One of the major findings of the Exome Aggregation Consortium (ExAC), the largest-ever catalogue of genetic variation in the protein-coding regions of the human genome, is that many genetic mutations have been misclassified as harmful (M. Lek et al. Nature 536, 285–291; 2016). Authors of that study estimate that each person has lurking in their genome an average of 54 mutations that are currently considered pathogenic — but that about 41 of these occur so frequently in the human population that they aren’t in fact likely to cause severe disease. That finding is having major consequences for some people with such variants, lifting the equivalent of genetic death sentences.
That raises two challenges for researchers: how to sort out which mutations currently considered pathogenic are actually benign, and how to apply more rigorous tests to future research that aims to find the genetic causes of disease.
Working out which mutations are actually linked to illness will be a long and arduous task. For instance, geneticist and physician Leslie Biesecker of the US National Human Genome Research Institute in Bethesda, Maryland, found that a patient referred to him for diagnosis harboured a genetic variant that had been linked to kidney failure. Yet it turned out that the variant was too common in ExAC to realistically be causing a rare kidney ailment. So Biesecker checked genome sequences from 950 people whom he had previously sequenced in a study called ClinSeq (K. L. Lewis et al. PLoS ONE 10, e0132690; 2015). Five of them had the same variant, with no history of kidney disease, indicating that the variant probably does not actually cause this illness. To probe further, Biesecker is now recontacting the five ClinSeq participants with the variant to ask them to take part in follow-up tests to check whether they have normal kidney function, including collecting multiple urine samples over a 24-hour period.
To reassess the links between diseases and mutations, researchers must have access to a group of people whose detailed genetic and clinical information are known, and that’s rare. It also takes time and some cost; multiply that by the huge numbers of ‘pathogenic’ variants that have been called into question, and researchers are looking at a major undertaking. It’s a crucial one, because geneticists are being asked every day to make judgements about the harm that could be caused by mutations found in patients’ genomes. Biesecker hopes that planned or existing projects to link people’s genomes to their detailed health records — such as the US president’s Precision Medicine Initiative, which aims to sequence at least 1 million Americans, and the UK 100,000 Genomes Project — will help.
“Many have not required enough evidence before asserting that a particular variant is harmful.”
The rethink on pathogenicity shows that researchers who hunt for genetic mutations likely to cause disease need to be cautious. Many, it seems, have not required enough evidence before asserting that a particular variant is harmful.
Early efforts to discover the genetic underpinnings of disease started with families in which a particular condition recurred, generation after generation. By studying their extensive pedigrees, researchers could see strong evidence that certain mutations caused the disease. But in recent years, researchers have switched tactics: for instance, searching for evidence of pathogenicity by scanning for mutations that are more common in people with disease than in those without. It is becoming clear that many human genetic variations are relatively rare, and when researchers do not examine large enough groups of people with and without disease when scanning for pathogenic mutations, they are likely to mistakenly conclude that particular variants of interest turn up only in people with disease. The truth may be that they just haven’t looked hard enough for these variants elsewhere.
These conclusions have consequences for real people, and so researchers must go about this work differently. When they suspect that a variant is linked to disease, they should check to see how common it is in databases such as ExAC. Even better, they should hunt for evidence that the mutation has a functional role in disease before declaring that it is pathogenic. Let the reckoning begin.
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