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Melanotan 2(MT2) is a synthetic cyclic heptapeptide that is mainly used to increase tanning. It stimulates a natural increase in melanin production. Melanin is the main determinant of skin color in humans. Melanin is a brown pigment which causes skin to become darker in appearance when exposed to UV rays.
Melanotan II was first synthesized at the University of Arizona when looking at possible ways to treat skin cancer. They hypothesized that an effective way to reduce skin cancer rates in people would be to induce the body's natural pigmentary system to produce a protective tan prior to UV exposure.
Clinical trials have shown that Melanotan 2 safely promotes melanogenesis. This is a process were melanocytes produce melanin. Lighter-skinned people have low base levels of melanogenesis. Exposure to UV-B radiation causes an increased melanogenesis. The purpose of the melanogenesis is to protect the hypodermis, the layer under the skin, from the UV-B light that can damage it. It does this by absorbing all the UV-B light and blocking it from passing the skin layer.
MT2 has also been shown to have aphrodisiac effects. Giuliano F et al. (2006) showed MT2 exerting a dose-dependent effect on erections in anesthetized rats. They went on to show MT2 having inducer and facilitator activities on erection depending upon delivery route of the peptide. There are various studies showing similar results in both animals and humans. Wessells H et al. (2000) highlighted the positive effect MT2 has on sexual desire and erections in men suffering with erectile dysfunction and various organic risk factors.
Through clinical research it has been shown MT2 has excellent fat burning effects. It was previously thought that it assisted weight loss indirectly due to its appetite-reducing effect. Echter, it now appears that MT2 has direct fat burning effects. Strader AD et al. (2007) is a great example of the direct fat burning effect. They conducted a series of tests including one that shown MT2 treatment led to ageneral reduction in both visceral and subcutaneous fat tissue in high-fat-fed mice. Choi YH et al. (2003) also showed in addition to reducing food intake and inhibiting body weight gain, administration of MT2 reduces fat mass. They concluded this was most likely by accelerated lipid mobilization, but not by apoptosis (cell death).
A very interesting effect MT2 brings about is its ability to increase insulin sensitivity during researchers' trials. Heijboer AC et al (2005) studied the effects MT2 has on hepatic and whole-body insulin sensitivity. Results showed administration of MT2 increased insulin-mediated glucose disposal but did not affect the capacity of insulin to suppress EGP. MT2's acute effect on insulin sensitivity was further highlighted during studies done by the Nagoya University Graduate School of Medicine. Banno R et al. (2007) examined the effects MT2 had on insulin sensitivity in diet-induced obese rats. The insulin tolerance test showed that insulin sensitivity was significantly improved in the MT2 group compared to the pair-fed group. Verder, MT2 treatment increased the number of small-sized adipocytes in epididymal white adipose tissues, suggesting that MT2 increased insulin sensitivity through action on the white adipose tissues.
[Sc:signoff-sod]PS, here are some related links to discussions about Melanotan 2 op de EliteFitness.com forums:
Gebruiksinstructies voor Melanotan 2
Melanotan lange termijn neveneffect = Skin Cancer ?
Melanotan II dosering - Huidtype II
Referenties:
1. Giuliano F, Clément P, Droupy S, Alexandre L, Bernabé J (2006) Melanotan-II: Investigation of the inducer and facilitator effects on penile erection in anaesthetized rat. PMID: 16360286 [PubMed - geïndexeerd MEDLINE].
2. Choi YH, Li C, Hartzell DL, Lin J, Della-Fera MA, Baile CA (2003) MTII administered peripherally reduces fat without invoking apoptosis in rats. PMID: 12834806 [PubMed - geïndexeerd MEDLINE].
3. Strader AD, Shi H, Ogawa R, Seeley RJ, Reizes O (2007) The effects of the melanocortin agonist (MT-II) on subcutaneous and visceral adipose tissue in rodents. PMID: 17567964 [PubMed - geïndexeerd MEDLINE].
4. Banno R, Arima H, Hayashi M, Goto M, Watanabe M, Sato I, Ozaki N, Nagasaki H, Ozaki N, Oiso Y (2007) Central administration of melanocortin agonist increased insulin sensitivity in diet-induced obese rats. PMID: 17321524 [PubMed - geïndexeerd MEDLINE].
5. Heijboer AC, van den Hoek AM, Pijl H, Voshol PJ, Havekes LM, Romijn JA, Corssmit EP (2005) Intracerebroventricular administration of melanotan II increases insulin sensitivity of glucose disposal in mice. PMID: 15971058 [PubMed - geïndexeerd MEDLINE].
6. Wessells H, Gralnek D, Dorr R, Hruby VJ, Hadley ME, Levine N (2000) Effect of an alpha-melanocyte stimulating hormone analog on penile erection and sexual desire in men with organic erectile dysfunction. PMID: 11018622 [PubMed - geïndexeerd MEDLINE].