Mitochondria Play Important role
in Human Evolution and Disease
A pioneering scientist in
mitochondrial biology, Douglas C. Wallace, synthesizes evidence for the
importance of mitochondria in a provocative Perspective article today in the
journal Cell.
Residing in large numbers outside
the nucleus of every cell, mitochondria contain their own DNA, with unique
features that "may require a reassessment of some of our core assumptions
about human genetics and evolutionary theory," concludes Wallace, director
of the Center for Mitochondrial and Epigenomic Medicine at The Children's
Hospital of Philadelphia.
Wallace has investigated
mitochondria for more than 40 years. In 1988, he was the first to show that
mutations in mitochondrial DNA (mtDNA) can cause inherited human disease. His
body of research has focused on how mtDNA mutations contribute to both rare and
common diseases by disrupting bioenergetics -- chemical reactions that generate
energy at the cellular level.
Wallace and colleagues previously
showed in the late 1970s that human mitochondrial DNA is inherited exclusively
through the mother. They then used this knowledge to reconstruct the ancient
migrations of women by comparing variation in mtDNA among populations
throughout the world. From such studies, scientists have concluded that humans
arose in Africa about 200,000 years ago and that only two mtDNA lineages
successfully left Africa about 65,000 years ago to colonize the rest of the
world.
Based on insights from these
human migration studies, Wallace takes up a longstanding scientific question
raised by Darwinian evolution -- both in humans and other species. As
subpopulations moved into isolated areas, how did they remain isolated over a
long enough time for new species-defining traits to arise in nuclear genes and
become enriched by natural selection to permit speciation?
The vast majority of our 20,000
or so genes exist in the DNA within each cell's nucleus, as distinct from the
13 protein-coding genes inside mtDNA. However, Wallace argues that mtDNA
mutations provide faster and more flexible adaptations to changing environments
than do nuclear DNA mutations. The mtDNA has a much higher mutation rate than
nuclear DNA, which by itself might imperil species survival, because most DNA
mutations are deleterious. However, mtDNA mutations alter physiology at the
single-cell level. Therefore, cells in the mother's ovary that harbor the most
deleterious mtDNA mutations can be eliminated by natural selection prior to
fertilization. Thus only mild mtDNA variants, a subset of which may be
potentially beneficial, are introduced into the population.
The high mutation rate in mtDNA
plus ovarian selection thus provides a powerful tool for humans (and animals)
to adapt to an environmental change, without endangering a population's overall
survival. Mitochondrial DNA also exchanges signals with nuclear DNA, and the
interaction helps drive the evolution of physiological processes over time.
Populations that expand into a marginal environmental space, Wallace argues,
adapt their physiology through mtDNA mutation to better exploit the limited
food sources and other resources in that environment. This permits prolonged
occupation of the marginal environment, giving sufficient time for nuclear DNA mutations
to generate anatomical structures appropriate for exploiting more abundant food
resources in the new environment.
To support this hypothesis,
Wallace proposes that mitochondria variation can result in crucial energy
tradeoffs. At the cellular level, mitochondria convert oxygen and nutrients to
the energy-rich chemical ATP, while also producing heat. In tropical climates,
this coupling process is maximally effective, permitting more efficient
production of ATP with minimal heat production. In the Arctic, the conversion
of food to ATP is less efficient, requiring more calories to be consumed for
the same amount of ATP, and this generates more heat. So different patterns of
mtDNA variation are likely beneficial in warm versus cold climates. Similarly, certain
mtDNA variants are enriched in Tibetan populations, suggesting that mtDNA
variation may permit adaptation to the low oxygen tension at high altitude.
Wallace also cites multiple
studies that show that regional mtDNA variation correlates with predilection to
a wide variety of metabolic and degenerative diseases, including Alzheimer and
Parkinson disease, diabetes, obesity, and cardiovascular disease.
Biologists have long known that
adaptations that confer an advantage in one environment can become less
beneficial in another environment. Wallace suggests an important contributor to
this phenomenon could be the physiological adaptation of mtDNA variation. He
postulates that as populations migrate and dietary patterns become globalized,
people with mtDNA optimized to one environment, where they eat a sub-Saharan
African diet, may not be well adapted to another environment, where they may
consume a Central European diet. "Because mitochondria have such a crucial
role in our physiology, changes in mitochondrial DNA can have profound effects
on human biology," he adds.
