Tesamorelin
$30.00 – $95.00
★★★★★ 4.9 stars
Tesamorelin is a growth hormone releasing hormone analog that increases IGF-1 levels in men and women, by an average of 181 micrograms/liter. It binds to and stimulates GHRH receptors with similar potency as endogenous GHRH. It has a host of other benefits including nootropic effects and reducing triglycerides.<br>
Tesamorelin has subsequently been shown to decrease carotid intima-media thickness (cIMT), visceral adipose tissue (VAT), and c-reactive protein (CRP). It has not been linked to
significantly affect other pituitary hormones and their respective mechanisms in the body. Additionally, it can improve cognitive function for healthy seniors and patients with an increased risk of Alzheimer’s disease, due to mild cognitive impairment.
Similar sustained beneficial effects were seen for tesamorelin 2 mg (n = 273) or placebo (n = 137) s.c. daily total cholesterol, but high-density lipoprotein decreased for 26 weeks. At week 26, patients originally on minimally over 52 weeks. Upon discontinuation of tesamorelin were rerandomized to 2 mg tesamorelin (T-T tesamorelin, VAT reaccumulated. Treatment with group, n = 154) or placebo (T-P group, n = 50), whereas tesamorelin was generally well tolerated and resulted in patients originally on placebo were switched to sustained decreases in VAT and triglycerides over 52 weeks tesamorelin (P-T group, n = 111). Safety included adverse events and glucose parameters. Tesamorelin was generally without aggravating glucose. Though effects on VAT are sustained during treatment for 52 weeks, these effects do well tolerated. The prevalence of adverse events and serious not last beyond the duration of treatment.
Falutz, Julian & Allas, Soraya & Mamputu, Jean-Claude & Potvin, Diane & Kotler, Donald & Somero, Michael & Berger, Daniel & Brown, Stephen & Richmond, Gary & Fessel, Jeffrey & Turner, Ralph & Grinspoon, Steven. (2008). Long-term safety and effects of tesamorelin, a growth hormone-releasing factor analogue, in HIV patients with abdominal fat accumulation. AIDS (London, England). 22. 1719-28.”
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