Oxandrolone Anavar Female Oral Anabolic Androgenic Steroids 53-39-4
Chemical Name: 5alpha-androstan-2-oxa-17alpha-methyl-17beta-ol-3-one
Assay: 99% min.
Molecular Formula: C19H30O3
Molecular weight: 306.4
Packing: foil bag or tin.
Delivery: Express courier.
Character: White crystalline powder.
Categories: Miscellaneous; Biochemistry; Steroids (Others)
Usage: pharmaceutical material, Steroid hormone, Anabolin. As a male hormone and anabolic hormones.
|Description||White or Almost White Crystalline Powder||white crystalloid powder|
|Specific Rotation||-18° ~ -24°||-22.0°|
|Loss On Drying||1.0%max||0.13%|
|Organic Volatile Impurities||meets the requirements||Conforms|
|Residual Solvents||meets the requirements||Conforms|
|Residue On Ignition||0.2%max||0.05%|
|Conclusion||The specification conform with USP30 standard|
Anavar recipe injection :
1)Highest concentration made -50ml @ 20mg/ml 1 gram of powder
9.8 ml's of PEG 300
39.2 ml's of 190 Proof Grain Alcohol
2)50ml @ 50mg/ml
2.5 grams Anavar (2.5ml) 2.5ml BA
2.5ml BB 5ml guaiacol 37.5ml Oil
Anavar Oxandrolone Half Life
Anavar does not aromatize or convert to DHT, and has an 8 hour half-life. Thus, a moderate dose taken in the morning is largely out of the system by night, yet supplies reasonable levels of androgen during the day and early evening.
One study found oxandrolone to be superior to testosterone and to Deca (nandrolone) for reducing abdominal fat in men, or at least in obese older men at the specific low doses studied, which were not necessarily equipotent. From this, some have made broad generalizations to bodybuilding. However, this does not necessarily carry over to anabolic steroid cycles at doses commonly used in bodybuilding. In the case of the study in question, I expect the difference in outcomes was dose-related.
In practice, at total androgen doses typically used, one can cut just as effectively without oxandrolone as with, given any of various possible substitutions for the oxandrolone. This is not to say this drug is ineffective, but rather that other androgens including testosterone are also effective at high dose for abdominal fat loss.
In the case of low-dose use however, I do think it is a correct conclusion that for most, low dose Anavar use is more effective for cutting than equal dosages of most other anabolic steroids. This may be partly or entirely from additive effect with natural testosterone: such oxandrolone use may not suppress such its production, the user may enjoy both the full effect of his natural testosterone and the effect of the oxandrolone. In contrast, low-dose testosterone or nandrolone use results in substantial suppression of natural testosterone, and so there is less total effect.
Oxandrolone, as with other 17-alkylated steroids, is hepatotoxic. At one time it was thought that it is not, but both clinical and practical experience with Oxandrin has shown that liver toxicity can indeed be an issue with prolonged use. I believe the usual principle of limiting 17-alkylated use to 6 weeks at a time should be applied when oxandrolone is used, just as with any alkylated oral.
Trenbolone or Primobolan are suitable substitutes for Anavar, without the liver toxicity issues. As a substitute, Primobolan shares the property of being low-suppressive, while trenbolone does not.
An interesting application of the drug that takes advantage of its oral administration is use as a morning-only bridging agent between cycles, which in my opinion should be done - if done - only after fully recovering normal testosterone production from the last cycle. At least 20 mg is usually acceptable in this application. Ideally, testosterone levels will be measured to monitor such bridging. A factor limiting to such bridging is the liver toxicity issue.
With regard to use by women, while there is a common belief that Anavar is minimally virilizing to female, in fact virilization is not unusual at 20 mg/day and can occur at considerably lower doses than that. Even 5 mg/day is not side-effect-free for all.
During a cycle, oxandrolone is not particularly recommended because there are more cost-efficient choices that will fully accomplish the same goals and do not add to liver toxicity.
The two best uses for Anavar are in optional bridging periods between cycles, if such are employed, while keeping care to avoid excessive duration of continuous 17-alkylated use; and, if short-acting injectables are not available, to supplement cycles as levels fall between the time of last injection and the start of post-cycle therapy so that that time period can remain effective for gains.
|Contact Person :||Anne|