Neanderthal DNA has subtle but significant impact on human traits

Latest study confirms and expands on what scientists have suggested about the effect of Neanderthal DNA on modern humans.

VANDERBILT UNIVERSITY—Since 2010 scientists have known that people of Eurasian origin have inherited anywhere from 1 to 4 percent of their DNA from Neanderthals.

The discovery spawned a number of hypotheses about the effects these genetic variants may have on the physical characteristics or behavior of modern humans, ranging from skin color to heightened allergies to fat metabolism…generating dozens of colorful headlines including “What your Neanderthal DNA is doing for you” and “Neanderthals are to blame for our allergies” and “Did Europeans Get Fat From Neanderthals?”

Now, the first study* that directly compares Neanderthal DNA in the genomes of a significant population of adults of European ancestry with their clinical records confirms that this archaic genetic legacy has a subtle but significant impact on modern human biology.

“Our main finding is that Neanderthal DNA does influence clinical traits in modern humans: We discovered associations between Neanderthal DNA and a wide range of traits, including immunological, dermatological, neurological, psychiatric and reproductive diseases,” said John Capra, senior author of the paper “The phenotypic legacy of admixture between modern humans and Neanderthals” published in the Feb. 12 issue of the journal Science. The evolutionary geneticist is an assistant professor of biological sciences at Vanderbilt University.

Some of the associations that Capra and his colleagues found confirm previous hypotheses. One example is the proposal that Neanderthal DNA affects cells called keratinocytes that help protect the skin from environmental damage such as ultraviolet radiation and pathogens. The new analysis found Neanderthal DNA variants influence skin biology in modern humans, in particular the risk of developing sun-induced skin lesions called keratosis, which are caused by abnormal keratinocytes.

In addition, there were a number of surprises. For example, they found that a specific bit of Neanderthal DNA significantly increases risk for nicotine addiction. They also found a number of variants that influence the risk for depression: some positively and some negatively. In fact, a surprising number of snippets of Neanderthal DNA were associated with psychiatric and neurological effects, the study found.

“The brain is incredibly complex, so it’s reasonable to expect that introducing changes from a different evolutionary path might have negative consequences,” said Vanderbilt doctoral student Corinne Simonti, the paper’s first author.

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This graphic shows Neanderthal-influenced traits. Credit: Deborah Brewington, Vanderbilt University

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According to the researchers, the pattern of associations that they discovered suggest that today’s population retains Neanderthal DNA that may have provided modern humans with adaptive advantages 40,000 years ago as they migrated into new non-African environments with different pathogens and levels of sun exposure. However, many of these traits may no longer be advantageous in modern environments.

One example is a Neanderthal variant that increases blood coagulation. It could have helped our ancestors cope with new pathogens encountered in new environments by sealing wounds more quickly and preventing pathogens from entering the body. In modern environments this variant has become detrimental, because hypercoagulation increases risk for stroke, pulmonary embolism and pregnancy complications.

In order to discover these associations, the researchers used a database containing 28,000 patients whose biological samples have been linked to anonymized versions of their electronic health records. The data came from eMERGE – the Electronic Medical Records and Genomics Network funded by the National Human Genome Research Institute – which links digitized records from Vanderbilt University Medical Center’s BioVU databank and eight other hospitals around the country.

This data allowed the researchers to determine if each individual had ever been treated for a specific set of medical conditions, such as heart disease, arthritis or depression. Next they analyzed the genomes of each individual to identify the unique set of Neanderthal DNA that each person carried. By comparing the two sets of data, they could test whether each bit of Neanderthal DNA individually and in aggregate influences risk for the traits derived from the medical records.

“Vanderbilt’s BioVU and the network of similar databanks from hospitals across the country were built to enable discoveries about the genetic basis of disease,” said Capra. “We realized that we could use them to answer important questions about human evolution.”

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 Neanderthal DNA influences many physical traits in people of Eurasian heritage. Credit: Michael Smeltzer, Vanderbilt University

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According to the evolutionary geneticist, this work establishes a new way to investigate questions about the effects of events in recent human evolution.

The current study was limited to associating Neanderthal DNA variants with physical traits (phenotypes) included in hospital billing codes, but there is a lot of other information contained in the medical records, such as lab tests, doctors’ notes, and medical images, that Capra is working on analyzing in a similar fashion.

Source: Vanderbilt University news release

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*”The phenotypic legacy of admixture between modern humans and Neandertals,” by C.N. Simonti; L. Bastarache; D.M. Roden; J.D. Prato; J.C. Denny; J.A. Capra at Vanderbilt University in Nashville, TN; B. Vernot; D.R. Crosslin; G.P. Jarvik; J.M. Akey at University of Washington in Seattle, WA; E. Bottinge at Mount Sinai School of Medicine in New York, NY; D.S. Carrell; D.R. Crosslin; G.P. Jarvik at University of Washington Medical Center in Seattle, WA; R.L. Chisholm at Northwestern University in Chicago, IL.  All authors include: Lisa Bastarache, Dan Roden, Jeffrey Prato and Joshua Denny from Vanderbilt; Benjamin Vernot, David Carrell, David Crosslin, Gail Jarvik and Joshua Akey from the University of Washington; Erwin Bottinger from Mount Sinai School of Medicine; Rex Chisholm from Northwestern University; Scott Hebbring from the Marshfield Clinic; Iftikhar Kullo and Jyotishman Pathak from the Mayo Clinic; Rongling Li from the National Human Genome Research Institute; Marylynn Ritchie and Shefali Verma from Pennsylvania State University; Gerard Tromp from the Geisinger Health System; and William Bush from Case Western Reserve University.

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