Quantifying prion disease penetrance using large population control cohorts

EV Minikel, SM Vallabh, M Lek, Karol Estrada Gil, KE Samocha, JF Sathirapongsasuti, CY McLean, JY Tung, LPC Yu, P Gambetti, J Blevins, SL Zhang, Y Cohen, W Chen, M Yamada, T Hamaguchi, N Sanjo, H Mizusawa, Y Nakamura, T KitamotoSJ Collins, A Boyd, RG Will, R Knight, C Ponto, I Zerr, TFJ Kraus, S Eigenbrod, A Giese, M Calero, J de Pedro-Cuesta, S Haik, JL Laplanche, E Bouaziz-Amar, JP Brandel, S Capellari, P Parchi, A Poleggi, A Ladogana, AH O'Donnell-Luria, KJ Karczewski, JL Marshall, M Boehnke, M Laakso, KL Mohlke, A Kahler, K Chambert, S McCarroll, PF Sullivan, CM Hultman, SM Purcell, P Sklar, Sven van der Lee, A Rozemuller, C Jansen, Bert Hofman, Robert Kraaij, Jeroen van Rooij, Arfan Ikram, André Uitterlinden, Cornelia Duijn, MJ Daly, DG MacArthur

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268 Citations (Scopus)

Abstract

More than 100,000 genetic variants are reported to cause Mendelian disease in humans, but the penetrance-the probability that a carrier of the purported disease-causing genotype will indeed develop the disease-is generally unknown. We assess the impact of variants in the prion protein gene (PRNP) on the risk of prion disease by analyzing 16,025 prion disease cases, 60,706 population control exomes, and 531,575 individuals genotyped by 23andMe Inc. We show that missense variants in PRNP previously reported to be pathogenic are at least 30 times more common in the population than expected on the basis of genetic prion disease prevalence. Although some of this excess can be attributed to benign variants falsely assigned as pathogenic, other variants have genuine effects on disease susceptibility but confer lifetime risks ranging from < 0.1 to similar to 100%. We also show that truncating variants in PRNP have position-dependent effects, with true loss-of-function alleles found in healthy older individuals, a finding that supports the safety of therapeutic suppression of prion protein expression.
Original languageUndefined/Unknown
JournalScience Translational Medicine
Volume8
Issue number322
DOIs
Publication statusPublished - 2016

Research programs

  • EMC MM-01-39-09-A
  • EMC NIHES-01-64-01

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