NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study

BACKGROUND: Despite NUDT15 variants showing significant association with thiopurine-induced adverse events (AEs) in Asians, it remains unclear which variants of NUDT15 or whether additional genetic variants should be tested to predict AEs. To clarify the best pharmacogenetic test to be used clinical...

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Autores principales: Kakuta, Yoichi, Kawai, Yosuke, Okamoto, Daisuke, Takagawa, Tetsuya, Ikeya, Kentaro, Sakuraba, Hirotake, Nishida, Atsushi, Nakagawa, Shoko, Miura, Miki, Toyonaga, Takahiko, Onodera, Kei, Shinozaki, Masaru, Ishiguro, Yoh, Mizuno, Shinta, Takahara, Masahiro, Yanai, Shunichi, Hokari, Ryota, Nakagawa, Tomoo, Araki, Hiroshi, Motoya, Satoshi, Naito, Takeo, Moroi, Rintaro, Shiga, Hisashi, Endo, Katsuya, Kobayashi, Taku, Naganuma, Makoto, Hiraoka, Sakiko, Matsumoto, Takayuki, Nakamura, Shiro, Nakase, Hiroshi, Hisamatsu, Tadakazu, Sasaki, Makoto, Hanai, Hiroyuki, Andoh, Akira, Nagasaki, Masao, Kinouchi, Yoshitaka, Shimosegawa, Tooru, Masamune, Atsushi, Suzuki, Yasuo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Japan 2018
Materias:
Original Article—Alimentary Tract
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6132901/
https://www.ncbi.nlm.nih.gov/pubmed/29923122
http://dx.doi.org/10.1007/s00535-018-1486-7
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author Kakuta, Yoichi
Kawai, Yosuke
Okamoto, Daisuke
Takagawa, Tetsuya
Ikeya, Kentaro
Sakuraba, Hirotake
Nishida, Atsushi
Nakagawa, Shoko
Miura, Miki
Toyonaga, Takahiko
Onodera, Kei
Shinozaki, Masaru
Ishiguro, Yoh
Mizuno, Shinta
Takahara, Masahiro
Yanai, Shunichi
Hokari, Ryota
Nakagawa, Tomoo
Araki, Hiroshi
Motoya, Satoshi
Naito, Takeo
Moroi, Rintaro
Shiga, Hisashi
Endo, Katsuya
Kobayashi, Taku
Naganuma, Makoto
Hiraoka, Sakiko
Matsumoto, Takayuki
Nakamura, Shiro
Nakase, Hiroshi
Hisamatsu, Tadakazu
Sasaki, Makoto
Hanai, Hiroyuki
Andoh, Akira
Nagasaki, Masao
Kinouchi, Yoshitaka
Shimosegawa, Tooru
Masamune, Atsushi
Suzuki, Yasuo
author_facet Kakuta, Yoichi
Kawai, Yosuke
Okamoto, Daisuke
Takagawa, Tetsuya
Ikeya, Kentaro
Sakuraba, Hirotake
Nishida, Atsushi
Nakagawa, Shoko
Miura, Miki
Toyonaga, Takahiko
Onodera, Kei
Shinozaki, Masaru
Ishiguro, Yoh
Mizuno, Shinta
Takahara, Masahiro
Yanai, Shunichi
Hokari, Ryota
Nakagawa, Tomoo
Araki, Hiroshi
Motoya, Satoshi
Naito, Takeo
Moroi, Rintaro
Shiga, Hisashi
Endo, Katsuya
Kobayashi, Taku
Naganuma, Makoto
Hiraoka, Sakiko
Matsumoto, Takayuki
Nakamura, Shiro
Nakase, Hiroshi
Hisamatsu, Tadakazu
Sasaki, Makoto
Hanai, Hiroyuki
Andoh, Akira
Nagasaki, Masao
Kinouchi, Yoshitaka
Shimosegawa, Tooru
Masamune, Atsushi
Suzuki, Yasuo
author_sort Kakuta, Yoichi
collection PubMed
description BACKGROUND: Despite NUDT15 variants showing significant association with thiopurine-induced adverse events (AEs) in Asians, it remains unclear which variants of NUDT15 or whether additional genetic variants should be tested to predict AEs. To clarify the best pharmacogenetic test to be used clinically, we performed association studies of NUDT15 variants and haplotypes with AEs, genome-wide association study (GWAS) to discover additional variants, and ROC analysis to select the model to predict severe AEs. METHODS: Overall, 2630 patients with inflammatory bowel disease (IBD) were enrolled and genotyped for NUDT15 codon 139; 1291 patients were treated with thiopurines. diplotypes were analyzed in 970 patients, and GWASs of AEs were performed with 1221 patients using population-optimized genotyping array and imputation. RESULTS: We confirmed the association of NUDT15 p.Arg139Cys with leukopenia and alopecia (p = 2.20E−63, 1.32E−69, OR = 6.59, 12.1, respectively), and found a novel association with digestive symptoms (p = 6.39E−04, OR = 1.89). Time to leukopenia was significantly shorter, and when leukopenia was diagnosed, thiopurine doses were significantly lower in Arg/Cys and Cys/Cys than in Arg/Arg. In GWASs, no additional variants were found to be associated with thiopurine-induced AEs. Despite strong correlation of leukopenia frequency with estimated enzyme activities based on the diplotypes (r(2) = 0.926, p = 0.0087), there were no significant differences in the AUCs of diplotypes from those of codon 139 to predict severe AEs (AUC = 0.916, 0.921, for acute severe leukopenia, AUC = 0.990, 0.991, for severe alopecia, respectively). CONCLUSIONS: Genotyping of NUDT15 codon 139 was sufficient to predict acute severe leukopenia and alopecia in Japanese patients with IBD. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00535-018-1486-7) contains supplementary material, which is available to authorized users.
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spelling pubmed-61329012018-09-13 NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study Kakuta, Yoichi Kawai, Yosuke Okamoto, Daisuke Takagawa, Tetsuya Ikeya, Kentaro Sakuraba, Hirotake Nishida, Atsushi Nakagawa, Shoko Miura, Miki Toyonaga, Takahiko Onodera, Kei Shinozaki, Masaru Ishiguro, Yoh Mizuno, Shinta Takahara, Masahiro Yanai, Shunichi Hokari, Ryota Nakagawa, Tomoo Araki, Hiroshi Motoya, Satoshi Naito, Takeo Moroi, Rintaro Shiga, Hisashi Endo, Katsuya Kobayashi, Taku Naganuma, Makoto Hiraoka, Sakiko Matsumoto, Takayuki Nakamura, Shiro Nakase, Hiroshi Hisamatsu, Tadakazu Sasaki, Makoto Hanai, Hiroyuki Andoh, Akira Nagasaki, Masao Kinouchi, Yoshitaka Shimosegawa, Tooru Masamune, Atsushi Suzuki, Yasuo J Gastroenterol Original Article—Alimentary Tract BACKGROUND: Despite NUDT15 variants showing significant association with thiopurine-induced adverse events (AEs) in Asians, it remains unclear which variants of NUDT15 or whether additional genetic variants should be tested to predict AEs. To clarify the best pharmacogenetic test to be used clinically, we performed association studies of NUDT15 variants and haplotypes with AEs, genome-wide association study (GWAS) to discover additional variants, and ROC analysis to select the model to predict severe AEs. METHODS: Overall, 2630 patients with inflammatory bowel disease (IBD) were enrolled and genotyped for NUDT15 codon 139; 1291 patients were treated with thiopurines. diplotypes were analyzed in 970 patients, and GWASs of AEs were performed with 1221 patients using population-optimized genotyping array and imputation. RESULTS: We confirmed the association of NUDT15 p.Arg139Cys with leukopenia and alopecia (p = 2.20E−63, 1.32E−69, OR = 6.59, 12.1, respectively), and found a novel association with digestive symptoms (p = 6.39E−04, OR = 1.89). Time to leukopenia was significantly shorter, and when leukopenia was diagnosed, thiopurine doses were significantly lower in Arg/Cys and Cys/Cys than in Arg/Arg. In GWASs, no additional variants were found to be associated with thiopurine-induced AEs. Despite strong correlation of leukopenia frequency with estimated enzyme activities based on the diplotypes (r(2) = 0.926, p = 0.0087), there were no significant differences in the AUCs of diplotypes from those of codon 139 to predict severe AEs (AUC = 0.916, 0.921, for acute severe leukopenia, AUC = 0.990, 0.991, for severe alopecia, respectively). CONCLUSIONS: Genotyping of NUDT15 codon 139 was sufficient to predict acute severe leukopenia and alopecia in Japanese patients with IBD. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00535-018-1486-7) contains supplementary material, which is available to authorized users. Springer Japan 2018-06-19 2018 /pmc/articles/PMC6132901/ /pubmed/29923122 http://dx.doi.org/10.1007/s00535-018-1486-7 Text en © The Author(s) 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Original Article—Alimentary Tract
Kakuta, Yoichi
Kawai, Yosuke
Okamoto, Daisuke
Takagawa, Tetsuya
Ikeya, Kentaro
Sakuraba, Hirotake
Nishida, Atsushi
Nakagawa, Shoko
Miura, Miki
Toyonaga, Takahiko
Onodera, Kei
Shinozaki, Masaru
Ishiguro, Yoh
Mizuno, Shinta
Takahara, Masahiro
Yanai, Shunichi
Hokari, Ryota
Nakagawa, Tomoo
Araki, Hiroshi
Motoya, Satoshi
Naito, Takeo
Moroi, Rintaro
Shiga, Hisashi
Endo, Katsuya
Kobayashi, Taku
Naganuma, Makoto
Hiraoka, Sakiko
Matsumoto, Takayuki
Nakamura, Shiro
Nakase, Hiroshi
Hisamatsu, Tadakazu
Sasaki, Makoto
Hanai, Hiroyuki
Andoh, Akira
Nagasaki, Masao
Kinouchi, Yoshitaka
Shimosegawa, Tooru
Masamune, Atsushi
Suzuki, Yasuo
NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study
title NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study
title_full NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study
title_fullStr NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study
title_full_unstemmed NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study
title_short NUDT15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in Japanese patients with inflammatory bowel disease: a multicenter study
title_sort nudt15 codon 139 is the best pharmacogenetic marker for predicting thiopurine-induced severe adverse events in japanese patients with inflammatory bowel disease: a multicenter study
topic Original Article—Alimentary Tract
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6132901/
https://www.ncbi.nlm.nih.gov/pubmed/29923122
http://dx.doi.org/10.1007/s00535-018-1486-7
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