Drostanolone Propionate 100 mg/ml by Hilma Biocare

Drostanolone Propionate 100 mg/ml by Hilma Biocare
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  • Brand: Hilma Biocare
  • Product Code: Propionate
  • Reward Points: 52
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  • $65.00 $52.00
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  • Price in reward points: 520

Tags: masteron

Drostanolone Propionate, by Hilma Biocare



Brand: Hilma Biocare



100mg/ml, 10ml/vial

Drug name: Drostanolone propionate

Drug class: Anabolic / androgenic steroids

 

Use and effective range:

Applications: quality, competition, diet

Anabolic components: moderate

Androgenic components: strong

 

Dose range and duration of use:

Beginners: not suitable

Hobby: 50-100mg every other day

Professional range: 100mg/day every 1-2 days

Women: 100-150mg / week with restrictions

Application period: 4 - 12 weeks

 

Active Life: 2-3 days

Drug Class: Androgenic/Anabolic steroid (For injection)

Average Reported Dosage: Men 300-500-mg weekly Women 100-150mg weekly

Acne: Yes

Water Retention: None

High Blood Pressure: Rare

Liver Toxic: None

Aromatization: None

Noted Comments: High Androgenic/Moderate Anabolic/Moderate

anti-estrogenic DHT Conversion: None, DHT derivative

Decreases HPTA Function: Low suppression in most cases

 

Drostanolone propionate (Masteron) is a highly androgenic injectable steroid that is a synthetic derivative of DHT (dihydrotestosterone). Since DHT does not aromatize to estrogens, there was no noted water retention during administration. If a bodybuilder had achieved a low body fat level, this drug was reported to dramatically improved shape and hardness in muscle tissue while augmenting the vascular appearance of a contest ready athlete. Normally, Masteron was used only during the last 3-5 weeks before a show as part of a pre-contest stack. In this case, 100-mg was commonly injected every second or third day (2-3 times weekly) by males and at a dosage of 50mg every other day by most women whom reported use. Additionally, according to available literature, Masteron is quite anticatabolic and anti-estrogenic in nature due to receptor inhibition. So the reported characteristics of this drug do have supportive clinical validation to consider.

 

Combined with so- called mass steroids, Masteron did aid in a rapid build-up of strength and mass even with its relatively moderate anabolic qualities. However, Masteron was not reported to be the best choice for this purpose by those polled. DHT can promote hair loss and prostate disorders in prone individuals though it is not well documented as to whether or not deviants of the DHT structure can in all case do the same.

 

Masteron has a receptor binding ability 3-5 times greater than that of testosterone. This means that the drug can hang out longer in androgen receptor-sites and is not easily displaced. The result should be increased AAS activity.

 

An interesting facet of Masteron is the way it acts as an anti-estrogen. This is due to its ability to compete for the aromatase receptor. As the reader is aware of by now, many AAS are capable of conversion to estrogens. The process is caused by an enzyme called aromatase. (Of course the process of AAS conversion to estrogen is referred to as aromatization) If a drug has the ability to inhibit the enzyme at its own receptor and still act as a powerful non-aromatizing AAS, its interesting and unusual to me.

 

My personal experiences with this drug have always been favorable with no negative side effects. Additionally I feel that the drug has had value as a sort of AAS moderator. Let me explain this. Masteron has a high SHBG and albumin binding rate.

 

Since these two hormone binding proteins prevent AAS from mening with their receptors, some would assume this is a bad thing. Masteron is 3-5 times more active than testosterone, so the unbound portion circulating in the blood stream goes a long way. Since the drug binds a higher percentage of SHBG and albumin, any other AAS co-administered with it remains in an unbound/active/free state to a greater extent and is able to induce a greater response. This is an example of noted drug synergy common to protocols reported as most effective yet requiring lower dosages to accomplish a specific result. The implication is that lower dosages of co-administered drugs allowed a decrease in negative side effects.


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