Testosterone synthesis from DHEA

MikeBlast

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Below is the synthesis of testosterone from DHEA provided by Patrick Arnold. Protection group has been inferred and reduction method is unknown.

1. 3β-O Protection with TMSCl
2. 17β Enantioselective reduction
3. 17β Esterification
4. 3β-O Deprotection with TBAF
5. 3-O Oppenauer oxidation with simultaneous alkene rearrangement to conjugated position
 

G.Patton

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Hello. What is the value of your post without detailed explanation?
 

MikeBlast

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My intention was to start the discussion of testosterone synthesis as I couldn't find much online. If this is the wrong place to make my post I apologize.
 

G.Patton

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No problem. I would in your place state clearly an intention in a post :)
 

MikeBlast

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It looks like this can be simplified into a 3 step process.
1. 3-O Oppenauer oxidation with simultaneous alkene rearrangement to conjugated position
2. 17β Enantioselective reduction by Saccharomyces cerevisiae (bakers/brewers yeast)
3. 17β Esterification

I haven't found yields for androstenedione -> testosterone but based on similar substrates in Microbial Transformations of Steroids it would likely be around 70%

Microbial Transformations of Steroids. A Handbook. Willium Charney and Hershel L. Herzog. Academic Press, New York, 1967​

 

MikeBlast

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It turns out 17β is the kinetic product and can be produced with good selectivity (17α: 3%, 17β: 97%) using NaBH4 alone.
https://chemistry-europe.onlinelibrary.wiley.com/doi/pdf/10.1002/chem.202100967

The above study also shows MPV reduction has moderate selectivity (17α: 34%, 17β: 66%). I would be interested to know if simultaneous oxidation and reduction of the 3 and 17 positions can be achieved using an Al catalyst. I would imagine the conjugated 3 keto form would be favored, driving the reaction forwards.

More details about the oppenauer oxidation for my own reference https://doi.org/10.1002/recl.19370560206
 

HerrHaber

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Biochemist me advises not to consume any racemic steroids since it may lead to irreversible damage that will be observed too late.
 

MikeBlast

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Do you have any reason to believe 17α-testosterone (epitestosterone) is toxic? It is an endogenous steroid that exists at concentrations of approximately equal to testosterone.
 
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HerrHaber

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I'm more concerned about it's function (there are more modern testosterone modulators with much less side effects)
 

MikeBlast

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Epitestosterone is a positive allosteric modulator of the GABAA receptor. It appears to be neuroprotective and a high testosterone / epitestosterone ratio seems to be correlated with autism.

SARMs are definitely something I am looking into. They seem to have their own disadvantages such as reducing estrogen levels. Once I figure out the synthesis of testosterone I will look into more tissue selective steroids like boldenone and DHT. Synthesizing fluorinated SARMs is beyond me at this point.
 

HerrHaber

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I hope to have been involved in motivating you to further document as I used to dive into science abbysally deep... then find my way out. I like your thinking!
 

MikeBlast

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You have been. I really appreciate the feedback. I don't have a formal background in chemistry or pharmacology, so I was hoping to my work checked by this forum :)
 

HerrHaber

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passion is key... I will try to be attentive and help you whenever
 

HerrHaber

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you are most welcome!
 
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