Clinical impact of pharmacogenetic risk variants in a large chinese cohort

Chun Yu Wei; Ming Shien Wen; Chih Kuang Cheng; Yi Jing Sheen; Tsung Chieh Yao; Sing Lian Lee; Jer Yuarn Wu; Ming Fang Tsai; Ling Hui Li; Chun Houh Chen; Cathy S.J. Fann; Hsin Chou Yang; Yen Tsung Huang; Hung Hsin Chen; Yi Min Liu; Erh Chan Yeh; Yu Ching Peng; Shuu Jiun Wang; Shih Pin Chen; Ming Tsun Tsai; Teh Ia Huo; Chien Wei Su; Der-Cherng Tarng; Chin-Chou Huang; Jong Ling Fuh; Keng Hsin Lan; Yo Tsen Liu; Ching Liang Lu; Yi Chung Lee; Yi-Hsiang Huang; Chung Pin Li; Yen Feng Wang; Yu Cheng Hsieh; Yi Ming Chen; Tzu Hung Hsiao; Ching Heng Lin; Yen Ju Chen; I. Chieh Chen; Chien Lin Mao; Shu Jung Chang; Yen Lin Chang; Yi Ju Liao; Chih Hung Lai; Wei Ju Lee; Hsin Tung; Ting Ting Yen; Hsin Chien Yen; Jer Hwa Chang; Chun Yao Huang; Lung Chan; Yung Wei Lin; Bu Yuan Hsiao; Chaur Jong Hu; Yung Kuo Lin; Yung Feng Lin; Tung Cheng Chang; Deng Chyang Wu; Jung Yu Kan; Chung Yao Hsu; Szu Chia Chen; Ching Chia Li; Chung Feng Huang; Chau Chyun Sheu; Lii Jia Yang; Chung Hwan Chen; Kuan Mao Chen; Shu Min Chang; Min Shiuan Liou; Shi Ping Wang; Kuan Ting Lin; Hui Ping Chuang; Ying Ju Chen; Joey Sin; Ying Ting Chen; Chiung Chih Chang; Chang Fu Kuo; Jing Chi Lin; Ho Chang Kuo; Tien Min Chan; Chao Wei Lee; Jenn Haung Lai; Shue Fen Luo; Hao Tsai Cheng; Lian Yu Lin; Li Chun Chang; Chia Ti Tsai; Hsien Li Kao; Jian Jyun Yu; Jiann Shing Jeng; Min Chin Chiu; Tzu Chan Hong; Shun Fa Yang; Hsueh Ju Lu; Sheng Chiang Su; Pauling Chu; Peng Fei Li; Chia Lin Tsai; Chia Kuang Tsai; Shih En Tang; Chien Ming Lin; Yung Fu Wu; Chih Yang Huang; Shinn Zong Ling; Chun Chun Chang; Tzu Kai Lin; Sheng Mou Hsiao; Chih Hung Chang; Chih Dao Chen; Gwo Chin Ma; Ting Yu Chang; Juey Jen Hwang; Chien Lin Lu; Kuo Jang Kao; Chen Fang Hung; Shiou Sheng Chen; Po Yueh Chen; Kochung Tsui; Yuan Tsong Chen; Chien Hsiun Chen; Chih Cheng Chien; Han Sun Chiang; Yen Ling Chiu; Hsiang Cheng Chen; Pui Yan Kwok

doi:10.1038/s41467-025-61644-x

Clinical impact of pharmacogenetic risk variants in a large chinese cohort

Chun Yu Wei^*
, Ming Shien Wen
, Chih Kuang Cheng
, Yi Jing Sheen
, Tsung Chieh Yao
, Sing Lian Lee
, Jer Yuarn Wu
, Ming Fang Tsai
, Ling Hui Li
, Chun Houh Chen
, Cathy S.J. Fann
, Hsin Chou Yang
, Yen Tsung Huang
, Hung Hsin Chen
, Yi Min Liu
, Erh Chan Yeh
, Yu Ching Peng
, Shuu Jiun Wang
, Shih Pin Chen
, Ming Tsun Tsai

Teh Ia Huo, Chien Wei Su, Der-Cherng Tarng, Chin-Chou Huang, Jong Ling Fuh, Keng Hsin Lan, Yo Tsen Liu, Ching Liang Lu, Yi Chung Lee, Yi-Hsiang Huang, Chung Pin Li, Yen Feng Wang, Yu Cheng Hsieh, Yi Ming Chen, Tzu Hung Hsiao, Ching Heng Lin, Yen Ju Chen, I. Chieh Chen, Chien Lin Mao, Shu Jung Chang, Yen Lin Chang, Yi Ju Liao, Chih Hung Lai, Wei Ju Lee, Hsin Tung, Ting Ting Yen, Hsin Chien Yen, Jer Hwa Chang, Chun Yao Huang, Lung Chan, Yung Wei Lin, Bu Yuan Hsiao, Chaur Jong Hu, Yung Kuo Lin, Yung Feng Lin, Tung Cheng Chang, Deng Chyang Wu, Jung Yu Kan, Chung Yao Hsu, Szu Chia Chen, Ching Chia Li, Chung Feng Huang, Chau Chyun Sheu, Lii Jia Yang, Chung Hwan Chen, Kuan Mao Chen, Shu Min Chang, Min Shiuan Liou, Shi Ping Wang, Kuan Ting Lin, Hui Ping Chuang, Ying Ju Chen, Joey Sin, Ying Ting Chen, Chiung Chih Chang, Chang Fu Kuo, Jing Chi Lin, Ho Chang Kuo, Tien Min Chan, Chao Wei Lee, Jenn Haung Lai, Shue Fen Luo, Hao Tsai Cheng, Lian Yu Lin, Li Chun Chang, Chia Ti Tsai, Hsien Li Kao, Jian Jyun Yu, Jiann Shing Jeng, Min Chin Chiu, Tzu Chan Hong, Shun Fa Yang, Hsueh Ju Lu, Sheng Chiang Su, Pauling Chu, Peng Fei Li, Chia Lin Tsai, Chia Kuang Tsai, Shih En Tang, Chien Ming Lin, Yung Fu Wu, Chih Yang Huang, Shinn Zong Ling, Chun Chun Chang, Tzu Kai Lin, Sheng Mou Hsiao, Chih Hung Chang, Chih Dao Chen, Gwo Chin Ma, Ting Yu Chang, Juey Jen Hwang, Chien Lin Lu, Kuo Jang Kao, Chen Fang Hung, Shiou Sheng Chen, Po Yueh Chen, Kochung Tsui, Yuan Tsong Chen, Chien Hsiun Chen^*, Chih Cheng Chien^*, Han Sun Chiang^*, Yen Ling Chiu^*, Hsiang Cheng Chen^*, Pui Yan Kwok^*

^*此作品的通信作者

研究成果 › 同行評審

7 引文斯高帕斯（Scopus）

摘要

Incorporating pharmacogenetics into clinical practice promises to improve therapeutic outcomes by optimizing drug selection and dosage based on genetic factors affecting drug response. A key advantage of PGx-guided therapy is to decrease the likelihood of adverse events. To evaluate the clinical impact of PGx risk variants, we performed a retrospective study using genetic and clinical data from the largest Han Chinese cohort, comprising 486,956 individuals, assembled by the Taiwan Precision Medicine Initiative. We found that nearly all participants carried at least one genetic variant that could affect drug response, with many carrying multiple risk variants. Here we show the detailed analyses of four gene-drug pairs, azathioprine (NUDT15/TPMT), clopidogrel (CYP2C19), statins (ABCG2/CYP2C9/SLCO1B1), and NSAIDs (CYP2C9), for which sufficient data exists for statistical power. While the results validate previous findings that PGx risk variants are significantly associated with drug-related adverse events or ineffectiveness, the excess risk of adverse events or lack of efficacy is small compared to that found in those without the PGx risk variants, and most patients with PGx variants do not suffer from adverse events. Our results point to the complexity of implementing PGx in clinical practice and the need for integrative approaches to optimize precision medicine.

原文	English
文章編號	6344
期刊	Nature Communications
卷	16
發行號	1
DOIs	https://doi.org/10.1038/s41467-025-61644-x
出版狀態	Published - 12月 2025

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10.1038/s41467-025-61644-x

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引用此

Wei, C. Y., Wen, M. S., Cheng, C. K., Sheen, Y. J., Yao, T. C., Lee, S. L., Wu, J. Y., Tsai, M. F., Li, L. H., Chen, C. H., Fann, C. S. J., Yang, H. C., Huang, Y. T., Chen, H. H., Liu, Y. M., Yeh, E. C., Peng, Y. C., Wang, S. J., Chen, S. P., ... Kwok, P. Y. (2025). Clinical impact of pharmacogenetic risk variants in a large chinese cohort. Nature Communications, 16(1), 文章 6344. https://doi.org/10.1038/s41467-025-61644-x

@article{afa77cb6e016442b8f62b32b5ee381e4,

title = "Clinical impact of pharmacogenetic risk variants in a large chinese cohort",

abstract = "Incorporating pharmacogenetics into clinical practice promises to improve therapeutic outcomes by optimizing drug selection and dosage based on genetic factors affecting drug response. A key advantage of PGx-guided therapy is to decrease the likelihood of adverse events. To evaluate the clinical impact of PGx risk variants, we performed a retrospective study using genetic and clinical data from the largest Han Chinese cohort, comprising 486,956 individuals, assembled by the Taiwan Precision Medicine Initiative. We found that nearly all participants carried at least one genetic variant that could affect drug response, with many carrying multiple risk variants. Here we show the detailed analyses of four gene-drug pairs, azathioprine (NUDT15/TPMT), clopidogrel (CYP2C19), statins (ABCG2/CYP2C9/SLCO1B1), and NSAIDs (CYP2C9), for which sufficient data exists for statistical power. While the results validate previous findings that PGx risk variants are significantly associated with drug-related adverse events or ineffectiveness, the excess risk of adverse events or lack of efficacy is small compared to that found in those without the PGx risk variants, and most patients with PGx variants do not suffer from adverse events. Our results point to the complexity of implementing PGx in clinical practice and the need for integrative approaches to optimize precision medicine.",

author = "Wei, \{Chun Yu\} and Wen, \{Ming Shien\} and Cheng, \{Chih Kuang\} and Sheen, \{Yi Jing\} and Yao, \{Tsung Chieh\} and Lee, \{Sing Lian\} and Wu, \{Jer Yuarn\} and Tsai, \{Ming Fang\} and Li, \{Ling Hui\} and Chen, \{Chun Houh\} and Fann, \{Cathy S.J.\} and Yang, \{Hsin Chou\} and Huang, \{Yen Tsung\} and Chen, \{Hung Hsin\} and Liu, \{Yi Min\} and Yeh, \{Erh Chan\} and Peng, \{Yu Ching\} and Wang, \{Shuu Jiun\} and Chen, \{Shih Pin\} and Tsai, \{Ming Tsun\} and Huo, \{Teh Ia\} and Su, \{Chien Wei\} and Der-Cherng Tarng and Chin-Chou Huang and Fuh, \{Jong Ling\} and Lan, \{Keng Hsin\} and Liu, \{Yo Tsen\} and Lu, \{Ching Liang\} and Lee, \{Yi Chung\} and Yi-Hsiang Huang and Li, \{Chung Pin\} and Wang, \{Yen Feng\} and Hsieh, \{Yu Cheng\} and Chen, \{Yi Ming\} and Hsiao, \{Tzu Hung\} and Lin, \{Ching Heng\} and Chen, \{Yen Ju\} and Chen, \{I. Chieh\} and Mao, \{Chien Lin\} and Chang, \{Shu Jung\} and Chang, \{Yen Lin\} and Liao, \{Yi Ju\} and Lai, \{Chih Hung\} and Lee, \{Wei Ju\} and Hsin Tung and Yen, \{Ting Ting\} and Yen, \{Hsin Chien\} and Chang, \{Jer Hwa\} and Huang, \{Chun Yao\} and Lung Chan and Lin, \{Yung Wei\} and Hsiao, \{Bu Yuan\} and Hu, \{Chaur Jong\} and Lin, \{Yung Kuo\} and Lin, \{Yung Feng\} and Chang, \{Tung Cheng\} and Wu, \{Deng Chyang\} and Kan, \{Jung Yu\} and Hsu, \{Chung Yao\} and Chen, \{Szu Chia\} and Li, \{Ching Chia\} and Huang, \{Chung Feng\} and Sheu, \{Chau Chyun\} and Yang, \{Lii Jia\} and Chen, \{Chung Hwan\} and Chen, \{Kuan Mao\} and Chang, \{Shu Min\} and Liou, \{Min Shiuan\} and Wang, \{Shi Ping\} and Lin, \{Kuan Ting\} and Chuang, \{Hui Ping\} and Chen, \{Ying Ju\} and Joey Sin and Chen, \{Ying Ting\} and Chang, \{Chiung Chih\} and Kuo, \{Chang Fu\} and Lin, \{Jing Chi\} and Kuo, \{Ho Chang\} and Chan, \{Tien Min\} and Lee, \{Chao Wei\} and Lai, \{Jenn Haung\} and Luo, \{Shue Fen\} and Cheng, \{Hao Tsai\} and Lin, \{Lian Yu\} and Chang, \{Li Chun\} and Tsai, \{Chia Ti\} and Kao, \{Hsien Li\} and Yu, \{Jian Jyun\} and Jeng, \{Jiann Shing\} and Chiu, \{Min Chin\} and Hong, \{Tzu Chan\} and Yang, \{Shun Fa\} and Lu, \{Hsueh Ju\} and Su, \{Sheng Chiang\} and Pauling Chu and Li, \{Peng Fei\} and Tsai, \{Chia Lin\} and Tsai, \{Chia Kuang\} and Tang, \{Shih En\} and Lin, \{Chien Ming\} and Wu, \{Yung Fu\} and Huang, \{Chih Yang\} and Ling, \{Shinn Zong\} and Chang, \{Chun Chun\} and Lin, \{Tzu Kai\} and Hsiao, \{Sheng Mou\} and Chang, \{Chih Hung\} and Chen, \{Chih Dao\} and Ma, \{Gwo Chin\} and Chang, \{Ting Yu\} and Hwang, \{Juey Jen\} and Lu, \{Chien Lin\} and Kao, \{Kuo Jang\} and Hung, \{Chen Fang\} and Chen, \{Shiou Sheng\} and Chen, \{Po Yueh\} and Kochung Tsui and Chen, \{Yuan Tsong\} and Chen, \{Chien Hsiun\} and Chien, \{Chih Cheng\} and Chiang, \{Han Sun\} and Chiu, \{Yen Ling\} and Chen, \{Hsiang Cheng\} and Kwok, \{Pui Yan\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

month = dec,

doi = "10.1038/s41467-025-61644-x",

language = "English",

volume = "16",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Publishing Group",

number = "1",

}

Wei, CY, Wen, MS, Cheng, CK, Sheen, YJ, Yao, TC, Lee, SL, Wu, JY, Tsai, MF, Li, LH, Chen, CH, Fann, CSJ, Yang, HC, Huang, YT, Chen, HH, Liu, YM, Yeh, EC, Peng, YC, Wang, SJ , Chen, SP, Tsai, MT, Huo, TI, Su, CW, Tarng, D-C, Huang, C-C, Fuh, JL, Lan, KH, Liu, YT, Lu, CL, Lee, YC, Huang, Y-H, Li, CP, Wang, YF, Hsieh, YC, Chen, YM, Hsiao, TH, Lin, CH, Chen, YJ, Chen, IC, Mao, CL, Chang, SJ, Chang, YL, Liao, YJ, Lai, CH, Lee, WJ, Tung, H, Yen, TT, Yen, HC, Chang, JH, Huang, CY, Chan, L, Lin, YW, Hsiao, BY, Hu, CJ, Lin, YK, Lin, YF, Chang, TC, Wu, DC, Kan, JY, Hsu, CY, Chen, SC, Li, CC, Huang, CF, Sheu, CC, Yang, LJ, Chen, CH, Chen, KM, Chang, SM, Liou, MS, Wang, SP, Lin, KT, Chuang, HP, Chen, YJ, Sin, J, Chen, YT, Chang, CC, Kuo, CF, Lin, JC, Kuo, HC, Chan, TM, Lee, CW, Lai, JH, Luo, SF, Cheng, HT, Lin, LY, Chang, LC, Tsai, CT, Kao, HL, Yu, JJ, Jeng, JS, Chiu, MC, Hong, TC, Yang, SF, Lu, HJ, Su, SC, Chu, P, Li, PF, Tsai, CL, Tsai, CK, Tang, SE, Lin, CM, Wu, YF, Huang, CY, Ling, SZ, Chang, CC, Lin, TK, Hsiao, SM, Chang, CH, Chen, CD, Ma, GC, Chang, TY, Hwang, JJ, Lu, CL, Kao, KJ, Hung, CF, Chen, SS, Chen, PY, Tsui, K, Chen, YT, Chen, CH, Chien, CC, Chiang, HS, Chiu, YL, Chen, HC & Kwok, PY 2025, 'Clinical impact of pharmacogenetic risk variants in a large chinese cohort', Nature Communications, 卷 16, 編號 1, 6344. https://doi.org/10.1038/s41467-025-61644-x

TY - JOUR

T1 - Clinical impact of pharmacogenetic risk variants in a large chinese cohort

AU - Wei, Chun Yu

AU - Wen, Ming Shien

AU - Cheng, Chih Kuang

AU - Sheen, Yi Jing

AU - Yao, Tsung Chieh

AU - Lee, Sing Lian

AU - Wu, Jer Yuarn

AU - Tsai, Ming Fang

AU - Li, Ling Hui

AU - Chen, Chun Houh

AU - Fann, Cathy S.J.

AU - Yang, Hsin Chou

AU - Huang, Yen Tsung

AU - Chen, Hung Hsin

AU - Liu, Yi Min

AU - Yeh, Erh Chan

AU - Peng, Yu Ching

AU - Wang, Shuu Jiun

AU - Chen, Shih Pin

AU - Tsai, Ming Tsun

AU - Huo, Teh Ia

AU - Su, Chien Wei

AU - Tarng, Der-Cherng

AU - Huang, Chin-Chou

AU - Fuh, Jong Ling

AU - Lan, Keng Hsin

AU - Liu, Yo Tsen

AU - Lu, Ching Liang

AU - Lee, Yi Chung

AU - Huang, Yi-Hsiang

AU - Li, Chung Pin

AU - Wang, Yen Feng

AU - Hsieh, Yu Cheng

AU - Chen, Yi Ming

AU - Hsiao, Tzu Hung

AU - Lin, Ching Heng

AU - Chen, Yen Ju

AU - Chen, I. Chieh

AU - Mao, Chien Lin

AU - Chang, Shu Jung

AU - Chang, Yen Lin

AU - Liao, Yi Ju

AU - Lai, Chih Hung

AU - Lee, Wei Ju

AU - Tung, Hsin

AU - Yen, Ting Ting

AU - Yen, Hsin Chien

AU - Chang, Jer Hwa

AU - Huang, Chun Yao

AU - Chan, Lung

AU - Lin, Yung Wei

AU - Hsiao, Bu Yuan

AU - Hu, Chaur Jong

AU - Lin, Yung Kuo

AU - Lin, Yung Feng

AU - Chang, Tung Cheng

AU - Wu, Deng Chyang

AU - Kan, Jung Yu

AU - Hsu, Chung Yao

AU - Chen, Szu Chia

AU - Li, Ching Chia

AU - Huang, Chung Feng

AU - Sheu, Chau Chyun

AU - Yang, Lii Jia

AU - Chen, Chung Hwan

AU - Chen, Kuan Mao

AU - Chang, Shu Min

AU - Liou, Min Shiuan

AU - Wang, Shi Ping

AU - Lin, Kuan Ting

AU - Chuang, Hui Ping

AU - Chen, Ying Ju

AU - Sin, Joey

AU - Chen, Ying Ting

AU - Chang, Chiung Chih

AU - Kuo, Chang Fu

AU - Lin, Jing Chi

AU - Kuo, Ho Chang

AU - Chan, Tien Min

AU - Lee, Chao Wei

AU - Lai, Jenn Haung

AU - Luo, Shue Fen

AU - Cheng, Hao Tsai

AU - Lin, Lian Yu

AU - Chang, Li Chun

AU - Tsai, Chia Ti

AU - Kao, Hsien Li

AU - Yu, Jian Jyun

AU - Jeng, Jiann Shing

AU - Chiu, Min Chin

AU - Hong, Tzu Chan

AU - Yang, Shun Fa

AU - Lu, Hsueh Ju

AU - Su, Sheng Chiang

AU - Chu, Pauling

AU - Li, Peng Fei

AU - Tsai, Chia Lin

AU - Tsai, Chia Kuang

AU - Tang, Shih En

AU - Lin, Chien Ming

AU - Wu, Yung Fu

AU - Huang, Chih Yang

AU - Ling, Shinn Zong

AU - Chang, Chun Chun

AU - Lin, Tzu Kai

AU - Hsiao, Sheng Mou

AU - Chang, Chih Hung

AU - Chen, Chih Dao

AU - Ma, Gwo Chin

AU - Chang, Ting Yu

AU - Hwang, Juey Jen

AU - Lu, Chien Lin

AU - Kao, Kuo Jang

AU - Hung, Chen Fang

AU - Chen, Shiou Sheng

AU - Chen, Po Yueh

AU - Tsui, Kochung

AU - Chen, Yuan Tsong

AU - Chen, Chien Hsiun

AU - Chien, Chih Cheng

AU - Chiang, Han Sun

AU - Chiu, Yen Ling

AU - Chen, Hsiang Cheng

AU - Kwok, Pui Yan

PY - 2025/12

Y1 - 2025/12

N2 - Incorporating pharmacogenetics into clinical practice promises to improve therapeutic outcomes by optimizing drug selection and dosage based on genetic factors affecting drug response. A key advantage of PGx-guided therapy is to decrease the likelihood of adverse events. To evaluate the clinical impact of PGx risk variants, we performed a retrospective study using genetic and clinical data from the largest Han Chinese cohort, comprising 486,956 individuals, assembled by the Taiwan Precision Medicine Initiative. We found that nearly all participants carried at least one genetic variant that could affect drug response, with many carrying multiple risk variants. Here we show the detailed analyses of four gene-drug pairs, azathioprine (NUDT15/TPMT), clopidogrel (CYP2C19), statins (ABCG2/CYP2C9/SLCO1B1), and NSAIDs (CYP2C9), for which sufficient data exists for statistical power. While the results validate previous findings that PGx risk variants are significantly associated with drug-related adverse events or ineffectiveness, the excess risk of adverse events or lack of efficacy is small compared to that found in those without the PGx risk variants, and most patients with PGx variants do not suffer from adverse events. Our results point to the complexity of implementing PGx in clinical practice and the need for integrative approaches to optimize precision medicine.

AB - Incorporating pharmacogenetics into clinical practice promises to improve therapeutic outcomes by optimizing drug selection and dosage based on genetic factors affecting drug response. A key advantage of PGx-guided therapy is to decrease the likelihood of adverse events. To evaluate the clinical impact of PGx risk variants, we performed a retrospective study using genetic and clinical data from the largest Han Chinese cohort, comprising 486,956 individuals, assembled by the Taiwan Precision Medicine Initiative. We found that nearly all participants carried at least one genetic variant that could affect drug response, with many carrying multiple risk variants. Here we show the detailed analyses of four gene-drug pairs, azathioprine (NUDT15/TPMT), clopidogrel (CYP2C19), statins (ABCG2/CYP2C9/SLCO1B1), and NSAIDs (CYP2C9), for which sufficient data exists for statistical power. While the results validate previous findings that PGx risk variants are significantly associated with drug-related adverse events or ineffectiveness, the excess risk of adverse events or lack of efficacy is small compared to that found in those without the PGx risk variants, and most patients with PGx variants do not suffer from adverse events. Our results point to the complexity of implementing PGx in clinical practice and the need for integrative approaches to optimize precision medicine.

UR - https://www.scopus.com/pages/publications/105010520587

U2 - 10.1038/s41467-025-61644-x

DO - 10.1038/s41467-025-61644-x

M3 - Article

C2 - 40634300

AN - SCOPUS:105010520587

SN - 2041-1723

VL - 16

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 6344

ER -

Clinical impact of pharmacogenetic risk variants in a large chinese cohort

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