I study genetics of aging in the
nematode worm Caenorhabditis elegans. C. elegans is a simple animal model
organism that has been studied in the lab for a few decades. The adult
roundworm is about 1mm long and consists of about 1000 cells. Conveniently, the
fate of every cell division from fertilization until the worm reaches adulthood
(which takes about 3 days) has been mapped out by scientists, so that we know
exactly how every cell division occurs in order for the worm to develop into an
organism of multiple tissues and specialized cell types. Additionally,
scientists have also sequenced the entire C. elegans genome, so we can study
any gene with any particular function of interest. These two key features,
along with many other lab techniques that have been well-established when
studying worms, make C. elegans an attractive animal model system. Scientists
may utilize C. elegans to study neurobiology, development, stem cell biology,
etc. I utilize C. elegans as a model for studying aging because many genes
important for regulating aging process (such as genes in hormonal pathways, genes
involved in nutrient uptake, and genes expressed in the mitochondria) are
conserved from C. elegans to humans. Additionally, C. elegans adult worms only
live for 2-3 weeks, so I can easily conduct multiple experiments over the
entire lifespan of a worm in a short amount of time.
While perusing through recent scientific articles about C. elegans aging, I came across an article by Yoko Honda and colleagues, entitled “Genes down-regulated in spaceflight are involved in the control of longevity in Caenorhabditis elegans” (Scientific Reports 2: 487, 2012). Here is the article link: http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3390002/pdf/srep00487.pdf. The title immediately caught my attention, not just because I am interested in genes that regulate longevity in C. elegans, but mostly because these scientists studied longevity of C. elegans in space! Their research is literally out of this world! (Sorry for the cheesy pun.) Oftentimes a space exploration will also carry some lab specimens along for the ride, so that we can learn more about how spaceflight impacts living things. Honda and colleagues claim that studying the impact of spaceflight on C. elegans aging is important because soon humans will be spending more time in space as we explore other planets or colonize the moon. These statements are a bit far-fetched because our daily lives will not resemble an episode of “Futurama” any time soon; however, we can argue that studying the effect of spaceflight on aging is intriguing from a physics standpoint; remember learning about Albert Einstein’s theory that if you travel into space and come back to Earth, you will be much younger than you were supposed to be? This is part of the theory of relativity: the faster you travel through space, the slower you will travel through time.
While perusing through recent scientific articles about C. elegans aging, I came across an article by Yoko Honda and colleagues, entitled “Genes down-regulated in spaceflight are involved in the control of longevity in Caenorhabditis elegans” (Scientific Reports 2: 487, 2012). Here is the article link: http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3390002/pdf/srep00487.pdf. The title immediately caught my attention, not just because I am interested in genes that regulate longevity in C. elegans, but mostly because these scientists studied longevity of C. elegans in space! Their research is literally out of this world! (Sorry for the cheesy pun.) Oftentimes a space exploration will also carry some lab specimens along for the ride, so that we can learn more about how spaceflight impacts living things. Honda and colleagues claim that studying the impact of spaceflight on C. elegans aging is important because soon humans will be spending more time in space as we explore other planets or colonize the moon. These statements are a bit far-fetched because our daily lives will not resemble an episode of “Futurama” any time soon; however, we can argue that studying the effect of spaceflight on aging is intriguing from a physics standpoint; remember learning about Albert Einstein’s theory that if you travel into space and come back to Earth, you will be much younger than you were supposed to be? This is part of the theory of relativity: the faster you travel through space, the slower you will travel through time.
By
using C. elegans as a model system, Honda and colleagues have shown that this
is actually true – worms do slow down the natural process of aging when they
are in space! The researchers were able to make this claim based on a few findings from
their research. They utilized data from the International C. elegans
Experiment First Project, in which they compared data from “space-flown” vs.
“ground control worms” over a 16-day period, where the worms were either on
ground for 16 days or were or ground for 5 days and then space-flown for 11
days.
In the first experiment, the
scientists looked at the accumulation of protein aggregates consisting of 35-glutamine
repeats. It was previously shown that these aggregates accumulate with
increasing age in the worm; in fact, these are the same type of aggregates that
accumulate in the brain of patients with polyglutamine diseases like
Huntington’s Disease. The researchers tagged these aggregates with a
fluorescent protein in order to easily count the number of aggregates under the
microscope by looking at the amount of fluorescence. They saw that spaceflight
reduced the accumulation of these polyglutamine aggregates, in which worms of
the same age that were space-flown had fewer aggregates than worms that were
not space-flown. As accumulation of these aggregates is a biomarker for aging,
this means that the space-flown worms were aging more slowly!
The
second experiment which showed that spaceflight slows down worm aging was
conducted by using a DNA microarray, which is a technique to measure changes in
gene expression between two different conditions. (This is where the sequenced
genome of C. elegans comes in handy because the DNA microarray allows you to
look at many, many genes at once.) For this experiment, scientists compared
gene expression between space-flown vs. ground control worms. There were many
genes that were either up- or down-regulated compared between the two different
environmental conditions. However, Honda and colleagues analyzed this data and noticed
that seven genes important for neuronal and endocrine signaling were
down-regulated in the space-flown worms compared to the ground control worms. By
applying certain lab techniques to worms that were not space-flown, the
researchers saw that inactivation of these same seven genes resulted in
increased longevity of the worms. Therefore, when these genes are not
functioning, the worms live longer, which means that these genes antagonize
longevity. Since the space-flown worms had much lower expression levels of
these genes, this indicates that the space-flown worms were aging more slowly
than their ground control counterparts. The researchers went on to demonstrate
that, for three of these seven genes, there is less accumulation of
polyglutamine aggregates when the genes are inactivated, further indicating
that these genes antagonize longevity when functioning normally.
Honda and colleagues concluded from
these experiments that C. elegans worms age more slowly due to a neuronal and
endocrine response to cues from their space-flight environment, as compared to
worms that are aging and are not space-flown. By utilizing this model
organism, the researchers demonstrated through a few experiments that
biological aging is, in fact, affected by space flight, just as Albert Einstein
had predicted.
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