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New Peptide

FindNemo

New member
Newbies
Joined
Apr 11, 2009
Messages
11
FYI... Keep reading and you will see the tie in w/ IGF1, anti-aging, and MUSCLE REPAIR ....

Humanin Peptide May Be New Drug Target For Diabetes, Alzheimer's Disease
ScienceDaily (Apr. 23, 2009) — Recent studies have shown that the mitochondrial peptide Humanin (HN) protects against neuronal cell death such as happens in Alzheimer's disease. Now, in a study presented April 22 at Experimental Biology 2009 in New Orleans, Dr. Nir Barzilai reports that a small infusion of HN is the most potent regulator of insulin metabolism that his research team has ever seen, significantly improving overall insulin sensitivity and sharply decreasing the glucose levels of diabetic rats.

The finding is the first evidence of a role for HN in glucose metabolism and provides new insight into how this metabolism may be involved in the development of seemingly diverse age-related diseases such as Type 2 Diabetes Mellitus and Alzheimer's. The finding also provides support for the growing understanding that the brain (not just the pancreas, liver and other peripheral organs) is heavily involved in glucose metabolism.

Furthermore, says Dr. Barzilai, the Ingeborg and Ira Leon Rennert Chair of Aging Research and Director of the Institute for Aging Research at the Albert Einstein College of Medicine, the power of HN on insulin action suggests a new therapeutic approach to diabetes. Further understanding of how HN interactions with the growth hormone/insulin-like growth factor system may also lead to strategies to protect against age-related diseases including Alzheimer's.

Dr. Barzilai's presentation at Experimental Biology 2009 is part of the scientific program of the American Society for Biochemistry and Molecular Biology.

Dr. Barzilai is internationally known as a leading discoverer of longevity genes, especially those he has identified in a well-established group of almost 500 Ashkenazi Jews, aged 95 to 112, and their families. Last year, he reported that some of the oldest in this group have mutations in the gene for insulin-like growth factor 1 (IGF-1) receptor, genetic alterations that have been shown to prolong life span in worms and some mammals. In this Experimental Biology presentation, he reports that, while the production of HN generally decreases as people age, it decreases less in the centenarians and is the highest in their offspring. Studies are now underway at the Institute for Aging Research to determine if the centenarians have a mutation in the HN gene in the mitochondria.

How do these genes fit together? Although there is still much to learn, says Dr. Barzilai, his team increasingly understands how HN interacts with the GH/IGF system. In earlier studies, the team found that insulin-like growth factor binding protein-3 (IGFBP-3) binds Humanin and tempers its effects on promotion of cell survival.

In this new study, the effects of HN on insulin action also were found to be tempered by IGFBP-3. Inhibiting IGFBP-3 allowed the peptide to exert a more potent effect. That suggests a drug target, says Dr. Barzilai.

He says that in this preclinical testing period, it is still too soon to know how HN would perform in humans, but he believes the naturally occurring peptide's ability to preserve cells is promising. One concern of anti-diabetic drugs is increased risk for cardiovascular disease. When Dr. Barzilai's team administered Humanin to rats before or after they were induced to have heart attacks, however, the area of infarction (area of dead cells caused by lack of blood) actually decreased by almost 50 percent, compared to that in rats not given the peptide.

Funding for the study came from the National Institute on Aging and the Paul Glenn Foundation.


--------------------------------------------------------------------------------

Adapted from materials provided by Federation of American Societies for Experimental Biology, via EurekAlert!, a service of AAAS.
 
Ok.......so this new peptide will allow people to live longer. That doesn't help bbers in terms of gaining mass or burning fat. I mean sure it's great that it might help people live longer but from what I'm reading, it has no purpose in bbing.
 
Do you think IGF1 or GHRP has any place in bbing? This is the peptide and growth factor forum, not the steroid forum. If you're looking for mass, check out steroids. GHRP is a gherlin mimetic that increases IGF1 systemically.

This article posits a link between igf1 and this peptide and longevity, muscle repair.... etc.
I am just throwing this out there right now and will do my homework this weekend.

Anyways, when you get older, you will realize that your ability to keep going to the gym depends on your muskuloskeletal (muscles, tendons, ligaments) system being in good shape. This in turn, ultimately affects your ability to do "body building".
 
Ok.......so this new peptide will allow people to live longer. That doesn't help bbers in terms of gaining mass or burning fat. I mean sure it's great that it might help people live longer but from what I'm reading, it has no purpose in bbing.

JM you crack me up. At the rate most of these hobbiest bodybuilders are progressing its going to take a long life to get there.

"...a small infusion of HN is the most potent regulator of insulin metabolism that his research team has ever seen."

Did you miss this... :)
 
FindNemo thank you, thank you, thank you!!!!

This is pretty awesome... I have been waiting for an advancement like this, because it is the link I have circled in my longevity cascade.

I was going to get some sleep but now I have to go pull some research on the peptide Humanin.

Thanks again.
 
Dat, Looking forward to reading whatever you find on this.

I will finish your thread on CJC/GHRP & then start on Humanin.
 
JM you crack me up. At the rate most of these hobbiest bodybuilders are progressing its going to take a long life to get there.

"...a small infusion of HN is the most potent regulator of insulin metabolism that his research team has ever seen."

Did you miss this... :)

I guess I did miss that part bro. My bad.
 
having done some biomedical courses in university just to satisfy some interest in the subjects, this is VERY interesting to me! Sounds like a step towards some more cool research and discovery
 
Here is the study upon which the article was based. I am curious to investigate the Humanin analogues.


Novel neuro-regulation of peripheral metabolism in aging, Nir Barzilai *, The FASEB Journal. 2009;23:425.2

* Department of Medicine and Genetics, Institute for Aging Research, Albert Einstein College of Medicine, Bronx, NY

ABSTRACT

Decline in insulin action is a metabolic feature of aging and may be involved in the development of age related diseases including Type 2 Diabetes Mellitus (T2DM) and Alzheimer's disease (AD). A novel mitochondrial peptide, Humanin(HN) has been recently recognized for its neuro-protective role against AD-related neurotoxicity, and an IGFBP3 partner. Here we show that, in addition to its neuro-survival effects, HN regulates both hepatic and peripheral insulin action via the hypothalamus.

Infusion of HN ICV significantly improves overall insulin sensitivity, both at the liver and skeletal muscle. The central effects of HN on insulin action are associated with activation of hypothalamic STAT-3 signaling; effects that are negated by co-inhibition of hypothalamic STAT-3. Furthermore, endogenous IGFBP-3 in the hypothalamus tempers the effects of HN on glucose metabolism.

Peripheral infusions of novel HN derivatives reproduce the insulin-sensitizing effects of central HN. HN represents a novel link between diabetes and neurodegeneration and along with its analogues offers a potential therapeutic tool to improve insulin action and treat T2DM. Importantly, acute regulation of peripheral insulin action is probably elicited in the hypothalamus and the integrity of GH/IGF system is probably needed to ensure normal metabolism with aging. This line of investigation may lead to strategies of blocking IGF-1 effects in the periphery (reducing risk for cancer), while protecting against other age-related disease with central origins (T2DM and Alzheimer's).​
 

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