Source : Uppsala University
In a new study,
researchers at Uppsala University now demonstrate that one night of sleep loss
has a tissue-specific impact on the regulation of gene expression and
metabolism in humans. This may explain how shift work and chronic sleep loss
impairs our metabolism and adversely affects our body composition. The study is
published in the scientific journal Science
Advances.
Epidemiological
studies have shown that the risk for obesity and type 2 diabetes is elevated in
those who suffer from chronic sleep loss or who carry out shift work. Other
studies have shown an association between disrupted sleep and adverse weight
gain, in which fat accumulation is increased at the same time as the muscle
mass is reduced -- a combination that in and of itself has been associated with
numerous adverse health consequences. Researchers from Uppsala and other groups
have in earlier studies shown that metabolic functions that are regulated by
e.g. skeletal muscle and adipose tissue are adversely affected by disrupted
sleep and circadian rhythms. However, until now it has remained unknown whether
sleep loss per se can cause molecular changes at the tissue level that can
confer an increased risk of adverse weight gain.
In the new study, the
researchers studied 15 healthy normal-weight individuals who participated in
two in-lab sessions in which activity and meal patterns were highly
standardised. In randomised order, the participants slept a normal night of
sleep (over eight hours) during one session, and were instead kept awake the
entire night during the other session. The morning after each night-time
intervention, small tissue samples (biopsies) were taken from the participants'
subcutaneous fat and skeletal muscle. These two tissues often exhibit disrupted
metabolism in conditions such as obesity and diabetes. At the same time in the
morning, blood samples were also taken to enable a comparison across tissue
compartments of a number of metabolites. These metabolites comprise sugar
molecules, as well as different fatty and amino acids.
The tissue samples
were used for multiple molecular analyses, which first of all revealed that the
sleep loss condition resulted in a tissue-specific change in DNA methylation,
one form of mechanism that regulates gene expression. DNA methylation is a
so-called epigenetic modification that is involved in regulating how the genes
of each cell in the body are turned on or off, and is impacted by both
hereditary as well as environmental factors, such as physical exercise.
"Our research
group were the first to demonstrate that acute sleep loss in and of itself
results in epigenetic changes in the so-called clock genes that within each
tissue regulate its circadian rhythm. Our new findings indicate that sleep loss
causes tissue-specific changes to the degree of DNA methylation in genes spread
throughout the human genome. Our parallel analysis of both muscle and adipose
tissue further enabled us to reveal that DNA methylation is not regulated
similarly in these tissues in response to acute sleep loss," says Jonathan
Cedernaes who led the study.
"It is
interesting that we saw changes in DNA methylation only in adipose tissue, and
specifically for genes that have also been shown to be altered at the DNA
methylation level in metabolic conditions such as obesity and type 2 diabetes.
Epigenetic modifications are thought to be able to confer a sort of metabolic
"memory" that can regulate how metabolic programmes operate over
longer time periods. We therefore think that the changes we have observed in
our new study can constitute another piece of the puzzle of how chronic
disruption of sleep and circadian rhythms may impact the risk of developing for
example obesity," notes Jonathan Cedernaes.
Further analyses of
e.g. gene and protein expression demonstrated that the response as a result of
wakefulness differed between skeletal muscle and adipose tissue. The
researchers say that the period of wakefulness simulates the overnight
wakefulness period of many shift workers assigned to nightwork. A possible
explanation for why the two tissues respond in the observed manner could be
that overnight wakefulness periods exert a tissue-specific effect on tissues'
circadian rhythm, resulting in misalignment between these rhythms. This is
something that the researchers found preliminary support for also in this
study, as well as in an earlier similar but smaller study.
"In the present
study we observed molecular signatures of increased inflammation across tissues
in response to sleep loss. However, we also saw specific molecular signatures
that indicate that the adipose tissue is attempting to increase its capacity to
store fat following sleep loss, whereas we instead observed signs indicating
concomitant breakdown of skeletal muscle proteins in the skeletal muscle, in
what's also known as catabolism. We also noted changes in skeletal muscle
levels of proteins involved handling blood glucose, and this could help explain
why the participants' glucose sensitivity was impaired following sleep loss.
Taken together, these observations may provide at least partial mechanistic
insight as to why chronic sleep loss and shift work can increase the risk of
adverse weight gain as well as the risk of type 2 diabetes," says Jonathan
Cedernaes.
The researchers have
only studied the effect of one night of sleep loss, and therefore do not know
how other forms of sleep or disruption of circadian misalignment would have affected
the participants' tissue metabolism.
"It will be
interesting to investigate to what extent one or more nights of recovery sleep
can normalise the metabolic changes that we observe at the tissue level as a
result of sleep loss. Diet and exercise are factors that can also alter DNA
methylation, and these factors can thus possibly be used to counteract adverse
metabolic effects of sleep loss," says Jonathan Cedernaes.
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