There are some benign negative effects, but we have learned that it
is the hormone released on fasting rather than the fasting itself
that extends life. This is a much easier protocol to work around.
In fact it is inevitable that we will all end up taking advantage of
this.
It also suggests that a healthy lifestyle can be extended for early
adopters who begin supplementation in their twenties into the century
mark but not much beyond. Modern lifespans are averaging out to
around eighty years. This should permit that span to reach 100.
This is good news that should be available in some form or the other
rather quickly or at least inside five years.
Starvation hormone
markedly extends mouse life span, researchers report
DALLAS – Oct. 16,
2012 – A study by UT Southwestern Medical Center researchers finds
that a starvation hormone markedly extends life span in mice without
the need for calorie restriction.
“Restricting food
intake has been shown to extend lifespan in several different kinds
of animals. In our study, we found transgenic mice that produced more
of the hormone fibroblast growth factor-21 (FGF21) got the benefits
of dieting without having to limit their food intake. Male mice that
overproduced the hormone had about a 30 percent increase in average
life span and female mice had about a 40 percent increase in average
life span,” said senior author Dr. Steven Kliewer, professor
of molecular biology and pharmacology.
The study published
online in eLife – a new peer-reviewed, open access
journal – defined average life span as the point at which half the
members of a given test group remained alive. A study to determine
differences in maximum life span is ongoing: While none of the
untreated mice lived longer than about 3 years, some of the female
mice that overproduced FGF21 were still alive at nearly 4 years, the
researchers report.
FGF21 seems to provide
its health benefits by increasing insulin sensitivity and blocking
the growth hormone/insulin-like growth factor-1 signaling pathway.
When too abundant, growth hormone can contribute to insulin
resistance, cancer, and other diseases, the researchers said.
FGF21 is a hormone
secreted by the liver during fasting that helps the body adapt to
starvation. It is one of three growth factors that are considered
atypical because they behave like hormones, which are substances
created by one part of the body that have effects in other parts, the
researchers said.
“Prolonged
overproduction of the hormone FGF21 causes mice to live extraordinary
long lives without requiring a decrease in food intake. It mimics
the health benefits of dieting without having to diet,” said
co-author Dr. David Mangelsdorf, chairman of pharmacology and a
Howard Hughes Medical Institute (HHMI) investigator at UT
Southwestern.
“Aging and
aging-related diseases represent an increasing burden on modern
society. Drugs that slow the aging process would be very desirable.
These findings raise the possibility of a hormone therapy to extend
life span,” said Dr. Mangelsdorf, who runs a research laboratory
with Dr. Kliewer. They first identified FGF21’s starvation-fighting
effects in a 2007 study.
Lead author Dr.
Yuan Zhang, an instructor of pharmacology, said the study was
considered risky because all involved understood it would be at least
two years – an average mouse life span – before there would be
any evidence of whether elevated production of FGF21 would affect
longevity. Previous research has found that FGF21 can reduce weight
in obese mice. The mice that overproduced FGF21 in this latest study
were lean throughout their lives and remained lean even while eating
slightly more than the wild-type mice, the researchers said.
The hormone does have
some downsides: FGF21 overproducers tended to be smaller than
wild-type mice and the female mice were infertile. While FGF21
overproducers had significantly lower bone density than wild-type
mice, the FGF21-abundant mice exhibited no ill effects from the
reduced bone density and remained active into old age without any
broken bones, the researchers said.
“FGF21 is not
affecting their mobility. These guys are spry. They live nice, long
lives,” Dr. Kliewer said. “But the decreased bone density and
female infertility will require additional research to determine if
it is possible to separate out the hormone’s life span-extending
effects from its effect on bone,” he added.
The study was
supported by the National Institutes of Health, the Robert
A. Welch Foundation, the Leona M. and Harry B. Helmsley
Charitable Trust,and the HHMI.
UT Southwestern
co-authors are Dr. Yang Xie, assistant professor of clinical
sciences; Dr. Eric Berglund, postdoctoral researcher in the Division
of Hypothalamic Research; Dr. Katie Colbert Coate, postdoctoral
researcher in pharmacology; Dr. Tian Teng He, senior research
associate in the Advanced Imaging Research Center; Dr. Takeshi
Katafuchi, instructor of pharmacology; Dr. Guanghua Xiao,
assistant professor of clinical sciences; Drs. Matthew Potthoff and
Wei Wei, both postdoctoral researchers in pharmacology; and Dr.
Yihong Wan, assistant professor of pharmacology. Drs. Ruth Yu and
Ronald Evans of the Salk Institute in San Diego also participated in
the research.
No comments:
Post a Comment