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Thread: Took Anabolic Steroids by mistake, advice on how best way to stop taking them

  1. #1
    anabolicmistake is offline New Member
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    Exclamation Took Anabolic Steroids by mistake, advice on how best way to stop taking them

    My friend and i are rugby players that are recovering from a few injuries and would like to get back to our original strength and so forth.

    We got tired of not making a lot of progress due to our minor injuries and decided some form of test booster or prohormone would help out with recovery.

    We went to a supplement store in SD and asked for the best stuff he had. The guy sold us "Tren 50" buy Silver Pharma, or Silver Star Pharma. We didnt expect it to be anything legit, turns out it was straight up Tren. Estra-4, 9-diene-3, 17-dione.

    We didnt really pay attention to it until this weekend. Once we looked it up we realized we weren't exactly prepared to take a full blown cycle of tren, especially since this would be our first time with any form of performance enhancement.

    our question. How to get of it safely without any crazy side effects?

    we have been on for about 2 weeks taking the bottle recommended dosage of 1 pill twice a day, 50 mgs per pill. so 100 mgs a day.

  2. #2
    austinite's Avatar
    austinite is offline HRT Specialist ~ AR-Platinum Elite-Hall of Famer ~
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    Well, I don't see how that's tren . Anyway, just stop taking it and get some NAC to clean up your liver.
    ~ PLEASE DO NOT ASK FOR SOURCE CHECKS ~

    "It's human nature in a 'more is better' society full of a younger generation that expects instant gratification, then complain when they don't get it. The problem will get far worse before it gets better". ~ kelkel

  3. #3
    ChiveOn's Avatar
    ChiveOn is offline Senior Member
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    This is not actual trenbolone .

    I belive the chemical name for oral trenbolone is metribolone.

    Metribolone

    Pharmaceutical Name: Methyltrienolone
    Chemical structure: 17-methylestra-4,9,11-trien-3-one,17b-ol
    Molecular weight of base: 284.3974

    Effective dose: 5-15 mg / day
    Average Street-price: Only available for research purposes.
    Available Doses: None

    Brands & Products: Originally produced by Negma, but never approved for production.

    Characteristics:

    Methyltrienolone is structurally similar to trenbolone (Parabolan /Finaplix ), a well-liked and powerful androgen that does not aromatize to estrogen. The difference is the attachment of a 17-alpha-methyl group for oral activity. So one could refer to methyltrienolone as oral trenbolone. It was first explored quite some time ago by Negma in France, the same company that marketed Parabolan (trenbolone). But the drug was never approved by the French government and was hence never produced. The reason was extreme hepatoxicity. Bill Roberts, the biochemist, once commented that taking methyltrienolone made taking insane doses of anadrol and Halotestin together look mild on the liver. While I was unable to find anything in the literature that describes the extent of the liver toxicity, it's a generally accepted fact. That's also why, to the dissapointment of many, you will never find a commercially marketed methyltrienolone product. Its only sold in bulk to labs and universities for research studies involving androgens.

    Mainly because (and those who wish it was available will wish so even more now) its such a potent androgen. There is some conflicting information in that regard however. Organic chemist Patrick Arnold, head of LPJ research, once stated that methyltrienolone was the most powerful steroid ever, and that statement has been blown out of proportion and taken on a life of its own. While androgenically a very potent steroid, methyltrienolone is still basically trenbolone with a 17-alpha-methyl group. A group that has the tendency to actually reduce the androgenic potency. So it may actually be somewhat milder than trenbolone, on the contrary to what many pseudo steroid guru's are now claiming after reading Pat Arnold's statement. I can't find any other documented effects of the 17-alpha-alkylation influencing androgen binding in a positive way. It's a potent androgen, with more binding than even DHT, but the study that claims that is mild at the very best about quantifications, whereas people have used the term 1000 times more powerful than testosterone , which is surely exaggerated.

    What is interesting is that it seems to show nearly no binding for sex-hormone binding proteins, which makes it a popular choice in androgen receptor studies, since it will demonstrate equal binding in all tissues regardless of the presence and amount of these proteins. No doubt this plays a role in its supposed binding capacity. In this instance the 17-alpha-alkylation may have played a key role, since it has been demonstrated a multitude of times that 17-alpha-methyl groups decrease the binding for sex-hormone binding proteins as well as most other structures, and due to its triple double bond, trenbolone really didn't bind well to these to begin with.

    One of the findings made in clinical tests with methyltrienolone was the discovery of high amounts of the DHT-deactivating enzyme 3alpha-hydroxysteroid dehydrogenase in muscle tissue. Once again proof that God meant to keep us humans weak. Hurray for science. Follow-up studies then went on to show that DHT nonetheless showed similar binding in the prostate, and showing little or no presence of the deactivating enzyme. So God would rather have us all die of prostate cancer than gain a few ounces of muscle. It's a comforting thought, no?

    What methyltrienolone, despite its amazing capacity, still doesn't overcome are the basic problems with any 19Nor compound. First of all its effects on libido. Methyltrienolone still seems to affect our sex drive in such a potent manner that the dreaded Deca Dick (temporary impotence) is a very real threat. Another is that it still binds almost equipotently to the progesterone receptor. The latter would be of little concern as long as no circulating estrogen is present since methyltrienolone does not aromatize, but could cause problems such as aggravating water retention and gyno (growth of breast tissue in men) if combined with an aromatizing androgen or an estrogen.

    While many may wish that an incredibly strong androgenic, non-aromatizing compound as this was available for daily use, its not. And if the indications are true, its probably best. I've warned many people for the toxicity of fluoxymesterone, and everything points to it that methyltrienolone makes fluoxymesterone look like Tums tablets in terms of liver toxicity.

    Stacking and Use:

    Obviously this section is mostly useless, as any who would use, let alone stack methyltrienolone for any decent period of time, wouldn't really be around long enough to tell us how well it worked. Ideally one would use it alone, while dieting or for the purpose of gaining lean mass. The androgenic potency is slightly higher than that of trenbolone, so the risk for aggravated hair loss, acne, prostate hypertrophy and deepening of voice is not only realistic, but almost likely. If one were to use it, you would probably have to use every trick in the book to protect your liver and stay alive: Alpha Lipoic Acid, Milk thistle, dessicated liver and Vitamin B6. The blood pressure raise would not be mild either. So something to lower blood pressure is advised as well.

    Hope this helps!! I have a friend who has it and plans on using it mid cycle during a high weight/low rep phase in his training for 30 days @ 5 to 10mg/day.
    Java Man likes this.

  4. #4
    anabolicmistake is offline New Member
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    When we looked up the active ingredient, we found a few things saying it was a different form of tren . I dont know anything significant about any AAS. Our main question is that if should we cycle off it a bit, lower our dosage for a few days before we quit? or just stop taking it all together. we are concerned with lowered testosterone production and if quitting cold turkey would cause any type of problems

  5. #5
    austinite's Avatar
    austinite is offline HRT Specialist ~ AR-Platinum Elite-Hall of Famer ~
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    You don't need to taper off. Just stop taking it and clean up your liver. That's it. 2 weeks didn't do much.
    ~ PLEASE DO NOT ASK FOR SOURCE CHECKS ~

    "It's human nature in a 'more is better' society full of a younger generation that expects instant gratification, then complain when they don't get it. The problem will get far worse before it gets better". ~ kelkel

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    anabolicmistake is offline New Member
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    Okay, by NAC you are talking about N-Acetyl Cysteine? again i dont know much lol
    would i be able to find this at almost any health supplement store?

    and if this is not tren or anything hardcore, would result be favorable with continued use? and would a SERM, and which serm, would be required after (read this on an old forum post)

  7. #7
    austinite's Avatar
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    ^ yeah. Take 600mg a day till the bottle is finished. Prohormones are garbage. Just trash what you have.

    Serm for what?
    ~ PLEASE DO NOT ASK FOR SOURCE CHECKS ~

    "It's human nature in a 'more is better' society full of a younger generation that expects instant gratification, then complain when they don't get it. The problem will get far worse before it gets better". ~ kelkel

  8. #8
    Java Man's Avatar
    Java Man is offline Known Troll
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    Quote Originally Posted by ChiveOn View Post
    This is not actual trenbolone .

    I belive the chemical name for oral trenbolone is metribolone.

    Metribolone

    Pharmaceutical Name: Methyltrienolone
    Chemical structure: 17-methylestra-4,9,11-trien-3-one,17b-ol
    Molecular weight of base: 284.3974

    Effective dose: 5-15 mg / day
    Average Street-price: Only available for research purposes.
    Available Doses: None

    Brands & Products: Originally produced by Negma, but never approved for production.

    Characteristics:

    Methyltrienolone is structurally similar to trenbolone (Parabolan /Finaplix ), a well-liked and powerful androgen that does not aromatize to estrogen. The difference is the attachment of a 17-alpha-methyl group for oral activity. So one could refer to methyltrienolone as oral trenbolone. It was first explored quite some time ago by Negma in France, the same company that marketed Parabolan (trenbolone). But the drug was never approved by the French government and was hence never produced. The reason was extreme hepatoxicity. Bill Roberts, the biochemist, once commented that taking methyltrienolone made taking insane doses of anadrol and Halotestin together look mild on the liver. While I was unable to find anything in the literature that describes the extent of the liver toxicity, it's a generally accepted fact. That's also why, to the dissapointment of many, you will never find a commercially marketed methyltrienolone product. Its only sold in bulk to labs and universities for research studies involving androgens.

    Mainly because (and those who wish it was available will wish so even more now) its such a potent androgen. There is some conflicting information in that regard however. Organic chemist Patrick Arnold, head of LPJ research, once stated that methyltrienolone was the most powerful steroid ever, and that statement has been blown out of proportion and taken on a life of its own. While androgenically a very potent steroid, methyltrienolone is still basically trenbolone with a 17-alpha-methyl group. A group that has the tendency to actually reduce the androgenic potency. So it may actually be somewhat milder than trenbolone, on the contrary to what many pseudo steroid guru's are now claiming after reading Pat Arnold's statement. I can't find any other documented effects of the 17-alpha-alkylation influencing androgen binding in a positive way. It's a potent androgen, with more binding than even DHT, but the study that claims that is mild at the very best about quantifications, whereas people have used the term 1000 times more powerful than testosterone , which is surely exaggerated.

    What is interesting is that it seems to show nearly no binding for sex-hormone binding proteins, which makes it a popular choice in androgen receptor studies, since it will demonstrate equal binding in all tissues regardless of the presence and amount of these proteins. No doubt this plays a role in its supposed binding capacity. In this instance the 17-alpha-alkylation may have played a key role, since it has been demonstrated a multitude of times that 17-alpha-methyl groups decrease the binding for sex-hormone binding proteins as well as most other structures, and due to its triple double bond, trenbolone really didn't bind well to these to begin with.

    One of the findings made in clinical tests with methyltrienolone was the discovery of high amounts of the DHT-deactivating enzyme 3alpha-hydroxysteroid dehydrogenase in muscle tissue. Once again proof that God meant to keep us humans weak. Hurray for science. Follow-up studies then went on to show that DHT nonetheless showed similar binding in the prostate, and showing little or no presence of the deactivating enzyme. So God would rather have us all die of prostate cancer than gain a few ounces of muscle. It's a comforting thought, no?

    What methyltrienolone, despite its amazing capacity, still doesn't overcome are the basic problems with any 19Nor compound. First of all its effects on libido. Methyltrienolone still seems to affect our sex drive in such a potent manner that the dreaded Deca Dick (temporary impotence) is a very real threat. Another is that it still binds almost equipotently to the progesterone receptor. The latter would be of little concern as long as no circulating estrogen is present since methyltrienolone does not aromatize, but could cause problems such as aggravating water retention and gyno (growth of breast tissue in men) if combined with an aromatizing androgen or an estrogen.

    While many may wish that an incredibly strong androgenic, non-aromatizing compound as this was available for daily use, its not. And if the indications are true, its probably best. I've warned many people for the toxicity of fluoxymesterone, and everything points to it that methyltrienolone makes fluoxymesterone look like Tums tablets in terms of liver toxicity.

    Stacking and Use:

    Obviously this section is mostly useless, as any who would use, let alone stack methyltrienolone for any decent period of time, wouldn't really be around long enough to tell us how well it worked. Ideally one would use it alone, while dieting or for the purpose of gaining lean mass. The androgenic potency is slightly higher than that of trenbolone, so the risk for aggravated hair loss, acne, prostate hypertrophy and deepening of voice is not only realistic, but almost likely. If one were to use it, you would probably have to use every trick in the book to protect your liver and stay alive: Alpha Lipoic Acid, Milk thistle, dessicated liver and Vitamin B6. The blood pressure raise would not be mild either. So something to lower blood pressure is advised as well.

    Hope this helps!! I have a friend who has it and plans on using it mid cycle during a high weight/low rep phase in his training for 30 days @ 5 to 10mg/day.
    That.was awesome. I hadn't heard of methyltrienolone until now. C17a tren ... Very interesting read.

  9. #9
    dickster is offline Associate Member
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    What's NAC?, whoops should have kept reading, sorry.
    Last edited by dickster; 07-25-2013 at 02:12 AM.

  10. #10
    anabolicmistake is offline New Member
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    an serm to counter any effects estrogenic effects? i have no idea. again this is all through random research from the internet. one forum said make sure to take a SERM after finishing a cycle of this stuff.

    also another seemingly legit site made this sound like it is a legit steroid and would effect the body almost as if real it was real tren

    so if i kept taking it with liver support i would be fine?

  11. #11
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    krugerr is offline Knowledgeable Member
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    You wouldnt find oral tren in a supplement store. You wouldnt find Oral tren anywhere. Its a prohormone as previously stated, which are written and described to make the user believe they're real steroids , and they name them as the street names of real steroids. As suggested already, just stop taking them, they're trash. If you have worries use something to help flush the liver, something with a little liver protection. You wont have done any damage in the two weeks.

    Serms are for Estrogen receptors. Trenbolone is a Progestin, meaning you would need to use a Prolactin Antagonist, such a Cabergoline. However, you havent got real tren, so dont worry.

  12. #12
    austinite's Avatar
    austinite is offline HRT Specialist ~ AR-Platinum Elite-Hall of Famer ~
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    Quote Originally Posted by anabolicmistake View Post
    an serm to counter any effects estrogenic effects? i have no idea. again this is all through random research from the internet. one forum said make sure to take a SERM after finishing a cycle of this stuff.

    also another seemingly legit site made this sound like it is a legit steroid and would effect the body almost as if real it was real tren

    so if i kept taking it with liver support i would be fine?
    All you need to do is 2 things. Throw away this drug, and supplement with NAC.

    That's it.
    ~ PLEASE DO NOT ASK FOR SOURCE CHECKS ~

    "It's human nature in a 'more is better' society full of a younger generation that expects instant gratification, then complain when they don't get it. The problem will get far worse before it gets better". ~ kelkel

  13. #13
    ChiveOn's Avatar
    ChiveOn is offline Senior Member
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    Quote Originally Posted by Java Man View Post
    That.was awesome. I hadn't heard of methyltrienolone until now. C17a tren... Very interesting read.
    I seem to remember several knowledgeable member discussing oral tren months ago when I was deciding to use tren in a cycle for the first time and I did some reading on it. I wish I could find the thread I'm referring to, but ain't nobody got time for that!
    I thought it was out there and doses were in the mcg range it was just very very hard to find.

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