Large-scale integration of omics and electronic health records to identify potential risk protein biomarkers and therapeutic drugs for cancer prevention and intervention

Author:

Li QingORCID,Song Qingyuan,Chen Zhishan,Choi Jungyoon,Moreno Victor,Ping JieORCID,Wen Wanqing,Li Chao,Shu Xiang,Yan Jun,Shu Xiao-ou,Cai Qiuyin,Long Jirong,Huyghe Jeroen R,Pai Rish,Gruber Stephen B,Casey Graham,Wang Xusheng,Toriola Adetunji T.,Li Li,Singh Bhuminder,Lau Ken S,Zhou Li,Wu ChongORCID,Peters Ulrike,Zheng Wei,Long Quan,Yin Zhijun,Guo Xingyi

Abstract

AbstractIdentifying risk protein targets and their therapeutic drugs is crucial for effective cancer prevention. Here, we conduct integrative and fine-mapping analyses of large genome-wide association studies data for breast, colorectal, lung, ovarian, pancreatic, and prostate cancers, and characterize 710 lead variants independently associated with cancer risk. Through mapping protein quantitative trait loci (pQTL) for these variants using plasma proteomics data from over 75,000 participants, we identify 365 proteins associated with cancer risk. Subsequent colocalization analysis identifies 101 proteins, including 74 not reported in previous studies. We further characterize 36 potential druggable proteins for cancers or other disease indications. Analyzing >3.5 million electronic health records, we uncover five drugs (Haloperidol, Trazodone, Tranexamic Acid, Haloperidol, and Captopril) associated with increased cancer risk and two drugs (Caffeine and Acetazolamide) linked to reduced colorectal cancer risk. This study offers novel insights into therapeutic drugs targeting risk proteins for cancer prevention and intervention.

Publisher

Cold Spring Harbor Laboratory

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