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Monday, November 29, 2010

Premature ageing can be reversed by reactivating an enzyme that protects the tips of chromosomes

In Nature News Today
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Premature ageing can be reversed by reactivating an enzyme that protects the tips of chromosomes, a study in mice suggests.
Mice engineered to lack the enzyme, called telomerase, become prematurely decrepit. But they bounced back to health when the enzyme was replaced. The finding, published online today in Nature1, hints that some disorders characterized by early ageing could be treated by boosting telomerase activity.
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Researchers have identified targets that could help produce old-age-defying drugs and a fountain of youth for the baby boomer population… but haven’t we heard this all before?
The study, published in Nature this week, used the enzyme telomerase to stop and actually reverse the aging process in prematurely-aged mice.

Telomerase keeps chromosomes structurally sound by beefing up telomeres, the repetitive segments of junk DNA at the ends of chromosomes. Telomeres act as protective buffers for the chromosome’s working genes during cell division, when the chromosome is shortened and genetic material at the tips is lost.

For the new study, researchers created special mice whose telomerase activity could be switched on and off. When telomerase was turned off, the mice aged prematurely.
These animals age much faster than normal mice–they are barely fertile and suffer from age-related conditions such as osteoporosis, diabetes and neurodegeneration. They also die young. “If you look at all those data together, you walk away with the idea that the loss of telomerase could be a very important instigator of the ageing process,” says [lead author Ronald] DePinho.

The mice were grown to adulthood without activating the telomerase gene. Then, the researchers turned telomerase on for a month to see what happened to the mice. By giving the mice back telomerase activity, they were able to not just stop but undo the premature aging.
“What really caught us by surprise was the dramatic reversal of the effects we saw in these animals,” says DePinho. He describes the outcome as “a near ‘Ponce de Leon’ effect” — a reference to the Spanish explorer Juan Ponce de Leon, who went in search of the mythical Fountain of Youth. Shrivelled testes grew back to normal and the animals regained their fertility. Other organs, such as the spleen, liver and intestines, recuperated from their degenerated state.

The researchers say drugs that increase telomerase activity could be used to treat premature aging diseases in humans, and could possibly even reverse or delay normal aging. But DePinto and his colleagues stress that the study was just a ”proof-of-concept” experiment to show that changes to telomerase can affect aging.

Before these results can benefit humans who fear the bodily effects of time, many concerns must be answered. Some critics note that the researchers used prematurely-aged mice completely lacking telomerase activity instead of normal mice. Since some normal human cells express telomerase, but not all of them do, there is no telling what the effect of ramping up its activity would be. And even if telomerase-activating drugs do end up working in humans, they could be useful for diseases of premature aging, but wouldn’t necessarily combat normal aging. Says aging researcher David Harrison:
“They are not studying normal ageing, but ageing in mice made grossly abnormal.” [Nature News]

Though mice are often used to develop and test pharmaceuticals, many of those are revealed to be ineffective or unsafe in human trials. This is especially worrisome when mucking with telomerase, whose over-expression has been linked to cancer. The researchers didn’t observe any cancers in these test mice, but telomerase was only activated for one month.
The downside is that telomerase is often mutated in human cancers, and seems to help existing tumours grow faster. But DePinho argues that telomerase should prevent healthy cells from becoming cancerous in the first place by preventing DNA damage.
Researcher Tom Kirkwood told The Guardian that there are a host of other factors involved in aging that have been overlooked in this telomerase-based study.
“The key question is what might this mean for human therapies against age-related diseases? While there is some evidence that telomere erosion contributes to age-associated human pathology, it is surely not the only, or even dominant, cause, as it appears to be in mice engineered to lack telomerase.” [The Guardian]

It looks like anyone hoping for the fountain of youth will have to hang around a little longer while researchers work out the answers to all these questions.

1 comment:

  1. There is really no need for genetic engineerin­g to activate telomerase as was done in the Depinho mouse model. There is about 20 years of research on Telomere activation­. There are two receptors for estrogen on the TERT gene which controls this process. Whether you happen to be a human being or a mouse, the best way to increase telomerase activity, lengthen the telomeres and reverse aging is with the human bioidentic­­al hormone, 17-Beta-Es­­tradiol, also known as estrogen. In 1999, Kyo demonstrat­­ed that 17-Beta-Es­­tradiol activates telomerase via direct and indirect effects on the hTERT promoter region. This was confirmed in 2000 by Silvia Misiti and again in 2009 by Rodrigo T. Calado from the NIH.

    A recent December 2010 study from Imanishi from Japan showed that 17-Beta-Es­­tradiol (estrogen) augments telomerase activity, thereby accelerati­­ng recovery after injury and reducing the effects of aging (reducing senescence­­).

    Natural substances such as resveratrol, gingko and silymarin also activate telomeres.

    For more see:

    http://jeffreydach.com/2010/12/03/anti-aging-breakthrough-with-telomerase-knockout-mice-by-jeffrey-dach-md.aspx

    regards, jeffrey dach md

    ReplyDelete