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Neanderthals' genetic legacy:
Humans inherited variants affecting disease risk, infertility, skin and hair
characteristics
Date:
January 29,
2014
Source:
Harvard Medical School
Summary:
Remnants of Neanderthal DNA in
modern humans are associated with genes affecting type 2 diabetes, Crohn's
disease, lupus, biliary cirrhosis and smoking behavior. They also concentrate
in genes that influence skin and hair characteristics. At the same time,
Neanderthal DNA is conspicuously low in regions of the X chromosome and
testes-specific genes.
...................................
Remnants of
Neanderthal DNA in modern humans are associated with genes affecting type 2
diabetes, Crohn's disease, lupus, biliary cirrhosis and smoking behavior. They
also concentrate in genes that influence skin and hair characteristics. At the
same time, Neanderthal DNA is conspicuously low in regions of the X chromosome
and testes-specific genes.
The
research, led by Harvard Medical School geneticists and published Jan. 29 in Nature,
suggests ways in which genetic material inherited from Neanderthals has proven
both adaptive and maladaptive for modern humans. (A related paper by a separate
team was published concurrently in Science.)
"Now
that we can estimate the probability that a particular genetic variant arose
from Neanderthals, we can begin to understand how that inherited DNA affects
us," said David Reich, professor of genetics at HMS and senior author of
the paper. "We may also learn more about what Neanderthals themselves were
like."
In the past
few years, studies by groups including Reich's have revealed that present-day
people of non-African ancestry trace an average of about 2 percent of their
genomes to Neanderthals -- a legacy of interbreeding between humans and
Neanderthals that the team previously showed occurred between 40,000 to 80,000
years ago. (Indigenous Africans have little or no Neanderthal DNA because their
ancestors did not breed with Neanderthals, who lived in Europe and Asia.)
Several
teams have since been able to flag Neanderthal DNA at certain locations in the
non-African human genome, but until now, there was no survey of Neanderthal
ancestry across the genome and little understanding of the biological
significance of that genetic heritage.
"The
story of early human evolution is captivating in itself, yet it also has
far-reaching implications for understanding the organization of the modern
human genome," said Irene A. Eckstrand of the National Institutes of
Health's National Institute of General Medical Sciences, which partially funded
the research. "Every piece of this story that we uncover tells us more
about our ancestors' genetic contributions to modern human health and
disease."
Deserts and
Oases
Reich and
colleagues -- including Svante Pääbo of the Max Planck Institute for
Evolutionary Anthropology in Germany -- analyzed genetic variants in 846 people
of non-African heritage, 176 people from sub-Saharan Africa, and a
50,000-year-old Neanderthal whose high-quality genome sequence the team
published in 2013.
The most
powerful information the researchers used to determine whether a gene variant
came from a Neanderthal was if the variant appeared in some non-Africans and
the Neanderthal but not in the sub-Saharan Africans.
Using this
and other types of information, the team found that some areas of the modern
non-African human genome were rich in Neanderthal DNA, which may have been
helpful for human survival, while other areas were more like
"deserts" with far less Neanderthal ancestry than average.
The barren
areas were the "most exciting" finding, said first author Sriram
Sankararaman of HMS and the Broad Institute. "It suggests the introduction
of some of these Neanderthal mutations was harmful to the ancestors of
non-Africans and that these mutations were later removed by the action of
natural selection."
The team
showed that the areas with reduced Neanderthal ancestry tend to cluster in two
parts of our genomes: genes that are most active in the male germline (the
testes) and genes on the X chromosome. This pattern has been linked in many
animals to a phenomenon known as hybrid infertility, where the offspring of a
male from one subspecies and a female from another have low or no fertility.
"This
suggests that when ancient humans met and mixed with Neanderthals, the two
species were at the edge of biological incompatibility," said Reich, who
is also a senior associate member of the Broad Institute and an investigator at
the Howard Hughes Medical Institute. Present-day human populations, which can
be separated from one another by as much as 100,000 years (such as West
Africans and Europeans), are fully compatible with no evidence of increased
male infertility. In contrast, ancient human and Neanderthal populations
apparently faced interbreeding challenges after 500,000 years of evolutionary
separation.
"It is
fascinating that these types of problems could arise over that short a time
scale," Reich said.
A Lasting
Heritage
The team
also measured how Neanderthal DNA present in human genomes today affects
keratin production and disease risk.
Neanderthal
ancestry is increased in genes affecting keratin filaments. This fibrous
protein lends toughness to skin, hair and nails and can be beneficial in colder
environments by providing thicker insulation, said Reich. "It's tempting
to think that Neanderthals were already adapted to the non-African environment
and provided this genetic benefit to humans," he speculated.
The
researchers also showed that nine previously identified human genetic variants
known to be associated with specific traits likely came from Neanderthals.
These variants affect diseases related to immune function and also some
behaviors, such as the ability to stop smoking. The team expects that more
variants will be found to have Neanderthal origins.
The team has
already begun trying to improve their human genome ancestry results by
analyzing multiple Neanderthals instead of one. Together with colleagues in
Britain, they also have developed a test that can detect most of the
approximately 100,000 mutations of Neanderthal origin they discovered in people
of European ancestry; they are conducting an analysis in a biobank containing
genetic data from half a million Britons.
"I
expect that this study will result in a better and more systematic
understanding of how Neanderthal ancestry affects variation in human traits
today," said Sankararaman.
As another
next step, the team is studying genome sequences from people from Papua New
Guinea to build a database of genetic variants that can be compared to those of
Denisovans, a third population of ancient humans that left most of its genetic
traces in Oceania but little in mainland Eurasia.
This
research was supported by the Presidential Innovation Fund of the Max Planck
Society, NSF HOMINID grant 1032255, NIH grant GM100233 and the Howard Hughes
Medical Institute.
Story
Source:
The above
story is based on materials
provided by Harvard Medical School.
The original article was written by Stephanie Dutchen. Note: Materials may
be edited for content and length.
Journal
Reference:
- Sriram Sankararaman, Swapan Mallick, Michael Dannemann, Kay Prüfer, Janet Kelso, Svante Pääbo, Nick Patterson, David Reich. The genomic landscape of Neanderthal ancestry in present-day humans. Nature, 2014; DOI: 10.1038/nature12961
