Exome-wide association study to identify rare variants influencing COVID-19 outcomes: Results from the Host Genetics Initiative

Butler-Laporte, G.; Povysil, G.; Kosmicki, J.A.; Cirulli, E.T.; Drivas, T.; Furini, S.; Saad, C.; Schmidt, A.; Olszewski, P.; Korotko, U.; Quinodoz, M.; Çelik, E.; Kundu, K.; Walter, K.; Jung, J.; Stockwell, A.D.; Sloofman, L.G.; Jordan, D.M.; Thompson, R.C.; Del Valle, D.; Simons, N.; Cheng, E.; Sebra, R.; Schadt, E.E.; Kim-Schulze, S.; Gnjatic, S.; Merad, M.; Buxbaum, J.D.; Beckmann, N.D.; Charney, A.W.; Przychodzen, B.; Chang, T.; Pottinger, T.D.; Shang, N.; Brand, F.; Fava, F.; Mari, F.; Chwialkowska, K.; Niemira, M.; Pula, S.; Baillie, J.K.; Stuckey, A.; Salas Ellacuriaga, Antonio; Bello, X.; Pardo Seco, Jacobo José; Gómez Carballa, Alberto; Rivero Calle, Irene; Martinón Torres, Federico; Ganna, A.; Karczewski, K.J.; Veerapen, K.; Bourgey, M.; Bourque, G.; Eveleigh, R.J.; Forgetta, V.; Morrison, D.; Langlais, D.; Lathrop, M.; Mooser, V.; Nakanishi, T.; Frithiof, R.; Hultström, M.; Lipcsey, M.; Marincevic-Zuniga, Y.; Nordlund, J.; Schiabor Barrett, K.M.; Lee, W.; Bolze, A.; White, S.; Riffle, S.; Tanudjaja, F.; Sandoval, E.; Neveux, I.; Dabe, S.; Casadei, N.; Motameny, S.; Alaamery, M.; Massadeh, S.; Aljawini, N.; Almutairi, M.S.; Arabi, Y.M.; Alqahtani, S.A.; Al Harthi, F.S.; Almutairi, A.; Alqubaishi, F.; Alotaibi, S.; Binowayn, A.; Alsolm, E.A.; El Bardisy, H.; Fawzy, M.; Cai, F.; Soranzo, N.; Butterworth, A.; Geschwind, D.H.; Arteaga, S.; Stephens, A.; Butte, M.J.; Boutros, P.C.; Yamaguchi, T.N.; Tao, S.; Eng, S.; Sanders, T.; Tung, P.J.; Broudy, M.E.; Pan, Y.; Gonzalez, A.; Chavan, N.; Johnson, R.; Pasaniuc, B.; Yaspan, B.; Smieszek, S.; Rivolta, C.; Bibert, S.; Bochud, P.-Y.; Dabrowski, M.; Zawadzki, P.; Sypniewski, M.; Kaja, E.; Chariyavilaskul, P.; Nilaratanakul, V.; Hirankarn, N.; Shotelersuk, V.; Pongpanich, M.; Phokaew, C.; Chetruengchai, W.; Tokunaga, K.; Sugiyama, M.; Kawai, Y.; Hasegawa, T.; Naito, T.; Namkoong, H.; Edahiro, R.; Kimura, A.; Ogawa, S.; Kanai, T.; Fukunaga, K.; Okada, Y.; Imoto, S.; Miyano, S.; Mangul, S.; Abedalthagafi, M.S.; Zeberg, H.; Grzymski, J.J.; Washington, N.L.; Ossowski, S.; Ludwig, K.U.; Schulte, E.C.; Riess, O.; Moniuszko, M.; Kwasniewski, M.; Mbarek, H.; Ismail, S.I.; Verma, A.; Goldstein, D.B.; Kiryluk, K.; Renieri, A.; Ferreira, M.A.R.; Richards, J.B.
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Fecha de publicación
2022
Título de revista
PLoS genetics
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Article
Resumen
Host genetics is a key determinant of COVID-19 outcomes. Previously, the COVID-19 Host Genetics Initiative genome-wide association study used common variants to identify multiple loci associated with COVID-19 outcomes. However, variants with the largest impact on COVID-19 outcomes are expected to be rare in the population. Hence, studying rare variants may provide additional insights into disease susceptibility and pathogenesis, thereby informing therapeutics development. Here, we combined whole-exome and whole-genome sequencing from 21 cohorts across 12 countries and performed rare variant exome-wide burden analyses for COVID-19 outcomes. In an analysis of 5,085 severe disease cases and 571,737 controls, we observed that carrying a rare deleterious variant in the SARS-CoV-2 sensor toll-like receptor TLR7 (on chromosome X) was associated with a 5.3-fold increase in severe disease (95% CI: 2.75-10.05, p = 5.41x10-7). This association was consistent across sexes. These results further support TLR7 as a genetic determinant of severe disease and suggest that larger studies on rare variants influencing COVID-19 outcomes could provide additional insights.
Atribución 4.0 Internacional
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