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What
do we know right now?
Evolutionary biologists have known for some time that
round worms, yeast cells, and fruit flies all age differently
and have different life spans, e.g., the fruit fly, Drosophila
melanogaster, lives for about 30 or 40 days; whereas animals
like field mice live three years, dolphins 25, elephants almost
50, and the Galapagos tortoises can make it to 100.
Ever heard of the Frenchwoman Jeanne Calment ? She
was the oldest person ever documented, dying in August
1997 at age 122. (Madame Calment supposedly gave up smoking
just a few years ago because she couldn’t see well enough
to light her cigarettes. Don’t tell your parents that’s in
here, and don’t smoke because you will have a better chance
of making it to old age if you don’t.)
But these life spans pale in comparison to those of some species
of giant trees who live hundreds of years. (N.B. Life span
is the maximum length a species can live, whereas life expectancy
is usually less and varies from organism to organism.)
So
what makes all this work?
 To be honest, we still don't know for sure.
However, scientists like Judith Campisi, Ph.D., (head of the
Department of Cell and Molecular Biology at the University
of California at Berkeley) are testing the hypothesis that
the answer may lie in our cells. Actually cells senesce
(the process of becoming old) at different rates among different
organisms and among different people. Molecular biologists
know that our cells can duplicate up to 50 times in
vitro (meaning in a test tube or laboratory dish)
before they stop, or become senescent cells.
Leonard Hayflick discovered this almost 40 years ago,
but only recently have geneticists (scientists who study our
heredity) been able to isolate genes that can cause certain
cells to act differently, either age faster, that is, go through
their 50 duplications sooner, or extend the number of divisions
to almost 90.
What these scientists are looking for is the senescent
factor (SF), which may be the underlying cause of why
our billions of cells stop dividing and thus age. The elusive
SF has been viewed from either a "damage" theory or a "programmed"
theory point of view.
The
Theory of Aging
Damage
theories are based on the assumption that aging is the
result of accumulated errors from such sources as free radicals.
Now free radicals aren’t protestors who’ve been released from
jail. They are, according to Denham Harman’s 1956 theory,
atoms, ions, and molecules that contain an unpaired electron.
Based on Harman’s idea, the underlying cause of aging and
aging-related increases in diseases like cancer, is the accumulation
of structural damage to our cells  from being constantly bombarded by metabolically
generated free radicals. Oxygen free radicals are thought
to greatly increase the severity of, if not cause, such life-shortening
diseases as diabetes, strokes, and heart attacks. Since longer-lived
species have lower rates of free radical generation than do
shorter-lived ones, then life span may be dependent upon our
ability to prevent oxidative damage.
By contrast, programmed theories suggest the SF is
genetically regulated. While both theories are correct to
a certain degree, they are interconnected and have been thought
to create a fixed, maximum life span of between 120-130 years.
Now even the presumption of a fixed life span is being
questioned. Two researchers at MIT in Cambridge, MA, Drs.
David Sinclair and Leonard Guarente believe
they have discovered the "Holy Grail" of aging, the SF.
Believe it or not, it may all be a big mistake. These two
scientists think that bits of extra DNA – deoxyribonucleic
acid, the building blocks of life – accumulate within our
cells’ nuclei, and that this "junk" DNA builds up to levels
that clog normal cell action.
Our mothers have been telling us that junk food is bad for
us, now junk DNA may be, too! Actually, what Drs. Sinclair
and Guarente published in the prestigious journal, Cell,
was about brewer’s yeast cells; however, they believe that
this buildup of junk DNA from too many repeats of our ribosomes
– protein producing factories inside a cell’s nucleus – is
what also causes Werner’s syndrome in humans, which
is a fatal disease of premature aging.
Persons afflicted with Werner’s syndrome are normal until
they become teenagers, then they start developing signs of
accelerated aging like very wrinkled skin and die in their
30s. If the Cell paper’s conclusion is correct, then
knowing what the SF is may lead scientists to find ways to
slow down the mechanism of cellular senescence, or aging.
Our
Research
At Baylor
College of Medicine’s Huffington Center on Aging in Houston,
Texas, research teams led by Drs. James and Olivia
Pereira-Smith are studying the role that the SF
plays in reducing the number of cell divisions on such aging-related
health problems as osteoporosis (thinning bones that
break easily), declining immune function, cancer, liver impairment,
growth hormone declines, skin changes, and cardiovascular
disease.
These scientists know that at least four genes are involved
in cellular senescence and that three of them lie on human
chromosomes 1,4, and 7; they’ve even cloned the gene on
chromosome 4 for further study. They have also discovered
a protein – remember proteins are mainly those amino acids
that form the principal component of our cells – that inhibits
DNA synthesis on the surface of membranes of senescent cells.
Is this the SF? We’ll know soon, so check later editions of
Encarta to find out.
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