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Capsazepine Synthesis

Assured Fish - 5-5-2017 at 22:53

I found this compound about 2 weeks ago wile reading through whimsy, it was in a thread labelled "List of compounds that are too much of a challenge".
Anyway i saw this as a challenge and after combing through the compounds listed there capsazepine stuck out like a saw thumb.
This stuff looks waaaaaaay to fun to not at the very least discuss the preparation for but please don't give me any shit like "why don't people post practical procedures and do some real lab work instead of just coming up with theoretical preparations, i miss the old days when SM members spent more time in the lab than in front of the computer".
Because this stuff is really hard to make and also as i will highlight extremely dangerous at some points so their aint no way in hell im gonna try preparing it without first running through the practical implication with you guys first and even then im not sure if I am gonna make it any time soon as much as id love too.

Anywhooo My idea was to start from pyrocatechol obviously followed by protection of the dihydroxy groups in order to carry out a grignard reaction, to protect the dihydroxy groups i would propose either williamson with dihalomethane to prepare 1,3-benzodioxol or williamson with iodomethane to prepare 1,2-dimethoxybenzene followed by bromination with n-bromosuccinamide.
The reason i suggest benzodioxol over dimethoxybenzene is because from what i understand demethylation of vanillan is an absolute bitch and demethylation of benzodioxol is as simple as refluxing in a strong acid such as HBr or HCl but id like to hear you guys thoughts on this?

Once the bromide is prepared and dried it would then be reacted with magnesium turnings in diethyl ether or THF to prepare a grignard reagent, this grignard reagent would then be filtered and put into an addition funnel and dripped over 2-bromo nitroethane followed by acidic work up in the usual fassion to prepare 3,4-methylendioxy-phenyl-2-nitroethane or 3,4-dihydroxy-phenyl-2-nitroethane.
Which ever was prepared would then need to be demethylated to reform the dihydroxybenzene followed by reduction of the nitro group using either thiourea dioxide or sodium dithionite or catalyst/hydrogen, Id recommend thiourea dioxide simply because of ease of use and availability despite never having used it myself.
The 2-bromo-nitroethane could be prepared by bromination of 2-nitroethanol which may again be prepared by the reaction of formaldehyde and nitromethane.

https://de.wikipedia.org/wiki/2-Nitroethanol
http://www.orgsyn.org/demo.aspx?prep=CV5P0833

The next compound gives me pause as its a short chain thiol.
This compound is 3-hydroxy-1-propanethiol which sigma has named 3-Mercapto-1-propanol:
http://www.sigmaaldrich.com/catalog/product/aldrich/405736?l...
I unfortunetely have no idea as to how potentially dangerous this compound is to handle but i have an idea for its preparation. First reacting allyl alcohol with HBr to get allyl bromide then reacting allyl bromide with sodium hydrosulfite to prepare allyl thiol which could then be reacted with HBr in the presence of peroxide in a reverse markovnikov to get both 2-bomo-1-propanethiol and in higher yields the desired 3-bromo-1-propanethiol, Sigma says the bp of 3-Chloro-1-propanethiol is 145*C and so the bromide should be a few tens of degrees higher, The 2 and 3 bromo propanthiols could be hopefully separated via simple distillation, fractional might be necessary but i personally have never tried fractional distillation at those kind of temperatures.
Sodiumhydrosulfite however can be prepared by reaction of hydrogen sulfide with sodium alkoxide, Scary.
http://www.sigmaaldrich.com/catalog/product/aldrich/c68601?l...

Once the 3-bromo-1-propanethiol and 3,4-dihydroxyphenyl-2-ethylamine is prepared neucliophilic alophatic substitution between both componants while keeping the bromide at an excess in order to limit di and tri alkyation.
The unreacted amine and the di and tri alkylamine would then have to be separated although their shouldn't be to much to separate if done carefully enough, since distillation is out of the question for these kinda compounds i suspect liquid layer chromatography will have to be employed :mad:

The next part is where it get interesting.

https://www.heterocycles.jp/newlibrary/payments/form/00401/P...

This would employ a pummerer rearrangement to close the ring followed by reduction of the thiol using nickel chloride and sodium borohydride to close the benzazepine and yield 5,6-dihydroxybenzazepine

Unfortunately i think this may also yield 4,5-dihydroxybenzazepine but i don't have access to the paper.

Ok now this is where things get difficult, we need to substitute the amine with thioamide and i can only find 3 ways of doing this first is the kindler thioamide synthesis which would have to probably follow N substitution with acetyl chloride.
http://www.organic-chemistry.org/namedreactions/willgerodt-k...

The next method used a rather difficult to prepare reagent called the lawesons reagent or possibly phosphorous pentasulfide, by reacting either of these with the preprepared carbamide which im still a little iffy on how to prepare and also combined with the general un availability of lawsons reagent im not really gonna go into this method.

The third looks most promissing but also the most dangerous, it involves N substitution using cyanogen bromide and then proceeding in a similar manner as to how thiourea is prepared:

https://en.wikipedia.org/wiki/Thiourea

The LiAlHSH should not be too difficult to prepare provide LAH is on hand and cyanogen bromide can be conviently prepared by reaction of bromine with sodium cyanide.
NaCN + Br2 ---> BrCN + NaBr
https://erowid.org/archive/rhodium/chemistry/eleusis/cnbr.ht...

This leave us finally with the preparation of p-chloro phenyl-2-ethylbromide,
My idea for this was again simple, starting from styrene followed by chlorination with ferric chloride under dry conditions followed by distillation. Bp of p chlorostyrene is 192*C
http://www.chemspider.com/Chemical-Structure.13465.html
Bp of o chlorostyrene is 189*C
http://www.chemspider.com/Chemical-Structure.14205.html
For separation of the ortho and para isomers i recommend taking advantage of sterric hinderance in the same way that nerdrage did in his separation of chlorotoluene video only at much higher temperatures, around 200*C maybe a bit higher in a dean stark set up, hopefully they don't decompose to much at these temps.

The other much more lengthy method would be para nitration of styrene using acyl nitrate in zeolite:
http://www.sciencedirect.com/science/article/pii/S0167299199...
This p-nitrostyrene would then have to be reduced to an amine followed by diazatization with sodium nitrite and then finally reaction with copper chloride to get p-chlorstyrene.

The p-chlorostyrene could then be reacted with HBr in the presence of a peroxide again in a reverse markovnikov to get a mixture of phenyl alpha and beta brominated substrates, however im pretty sure phenyl-alpha-bromoethane undergoes hydrolysis to yield phenyl-alpha-hydroxyethane which would make separation considerably easier, possibly simple distillation if we can find the bp of p-chlor-phenyl-alpha-hydroxyethane.
https://www.alfa.com/en/catalog/A16839/

Then to finally arrive at our final destination neucliophilic alophatic substitution of p-chloro-phenyl-beta-bromoethane with N-thiourea-5,6-dihydroxybenzazepine wile keeping the benzazepine in excess to yield Capsazepine.
:cool:

Alice - 6-5-2017 at 01:53

Would be nice (and probably would bring more resonance) if you would provide a scheme containing the whole synthesis route including arrows with reagents, solvents, and reaction conditions. That would help greatly to understand your route and to identify potential problems faster..

Just as a small comment, I think LAH is a problem to get. It looks like most reagents in the synthesis need to be prepared first. Would be a huge amount of work.

EDIT:

Another point is the Grignard reaction with 2-bromonitroethane will lead to attack of the nitro group, additionally the grignard reagent may simply deprotonate 2-bromonitroethane leading to elimination of bromide with nitroethene as the product. Grignards usually are quite strong bases.

EDIT2:

2-Bromonitroethane will lead to the wrong chain length anyway, doesn't it?

[Edited on 6-5-2017 by Alice]

[Edited on 6-5-2017 by Alice]

DJF90 - 6-5-2017 at 07:53

I think you're making it much more complicated than it needs to be, and as Alice mentions you wouldn't even get the right product assuming it all worked. In fact I gave up reading when I noticed this.

Anyway, what makes catechol the "obvious" starting material for this? To my trained eye, I'd suspect either vanillin or eugenol to be better precursors, seeing how you're able to incorporate either the single or three sequential carbons of the azepine ring (respectively) and the "diol" is already half protected. Both also provide functionality amenable to introduction of the nitrogen for the azepane ring also. They are probably easier to aquire, too.

[Edited on 6-5-2017 by DJF90]

CuReUS - 6-5-2017 at 10:08

The best way to make the compound would be through a convergent synthesis.Divide the molecular into 2 halves at the bond between the thiourea C and the benzazepine N

Synthesis of the right half:-
1a) Convert fenclonine to p-chlorophenacetonitrile - https://www.sciencemadness.org/whisper/viewthread.php?tid=65...
2a) p-chlorophenacetontrile to p-chlorophenethylamine - http://pubs.acs.org/doi/abs/10.1021/ol403668e
3a) p-chlorophenethylamine to the isothiocyanate - http://www.tandfonline.com/doi/abs/10.1080/00304949209355899

Synthesis of the left half:-
1b)convert safrole to MD-butanoic acid (pg 5 of pdf) - https://www.jstage.jst.go.jp/article/cpb1958/44/3/44_3_500/_...
2b)intramolecular cyclisation of MD-butanoic acid to the ketone - http://www.tandfonline.com/doi/abs/10.1080/00304949109458304
3b)Modified schmidt reaction on the ketone - http://onlinelibrary.wiley.com/doi/10.1002/cmdc.201000101/fu...
4b)reduction of the lactam (pg 8 of pdf) - http://www.sciencedirect.com/science/article/pii/S0040402001...

If eugenol is used,an additional methylation step has to be done
1c) methylation of eugenol- http://www.sciencedirect.com/science/article/pii/S0040403998...
2c)O-methyleugenol to the butanoic acid - same ref as in 1b)
3c )intamolecular cyclisation of the acid to ketone - http://www.tandfonline.com/doi/full/10.1080/0039791080266339...
4c)modified schimdt - same ref as in 3b)
5c) reduction of the lactam - same ref as in 4b) or http://pubs.acs.org/doi/abs/10.1021/jm00039a006 (pg 2,scheme 1)

Putting it all together - react the right and the left halves -
http://onlinelibrary.wiley.com/doi/10.1002/chem.201102097/fu...

Quote:

Isothiocyanates are weak electrophiles. Akin to the reactions of carbon dioxide, nucleophiles attack at carbon

https://en.wikipedia.org/wiki/Isothiocyanate#Synthesis_and_r...
here,the isothiocyanate is the right half and the nucleophile is the benzazepine N of the left half.

finally,deprotect the diol of safrole -http://pubs.acs.org/doi/abs/10.1021/jo9910740
eugenol demethylation (also works for safrole) - http://pubs.acs.org/doi/abs/10.1021/jo961191k

I have 2 doubts for the deprotection step:-
1. could HBr be used or would it also destroy the thiourea bridge ?
2. should the deprotection be done at the end or can it be done before putting together the 2 halves (i.e would the diols be nucleophilic enough to compete with the bezazepine N to react with the isothiocyanate ? )

[Edited on 7-5-2017 by CuReUS]

Assured Fish - 6-5-2017 at 16:34

Quote:

Would be nice (and probably would bring more resonance) if you would provide a scheme containing the whole synthesis route including arrows with reagents, solvents, and reaction conditions. That would help greatly to understand your route and to identify potential problems faster..

If i can figure out a good place to host photos i can draw it all out and then post photos of that on here but i am having trouble finding a good way to do this, starting to feel like an computer illiterate old person.
I unfortunately cannot find usable pictures online for most of the scheme either.

Quote:

Another point is the Grignard reaction with 2-bromonitroethane will lead to attack of the nitro group, additionally the grignard reagent may simply deprotonate 2-bromonitroethane leading to elimination of bromide with nitroethene as the product. Grignards usually are quite strong bases.

I was afraid this might be the case i had found a few examples of nitros reacting with grignards but these were always aromatic and most organics literature doesn't talk about the reactions of nitros with grignards.
As for the deprotonation, is the grignard able to deprotonate due to the close proximity of the electron withdrawing nitro, i know their are examples of condensation between halo arenes and halo alkanes but im not sure about their limitations.

Quote:

2-Bromonitroethane will lead to the wrong chain length anyway, doesn't it?

Holy shit you're right, i just realized an enormous screw up on my part, although this does at least make a mannich reaction feasible for forming the phenylmethylamine chain.

Quote:

Anyway, what makes catechol the "obvious" starting material for this? To my trained eye, I'd suspect either vanillin or eugenol to be better precursors

I did look at vanillin briefly but due to my error in assuming the wrong chain length of the phenylalkylamine I had trouble figuring out how to prepare the phenethylamine from the benzaldehyde. The other issue i had with vanillin was that it was methylated and i didn't like the idea of demethylating the methoxide to hydroxide although in hindsight the pyridine/thiourea and AlCl3 are probably some of the easiest things to acquire in this synthesis.

Quote:

Synthesis of the right half:- 1a) Convert fenclonine to p-chlorophenacetonitrile - https://www.sciencemadness.org/whisper/viewthread.php?tid=65... 2a) p-chlorophenacetontrile to p-chlorophenethylamine - http://pubs.acs.org/doi/abs/10.1021/ol403668e 3a) p-chlorophenethylamine to the isothiocyanate - http://www.tandfonline.com/doi/abs/10.1080/00304949209355899

This makes thing a hell of a lot easier, as you can see by my origional idea starting from styrene there where way to many issues with high temperatures, I like the idea of forming the thiourea bridge from isothiocyanate as this nullifies the danger of pissing around with dangerous thiolating reagents. The only pain in the ass part i see here is gettin your hands on carbon disulfide but if i recall correctly their are a few rather OTC ways to make carbon disulfide floating around here on the forum.

Quote:

Part 2- synthesis of the left half from 3-(3,4-dimethoxyphenyl)propan-1-amine (pg 2 ,scheme 1) - http://pubs.acs.org/doi/abs/10.1021/jm00039a006

You don't specify as to how you would form the benzazepine ring from the phenylpropylamine so im assuming this is specified in the reference you gave, i unfortunately don't have access

but i will put a request in References.

Thanks for all your replies.

Alice this might help

Assured Fish - 6-5-2017 at 19:33

I was having issues uploading the photos from my camera, for some reason they registered as being to big but i have managed do this using my phone so apologies for the bad quality, also I don't have much light so they arn't the easiest to read.
This is my origional idea however i haven't drawed out the route to the p-chloro-phenyl-2-bromoethane.

I skipped drawing out the reduction of the nitro group and the deprotection/demethylation of the diol.

I will try drawing out the route suggested by CuReUS soon.

Again given recent posts this method wont work, however it may work if we were to replace the grignard between the bromobenzene and 2-bromo-nitroethane with possibly a mannich reaction between catechol ammonia and formaldehyde however im not sure if this would be specific enough to just alkalate the desired position and we may end up with 2,3-dihydroxy-phenylmethylamine as a side product.

Alice - 7-5-2017 at 04:50

Assured Fish, thanks for the pics. Now as you can see, in the second pic, there is a carbon vanishing.

For drawing such schemes, either use the chemdraw trial version or the ChemSketch freeware.
For the bromination, NBS is not OTC, but as this is an activated arene there is a vast number of halogeation reactions available. Br2 being one of them or just in situ generated Br2.

Quote:

As for the deprotonation, is the grignard able to deprotonate due to the close proximity of the electron withdrawing nitro, i know their are examples of condensation between halo arenes and halo alkanes but im not sure about their limitations.

Yes, either there is a concerted elimination of HBr or the negative charge is resonance-stabilized by the nitro group before elimination happens. See Henry reaction where deprotonation is intended in order to generate a nucleophile. Bromonitromethane won't solve the problem either as it's deprotonated too.

For the next step the reagent you suggest is 3-bromopropane-1-thiol. This will also react with itself and reacts twice with the benzylamine, as such a reaction would be performed with an auxiliary base, otherwise HBr formed blocks benzylamine for further reaction or may deprotect the phenolic groups. A short search reveals for such reagents the thiol is often protected as thioacetate.

For the other routes, CS2 isn't the only problem. For the other reactions stuff like phosgene, diborane, TiCl4, ethyl chloroformate, NaN3, POCl3, trichloroacetic anhydride, and TEMPO are required. Reagents difficult to make or pretty much dangerous to handle. This is hardly pratical and for being OTC something more straight forward and easier would be nice.

Additionally, the most crucial part for all of these reactions isn't the reactions themselfes or the various reagent preparations, but how to purify the products and how to make sure the compounds are the compounds intended. I count about 10-11 transformations not including the reagent preparations.

[Edited on 7-5-2017 by Alice]

UserPrevKnownAsVanta - 7-5-2017 at 08:08

Quote: Originally posted by Assured Fish

I will try drawing out the route suggested by CuReUS soon.

Chemdraw pls

CuReUS - 7-5-2017 at 08:12

Quote: Originally posted by Alice

For the bromination, NBS is not OTC

Not directly,but it can be made from OTC chemicals -http://www.sciencemadness.org/talk/viewthread.php?tid=3366
succinic acid is sold as food and dietary supplement - https://en.wikipedia.org/wiki/Succinic_acid#Food_and_dietary...

Quote:

For the other routes, CS2 isn't the only problem. For the other reactions stuff like phosgene, diborane, TiCl4, ethyl chloroformate, NaN3, POCl3, trichloroacetic anhydride, and TEMPO are required. Reagents difficult to make or pretty much dangerous to handle.

In case you haven't noticed,I have changed my initial route.You only need NaN₃ and TiCl₄ now.Azide is OTC or can be made from OTC chemicals - http://chemistry.mdma.ch/hiveboard/acquisition/000435713.htm....As for the latter,it can be bought.And you don't neccesarily have to use TCAA,using that just gives the best yield.Other cyclising agents could also be used.

Quote:

This is hardly practical and for being OTC something more straight forward and easier would be nice.

stop suffering from OTC OCD.

.This isn't a nitrobenzene to aniline type of synthesis.Desperate compounds call for desperate measures. :cool:

Quote:

Additionally, the most crucial part for all of these reactions isn't the reactions themselfes or the various reagent preparations, but how to purify the products and how to make sure the compounds are the compounds intended. I count about 10-11 transformations not including the reagent preparations.

instead of laughing at other people's syntheses,why don't you come up with a "simple, straight forward,practical and easy route" which uses safe reagents and is 100% OTC ? :mad:

[Edited on 7-5-2017 by CuReUS]

Alice - 7-5-2017 at 08:49

CuReUS, I just thought that something has changed. BTW I'm not laughing at other people's synthesis at all. That was just my way expressing this synthesis isn't trivial - not bad.

Of course, with enough energy and time it's possible achieving a lot OTC, but if really nothing is available and everthing has to be prepared in one or multiple steps in a more or less complicated manner it's just getting impossible for normal people to afford the workload.

Fortunately I have indeed made my own thoughts on the problems I have named.

Here is my draft for the synthesis of the left part (benzazepine). I paid much attention making the synthesis OTC friendly using only chemicals which are either available or there are established OTC procedures for making them. I'm aware the last step (thermal cyclization) is the most critical step and may be substituted in one way or another, maybe by cleaving the benzyl ether beforehand. The preparation of 1,3-diiodopropane will take two steps. 1. Transformation of 1,3-propanediol by distillation from NaCl and a suitable acid into the dichloride. 2. Double Finkelstein reaction with NaI leading to Cl/I exchange.

EDIT: Forgot to provide the link for yeast mediated reduction of vanillin:

http://pubs.acs.org/doi/abs/10.1021/ed070pA155

EDIT3: Added more precise wording.

EDIT4: Update

In chemistry there is always room for optimization, a never ending story.

Possible side products of 1,3-dichloropropane (b.p. 121 °C) synthesis like allyl chloride (b.p. 45 °C) or 1,2-dichloropropane (b.p. 95 °C) will be removable by fractionated distillation, alcohols by washing the product multiple times with water. I assume removing the chlorinated products under reduced pressure during the reaction may be fortunate or even neccessary. I have chosen the chlorination over iodination or bromination because the boiling points are more practical and it's better starting with cheap stuff.

The Finkelstein reaction may be performed with just 1 eq. NaI, as the statistical yield of 3-iodo-1-chloropropane is 75%. Assuming a slight dependence on the second substituent, e.g. sterically, an even higher ratio may be obtained. This leads to a lower boiling product which might then be distilled under reduced pressure (aspirator vacuum) saving half of the sodium iodide. The Grignard will prefer substituting the iodide over the chloride while the chloride remains still reactive towards ammonia. The ammonia additon may be done one-pot, or just after removal of the salts, as it enables further acid-base extraction. At that point hopefully other side products not being an amine will be removed. A possible toxic side product is propylene-1,3-diamine which is water soluble and removed by acid base extraction.

[Edited on 7-5-2017 by Alice]

[Edited on 7-5-2017 by Alice]

[Edited on 8-5-2017 by Alice]

[Edited on 8-5-2017 by Alice]

Eddygp - 8-5-2017 at 01:12

I doubt you would lose methoxy like that in the 7-m. cyclisation step. Maybe a sulfonate ester would be better. In any case, a friend of mine actually devised a very plausible route to capsazepine, I'll redirect him to here.

Alice - 8-5-2017 at 02:16

@Eddygp. As I said I didn't suggest the last step because it sounds so promising, it would just be so interesting to know whether it works. As a temperature range I think about anything between 200 °C and pyrolysis. At least for me chemistry would become very boring if I never tried to check out where the limits are. :cool:

On the other hand the benzyl ether can be transformed into any other functional group, for example back to the aldehyde, which would give an imine then. Still easier to reduce than the lactam though. A quaternary benzylamine would be another idea.

[Edited on 8-5-2017 by Alice]

12thealchemist - 8-5-2017 at 02:35

As per request, I'll attach my synthesis here, starting from vanillin and styrene.
There are two possibilities for the reduction of the oxime because I found two different methods on YouTube by competent chemists. In writing a more detailed document, I included both of these.
Also, the use of boron tribromide as the demethylation agent was chosen since there was an OrgSyn reference for that procedure, and both boron and bromine are relatively OTC.

Alice - 8-5-2017 at 05:07

12thealchemist, I have four comments on your synthesis pointing out potental problems.

1. Styrene will yield mostly markovnikov product upon treatment with HCl.

2. For the alkylation of the benzylamine the question is if this stops at the secondary amine.

3. For the Friedel-Crafts mediated cyclization I suspect the intramolecular cyclization being less favored compared to intermolecular alkylation of another molecule's ortho-phenol position which might or might not be overcome by highly diluted solution. A phenol is more activated than a methoxybenzene.

4. Not sure if BBr3 is capable of chopping off the alkyl from the 7-membered ring again leading to some undefined tar but I don't know how the reaction conditions mayt be, favoring one reaction over the other. The Friedel-Crafts alkylation is reversible in general, leading to difficulties which limit its synthetic use. But I haven't checked the literature about how the scope of this individual reagent BBr3 is.

Finally the synthesis of the benzylamine and the isothiocyanate looks very good!

12thealchemist - 8-5-2017 at 05:33

Alice:

1. I was aware that styrene + HCl would give mainly the undesired product; I had forgotten to point that out in the post. My thinking was that since the precursors were cheap and readily available, one could obtain sufficient quantities for the main synthesis without too much difficulty. However, I appreciate the drawbacks of this idea, namely green chem.

2. Crossed-fingers

3. Not something I had given much thought to; the lecturers at my university have historically indicated that intramolecular reactions are kinetically favoured over intermolecular ones. However, your point raises another one - could it instead react ortho to the phenol instead of meta? This does form a bridged compound, however.

4. The orgsyn reference:
Org. Synth. 1969, 49, 50
DOI: 10.15227/orgsyn.049.0050
http://www.orgsyn.org/demo.aspx?prep=CV5P0412

[Edited on 8-5-2017 by 12thealchemist]

CuReUS - 8-5-2017 at 09:21

Quote: Originally posted by Alice

Fortunately I have indeed made my own thoughts on the problems I have named.

Or unfortunately,as we will soon see

First of all,any route is only as good as its references.Since you do not provide suitable references,your route fails there itself.
Now lets go through your synthesis

1.For the vanilin reduction using yeast,not everyone has a centrifuge lying around,you know.
2.You have problem using azide,but no problem using K ?Also MeI is a very safe reagent according to you ?
3.bromination will give other isomers too.Will you be able to separate them ? Also,the HBr formed as a side product might demethylate the ethers
4.Pls give a reference where an alkylation is performed using grignard alone
5.How will you prevent the formation of 2nd,3rd and quaternary amines ?
6.And last but not the least,The cyclisation you propose might work in wonderland,but it won't work here on earth

Quote: Originally posted by Alice

On the other hand the benzyl ether can be transformed into any other functional group, for example back to the aldehyde, which would give an imine then. Still easier to reduce than the lactam though.

What do you mean by "still easier to reduce".Do you mean the process or the reagent ? Because if its the former,the amount of work you would have to do to convert the benzyl ether to the amine(selective de-alkylation,controlled oxidation,imine formation,reduction while trying to prevent reductive alkylation of the amine by the aldehyde) will outweigh the effort required to reduce the lactam.And if its the latter,and you are shy of using LAH,you could just use Red-Al instead..

Quote:

A quaternary benzylamine would be another idea.

What do you plan to do with that ?

Quote: Originally posted by 12thealchemist

As per request, I'll attach my synthesis here, starting from vanillin and styrene.

Your route is quite simple,but the problem is that in organic chemistry,simplicity and selectivity do not go hand in hand

Quote:

There are two possibilities for the reduction of the oxime because I found two different methods on YouTube by competent chemists.

I don't know which competent chemists you are referring to,but both the chemists I know have run into problems trying to reduce oximes using Zn.Chemplayer said that the final product was inpure and had to be furthur purified whereas nile red failed to reduce it itself.Another youtuber claims to have done it,but he got a shitty yield of 36%

2.In the alkylation step,isn't there a chance of the propane dichloride reacting twice with NH₂ to form an azetidine ?
3.Even if the FC intramolecular cyclisation went well,that naked phenol and even the NH would react with the AlCl₃ to form tar
4.Demethylating the ether before reacting it with the isothiocyanate might lead to a competing reaction between the OH and the N,as I have mentioned before

As for the other half,you will have a warm time during the p-chlorination.Just ask Nurdrage.Also the last step is wrong,since isothiocyanates are extremely susceptible to hydrolysis,and the NaOH would react with it before the benzazepine even had a chance

[Edited on 9-5-2017 by CuReUS]

clearly_not_atara - 8-5-2017 at 13:46

If you lack drawing software: https://anonym.to/http://py-chemist.com/

====================================

edit: reading is hard

From safrole, treatment with Cp2ZrHCl followed by benzylamine in THF results in anti-Markovnikov hydroamination to 5-(3-benzylaminopropyl)benzodioxole.

https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3800136/

This reacts with formaldehyde in aqueous acid in a Mannich reaction to give N-benzylbenzodioxolo[5,6-c]azepane.

N-benzylbenzodioxolo[5,6-c]azepane is then debenzylated with Pd/C/H2 or Pd/C/triethylammonium formate.

This is treated with p-chlorophenethyl isothiocyanate to yield capsazepine methylenide. The methylenedioxy group can be cleaved by a number of standard methods such as:

https://www.jstage.jst.go.jp/article/cpb1958/42/3/42_3_500/_...

Safrole itself can be made by a number of methods; generally the bromination of benzodioxole:

BzdH + NH4Br + H2O2 [HOAc] >> BzdBr
https://erowid.org/archive/rhodium/chemistry/aromatic.bromin...

followed by the formation of an organozinc reagent in acetonitrile and reaction of this with allyl acetate:

BzdBr + Zn + CoBr2 [MeCn] >> BzdZnBr
BzdZnBr + allyl-OAc >> safrole + "ZnBrOAc"
http://pubs.acs.org/doi/abs/10.1021/ol0340641

would seem preferable based on what people don't want to be ordering from chemical companies (piperonal, eugenol, IBX, etc).

If safrole is an issue it may be possible to substitute 2,2-dimethylbenzodioxole made IIRC by the condensation of catechol with acetone. However I know less about the cleavage of this moiety. 2,2-dimethylsafrole is not illegal AFAIK (it is not a drug precursor)

[Edited on 9-5-2017 by clearly_not_atara]

Alice - 8-5-2017 at 16:50

Hi CuReUS.

Not getting my point isn't a reason behaving like a child as you have illustrated:

Quote:

Or unfortunately as we will soon see

First of all,any route is only as good as its references.Since you do not provide suitable references,your route fails there itself.
Now lets go through your synthesis

This also includes use of majestic plural and not setting white spaces properly in order to not provide good readability. If you won't stop this I will ignore you until you're acting like a grown up again.

I thought you're the one not being happy with laughing about other people's synthesis. I didn't, but you seem to have some weird double standards.

A route fails only if it doesn't work in the end. Reactions not working as expected may be modified or substituted. Only if that fails the route fails. There is nothing special about this. My route is as hypothetical as yours, no matter if it's based on literature procedures or not. And now for the third time, I'm aware the cyclization as shown in my draft is experimental!

Quote:

1.For the vanilin reduction using yeast,not everyone has a centrifuge lying around,you know.

Surely a centrifuge is the only way extracting vanillyl alcohol. :/

Quote:

2.You have problem using azide,but no problem using K ?Also the MeI is a very safe reagent according to you ?

I never said I have a problem working with azides, MeI or K. In fact I worked with all of them multiple times. I said it's a huge amount of work together with a lot of other comparably difficult procedures making it hardly affordable for many. Therefor the procedure for making MeI is a lot easier than making azide. But it's true MeI in particular doesn't suit the toxicity issue I have raised. I won't work with MeI at home as I don't have a fume hood, but others have a fume hood so handling MeI is relatively safe as long as the person handling it is trained and ventilation works properly. My reasoning to suggest MeI is simple preparation and effectiveness.

Quote:

3.The bromination will give other isomers also.Will you be able to separate them ?

I don't know many aromatic substitutions which don't give mixtures so I would be surprised if this reaction wouldn't give a mixture too. Fortunately substituents already there are leading to a more or less good regioselectivity, additionally the reactivity of the electrophile affects regioselectivity too. Making the benzyl ether in order to enhance regioselectivity isn't a coincidence. If you have a look at the substrate, there is only one possibility for a para-methoxy substitution having additionally the benzyl ether ortho which makes it the most activated position. Therefor the product of interest is formed in excess. Did you realize I was applying the rules of regioselectivity prediction? Further, recrystallization is the method of choice purifying the product.

Quote:

4.Pls give a reference where an alkylation is performed using grignard alone

I don't need a reference for my own hypothesis. My aim is starting as simple as possible, and only if this fails choosing a more advanced/less amateur-friendly alternative. So I'm familiar with the various additives and alternatives, I just want to use them only if it's really neccessary. This way I'm trying to end up keeping the route easy and practical.

Quote:

5.How will you prevent the formation of 2nd,3rd and quaternary amines ?

By using an excess of hot conc. ethanolic ammonia, with the halide being droped slowly into it. This means choosing a suitable amount of ammonia to outperform multiple alkylations of the product.

Quote:

6.And last but not the least,The cyclisation you propose might work in wonderland,but it won't work here on earth

I don't share your attitude of knowing beforehand what's possible and what's not. Once I heard a lecture of a professor who said to the students: if you are done with the master, try to forget as much as possible as it will just clog up your mind.

Of course that was meant polemic but the core message is: never be too sure.

Quote:

What do you mean by "still easier to reduce".Do you mean the process or the reagent ? Because if its the former,the amount of work you would have to convert the benzyl ether to aldehyde(selective de-alkylation followed by controlled oxidation) will outweigh the effort required to reduce the lactam.And if its the latter,and you are shy of using LAH,you could just use Red-Al instead..

No, the latter, making LAH or whatever needed. LAH or Red-Al aren't OTC and even if you have any source it still doesn't make it OTC in general. Maybe OTC has a different meaning for each of us. That may explain a lot.

Quote:

Quote:
>> A quaternary benzylamine would be another idea.

What do you plan to do with that ?

As an alternative starting material for thermal cyclization. Trimethylamine may be a better leaving group than methoxide.

Quote:

>> Quote: Originally posted by 12thealchemist
>> As per request, I'll attach my synthesis here, starting from vanillin and styrene.

Your route is quite simple,but the problem is that in organic chemistry,simplicity and selectivity do not go hand in hand

This wasn't directed to me, but I answer anyway: The search for simplicity even for complicated problems is one of the aims of green chemistry.

clearly_not_atara - 8-5-2017 at 17:45

Quote:

4.Demethylating the ether before reacting it with the isothiocyanate might lead to a competing reaction between the OH and the N,as I have mentioned before

The isothiocyanate will not react with the phenol, as phenols do not autoionize in non-aqueous solvents, so it is okay to deprotect before this coupling. I think a couple of people missed this. As another example, ammonium acetate is ionized in water but neutral in DMSO. The amine-isocyanate coupling would almost certainly be performed in a less polar solvent like methylene chloride.

======================================================================================================
Alice -- some thoughts

Grignard reagents will not generally react with alkyl halides without a copper catalyst.

I'm confused why you've chosen a likely problematic thermolysis (such reactions usually require a Lewis acid and occur in the gas phase, also often water is the product and the amine is inserted into the ether) over simply protecting the aldehyde with ethyene glycol and using intramolecular reductive amination (generally an easy reaction) at the end. You need a (likely acidic) deprotection step anyway after all. This also avoids using any alkali metal.

Quote:

excess of hot conc. ethanolic ammonia

I suggest you plug in the Henry's law constant calculated in this paper, estimate that the partial pressure of ammonia won't rise above half an atmosphere (and you better not have any sparks anywhere...), and calculate the corresponding solubility. I'm not expecting encouraging numbers.
http://www.sciencedirect.com/science/article/pii/S0378381211...
The Delepine reaction is more feasible.

Generally your route is constructed with a very lax attitude to flammability, which is strange for someone who claims to have experience working in a home lab. I would not recommend an air-free technique (such as the Grignard or potassium) to anyone who can't prepare cuprous iodide. By contrast I even recommended an alternative for hydrogen. It's something you might want to consider. Many home chemists die in fires.

[Edited on 9-5-2017 by clearly_not_atara]

AvBaeyer - 8-5-2017 at 18:52

Why not first read about what has already been accomplished rather than pissing in the wind about a whole lot of chemistry that ain't going to work.

Lithiated β-aminoalkyl sulfones as mono and dinucleophiles in the preparation of nitrogen heterocycles: Application to the synthesis of capsazepine
DA Alonso, A Costa, B Mancheño, C Nájera - Tetrahedron, 1997 - Elsevier
The lithiation of N-benzyl-β-tosylethanamine (10a) and N-benzyl-α-phenyl-β-
tosylethanamine (10b) with n-butyllithium at− 78° C leads to monoanions 11a and 11b, respectively. Intermediates 11 react with different monoelectrophiles (D2O, alkyl halides,
Cited by 31 Related articles All 4 versions Cite Save

A Facile and Practical Synthesis of Capsazepine, a Vanilloid Receptor Antagonist
J Lee, J Lee - Synthetic communications, 1999 - Taylor & Francis
Page 1. SYNTHETIC COMMUNICATIONS, 29(23), 4127-4140 (1999) A FACILE AND PRACTICAL SYNTHESIS OF CAPSAZEPINE, A VANlLLOlD RECEPTOR ANTAGONIST Jeewoo Lee* and Jiyoun Lee ... ABSTRACT: A facile and practical synthesis of capsazepine, a vanilloid receptor
Cited by 9 Related articles All 3 versions Cite Save

An efficient parallel synthesis of capsazepine and capsazepine analogs
L Tafesse, DJ Kyle - Combinatorial chemistry & high throughput …, 2004 - ingentaconnect.com
Capsazepine (CPZ, 1) is a well-known vanilloid receptor (VR1) antagonist that has been
cited widely used inthe literature. However the current synthetic methods used for the total
synthesis of CPZ are lengthy, involve multiple purification steps, and produce low yields.
Cited by 7 Related articles All 4 versions Cite Save

Maybe then you can speculate on alternate routes.

AvB

Assured Fish - 8-5-2017 at 21:53

Aaaaaand im late to the party.

The following scheme is what I think was origionally proposed by CuReUS starting from safrole or eugenol, however i am a little confused as to how you intended to use a modified schmidt reaction on the ketone/amide, i thought we would just want to reduce this completely using NaBH4 or LAH to get the benzazepine ring.

The formation of the benzazepine ring was taken from this reference that was sent to me from CuReUS. http://pubs.acs.org/doi/abs/10.1021/jm00039a006

Fenclonine to nitrile. http://www.sciencemadness.org/talk/viewthread.php?tid=32534

And his reference for the deprotection of the diol for which i don't have access to. http://pubs.acs.org/doi/abs/10.1021/jo9910740

I have a modification though for which i have not drawn out unfortunately.
Instead of forming the isothiocyanate from the amine using CS2 we could instead opt to convert the amine to an isonitrile using chloroform and a base which would be about as OTC as you get:

CHCl3 + NaOH/KOH -----> CCl2 + R-NH2 -----> R-NC

The isonitrile could then be reacted with sulfur like in the following reference:
http://www.organic-chemistry.org/abstracts/lit4/754.shtm

This would mean that we could do away with the CS2 and instead opt for an OTC approach using sulfur, chloroform and KOH to bridge the p-chlorophenethylamine and benzazepine forming the thiourea bridge.

Some references

Assured Fish - 8-5-2017 at 23:28

AvBaeyer i managed to get your second reference but i cannot find your first one and ive yet to get access to the third: lee1999

CuReUS this is your demethylation reference: brooks1999

Attachment: lee1999.pdf (371kB)
This file has been downloaded 546 times

Attachment: brooks1999.pdf (156kB)
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Alice - 9-5-2017 at 05:09

@atara, I know about the Grignard issue. But my stance is to check out if this particular reaction will work this way. In my previous post I explained why I think this is a good idea.

Quote:

I'm confused why you've chosen a likely problematic thermolysis (such reactions usually require a Lewis acid and occur in the gas phase, also often water is the product and the amine is inserted into the ether) over simply protecting the aldehyde with ethyene glycol and using intramolecular reductive amination (generally an easy reaction) at the end. You need a (likely acidic) deprotection step anyway after all. This also avoids using any alkali metal.

I never said what I've drawn in the draft is the most promising possibility. After all discussion can make a synthesis just becoming better, not worse. Acetal protection may be a very good idea and very OTC. The question is what influence it will have on bromination and cross-coupling. The question has to be answered for the benzyl ether too of course.

Quote:

Generally your route is constructed with a very lax attitude to flammability, which is strange for someone who claims to have experience working in a home lab.

Not sure what you mean. I don't think I've ever stated having much of a home lab. I don't think a ~10 step synthesis is suitable by any means for non trained experimenters. Where trained includes refusing doing potentially dangerous steps without proper equipement and safety measures. It also includes knowing when to grab the fire extinguisher and when to run. For working with ether, especially diethyl ether, a sufficiently strong airflow is advisable. But as a side note, diethyl ether introduces the fortune being good in moderating temperature as it cools quite strong upon evaporation. Additionally a Grignard doesn't have to be neccessarily done in an inert atmosphere as the ether protects the liquid more or less from air contact. Nevertheless inert gas is the better choice if available.

Quote:

It would be highly advisable collecting ammonia in some washing bottles anyway. You're right about the solubilitity. Doesn't sound very encouraging, but solubility isn't neccessarily a prerequisite. Bubbling ammonia through the solution might still do the job, especially for the iodoalkyl.
Sure, Delepine would provide a higher chance of success without much experimenting. Thanks for mentioning.

Quote:

I would not recommend an air-free technique (such as the Grignard or potassium) to anyone who can't prepare cuprous iodide. By contrast I even recommended an alternative for hydrogen. It's something you might want to consider. Many home chemists die in fires.

I wouldn't recommend any organic multi-step synthesis to someone not being able preparing cuprous iodide.

[Edited on 9-5-2017 by Alice]

Waffles SS - 9-5-2017 at 05:43

Possible ways for synthesis Capsazepine by reaxys

Attachment: Capsazepine Synthesis.pdf (106kB)
This file has been downloaded 485 times

CuReUS - 9-5-2017 at 06:21

Quote: Originally posted by Alice

Not getting my point isn't a reason behaving like a child as you have illustrated

learn to accept criticism.You go around poking holes in other people's syntheses but get offended when others do the same to you.What fun!

Quote:

This also includes use of majestic plural and not setting white spaces properly in order to not provide good readability.

I used plural because I wanted to point out the flaws in your route to others.As for the spaces,blame the site posting software,not me

Quote:

My route is as hypothetical as yours, no matter if it's based on literature procedures or not.

My route is logical and backed up by refs,whereas yours uses basic reactions hoping as if by miracle that they will give react exactly the way you want them to.

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Surely a centrifuge is the only way extracting vanillyl alcohol. :/

that's what they use in the only ref you linked,possibly to remove the crappy yeast cells.Don't shoot the messenger :mad:

Quote:

Did you realize I was applying the rules of regioselectivity prediction?

No I didn't,I got into chemistry yesterday

..Also since the ring in highly activated,you will have di/tri bromination to care of too

Quote:

Further, recrystallization is the method of choice purifying the product.

that's easier said than done for some isomers,if you don't have the proper refs detailing the separation.Just ask nurdrage https://www.youtube.com/watch?v=_wbqqI0IgY8&index=9&...

Quote:

so basically you want to do trial and error instead of saving time and money following well established research.An easy and practical route is useless if it doesn't work.

Quote:

By using an excess of hot conc. ethanolic ammonia, with the halide being droped slowly into it. This means choosing a suitable amount of ammonia to outperform multiple alkylations of the product.

I don't think you know how much NH₃ you would need to prevent polyalkylation if you decided to follow that primitive route.IIRC,the ratio of NH₃ to RX is 20:1

.Have fun working with that much NH₃

Quote: Originally posted by clearly_not_atara

The isothiocyanate will not react with the phenol, as phenols do not autoionize in non-aqueous solvents, so it is okay to deprotect before this coupling. I think a couple of people missed this.

actually,I had a doubt about this upthread.But since no one clarified it,I assumed it to be a potential side reaction,to be on the safer side.I am relieved that the deprotection can be done before the final coupling.It would have been a disaster to destroy the whole molecule just to take the protecting group out

Quote:

The amine-isocyanate coupling would almost certainly be performed in a less polar solvent like methylene chloride.

They used acetonitrile in the paper I linked - http://onlinelibrary.wiley.com/doi/10.1002/chem.201102097/fu...

Quote: Originally posted by Assured Fish

Aaaaaand im late to the party.

Man,your compound seriously heated up this thread

Quote:

The following scheme is what I think was origionally proposed by CuReUS starting from safrole or eugenol, however i am a little confused as to how you intended to use a modified schmidt reaction on the ketone/amide, i thought we would just want to reduce this completely using NaBH4 or LAH to get the benzazepine ring.

Brilliant drawing,but you have messed up a few steps

1.In the 2nd step,the acid undergoes an intramolecular FC acylation using TCAA to form the ketone
2.Then the modified schimdt is done on the ketone using HCl/NaN₃ to get the cyclic amide(lactam)
3.Finally,the lactam is reduced to benzazepine using LAH

As for the right half-
1.I just realized now that there is no need to convert fenclonine to the nitrile and then reduce it,it can be directly decarboxylated to the amine
https://erowid.org/archive/rhodium/chemistry/tryptophan.html
http://www.sciencemadness.org/talk/viewthread.php?tid=8574
2.The safrole is deprotected before the coupling,following atara's recommendation.
3. As I mentioned above,acetonitrile is used as the solvent in the coupling step,not toulene. Did you have any reason for using the latter

Quote:

Instead of forming the isothiocyanate from the amine using CS2 we could instead opt to convert the amine to an isonitrile using chloroform and a base which would be about as OTC as you get

from the ease with which you suggest making isonitrile,its obvious that you have never worked with them.I suggest you don't,they stink to high heavens and they are extremely toxic(I got poisoned from just one whiff the first time I made them

)

[Edited on 9-5-2017 by CuReUS]

Dr.Bob - 9-5-2017 at 07:13

The Lee paper, along with the Wadpole JMC article, would indicate that the coupling of the azepine to the isothiocyanate is not a problem, and the isothiocyanate can be made from the amine easily enough, so the route comes down to ways to make each part. I see few other practical ways to break the molecule apart. Making the azepine from the amide with diborane is the way Wadpole did it, along with HBr deprotection of the dimethoxy groups, which is not trivial, but diborane can be generated from NaBH4, so that is plausable. And HBr is not that hard to make or find. But the Lee route to the azepine seems more doable for OTC possibilities, and the LAH reduction could be swapped for diborane also, which simplifies the chemicals to acquire. So I would favor the Lee routes so far.

I have not seen the L Tafesse, DJ Kyle - Combinatorial chemistry & high throughput …, 2004 route yet, unless it is better, the Lee route could be the best way to start.

Alice - 9-5-2017 at 07:19

@AVBaeyer

Because it was clear to me from the beginning that the available synthesis most probably would have been developed with a different focus than I think is needed in order to achieve a practical OTC synthesis. So why not trust in ones own experience and creativity and discuss that here on SM. Just grabing the literature procedure to achieve (or not to achieve) the goal by force doesn't meet my philosophy. Not to cause any misunderstandings, I'm happy having my opinion and others having their opinion, even if this is pissing in the wind for others, although sounds cumbersome to me, no offence intended.

@Assured Fish

Great drawings. If I got that right the synthesis shown in the left pic changed. The butanoic acid is activated by some activating agent and then undergoes cyclization (Friedel-Crafts acylation), then the ring is expanded by the modified Schmidt reaction.

How about the Beckmann rearrangement utilizing hydroxylamine? EDIT: The Beckmann rearrangement leads mostly to the wrong product, known at least for the non substituted derivative.

[Edited on 9-5-2017 by Alice]

AvBaeyer - 9-5-2017 at 18:12

Alice,
No offense taken. I referenced the syntheses so that those interested in how capsazepine has been synthesized in the past could see the routes. Gathering this sort of information is important in planning any new or modified synthesis whether starting from OTC materials or chemical catalog materials. Designing a synthesis "de novo" without knowledge of prior work and a sound basis in organic chemistry, in my opinion, is pissing in the wind. Organic synthesis is an excersize in reasoning by analogy. It is unusual and mostly unheard of to invent truly new reactions for specific steps in a total synthesis. For example, look in detail at some of the great RB Woodward syntheses (eg reserpine, strychnine, vitamin B12). What you will find is no truly new chemistry but the ingenious application of standard chemistry to new situations.

In the case of casazepine, perhaps the most satisfying excersize would be figuring out how to synthesize some of the published starting materials from OTC sources. In a way, I think that this is the direction that this discussion may be moving which I heartily endorse. [see Dr Bob above]

I wish everyone a lot of fun in this excersize.

AvB

Assured Fish - 9-5-2017 at 22:05

Im inclined to agree with Dr.Bob, the lee ref using an intramolecular Mannich from phenylpropylamine kinda trumps most of the overly complicated routes any of us have suggested so far.
We could still even start from safrole or methylated eugenol and hydroaminate the alkene in an anti-Markovnikov fasion however separation of the 2 and 3 phenylpropylamines may prove troublesome but i am certain their are catalysts out their that could selectively aminate at the 3 position.

Quote:

Great drawings. If I got that right the synthesis shown in the left pic changed. The butanoic acid is activated by some activating agent and then undergoes cyclization (Friedel-Crafts acylation), then the ring is expanded by the modified Schmidt reaction.

Alice yes that has changed and also straight decarboxylation of fenconine was also suggested by CuReUS to go straight to the amine.
The only thing is that most decarboxylations of 3-amino-3-ethanoic acids are a pain in the ass to pull off e.g. tryptophan.
TCCA is OTC as fuck and a nitrile reduction to an amine is not all that difficult to achieve if you have hydrides on hand, LAH i know we are trying to avoid but the nickel boride reduction using NaBH4 and NiCL2 is quite straight forward and should get quite good yields.

I am still very confused as to how CuReUS's azepine ring cylization works though, you mention using TCAA i suspect trichloroacetic acid.

Quote:

In the 2nd step,the acid undergoes an intramolecular FC acylation using TCAA to form the ketone

CuReUS could you elaborate further or perhaps draw it out for us pretty please?

clearly_not_atara - 10-5-2017 at 01:30

Quote:

the lee ref using an intramolecular Mannich from phenylpropylamine kinda trumps most of the overly complicated routes any of us have suggested so far.

Hey I also used an intramolecular Mannich... although I severely underestimated the difficulty of reducing Cp2ZrCl2, which it turns out can pretty much only be done with aluminium hydride reagents. The best route I found so far uses DIBAL, which can be made OTC (or some similar replacements) but is well worth avoiding.

I think that you could actually get away with performing the radical addition of HBr to safrole. As long as the conditions are nonpolar enough, Br- ions won't be present, and the ether won't be protonated, which means it won't be cleaved. Probably benzene is the best solvent since I'm not sure how well safrole will dissolve in hexane. I'm also not sure what the best radical initiator is, but you can make something like AiBN by making butanone azine the usual way and converting the hydrazones to tetrahedral carbon atoms with a carbanion like ethyl acetoacetate. Or tert-butyl peroxide might be accessible somehow but I have no idea. I think methyl iodide and ultraviolet light counts as a radical initiator in some jurisdictions.

From there you can staple on the amine of your choice or potassium isocyanate if for some reason you actually want to use isocyanates like some people in this thread.

Actually it's possible that if you try to perform the Delepine on the benzodioxol-5-propyl bromide you'll end up forming the azepane because the transient iminium will attack the arene rather than being hydrolysed by water. It might even be possible to "force" this reaction by decomposing the hexamine onium with acid in the absence of water. This would be a particularly elegant approach if it worked:

EDIT: LOL there's an extra "N" in there somewhere, stupid drawing software

[Edited on 10-5-2017 by clearly_not_atara]

Alice - 10-5-2017 at 03:53

Here is another draft, applying some changes, especially four points mentioned by clearly_not_atara, which is avoiding K, avoiding ether at least in one step, acetal protection, and applying the Delépine reaction.

EDIT: Revised route.

Not sure about the Leuckart-Wallach and maybe the formaldehyde formed in the Delépine reaction may lead to some unwanted side reactions, which may be circumvented by using the Gabriel synthesis or succinimide as the amine donor. EDIT: Buffering the bromination may be neccessary in order to save the acetal from deprotection.

[Edited on 10-5-2017 by Alice]

@Assured Fish

Quote:

I think phenylalanine is relatively easy to decarboxylate. The problem with tryptophane is the indole moiety.

Quote:

TCCA is OTC as fuck and a nitrile reduction to an amine is not all that difficult to achieve if you have hydrides on hand, LAH i know we are trying to avoid but the nickel boride reduction using NaBH4 and NiCL2 is quite straight forward and should get quite good yields.

As you say, 'if at hand'. For me NaBH4 falls in the same category as LAH although its reactivity is weaker. Non OTC chemicals in my opinion. Diborane as a substitute has an autoignition temperature of 38 °C. Boranes are great rocket propellants.

Quote:

I am still very confused as to how CuReUS's azepine ring cylization works though, you mention using TCAA i suspect trichloroacetic acid.

It's the anhydride which leads to a mixed anhydride with the butanoic acid which in return is easy to cyclisize. In the mixed anhydride the trichloroacetyl part draws charge from the butanoic part making it very susceptible for the arene. Additionally trichloroacetate is a very good leaving group. There are loads of procedures published for alternate F-C-acylations. It's also possible cyclisizing acids directly, but the conditions are usually harsh. Maybe some milder conditions would work here as the attack happpens para to MDO.

[Edited on 10-5-2017 by Alice]

[Edited on 10-5-2017 by Alice]

Alice - 10-5-2017 at 07:59

Lee & Lee report, that the intramolecular Mannich reaction proceeds very sluggishly and yields not the right product as main product, but the N-methylated derivative. Their key finding is N-benzylation and a free phenol para to where the Mannich should happen. This means, the product of the reaction is benzylated and in a next step cleaved by H2 baloon and Pd/C. On the other hand I guess if both methoxy groups are cleaved beforehand the Mannich also happens in ortho-phenol position. If none are cleaved the reaction might also not give such good results.

CuReUS - 10-5-2017 at 08:11

Quote: Originally posted by Dr.Bob

But the Lee route to the azepine seems more doable for OTC possibilities,So I would favor the Lee
routes so far. the Lee route could be the best way to start.

I respectfully disagree.I don't think either trimethylphosphoacetate or isovanilin is available OTC and neither is 1,1'-thiocarbonyldi-2-(1H)-pyridone)

Quote: Originally posted by clearly_not_atara

The best route I found so far uses DIBAL, which can be made OTC

You know how to make hydrides at home ?

Quote: Originally posted by Assured Fish

Im inclined to agree with Dr.Bob, the lee ref using an intramolecular Mannich from phenylpropylamine kinda trumps most of the overly complicated routes any of us have suggested so far.

But keep in mind that the amine has to be protected and deprotected,like alice said above,which makes the reaction redundant

Quote:

We could still even start from safrole or methylated eugenol...

Not if we go via the mannich.Presence of a free para OH is essential for the reaction.Read the above post by alice.

Quote:

The only thing is that most decarboxylations of 3-amino-3-ethanoic acids are a pain in the ass to pull off e.g. tryptophan.

I am sorry,I should have given you a ref related to phenylalanine(table 2,entry 7).There is a slight misprint,the decarboxylation gives b-phenethylamine only,not alpha-https://erowid.org/archive/rhodium/chemistry/trp.decarbox.en...

Quote:

I am still very confused as to how CuReUS's azepine ring cylization works though, you mention using TCAA i suspect trichloroacetic acid.

That's where you are making a mistake.The cyclisation won't give you the azepine directly,it will only give the ketone.You will have to then convert the ketone in 2 steps(modified schimdt followed by reduction) to the azepine.
I am attaching a pic of the route.As for the cyclisation mechanism,Alice has hit the nail on the head and explained it beautifully.

Quote: Originally posted by Alice

On the other hand I guess if both methoxy groups are cleaved beforehand the Mannich also happens in ortho-phenol position.

Not to mention the crap formed by the reaction of HCHO with the diol

[Edited on 10-5-2017 by CuReUS]

Alice - 11-5-2017 at 06:49

Here is my third draft, reintroducing the yeast mediated reduction of vanillin and K for its global deprotonation. Not sure but would be fortunate if KOH works instead. A method for the extraction of vanillyl alcohol is required, which doesn't end up in a mess and too much chemistry in buckets.

EtI is introduced in order to avoid MeI. The second last step may be omitted which may reduce the synthesis to 7 steps (not counting reagent prearations). Although I suspect the resulting product will have a higher purity going for the quarternary ammonium salt, hopefully making intermolecular reactions especially between the amine and the benzyl bromide less likely.

Trimethylamine may be obtained by treatment of any available quaternary trimethyl ammonium salt with a strong base like KOH. In this synthesis a global deprotection (hopefully leading to the benzyl bromide intermediate) was chosen, avoiding an extra step for the aryl ether deprotection. I would not recommend isolating the bifunctional amine/bromide, just boiling off the HBr, adding it to a new solvent containing trimethylamine. Something which wasn't discussed before but I think is imporant to know is the deprotection utilizing HBr will yield bromoalkyls, so be aware of the gases formed.

Quote:

As for the cyclisation mechanism,Alice has hit the nail on the head and explained it beautifully.

Thanks!

Quote:

Not to mention the crap formed by the reaction of HCHO with the diol

Different types of resin.

[Edited on 11-5-2017 by Alice]

[Edited on 11-5-2017 by Alice]

CuReUS - 11-5-2017 at 10:22

Quote: Originally posted by Alice

The second last step may be omitted which may reduce the synthesis to 7 steps

You could have done the synthesis in 6 steps by hydrolysing the ethers and converting the benzyl alcohol to bromide in the 2nd step(acid hydrolysis) of the gabriel itself.But you would have to free base the bromide salt before the cyclisation,which would add one more step to make the synthesis 7 steps.

Alice - 11-5-2017 at 11:37

I thought about this. The reason I decided not to suggest it is a possible activation of the carboxylic groups by HBr with possible Friedel-Crafts products. This may be even a bigger problem as the phenols are deprotected then. If it turns out there is no such problem there is indeed a step to omit.

I think free basing is a very very critical step as there is no good reason why there would be no excessive chain formation. Would be a pitty losing lots of product in the last step and I don't know how the product may be separated other than a column. Therefor catching the benzyl bromide by trimethylamine may be the safer way, not just because the reaction is probably faster than either chain formation or cyclization but to additionally accomplish the following cyclization as controlled and clean as possible. This may be accomplished by preparing a hot solvent and to introduce the previously diluted quarternary ammonium compound as slowly as possible.

JJay - 11-5-2017 at 14:16

I have been following this thread with considerable interest, although for the most part it is a little over my head. I find the notion that baker's yeast can do reductions to be fascinating. Is this the same common bread/brewing/wild yeast that can be found almost everywhere or is it a special strain? Also, can it reduce aldehydes generally?

Alice - 11-5-2017 at 15:10

@JJay, the brand mentioned in the paper is Fleischmann's "active dry" yeast. I don't know this particular brand but it looks like usual baker's yeast. There are lots of publications focusing on yeast mediated reducion of ketones especially aryl alkyl ketones. I didn't know before it works for vanillin too. I didn't find much about aldehydes. If you are interested, did you know carrots can be used as well for ketone reductions into chiral alcohols?

That might be interesting for vanillin reduction too.

[Edited on 11-5-2017 by Alice]

JJay - 11-5-2017 at 16:09

Wow, that is pretty much the most garden variety of yeast I can think of. I actually have a stray packet of it sitting around here somewhere. Carrots, LoL. That is interesting, though....

CuReUS - 11-5-2017 at 17:32

Quote:

I think free basing is a very very critical step as there is no good reason why there would be no excessive chain formation.

But if you don't free base it,the NH₂-Br salt won't react with the benzyl bromide.Also,I just remembered that catechols get oxidised very fast in the presence of base,so the free-basing step is a necessary evil

Quote: Originally posted by JJay

I find the notion that baker's yeast can do reductions to be fascinating.

If you think of it,its nothing great actually.Yeast has been used for thousands of years for fermentation(breaking down sugars to acetaldehyde and then reducing it to ethanol).So its obvious that it can also be used to reduce other substrates.Read this review -http://pubs.acs.org/doi/abs/10.1021/cr00001a004

Quote: Originally posted by JJay

Wow, that is pretty much the most garden variety of yeast I can think of. I actually have a stray packet of it sitting around here somewhere.

if you are planning to do this reaction,keep in mind that you will need a centrifuge(according to the vanillin reduction paper),probably to separate out the yeast cells finely suspended throughout the mixture before you can get your product.

[Edited on 12-5-2017 by CuReUS]

Assured Fish - 11-5-2017 at 21:03

Quote:

But if you don't free base it,the NH2-Br salt won't react with the benzyl bromide.Also,I just remembered that catechols get oxidised very fast in the presence of base,so the free-basing step is a necessary evil

It is possible for us to freebase or demethylate a quarternary ammonium salt without using strong bases which might react with the catechol.

https://www.thevespiary.org/rhodium/Rhodium/Vespiary/talk/in...

from what i understand they suggested using a neucleophilic amine that is more neucliophilic than the ammonium salt they wish to freebase to which the alkyl halide would prefer, they suggested using ethanolamine and cited a reference to go with it.

Sigmatropic - 12-5-2017 at 02:10

I’ve seen this thread pop up more than once in today’s posts over the past weeks and have given the idea some thought.

First off I will go through this without any of the OTC fetish and establish the general scheme. Later I will comment on certain steps and suggest possible OTC alternatives. If you have any additional suggestions, blast away!

So I´d start from catechol and suitably protect this with some alkyl groups. Compound 1 would be then be subjected to Friedel-Crafts acylation with succinic anhydride. After separating the other possible isomer of 2, 2 would be subjected to a Curtius rearrangement in which the heating step would be performed in an anhydrous environment. This would hopefully give the isocyanate, which upon treatment with anhydrous acid would cyclisize to form 3. Reduction/deoxygenation under harsh conditions should furnish 4 which would be deprotected to 5 by refluxing in HBr.

Then onto the p-chlorophenethylamine isothiocyanate. Ring chlorination, radical benzylic chlorination and substitution with a cyanide salt as per NurdRage. Then reduce 8 with alane (fearing loss of the ring Cl when using straight LAH). Activation of 9 with thiophosgene should allow it to be attached to 5 and yield capsazepine.

Overall I think it is pretty atom efficient except for the steps where isomers can be formed: 12, 23 and PhMe6. I've looked in reaxys and most reaction are known, although not for the particular compounds. Having said that I'm sure I could provide credible references on most reactions if It weren't for me closing all the tabs and discarding the information last night.

The main problems for OTC style would be Curtius&cyclization 23, reduction 34, reduction 89 and 910.

23: instead of using DPPA or SOCl2 then NaN3 one could use TCCA to make the acid chloride and then make the acyl azide. Isolate that and heat it in anhydrous conditions to give the isocyanate.

34: Somewhat more problematic but possibly HI/Red P could work, although I have my doubts about reduction of the amide. These conditions may even do a tandem demethylation making it 35

89: May be achieved by aluminium amalgam reduction. There are plenty of routes to phenethylamines.

910: The reason why I think this is not an OTC style synth. and it is not worth bothering starting from absolute schratch. Although conceivably it is possible from C/SCS2 + Cl2 CSCl2

Alice - 12-5-2017 at 04:34

CuReUS, I think boiling 48% HBr isn't exactly a very good hydrolytic condition. In the following I show you what I'm afraid might happen.

Quote:

I didn't mean not to free base the amine at all, just that it won't be trivial, because chain formation will start instantly. I'm not familiar with the oxidation of catechol especially kinetics. If nothing else helps then intert gas (N2 balloon) is the answer.

In the meantime I checked the pKb in water for trimethylamine and butylamine (as a rough comparison), it's 4.19 for the former and 3.22 for the latter. This opens the door for not massively liberating the propylamine while adding trimethylamine, at least in equilibrium. In reality the interconversion happens fast but the reaction of equimolar amounts leads to an equilibrium constant of around 10:

propylammonium bromide + trimethylamine <=====> propylamine + trimethylammonium bromide

So the acid base reaction is 10 times faster from the right to the left than the other way round. Adding an equimolar amount dilute trimethylamine into the benzyl bromide (the propylamine still protonated) solution very slowly might be better than reverse.

@Assured Fish

Quote:

It is possible for us to freebase or demethylate a quarternary ammonium salt without using strong bases which might react with the catechol.

Why would you want to demethylate the quarternary ammonium salt? Free basing would mean to remove a proton from primary, secondary or tertiary amines ammonium salts. As the benzyltrimethylammonium salt doesn't have a proton attached to nitrogen (as it's quaternary) there is no possibility for free basing. If any group is gonna be displaced from the quaternary salt by a good nucleophile it's the trimethylamine part which is the leaving group then. But this is exactly my intention - reacting the free based propylamine in an intramolecular Sn2 reaction with the quarternary benzylammonium bromide.

Free basing in this context means liberating the propylamine from propylammonium bromide by neutralizing "HBr" with a base, which otherwise blocks the amine so it can't act as a nucleophile. In the protonated form there is no lone pair which could do that.

[Edited on 12-5-2017 by Alice]

CuReUS - 12-5-2017 at 06:46

Quote: Originally posted by Assured Fish

It is possible for us to freebase a quarternary ammonium salt without using strong bases which might react with the catechol.

The salt I am referring to here is a primary amine salt,not a quat

Quote: Originally posted by Sigmatropic

This would hopefully give the isocyanate, which upon treatment with anhydrous acid would cyclisize to form 3....

both the refs I found on FC acylation using isocyanate use BF₃.Et₂O

https://en.wikipedia.org/wiki/Curtius_rearrangement#Dievodia...
http://pubs.rsc.org/en/Content/ArticleLanding/2014/QO/c4qo00...

Quote: Originally posted by Sigmatropic

34: Somewhat more problematic but possibly HI/Red P could work, although I have my doubts about reduction of the amide.

HI/red P would break the lactam

Quote: Originally posted by Alice

CuReUS, I think boiling 48% HBr isn't exactly a very good hydrolytic condition. In the following I show you what I'm afraid might happen.

I think the succinic acid would react with the diol rather than undergoing a FC acylation.

Quote:

Free basing in this context means liberating the propylamine from propylammonium bromide by neutralizing "HBr" with a base, which otherwise blocks the amine so it can't act as a nucleophile. In the protonated form there is no lone pair which could do that.

what other context is there for free basing ? That's what it means in all contexts. :cool:

[Edited on 13-5-2017 by CuReUS]

Eddygp - 14-5-2017 at 03:34

OK, as a small incentive*, I'll offer ~2.5 g or so of fairly pure brominated cinnamic acid (synthesised by yours truly) and 0.5 g or so of very pure p-nitrophenyl benzoate to whoever manages to design a home-chemist-friendly route to capsazepine. By the 20th of June.

* Europe guaranteed; other continents... if you could enlighten me on shipping etc. that would help

[Edited on 14-5-2017 by Eddygp]

Alice - 14-5-2017 at 04:14

@CuReUS

EDIT:

Quote:

Of course the procedure I found was an educational example on very small scale, it doesn't mean it's always the case removing yeast by a centrifudge.
As I think the fermentation of vanillin is very interesting, I finally started doing a bit of literature research about how to remove the yeast other than by a centrifudge. I found loads of information about filtering techniques, so I think I will give it a try, as this might be interesting in general not just for the capsazepine synthesis.

Quote:

I think the succinic acid would react with the diol rather than undergoing a FC acylation.

Both isn't completely impossible, so I wouldn't exclude any possibility. Especially the esters may be activated by HBr and undergo acylation. If esters form, although it's reversible, it wouldn't solve the goal omitting a step, especially a polyester would be unfortunate.

Quote:

what other context is there for free basing ? That's what it means in all contexts. :cool:

I have explained what free basing means in general just in the previous paragraph. Context in this context means the molecule we're talking about. But I'm pretty sure you know how it was meant.

@AvB. Sorry for the late answer, I was busy. You are speaking very indirect and general, so I have no clue what you're talking about. Do you think I don't have a sound understanding of organic chemistry or do you think someone having no sound understanding of organic chemistry should do this and that instead of thinking about new total synthesis? Do you think I don't know anything about total synthesis or are you explaining total synthesis in general? Do you think I should utilize standard reactions or do you think others should utilize standard reactions? How would you define standard reactions and what would be non standard reactions then? If this happens to be a controversy, I'd like to know what's your point.

Quote:

In the case of casazepine, perhaps the most satisfying excersize would be figuring out how to synthesize some of the published starting materials from OTC sources.

I took a different path - as a conscious decision. Anyone can choose whatever exercize this may be. You named another one, more beginner friendly perhaps. As I tried to explain you before, you can either choose to develop OTC reagent synthesis for known routes or you can develop a route according to OTC reagent availability. Both has it's own charm, but there is no such thing like right and false here.

[Edited on 14-5-2017 by Alice]

[Edited on 14-5-2017 by Alice]

CuReUS - 14-5-2017 at 08:33

Quote: Originally posted by Alice

But I'm pretty sure you know how it was meant.

No I didn't,I swear.In fact,I feel like an idiot now for asking such a stupid question

Quote:

yeah,you are right.8 steps it will have to be
btw,I just noticed something funny.In the reaxys pdf posted by waffleSS,the benzazepine is first converted to the bromide salt before reacting it with the isothiocyanate.Why can't you just react it directly ?

Alice - 14-5-2017 at 11:00

Quote: Originally posted by CuReUS

Quote: Originally posted by Alice

But I'm pretty sure you know how it was meant.

No I didn't,I swear.In fact,I feel like an idiot now for asking such a stupid question:

I honestly thought you were just kidding me.

Quote:

yeah,you are right.8 steps it will have to be

Possibly adding sodium succinimide after the grignard one-pot would safe a work-up.

Quote:

btw,I just noticed something funny.In the reaxys pdf posted by waffleSS,the benzazepine is first converted to the bromide salt before reacting it with the isothiocyanate.Why can't you just react it directly ?

I think this has just something to do with the demethylation by HBr done before. I checked one paper (page 9) and in the following step, there is triethylamine added. So it has no impact on the reaction, the amine will just be stable for storage.

[Edited on 14-5-2017 by Alice]

[Edited on 14-5-2017 by Alice]

Assured Fish - 14-5-2017 at 21:35

Sorry i misunderstood what alice wanted to do with that reaction.
I must admit you guys tend to loose me alot in this thread, i feel like the fumbling bafoon trodding along after you guys with pockets full of stones

Quote:

OK, as a small incentive*, I'll offer ~2.5 g or so of fairly pure brominated cinnamic acid (synthesised by yours truly) and 0.5 g or so of very pure p-nitrophenyl benzoate to whoever manages to design a home-chemist-friendly route to capsazepine. By the 20th of June.

Exactly how "home-chemist-friendly" are we talking about here?
Because a lot of the routes suggested already are pretty damn close, with only a few issues arrising by the use of some niche reagents such as trichloroacetic anhydride, Diisobutylaluminium hydride, sulfides etc.
These reagents are difficult to synthesize for sure but could be achieved by a determined amateur chemist.
Also are hydrides and carbon disulfide sufficiently "home-chemist-friendly" for your liking? Hydrides can after all be bought from other members on the forum, although CS2 is a bitch to make.

[Edited on 15-5-2017 by Assured Fish]

CuReUS - 15-5-2017 at 03:27

Quote: Originally posted by Alice

Possibly adding sodium succinimide after the grignard one-pot would safe a work-up.

isn't there a chance that some of the unreacted dihalopropane might also react with the succinimide ?

Quote: Originally posted by Assured Fish

although CS2 is a bitch to make.

just buy it,for chemistry's sake :mad:

Alice - 15-5-2017 at 05:05

@Assured Fish

Quote:

I must admit you guys tend to loose me alot in this thread, i feel like the fumbling bafoon trodding along after you guys with pockets full of stones

Just a matter of practice and experience.

There are just so many things you don't think about if you don't have much experience (or a bad day

). That's normal.

Quote: Originally posted by CuReUS

isn't there a chance that some of the unreacted dihalopropane might also react with the succinimide ?

Sure, but 1,3-diaminopropane is soluble in water while the product amine supposedly isn't. And it has reportedly a logP_ow of -1.3 (wiki, not sure if this is calculated), which means it prefers the aqueous phase as the free base. Recrystallizaton of the substituted succinimides may be another way separating it.

Here is a paper introduced showing a modified Grignard adding 3 mol% anhydrous CuCl2 in THF. Examples are:

p-methoxyphenylmagnesium bromide (1.2 eq.) with octyl bromide (1 eq.): 97% yield

p-dimethylaminophenylmagnesium bromide (1.2 eq.) with 1-chloro-5-bromopentane (1 eq.): 93% yield

With a bit of luck this works good as well with diethyl ether and the two possible reagents 1,3-diiodopropane and 1-chloro-3-iodopropane. CuCl2 is about the most trivial additive I can think of and 3 mol% looks great.

[Edited on 15-5-2017 by Alice]

EDIT:

confused edit removed

[Edited on 15-5-2017 by Alice]

p-chlorophenethyamine prep?

Assured Fish - 15-5-2017 at 22:50

Ok so ive been searching around for a source of fenclonine and have found nadda, its like this stuff is a prescription med or something even though all the sources ive read on the stuff don't refer to it being prescription based. :mad:

So i propose a different route to synthesize pCPEA (p-chlorophenethyamine) based of the same concept but starting from phenylalinine.

The decarboxylation is still the same as the one previously proposed by CuReUS here:
https://erowid.org/archive/rhodium/chemistry/trp.decarbox.en...

Then selective para-chlorination using potassium peroxymonosulfate (oxone) as a catalyst and KCl in acetonitrile.
https://erowid.org/archive/rhodium/chemistry/oxone.aromatic....

The only thing is I don't have direct access to the product Oxone, but i have found a product that contains peroxymonosulfate on ebay that looks like oxone:
http://www.ebay.com/itm/saltscapes-chlorine-free-oxidizer-sh...

Also a source of phenylalinine that's pretty cheap: http://nootropicsdepot.com/dl-phenylalanine-powder/

Alice - 16-5-2017 at 01:44

@Assured Fish

Chlorinations (and halogenations in general) aren't compatible with amines, as it leads to chloramines. Just think about how the reaction works. Oxone oxidizes chloride to chlorine, which is an electrophile and can be either attacked by the pi system of the arene or by the amine. But it may work by protecting the amine. EDIT: Oxone may also directly oxidize the amine.

I was looking for a few possibilities avoiding CS2. The first couple of options involve the transformation of isonitriles into isothiocyanates by different catalysts with elemental sulfur:

R-NC + cat. Se (5 mol%) + Et3N + S in THF, 73 % yield for nBuNC (Link)

R-NC + cat. Te (0.02 mol%) + Et3N + S in THF, 73 % yield for nBuNC (Link)

R-NC + cat. RhH(PPh3)4 + S in acetone (Link)

Selenium and especially tellurium are easy to aquire OTC as far as I see. Buying triphenylphosphine gives no fortune compared to buying CS2, making it OTC is lots of work. The isonitriles can either be made from the amine and chloroform or from the halogen compound utilizing AgCN.

The next couple of reactions are thiocyanate <---> isothiocyanate isomerization based. Isomerizations lead to the thermodynamically more favorable isothiocyanates - if they work:

thermal isomerization in solution (may not be suitable for non activated primary alkyl thiocyanates)

gas phase isomerization (reactive distillation)

heating alkylthiocyanate with metal thiocyanates

utilizing a lewis acid like ZnCl2

https://books.google.com/books?id=cAm7rA_D25wC

https://books.google.com/books?id=-OWIAwAAQBAJ

Third possibility:

reaction of alkyl halogenides with Hg(SCN)2 (possibly bad yield for primary alkyl halogenides, works at least bad for BuBr) (Link)

EDIT2: Would also be interesting how AgSCN works on primary alkyl halogenides, it wasn't examined in the paper above.

This is just what I found via superficial literature search. There may be more options of course.

[Edited on 16-5-2017 by Alice]

[Edited on 16-5-2017 by Alice]

CuReUS - 16-5-2017 at 06:39

Quote: Originally posted by Assured Fish

Ok so ive been searching around for a source of fenclonine and have found nadda, its like this stuff is a prescription med or something even though all the sources ive read on the stuff don't refer to it being prescription based. :mad:

https://raypeatforum.com/community/threads/affordable-source...

Alice - 16-5-2017 at 09:28

Two new drafts for the second part, the first for p-chlorophenylethyl halogenide the second for p-chlorophenylethylamine. I dont suggest any specific chlorination for now, nor do I comment it, at least for now.

EDIT:

After I had a closer look at the first suggestion, it's a bit overcomplicated, so I made another draft:

The first step is taken from the literature, where NaBr is used (90% yield for phenylalanine). I speculate NaBr may be substituted by NaCl which hopefully works too. For the chlorination the procedure posted by Assured Fish may work good here, a closer look at the original publication reveals for isobutylbenzene yields of 72% para, 2% ortho, and 1% disubstitution (75% conversion). Fairly good! The substitution performed by AgCN is described in the literature, but I have to find a good source first. The decarboxylation hopefully works freely as known for similar structures. The literature source for the last step is described in my previous post and can be found here.

[Edited on 16-5-2017 by Alice]

[Edited on 16-5-2017 by Alice]

[Edited on 16-5-2017 by Alice]

Assured Fish - 16-5-2017 at 21:08

Quote:

Chlorinations (and halogenations in general) aren't compatible with amines, as it leads to chloramines. Just think about how the reaction works. Oxone oxidizes chloride to chlorine, which is an electrophile and can be either attacked by the pi system of the arene or by the amine. But it may work by protecting the amine. EDIT: Oxone may also directly oxidize the amine.

Fuck.

CuReUS i would incorage you to follow that link because its a dead end, even if you use the search engine on the site.
I did manage to find a source for fenclonine however its way over priced.
http://store.molbase.com/product-26118.html

Also please don't then give me this reference because I already checked it out and the product they are selling doesn't actually contain fenclonine, they sell Centrophenoxine which doesn't contain any fenclonine, it contains another compound called Meclofenoxate which is an ester of dimethylethanolamine and 4-chlorophenoxyacetic acid which is confusingly also named pCPA just to add confusion to a subject that the general public is already ignorant about.
http://www.aip-health.com/pcpa.html

@Alice
Thanks for the correction, looks like a protecting group of succinimide/phthalamide is the best way to go about it then and it could still be accomplished in 2 pots.

A small note though Alice regarding your first suggestion, the hunsdieker reaction requires the carboxylic acid to be converted to a silver, lithium or thalium carboxylate first, I also am pretty sure it has trouble proceeding on saturated alkyl carboxylates, it would be better to decarboxylate and then diazatize the amine followed by reaction with the halide salt to get the desired alkyl halide.

Quote:

I was looking for a few possibilities avoiding CS2. The first couple of options involve the transformation of isonitriles into isothiocyanates by different catalysts with elemental sulfur:

Yusss someone else thinks the isonitrile is a better route than CS2, try telling CuReUS that; he thinks we're mad.

Edit: just realised that phthalamide would also be chlorinated so succinimide is really the best option.

[Edited on 17-5-2017 by Assured Fish]

[Edited on 17-5-2017 by Assured Fish]

Alice - 17-5-2017 at 03:01

Quote: Originally posted by Assured Fish

@Alice
Thanks for the correction, looks like a protecting group of succinimide/phthalamide is the best way to go about it then and it could still be accomplished in 2 pots.

Found a comment from Nicodem on a very similar problem. He mentioned protonation of the amine may be sufficient. This may have implications on the type of chlorination reaction to be chosen. (Link).

Quote:

A small note though Alice regarding your first suggestion, the hunsdieker reaction requires the carboxylic acid to be converted to a silver, lithium or thalium carboxylate first, I also am pretty sure it has trouble proceeding on saturated alkyl carboxylates, it would be better to decarboxylate and then diazatize the amine followed by reaction with the halide salt to get the desired alkyl halide.

It may work better for unsaturated acids but I don't think it's limited to such cases. Honestly I was just looking if it works for aliphatic acids but didn't read into details. See The Degradation Of Carboxylic Acid Salts By Means Of Halogen - The Hunsdiecker Reaction:

Quote:

The greatest utility of the Hunsdiecker reaction lies in the preparation of aliphatic halides, and most of the investigations of the reaction have been in the aliphatic series.

Anyhow, I discarded the first route more or less, as like mentioned, it's a bit overcomplicated. About your second point, not sure if the reaction on primary amines works as excellent as the one I found. I remember there are some issues with alkene and alcohol formation.

Quote:

I was looking for a few possibilities avoiding CS2. The first couple of options involve the transformation of isonitriles into isothiocyanates by different catalysts with elemental sulfur:

Yusss someone else thinks the isonitrile is a better route than CS2, try telling CuReUS that; he thinks we're mad.

We're all mad here...

Quote:

Edit: just realised that phthalamide would also be chlorinated so succinimide is really the best option.

Probably not, as it's deactivated. The authors of the paper you referred to (KCl-Oxone system) didn't find any chlorinated product for benzoic acid for example.

Here is the 4th draft assuming there is no need for amine protection other than protonation. The first two steps may be done the other way round, additionally the second popular isocyanide formation reaction is shown, avoiding AgCN:

EDIT: As an additional note: THF utilized in the last step may be substituted by diethyl ether or dioxane making this reaction more OTC.

[Edited on 17-5-2017 by Alice]

[Edited on 17-5-2017 by Alice]

[Edited on 17-5-2017 by Alice]

CuReUS - 17-5-2017 at 05:59

Quote: Originally posted by Alice

Selenium and especially tellurium are easy to aquire OTC as far as I see.

really ?

Quote: Originally posted by Assured Fish

I also am pretty sure hunsdicker has trouble proceeding on saturated alkyl carboxylates

actually,the hunsdicker reaction gives excellent yields for saturated acyclic and alicyclic compounds.It gives shitty yields for aromatic COOH's

Quote: Originally posted by Assured Fish

Yusss someone else thinks the isonitrile is a better route than CS2, try telling CuReUS that; he thinks we're mad.

isonitriles and Te.What a wonderful combination to stimulate one's olfaction.

spring is going to come early for some this year

[Edited on 17-5-2017 by CuReUS]

Alice - 17-5-2017 at 06:14

Quote: Originally posted by CuReUS

Quote: Originally posted by Alice

Selenium and especially tellurium are easy to aquire OTC as far as I see.

really ?

I saw tellurium sold for element collections at ebay and as a money investment metal.

Good thing is as 0.0002 eq. are required, it makes 2.6 mg at 100 mmol scale.

[Edited on 17-5-2017 by Alice]

Alice - 21-5-2017 at 09:55

As I didn't mention this before, in my first route draft where I suggested cyclisizing the amine directly with the benzyl ether, displacing methoxide, it caused quite some doubts about how this might be possible. This idea came to me as I remembered having read a paper about the synthesis of levetiracetam (An alternate synthesis of levetiracetam) in the past and thought about if there is a possible cut through for the present synthesis. For some instances the case differs, but for others it doesn't, which I will explain in the following.

For the levetiracetam synthesis, 2-aminobutanol is reacted with gamma-butyrolactone whereas in the first step aminolysis with ring opening occurs resulting in an amide. Then the amide-N acts as a nucleophile and substitutes the hydroxy group. The first step isn't really sursprising, while the second one would probably not have been expected. It becomes more clear as in a former synthesis 4-chlorobutyryl chloride was utilized instead of gamma-butyrolacton, a much more expensive and hazardous reagent. The reaction is performed at different temperatures, 160 °C (8 h, 76% yield, 5 mol% H3PO4 as catalyst) and 225 °C (10 h, 93% yield, no catalyst) solvent-free. Additionally the reaction can also be enhanced by microwave irradiation providing lower temperatures and greatly reduced reaction times (1 h, 200 °C, 82% yield). The reaction works because five-membered ring formation is favored (Baldwin's rule), it even outperforms hydroxide being a bad leaving group and an amide being a bad nucleophile.

For the reaction I suggested, a less kinetically and less energetically favored 7-membered ring is proposed to form and the less favorable methoxide as the leaving group. Nevertheless, two out of six angles are sterically fixed, making the 7 membered ring already partially in place, the benzylic position is activated for substitution compared to an aliphatic position, and the amine is a good nucleophile. An interesting effect known for benzylic substitution reactions is the dependence of rate constants on aromatic substitution pattern. While EDGs in para and ortho position enhance reaction rates, destabilizing the bond between benzylic carbon and substituent and stabilization of the transition state. EWGs show the opposite effect. (See: Kinetics and Mechanism of the Pyridinolysis of Benzyl Bromides in Dimethyl Sulfoxide or https://books.google.com/books?id=AgU4AAAAIAAJ&pg=PA134).

As I mentioned before my suggestion is, in my opinion, a very experimental suggestion, but didn't come from nowhere.

The only question which matters for the proposed reaction is if it proceeds in a considerable speed before pyrolysis occurs. H3PO4 or microwave probably wouldn't hurt too

[Edited on 21-5-2017 by Alice]

tsathoggua1 - 30-5-2017 at 09:07

Having looked up fenclonine, I can more or less guarantee that, short of third-world or countries where pharmacists are bribable for more or less anything if somebody has the money, given its action that isn't a drug that is going to be OTC. Nasty looking stuff too, very similar in structure and action to the para-haloamphetamines, which, 4-fluoroamphetamine aside, are notorious serotonergic neurotoxins that cause profound, massive depletion of tryptophan hydroxylase. IIRC at one time para-chloroamphetamine was originally developed, or certainly, used, as a diet drug, until it became known quite what a noxious bunch of compounds they are. Certainly the alpha-methylated homologs are, and going from a quick glance at the wiki article, fenclonine is also (deliberately) used to knock out serotonin production in cases of carcinoid, which is the term for a serotonin-producing tumor. Not really the kind of thing one would pick up in a health food shop, nootropic vendor, or anything along those lines, or ingest without it being pretty essential.

As for the production of 1,3-chloroiodopropane, I recall that iodine monochloride adds to double bonds to give chloroiodides. If iodine is available or KI, NaI etc. then the synthesis would require only chlorine gas, I made a couple of oz of ICl a little while back actually and the synthesis is quite easy, if a little hairy.

Its water reactive, air reactive, doesn't much like prolonged exposure to sunlight from what I've observed over time (it appears like the dregs in a flask, left outside, since I haven't yet got round to unsticking some stuck joints on the still I used that have gotten gunked up with iodine and possibly ICl in the solid phase (its got weird melting kinetics, reasonable nominal melting point, but it can seemingly supercool and remain liquid for prolonged periods of time that are significantly below the supposed freezing point, plus two crystalline forms. I actually have mine stored in a glass bottle with a chemical resistant cap and seal, not sure what plastic since I didn't buy them, the filth raided my place on a bogus warrant ostensibly to 'take samples for analysis', and what they actually DID, was trash the place, place small quantities of various reagents in these resistant bottles they brought, which they then left on the fucking bench top, along with some opened bottles of ether, THF and Li. Bloody moronic cunts if they weren't deliberately trying to burn the house down (there is some history behind that thought, although I'll not go into too many details)

So I don't know what plastic the caps and seals are made of, I'd guess some kind of fluoropolymer because ICl is damned aggressive towards many plastics, although it hasn't attacked the teflon tape used to assist sealing the joints it made mincemeat of grease and of keck clips (they fell to bits at the rate that I'd used all but four of mine within a day or twos work. Didn't do much good to the straps on one of my gas masks either.) The dregs are still in the receiver flask, and it appears to dissociate in bright sunny weather to give greenish fumes within the still sealed flask, and reform itself overnight or during not so bright weather. Definitely not something to inhale, I'd treat it like bromine, only quite a bit nastier, a bit easier to confine and unlike bromine, it is very moisture sensitive, a drop into water dissociates instantly into sinking iodine particulate and a greenish yellow puff of chlorine gas. Synthesis is trivial though, a chlorine generator connected to a drying tube packed with anhydrous CaCl2 with a bit of sacrificial wire wool to hold the drying agent in place if using liquid-phase chemistry to generate your Cl2, and the dried Cl2 is run through a condenser, horizontally, set up as a distillation rig. A little excess I2 is advisable, since any formed iodine trichloride (a yellowish to orangey solid) that forms initially as a byproduct reacts with solid I2 in the condenser (I used two liebigs in series with one another, one to pack with I2, and the second to condense the vapors and the recieving flask in an ice-salt-water bath with a little ethylene or diethylene glycol (Forget which now, but this just serves to cool the recieving flask down so it isn't too important which, mainly because it really isn't something you want to work with outside of a hood, unless you do it outdoors (which I did)

As I recall, it adds across double bonds like a halogen forming mixed chloroiodides. Whether or not the two halogens add proximally or distally to each other on an allene I am not sure, but if the latter occurs to any extent then I would think propadiene, best diluted in a carrier gas such as argon, bubbled through a solution of ICl due to the potent oxidizing nature of the beast, in GAA (which is a compatible solvent for ICl, Sasha Shulgin (may his soul rest gloriously) used it during his synthesis of 2C-I for the iodination of 2C-H and he did so as a solution of the interhalogen in GAA. would thus serve, IF distal addition occurs rather than forming an tetrahalopropane, or hexahalide

Then it might serve to produce the 1-chloro-3-iodopropane.

clearly_not_atara - 30-5-2017 at 09:26

I think you can add halogens to cyclopropane and get 1,3-halopropanes. In some literature the related 1,3-dichloropropEne is used as a 1,3-linker that can attach each end separately.

Assured Fish - 30-5-2017 at 16:38

@tsathoggua1
propadiene exists at an equalibrium with propyne and therefore is likely to form 1,2 dihalogenated propane as a major side product. The other issue with halogenating propadiene is how the fuck you would produce propadiene in the first place.

Atara's suggestion for using cyclopropane would be preferable given that it can be produced by reaction of sodium metal with 1,3 dibromopropane.
However this would again just push us back to having to prepare 1,3 dibromopropane. I reckon a better way to prepare 1-chloro-3-iodopropane would be to first prepare allyl chloride by substitution of allyl alcohol with HCl in the presence of aluminium chloride, followed by distillation BP 45*C and then carry our a reverse markovnicov using hydriodic acid followed again by distillation, the BP of 1-chloro-3-iodopropane according to sigma is 170 - 172*C, as for the BP of 1-chloro-2-iodopropane I am unable to find any references but 1-chloro-2-bromopropane has a BP of 116-117*C and 1-chlor-3-bromopropane has a BP of 144-145*C and this would suggest that the iodides would also have a sufficiently different BP so that fractional distillation would be plausible.

https://en.wikipedia.org/wiki/Allyl_chloride

http://www.sigmaaldrich.com/catalog/product/aldrich/234478?l...

http://www.sigmaaldrich.com/catalog/product/aldrich/231274?l...

http://www.sigmaaldrich.com/catalog/product/aldrich/b62404?l...

Alice - 30-5-2017 at 17:09

Seems like I don't get the point. What's the problem with chlorinating 1,3-propanediol by NaCl/H3PO4 followed by Finkelstein reaction?

CuReUS - 31-5-2017 at 09:30

Quote: Originally posted by tsathoggua1

Having looked up fenclonine, I can more or less guarantee that, short of third-world or countries where pharmacists are bribable for more or less anything if somebody has the money, given its action that isn't a drug that is going to be OTC.

why do you want to buy it from a brick and mortar shop,you could just order it online.Don't tell me you take the literal meaning of the word OTC

clearly_not_atara - 31-5-2017 at 10:43

https://www.google.com/patents/US3927131
I thought this was a thing.

Glycerol + 3 HCl >> 1,2,3-trichloropropane

"" + base + [rare earth metal oxide?] >> 1,3-dichloropropylene

Quote: Originally posted by Alice

Seems like I don't get the point. What's the problem with chlorinating 1,3-propanediol by NaCl/H3PO4 followed by Finkelstein reaction?

You get a mixture of dichloropropane, chloroiodopropane, and diiodopropane. If you don't mind losing at least half of your starting material along with plenty of iodine it could be okay. Separating that mixture will require fractional distillation at least.

tsathoggua1 - 1-6-2017 at 00:22

Curious-guilty as charged, in that instance. Thats having a literally-inclined mind for you, it does that sometimes and realizes later

That, and I am not sure how much I trust online pharmacies, particularly ones I haven't in the past done business with. There are certainly plenty of skeezy thieving scumbags around, its just the sort of business that attracts such vermin like shit draws flies.

Also, whilst I don't know for sure, it looked like the kind of thing that might not survive the test of time, with regards to being in current use or not, owing to the discontinuation of para-chloroamphetamine, which, unfortunately, was used as a diet drug, until it was realized that the non-fluorinated para-halogenated amphetamines (and presumably para-cyano/4-nitro also) are seriously bad news and produce potential permanent or very very long lasting depletion of tryptophan hydroxylase. Although at least, the phenethylamine homolog might prove to be a better substrate for MAO-a without the alpha-substituent.

Didn't stop some bloody stupid and reckless online grey market vendors marketing para-bromo(meth)cathinone for some time, though. Which if its still around, could be an alternative with reduction of the ketone and finkelstein reaction, if an alpha-methyl substituent (using the nomenclature for numbering of phenethylamines and amphetamines) would produce an analog of capsazepine active at TRPV1 receptors.

As for the propadiene, its sold in my part of the world (UK of all the shitheaps) for use in welding. I hadn't realized about the equilibrium, or at least, wasn't sure how fast they would interconvert and had thought to distill it under a freezing mixture (or rather, let it distill itself, without external applied heat), the propyne in MAPP gas would come off first.. How fast do they interconvert? and what are the numbers like for the relative proportions of propyne and propadiene at RT and in the liquid phase? Perhaps letting it boil off a solid, porous substrate such, ideally, as that from an empty acetylene bottle since acetylene at least, doesn't particularly like to be stored in the liquid phase, although if not under pressure, would that not largely mitigate any explosion risk? if in an open system that is.

(if nothing else, at least some of those absorbents use DMF as a solvent, some use acetone, and some DMF which wouldn't exactly be a crappy booby prize for effort expended)

[Edited on 1-6-2017 by tsathoggua1]

[Edited on 1-6-2017 by tsathoggua1]

DJF90 - 1-6-2017 at 01:46

Actually most "MAPP" gas these days (at least here in the UK) is a propane/propylene/dimethyl ether mixture. Generally sold under the name "MAPP Pro" or something similar, and ironically doesn't contain MAPP. I believe this substitute product was formulated following a shortage of MAPP a few years back.

Alice - 1-6-2017 at 03:03

Quote:

You get a mixture of dichloropropane, chloroiodopropane, and diiodopropane.

Sure, but boiling points lie sufficiently apart (120 °C, 170 °C, 224 °C). Dichloropropane can be removed without vacuum, 1-chloro-3-iodopropane by aspirator vacuum, the diiodo compound remains and can be recycled or used for other reactions. I don't think this is a bad deal considering the easy preparation and workup.

EDIT: erroneous logic removed.

[Edited on 1-6-2017 by Alice]

EDIT2:

I was indeed using a model not suitable here which gave me 75% yield.

After having removed some errors, here is my revised numerical result for 1 eq. dichloropropane and 0.9 eq NaI. In the first place I tried out 1 eq. NaI, but it turned out this does no favor compared to 0.9 eq. and leads to a product ratio of 25% : 50% : 25% instead of 30% : 50% : 20% (rounded). The overall iodide efficiency therefor is 56%. Trying 0.8 eq NaI I obtained the following ratio: 36% : 48% : 16% giving a NaI efficiency of 60%. A is the dichloro, B NaI, C chloroiodo, and D is the diiodo compound. I hope this is free of silly errors now.

[Edited on 1-6-2017 by Alice]

[Edited on 2-6-2017 by Alice]

halogen - 8-6-2017 at 19:19

Azetidine might be an ideal way to introduce the C3 segment on to catechol, directly. Thereupon reaction with formaldehyde completes the cycle. More precisely an acid salt would be used.

Who has azetidine lying around? This preparation in orgsyn uses ethyl acrylate to protect the amine. http://orgsyn.org/demo.aspx?prep=CV6P0075

I wonder if it is possible to prepare by anodic oxidation in dilute solution, of any gamma amino butyrate salt azetidine itself or aminopropanol.

Though oxetane is much less toxic/carcinogenic than oxirane, apparently not being an alkylating agent, the greater equilibrium of the amine salt in the body could conceivably be relevant. I couldn't find anything to settle this, looking quickly. The relative difficulty of synthesis makes azetidines uncommon - so says wikipedia.

[Edited on 9-6-2017 by halogen]

Assured Fish - 8-6-2017 at 21:17

@halogen How would you go about attaching the catechol ring with the azetidine, The amount of effort required to prepare the azetidine might make other methods considerably more accessible.

halogen - 9-6-2017 at 07:23

That occurred to me. Actually, looking into it the O than the C seems more likely to be alkylated... in addition to the o/p problem. So, bad idea. Sorry.

GABA electrolysis might just work, though, being necessarily dilute, separating it would be inconvenient. I should take out a patent. Come to think of it, maybe the primary radical can be trapped by catechol, benzodioxole or something. That would be the final word in convenience.

[Edited on 9-6-2017 by halogen]

clearly_not_atara - 9-6-2017 at 12:49

On the subject of heterocycles, I thought of a way to use 2-aminothiazole in order to avoid using other sulfur compounds. Unfortunately, I'm not sure how to synthesize 2-aminothiazole, although I don't think it's too hard. For the direct synthesis you can make a bromoacetaldehyde synthon via the reaction of a vinyl ether with Br2 IIRC.

Anyway, step 1 is a Mannich reaction, step 2 is just the addition of p-chlorophenethyl iodide to the nitrogen.

Step 3 is ozonolysis: my guess was that alkylating the nitrogen makes thiazole lose its aromaticity, meaning the alkene can be oxidized. The resulting dicarboxylic acid should eliminate to the thiourea.