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MESO-Rx Exclusive New Article on Testosterone by Type-IIx Published in Ongoing Anabolic Steroid Series

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MESO-Rx is excited to unveil the latest installment in its 11-part series exploring the unique characteristics of various anabolic steroids. The new article, written by @Type-IIx, provides an in-depth look at testosterone.

“Testosterone is a unique anabolic-androgenic steroid (AAS), essential for male sexual function, muscle growth, and insulin sensitivity. It amplifies and aromatizes, unlike other AAS, contributing to its critical role in male physiology and bodybuilding practices.”

thinksteroids.com

Testosterone Insights: Unique Characteristics of Anabolic-Androgenic Steroids – Part 5

Discover the vital role of testosterone in male physiology and explore its benefits for sexual function, insulin sensitivity, and muscle anabolism.
thinksteroids.com thinksteroids.com
 
BigNattyMcGee said:
These just keep getting better @Type-IIx !! I can't wait to read about Oxymetholone and Nandrolone.
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When I was thinking through the AAS that offer unique features, I couldn't particularize anything too unique about Anadrol.

Oxymetholone (Anadrol) Particulars
I can probably boil it down to this: Anadrol acts principally as a prohormone (Schänzer view) to 17α-methyl-5α-androstane-3α,17β-diol, this is 17α-methylated-3α-diol [referred to in this very article]. I have modeled its activity using the SwissTargetPrediction & SwissADME tools that show that it is a good AR ligand as well as ER-β ligand. ER-β modulates muscle remodeling and tends to oppose classical ER-α effects, "putting the brakes on" effects like feminization/gynecomastia, etc.

The thing to understand about prohormones of the "-diol" class is that they are metabolized by 3α/β-HSD to oxidize 3-hydroxyl to 3-ketone as well, that typically but not always is a better AR ligand due to the importance of the 3-keto group to serve as an electron acceptor with its lone pair of electrons, forming a strong bond with the charged amino acids of the AR's N-terminus. My September Newsletter discusses the -diols, -diones, and 4- & 5- prodrugs in the section titled, §2. Prohormones and Designer Steroids, Redux – Prohormones were to Metabolic Trickery as Designer Steroids were to Legal Chicanery. I will publish this soon, so I encourage anyone who has not to visit Ampouletude: Home of Type-IIx and click "Sign Up for Type-IIx's Newsletter."

Still, acting principally as a prohormone is not unique to Anadrol, since Epistane is similar. Another quality of Anadrol is that it is estrogen-sensitizing a la progestagenic effects and also probably benefits joints, acting oppositely to Winstrol's effects on joints.
 
Type-IIx said:
When I was thinking through the AAS that offer unique features, I couldn't particularize anything too unique about Anadrol.

Oxymetholone (Anadrol) Particulars
I can probably boil it down to this: Anadrol acts principally as a prohormone (Schänzer view) to 17α-methyl-5α-androstane-3α,17β-diol, this is 17α-methylated-3α-diol [referred to in this very article]. I have modeled its activity using the SwissTargetPrediction & SwissADME tools that show that it is a good AR ligand as well as ER-β ligand. ER-β modulates muscle remodeling and tends to oppose classical ER-α effects, "putting the brakes on" effects like feminization/gynecomastia, etc.

The thing to understand about prohormones of the "-diol" class is that they are metabolized by 3α/β-HSD to oxidize 3-hydroxyl to 3-ketone as well, that typically but not always is a better AR ligand due to the importance of the 3-keto group to serve as an electron acceptor with its lone pair of electrons, forming a strong bond with the charged amino acids of the AR's N-terminus. My September Newsletter discusses the -diols, -diones, and 4- & 5- prodrugs in the section titled, §2. Prohormones and Designer Steroids, Redux – Prohormones were to Metabolic Trickery as Designer Steroids were to Legal Chicanery. I will publish this soon, so I encourage anyone who has not to visit Ampouletude: Home of Type-IIx and click "Sign Up for Type-IIx's Newsletter."

Still, acting principally as a prohormone is not unique to Anadrol, since Epistane is similar. Another quality of Anadrol is that it is estrogen-sensitizing a la progestagenic effects and also probably benefits joints, acting oppositely to Winstrol's effects on joints.
Click to expand...
Thanks @Type-IIx - much appreciate your explanations and linking back to other articles. Helps me connect the dots (albeit s l o w l y ).

I better understand why Anadrol and Winstrol have a complimentary pairing. I am curious if this pairing wouldn't just help offset potential joint issues from Winstrol, but also offset potential estrogen sensitivity issues from Anadrol (there is an experiment waiting to happen here. . )
 
BigNattyMcGee said:
Thanks @Type-IIx - much appreciate your explanations and linking back to other articles. Helps me connect the dots (albeit s l o w l y ).

I better understand why Anadrol and Winstrol have a complimentary pairing. I am curious if this pairing wouldn't just help offset potential joint issues from Winstrol, but also offset potential estrogen sensitivity issues from Anadrol (there is an experiment waiting to happen here. . )
Click to expand...
Yes, by virtue of its antagonizing PR, I believe that this is the case. The two are complementary in this regard, "middling-out" sensitivity to, e.g., gyno.
 
BigNattyMcGee said:
Thanks @Type-IIx - much appreciate your explanations and linking back to other articles. Helps me connect the dots (albeit s l o w l y ).

I better understand why Anadrol and Winstrol have a complimentary pairing. I am curious if this pairing wouldn't just help offset potential joint issues from Winstrol, but also offset potential estrogen sensitivity issues from Anadrol (there is an experiment waiting to happen here. . )
Click to expand...
One of my favorite ways to polish off the end of a bulk, is to run last 5-6 weeks of 100mg of anadrol and 50mg of winstrol on top of Test and Npp. The synergy between anadrol and Winstrol is truly amazing. If you are going to experiment with the 2, you will find that it definitely does offset the potential estrogen sensitivity issues that anadrol has been known to bring to the table, however, it also can help combat most of not all of the progestagenic effects cause by nandrolone and trenbolone, by combatting progesterone Winstrol indirectly lowers prolactin. Simple solution for guys that hate the effects of Caber, the only downside is winny's half life is shorter. 9 hrs. for oral and about
24hrs. for Injectable. Where as caber's half-life is somewhere in the ballpark of 63-69 hrs. So using Winstrol throughout an entire cycle to combat progestagenic effects is not ideal.
 
Type-IIx said:
When I was thinking through the AAS that offer unique features, I couldn't particularize anything too unique about Anadrol.

Oxymetholone (Anadrol) Particulars
I can probably boil it down to this: Anadrol acts principally as a prohormone (Schänzer view) to 17α-methyl-5α-androstane-3α,17β-diol, this is 17α-methylated-3α-diol [referred to in this very article]. I have modeled its activity using the SwissTargetPrediction & SwissADME tools that show that it is a good AR ligand as well as ER-β ligand. ER-β modulates muscle remodeling and tends to oppose classical ER-α effects, "putting the brakes on" effects like feminization/gynecomastia, etc.

The thing to understand about prohormones of the "-diol" class is that they are metabolized by 3α/β-HSD to oxidize 3-hydroxyl to 3-ketone as well, that typically but not always is a better AR ligand due to the importance of the 3-keto group to serve as an electron acceptor with its lone pair of electrons, forming a strong bond with the charged amino acids of the AR's N-terminus. My September Newsletter discusses the -diols, -diones, and 4- & 5- prodrugs in the section titled, §2. Prohormones and Designer Steroids, Redux – Prohormones were to Metabolic Trickery as Designer Steroids were to Legal Chicanery. I will publish this soon, so I encourage anyone who has not to visit Ampouletude: Home of Type-IIx and click "Sign Up for Type-IIx's Newsletter."

Still, acting principally as a prohormone is not unique to Anadrol, since Epistane is similar. Another quality of Anadrol is that it is estrogen-sensitizing a la progestagenic effects and also probably benefits joints, acting oppositely to Winstrol's effects on joints.
Click to expand...
For those of you whose interest was piqued by the following passage of this article:

The mid-2000s was a positive inflection point, though brief, for the revitalization of AAS research and development, ushering in the prohormone and designer steroid era (e.g., THG, 4-diols, 19-nor-diols, 17α-methyl analogues, 1-Testo). Again, criminalization was the public policy response that followed until the 2010s experienced a revitalization of… basic testosterone!
Click to expand...
The section referred to above will actually be in this month’s October Newsletter, that you can Sign Up for at Ampouletude: Home of Type-IIx
 
Whereas testosterone treatment is associated with increased blood serum and brain levels of allopregnanolone and DHEA, synthetic AAS reduce them, along with their corresponding unconjugated forms and precursors (e.g., 17-hydroxypregnenolone, 5-androstene-3β,17β-diol, progesterone). [13]. [14]. [15].
Click to expand...

So far I've not found a definite statement on whether or not neurosteroids cease with exogenous testosterone use or not. If I understand this quote correctly, exogenous test should not decrease allopregnenolone and dhea, right? I've read it's possible that when fully shut down through exogenous test, dhea and pregnenolone also shut down, which would be avoidable through HCG.

Is it individual, whether the neurosteroids decrease or not?
 
Rakusa said:
So far I've not found a definite statement on whether or not neurosteroids cease with exogenous testosterone use or not. If I understand this quote correctly, exogenous test should not decrease allopregnenolone and dhea, right? I've read it's possible that when fully shut down through exogenous test, dhea and pregnenolone also shut down, which would be avoidable through HCG.

Is it individual, whether the neurosteroids decrease or not?
Click to expand...
Go through the cites bro, T does not deplete neurosteroids but synthetic AAS do. This article pulls it all together. Don’t believe me? Gotta do the research yourself so, and everything you need is herein.
 
Type-IIx said:
Go through the cites bro, T does not deplete neurosteroids but synthetic AAS do. This article pulls it all together. Don’t believe me? Gotta do the research yourself so, and everything you need is herein.
Click to expand...
Just saw your edit, I was a little to fast with my comment. Great research!
 
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