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Starting this today - Monster Cycle!!

Why? What's the evidence of this?

Internet rumor? Wishful thinking?

Var is 17 alpha alkylated. That forces a strain on the liver not to break it down. That alone causes toxicity.

Not trying to bust on you bro, but let's be careful not to pass along erroneous information that some people may take as accurate.

find me a source that says var is as toxic as anadrol and ièll find yo a 100 sources that say otherwise.

right now this thread is about suspension and i could give two shits about var until im in my cruising phase bro. are we going to carry on this argument for the rest of the threadÉ
 
find me a source that says var is as toxic as anadrol and ièll find yo a 100 sources that say otherwise.

right now this thread is about suspension and i could give two shits about var until im in my cruising phase bro. are we going to carry on this argument for the rest of the threadÉ

Lol oh no the dreadful French Canadian keyboard layout that replaces your "?" with that "E"
 
even though I had great strength gains and hardness from var, after seeing my detailed blood test after it, I never plan to use it agaln. The doctor fraked out, hell even I did.So Nelson s opinion is very sensible on this
 
find me a source that says var is as toxic as anadrol and ièll find yo a 100 sources that say otherwise.

right now this thread is about suspension and i could give two shits about var until im in my cruising phase bro. are we going to carry on this argument for the rest of the threadÉ


Great -- I'll take just one study that says var isn't as toxic as anadrol.

I didn't realize it was an "argument." Unless of course you regard using facts as being argumentative.

Hey bro, it's about education and information. It's a message board. But hey, I get it. If you don't give two shits, that's fine too. No worries.
 
Great -- I'll take just one study that says var isn't as toxic as anadrol.

I didn't realize it was an "argument." Unless of course you regard using facts as being argumentative.

Hey bro, it's about education and information. It's a message board. But hey, I get it. If you don't give two shits, that's fine too. No worries.

I meant I couldn't give a shit about arguing for the sakes of arguing...you have opinions and I have mine. And the word "fact" is rather subjective on controversial topics. If it's an argument, I wouldnt call it a fact.

Read this:

Why is Anavar not Liver Toxic?
Anavar does not contain a C-17 alpha alkylated ion which makes it extremely safe and non-toxic to the liver. It also does not easily convert to estrogen like other steroids
As for toxicity of 17aa the only report i have to hand at the moment but will dig out more is:


From research conducted by Michael Mooney that this is particularly well noted with HIV patients who have been using Oxandrin, another brand name for oxandrolone Anavar is much less liver toxic than other 17-alpha alkylated steroids, probably because it is primarily metabolized outside of the liver, when metabolized, and much of it is excreted unchanged. At higher doses it can increase liver enzyme values, there seems to be no evidence that any cytotoxicity exists, as is the case with other 17-alpha alkylated steroids.




Anabolic Steroids and the Liver

Anabolic steroids are processed by the liver. As discussed earlier, C-17 alkylated oral steroids (steroids with an alkyl group added at the alpha position of the "C-17" or number 17 carbon atom of the molecule to withstand total degradation on their first pass through the liver [see Steroids 101 section above]) are unusually harsh on the liver. For this reason, even moderate short-term administration of these C-17 oral steroids can effect liver function test readings. Elevated liver counts indicating liver stress (toxicity) have been reported in recent studies of somewhat moderate oral anabolic steroid therapy (daily doses of 40 and 80 mg of oxandrolone [Oxandrin, formerly Anavar]) as reported in the online periodical Medibolics, edited by Michael Mooney (Medibolics: Table of Contents). However, these elevated liver function readings will return to normal after cessation of a moderate, short-term steroid cycle. I could find not one case to the contrary. Further, it is recognized that intense weight training alone often causes changes in liver function tests, including SGOT, SGPT and LDH (this is something that all physicians monitoring athletes using anabolics should be familiar with).

The more serious liver problems attributed to anabolic steroid use include hepatocellular carcinoma (liver cancer) and peliosis hepatitis (blood-filled sacs within the liver). But the majority of cases reporting liver problems have dealt with extremely sick and elderly patients treated with C-17 alkylated oral steroids for years of continuous use, and many of these patients had a particular type of anemia linked to liver tumors even without anabolic steroid therapy. A computer search of the medical literature looking for steroid-associated liver tumors could find only three in athletes (Friedl, 1990). Of the three athletes, one was using 700 mg of oxymetholone a week for five straight years, and one had a tumor more indicative of classic liver cancer than of steroid-associated tumors. Virtually all of the reported liver problems seemed to occur with the 17 alpha-alkylated oral steroids. There have been no cysts or liver tumors reported in athletes using the 17 beta-esterified injectable steroids (Wright & Cowart, p. 61). It has been noted that injectable steroids generally appear to have little effect on the liver at all (Haupt, 1993, p. 469).

Recent studies continue to suggest that reports of serious adverse effects of anabolic steroids upon the liver in healthy athletes may be highly overstated. In a study of athletes, of the 53 current or past steroid users who underwent laboratory testing, only one subject displayed an abnormal liver test (Pope & Katz, 1994, p. 379; incidentally, on physical examination, not one user displayed evidence of any major abnormalities possibly attributable to steroids, such as high blood pressure, edema, acne or hair loss.) Another study tested one of the most powerful and reputedly dangerously toxic anabolic steroids for 30 weeks on HIV positive men and women (Hengge et al.). Oxymetholone, formerly known as Anadrol in the U.S. and a C-17 alkylated oral steroid, was administered in a dosage of over 1,000 mg per week (more than that used by many bodybuilders, and for a much longer duration of uninterrupted use). The results were significant gains in lean muscle mass -- even without any weightlifting. Even more importantly - and surprisingly -- there were no significant problems with liver function, water retention, or virilization side effects (it will be interesting to see whether further studies yield consistent findings at such high dosages).

While the dangers of anabolics to athletes' livers appear to have been highly exaggerated, it must be recognized that an apparently healthy athlete with a previously existing but undiscovered liver problem could do serious damage to himself by self-administering C-17 oral anabolic steroids. For this reason alone, it would be quite irresponsible for any athlete to use anabolic steroids without having a physician regularly conduct blood tests to monitor liver function.

In conclusion, this is why it's not as toxic as other orals:

Anavar is much less liver toxic than other 17-alpha alkylated steroids, probably because it is primarily metabolized outside of the liver, when metabolized, and much of it is excreted unchanged. At higher doses it can increase liver enzyme values, there seems to be no evidence that any cytotoxicity exists, as is the case with other 17-alpha alkylated steroids.
 
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