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Aging News & Information
Failure of our System to Repair Damaged DNA in
Cells Results in Aging
Reducing damage by sources such as sunlight,
cigarette smoke, and our own metabolism delays aging
 December 20, 2006 - The accumulation of genetic
damage in our cells, which occurs as a result of cell metabolism or
environmental influences, such as from smoking, is a major contributor
to how we age, according to a study being published today in the journal
Nature by an international group of researchers. A connection between
aging and DNA damage has long been suspected.
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Related Stories |
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Senior Citizen Statistics
How Long Can You Expect to Live, How You May Die
Projected by Census Bureau
By Tucker Sutherland, editor
December 16, 2006 – "Adults and teens will spend
nearly five months (3,518 hours) next year watching television, surfing
the Internet, reading daily newspapers and listening to personal music
devices," so says the lead paragraph in the news release from the U.S.
Census Bureau announcing the Statistical Abstract of the United
States: 2007. But, let's dig down to the important information, like
how long are we expected to live now days and how might we meet our end.
That information is there, too.
Read more...
Shrinking Older Men at Increased Risk of Death with
Loss of Inch in Height
Underlying mechanism may contribute to both bone
loss, which leads to height loss, and coronary heart and other diseases
December 12, 2006 - Men who lose 3 centimeters
(slightly over an inch) or
more of height as they age have an increased risk of death and of
coronary heart diseases events, according to a report in the December
11/25 issue of Archives of Internal Medicine, one of the JAMA/Archives
journals. Read
more...
Researchers Learn What It Takes for Men to Reach Age
85 - One Major Surprise
No smoking, excessive drinking, hypertension or
obesity but need spouse
November 14, 2006 – Men who want to live to at
least age 85 now have a specific strategy that will help them get there
– but they need to start at age 54 to exactly fit this model. But give
or take a few years probably does not change the formula proposed by
this research, which says avoiding smoking, excessive drinking,
hypertension and being overweight should just about achieve the goal.
One problem, if you are not married you just probably are not going to
make it to 85. Read
more...
Naked Mole-Rat in News Again as Scientists find
Longevity Champs have Slower Metabolism
 These old rats studied for years still not
giving up secret of long life
October 10, 2006 - The world’s longest living rodent – the naked
mole-rat – is in the research news again today as scientists continue to
probe for the secret to its longevity. The latest study of the hairless
tunnel-dweller suggests that the thyroid may hold the answer to why they
live 10 times longer than most regular mice. They found that the naked
mole-rat has significantly lower levels of thyroid hormone, which speeds
metabolism, and hope this leads to the secret of aging.
Read more...
Read more
Aging News & Information |
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The study found that mice completely lacking a
critical gene for repairing damaged DNA grow old rapidly and have
physical, genetic and hormonal profiles very similar to mice that grow
old naturally. Furthermore, the premature aging symptoms of the mice led
to the discovery of a new type of human progeria, a rare inherited
disease in which affected individuals age rapidly and die prematurely.
"These progeroid mice, even though they do not live
very long, have remarkably similar characteristics to normal old mice,
from their physical symptoms, to their metabolic and hormonal changes
and pathology, right down to the level of similar changes in gene
expression," said corresponding author Jan Hoeijmakers, Ph.D., head of
the department of genetics at the Erasmus Medical Center in Rotterdam,
Netherlands.
"This provides strong evidence that failure to
repair DNA damage promotes aging— a finding that was not entirely
unexpected since DNA damage was already known to cause cancer. However,
it shows how important it is to repair damage that is constantly
inflicted upon our genes, even through the simple act of breathing."
The study found that a key similarity between the
progeria-like, or progeroid, mice and naturally old mice is the
suppression of genes that control metabolic pathways promoting growth,
including those controlled by growth hormone. How growth hormone
pathways are suppressed is not known, but this response appears to have
evolved to protect against stress caused by DNA damage or the
wear-and-tear of normal living.
The authors speculate that this stress response
allows each of us to live as long and as healthy a life as possible
despite the accumulation of genetic damage as we age.
Findings from this study help to reconcile two
conflicting hypotheses currently favored in the field of aging research
about why we get old, according to the authors. The first is that our
lifespan and how well we age is determined by the genes inherited from
our parents. The second is that lifespan and fitness in old age is
determined by how much damage we incur over our lifetime.
"Our study suggests that both of these hypotheses
are correct. Damage, including DNA damage, drives the functional decline
we all experience as we age. But how we respond to that damage is
determined genetically, in particular by genes that regulate the growth
hormone and insulin pathways," said Laura Niedernhofer, M.D., Ph.D.,
assistant professor of molecular genetics and biochemistry, University
of Pittsburgh School of Medicine, and first author of the study.
How the researchers came to study the relationship
between DNA damage and aging began almost serendipitously in the late
1990s while Dr. Niedernhofer was a post-doctoral fellow in Dr.
Hoeijmakers’ laboratory at Erasmus Medical Center, a well-known European
center for medical genetics, including the diagnosis of people with
unusual sensitivity to sunlight.
A German physician had contacted the center about a
15-year old Afghan boy who was highly sensitive to the sun and had other
debilitating symptoms including weight loss, muscle wasting, hearing
loss, visual impairment, anemia, hypertension and kidney failure. The
boy’s family had immigrated to Germany to seek better medical treatment
for his condition.
Extreme sensitivity to ultraviolet (UV) radiation
from sunlight is a hallmark of diseases caused by defective DNA
repair—an important mechanism by which skin and other cell types
normally cut out, or excise, damage to their DNA caused by UV light.
Defects in one DNA repair mechanism, nucleotide excision repair (NER),
causes xeroderma pigmentosum, a rare disease in which people have a
2,000-fold increased risk of skin cancer from sun exposure.
When the investigators obtained cells from the boy
and tested them for NER activity, they found almost none. Further
analysis of the boy’s DNA revealed a mutation in a gene known as XPF,
which codes for part of a key enzyme required for the removal of DNA
damage. The XPF portion of the enzyme harbors the DNA-cutting activity;
whereas a second portion, known as ERCC1, is essential for the enzyme to
bind to the damaged DNA. Mutations in either XPF or ERCC1 lead to
reduced activity of this key DNA repair enzyme.
"We were completely surprised by the finding that
the patient had a mutation in XPF, because mutations in this gene
typically cause xeroderma pigmentosum, which is a disease characterized
primarily by skin and other cancers rather than accelerated aging," said
Dr. Hoeijmakers. "This patient, therefore, has a unique disease, which
we named XPF-ERCC1, or XFE-progeroid syndrome."
To understand why this XPF mutation caused
accelerated aging, the investigators compared the expression pattern of
all of the genes (approximately 30,000) in the liver of 15-day-old mice
that had been generated in the laboratory to harbor a defect in their
XPF-ERCC1 enzyme and that had symptoms of rapidly accelerated aging to
the genes expressed by normal mice of the same age.
This comparison revealed a profound suppression of
genes in several important metabolic pathways in the progeroid mice.
Most notably, the progeroid mice had a profoundly suppressed somatotroph
(growth hormone) axis—a key pathway involved in the promotion of growth
and development—compared to normal mice.
The investigators also found low levels of growth
hormones in the progeroid mice and ruled out the possibility that this
suppression was due to problems with their hypothalamus or pituitary
glands, which regulate growth hormone secretion. Furthermore, they
demonstrated that if normal adult mice were exposed to a drug that
causes DNA damage, such as a cancer chemotherapy agent, the growth
hormone axis was similarly suppressed. In other words, DNA damage
somehow triggered hormonal changes that halted growth, while also
boosting maintenance and repair.
Because growth hormone levels go down as we get
older, contributing to loss of muscle mass and bone density, the
investigators systematically compared the gene expression pattern of
their progeroid mice to normal old mice to look for other similarities.
What they found was a striking similarity pattern between the progeroid
and normal-aged mice in several key pathways.
Indeed, for genes that influence the growth hormone
pathway, there was a greater than 95 percent correlation in changes in
gene expression between the DNA repair-deficient mice and old mice. And,
remarkably, there was a near 90 percent correlation between all other
pathways affected in the progeroid mice and the older mice.
"Because there were such high correlations between
these pathways in progeroid and normal older mice, we are quite
confident that DNA damage plays a significant role in promoting the
aging process. The bottom line is that avoiding or reducing DNA damage
caused by sources such as sunlight and cigarette smoke, as well as by
our own metabolism, also could delay aging," explained Dr. Niedernhofer.
Editor's Notes:
This research was supported by the National
Institute of Aging, the National Institute of Environmental Health
Sciences, the National Cancer Institute, the American Cancer Society,
the Dutch Cancer Society, the Dutch Science Foundation and the Ellison
Medical Foundation.
In addition to Drs. Hoeijmakers and Niedernhofer,
others involved in this study include Andria Rasile Robinson and Anwaar
Ahmad, University of Pittsburgh Cancer Institute; George Garinis, Anja
Raams, Astrid Lalai, Esther Appeldoorn, Hanny Odijk, Roos Oostendorp,
Arjan Theil, Wibeke van Leeuwen, Wim Kleijer, Wim Vermeulen, Bert van
der Horst and Koos Jaspers, Erasmus Medical Center, Rotterdam,
Netherlands; Peter Meinecke, Altonaer Kinder- Krankenhaus, Hamburg,
Germany; and Jan Vijg, The Buck Institute for Aging Research, Novato,
Ca.
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