Global Biobank analyses provide lessons for developing polygenic risk scores across diverse cohorts

Ying Wang; Shinichi Namba; Esteban A. Lopera-Maya; Sini Kerminen; Kristin Tsuo; Kristi Läll; Masahiro Kanai; Wei Zhou; Kuan-Han Wu; Marie-Julie Favé; Laxmi Bhatta; Philip Awadalla; Ben Brumpton; Patrick Deelen; Kristian Hveem; Valeria Lo Faro; Reedik Mägi; Yoshinori Murakami; Serena Sanna; Jordan W. Smoller; Jasmina Uzunović; Brooke N. Wolford; Wei Zhou; Masahiro Kanai; Kuan-Han Wu; Humaira Rasheed; Kristin Tsuo; Jibril Hirbo; Ying Wang; Arjun Bhattacharya; Huiling Zhao; Shinichi Namba; Ida Surakka; Brooke N. Wolford; Valeria Lo Faro; Esteban A. Lopera-Maya; Kristi Läll; Marie-Julie Favé; Sinéad B. Chapman; Juha Karjalainen; Mitja Kurki; Mutaamba Maasha; Juulia Partanen; Ben Brumpton; Sameer Chavan; Tzu‐Ting Chen; Michelle Daya; Yi Ding; Yen‐Chen Anne Feng; Christopher R. Gignoux; Sarah E. Graham; Whitney Hornsby; Nathan Ingold; Ruth Johnson; Triin Laisk; Kuang Lin; Jun Lv; Iona Y. Millwood; Priit Palta; Anita Pandit; Michael Preuß; Unnur Þorsteinsdóttir; Jasmina Uzunović; Matthew Zawistowski; Xue Zhong; Archie Campbell; Kristy Crooks; Geertruida H. de Bock; Nicholas J. Douville; Sarah Finer; Lars G. Fritsche; Chris Griffiths; Yu Guo; Karen A. Hunt; Takahiro Konuma; Riccardo E. Marioni; Jansonius Nomdo; Snehal Patil; Nicholas Rafaels; Anne Richmond; Jonathan Shortt; Péter Straub; Ran Tao; Brett Vanderwerff; Kathleen C. Barnes; Marike Boezen; Zhengming Chen; Chia‐Yen Chen; Judy H. Cho; George Davey Smith; Hilary K. Finucane; Lude Franke; Eric R. Gamazon; Andrea Ganna; Tom R. Gaunt; Tian Ge; Hailiang Huang; Jennifer E. Huffman; Jukka Koskela; Clara Lajonchere; Matthew H. Law; Liming Li; Cecilia M. Lindgren; Ruth J. F. Loos; Stuart MacGregor; Koichi Matsuda; Catherine M. Olsen; David J. Porteous; Jordan A. Shavit; Harold Snieder; Richard C. Trembath; Judith M. Vonk; David C. Whiteman; Stephen J. Wicks; Cisca Wijmenga; John Wright; Jie Zheng; Xiang Zhou; Philip Awadalla; Michael Boehnke; Nancy J. Cox; Daniel H. Geschwind; Caroline Hayward; Kristian Hveem; Eimear E. Kenny; Kuang Lin; Reedik Mägi; Hilary C. Martin; Sarah E. Medland; Yukinori Okada; Aarno Palotie; Bogdan Paşaniuc; Serena Sanna; Jordan W. Smoller; Kāri Stefánsson; David A. van Heel; Robin Walters; Sebastian Zöllner; Alicia R. Martin; Cristen J. Willer; Mark J. Daly; Benjamin M. Neale; Cristen J. Willer; Eric R. Gamazon; Nancy J. Cox; Ida Surakka; Yukinori Okada; Alicia R. Martin; Jibril Hirbo

doi:10.1016/j.xgen.2022.100241

Global Biobank analyses provide lessons for developing polygenic risk scores across diverse cohorts

Ying Wang(Broad Institute), Shinichi Namba(The University of Osaka), Esteban A. Lopera-Maya(University of Groningen), Sini Kerminen(University of Helsinki), Kristin Tsuo(Broad Institute), Kristi Läll(University of Tartu), Masahiro Kanai(Broad Institute), Wei Zhou(Broad Institute), Kuan-Han Wu(University of Michigan), Marie-Julie Favé(Ontario Institute for Cancer Research), Laxmi Bhatta(Norwegian University of Science and Technology), Philip Awadalla(Ontario Institute for Cancer Research), Ben Brumpton(Norwegian University of Science and Technology), Patrick Deelen(University of Groningen), Kristian Hveem(Norwegian University of Science and Technology), Valeria Lo Faro(Uppsala University), Reedik Mägi(University of Tartu), Yoshinori Murakami(The University of Tokyo), Serena Sanna(University of Groningen), Jordan W. Smoller(Massachusetts General Hospital), Jasmina Uzunović(Ontario Institute for Cancer Research), Brooke N. Wolford(Norwegian University of Science and Technology), Wei Zhou(Broad Institute), Masahiro Kanai(Broad Institute), Kuan-Han Wu(Vanderbilt University), Humaira Rasheed(University of Michigan), Kristin Tsuo(Broad Institute), Jibril Hirbo(Broad Institute), Ying Wang(Broad Institute), Arjun Bhattacharya(Broad Institute), Huiling Zhao(Broad Institute), Shinichi Namba(University of Michigan), Ida Surakka(University of Michigan), Brooke N. Wolford(Broad Institute), Valeria Lo Faro(Uppsala University), Esteban A. Lopera-Maya(Broad Institute), Kristi Läll(University of Tartu), Marie-Julie Favé(Ontario Institute for Cancer Research), Sinéad B. Chapman(The University of Osaka), Juha Karjalainen(University of Michigan), Mitja Kurki(Norwegian University of Science and Technology), Mutaamba Maasha(Uppsala University), Juulia Partanen(University of Groningen), Ben Brumpton(Norwegian University of Science and Technology), Sameer Chavan(Ontario Institute for Cancer Research), Tzu‐Ting Chen, Michelle Daya, Yi Ding, Yen‐Chen Anne Feng, Christopher R. Gignoux, Sarah E. Graham(Norwegian University of Science and Technology), Whitney Hornsby, Nathan Ingold, Ruth Johnson, Triin Laisk(Broad Institute), Kuang Lin, Jun Lv, Iona Y. Millwood, Priit Palta, Anita Pandit, Michael Preuß, Unnur Þorsteinsdóttir, Jasmina Uzunović(Ontario Institute for Cancer Research), Matthew Zawistowski, Xue Zhong, Archie Campbell, Kristy Crooks, Geertruida H. de Bock, Nicholas J. Douville, Sarah Finer(Ontario Institute for Cancer Research), Lars G. Fritsche, Chris Griffiths, Yu Guo, Karen A. Hunt, Takahiro Konuma, Riccardo E. Marioni, Jansonius Nomdo, Snehal Patil, Nicholas Rafaels, Anne Richmond(RIKEN Center for Integrative Medical Sciences), Jonathan Shortt, Péter Straub, Ran Tao, Brett Vanderwerff, Kathleen C. Barnes, Marike Boezen, Zhengming Chen, Chia‐Yen Chen, Judy H. Cho, George Davey Smith, Hilary K. Finucane, Lude Franke, Eric R. Gamazon(Vanderbilt University), Andrea Ganna, Tom R. Gaunt, Tian Ge, Hailiang Huang, Jennifer E. Huffman, Jukka Koskela, Clara Lajonchere(Vanderbilt University), Matthew H. Law, Liming Li, Cecilia M. Lindgren(Norwegian University of Science and Technology), Ruth J. F. Loos, Stuart MacGregor, Koichi Matsuda, Catherine M. Olsen, David J. Porteous, Jordan A. Shavit(Ontario Institute for Cancer Research), Harold Snieder, Richard C. Trembath, Judith M. Vonk, David C. Whiteman, Stephen J. Wicks, Cisca Wijmenga, John Wright(Massachusetts General Hospital), Jie Zheng, Xiang Zhou, Philip Awadalla(Ontario Institute for Cancer Research), Michael Boehnke, Nancy J. Cox(Vanderbilt University), Daniel H. Geschwind, Caroline Hayward, Kristian Hveem(Norwegian University of Science and Technology), Eimear E. Kenny(Broad Institute), Kuang Lin(Ontario Institute for Cancer Research), Reedik Mägi(University of Tartu), Hilary C. Martin(Vanderbilt University), Sarah E. Medland, Yukinori Okada(RIKEN Center for Integrative Medical Sciences), Aarno Palotie(Norwegian University of Science and Technology), Bogdan Paşaniuc, Serena Sanna(University of Groningen), Jordan W. Smoller(Massachusetts General Hospital), Kāri Stefánsson(Broad Institute), David A. van Heel, Robin Walters(RIKEN Center for Integrative Medical Sciences), Sebastian Zöllner, Alicia R. Martin(Broad Institute), Cristen J. Willer(University of Groningen), Mark J. Daly(Massachusetts General Hospital), Benjamin M. Neale, Cristen J. Willer(Norwegian University of Science and Technology), Eric R. Gamazon(Vanderbilt University), Nancy J. Cox(Vanderbilt University), Ida Surakka(Broad Institute), Yukinori Okada(Norwegian University of Science and Technology), Alicia R. Martin(Broad Institute), Jibril Hirbo(Vanderbilt University)

Cell Genomics

January 1, 2023

10.1016/j.xgen.2022.100241

Cited by 108Open Access

Full Text

Abstract

Polygenic risk scores (PRSs) have been widely explored in precision medicine. However, few studies have thoroughly investigated their best practices in global populations across different diseases. We here utilized data from Global Biobank Meta-analysis Initiative (GBMI) to explore methodological considerations and PRS performance in 9 different biobanks for 14 disease endpoints. Specifically, we constructed PRSs using pruning and thresholding (P + T) and PRS-continuous shrinkage (CS). For both methods, using a European-based linkage disequilibrium (LD) reference panel resulted in comparable or higher prediction accuracy compared with several other non-European-based panels. PRS-CS overall outperformed the classic P + T method, especially for endpoints with higher SNP-based heritability. Notably, prediction accuracy is heterogeneous across endpoints, biobanks, and ancestries, especially for asthma, which has known variation in disease prevalence across populations. Overall, we provide lessons for PRS construction, evaluation, and interpretation using GBMI resources and highlight the importance of best practices for PRS in the biobank-scale genomics era.

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