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Literature DB >> 24033692

UGT1A16, 1A73, and 1A9*22 genotypes predict severe neutropenia in FOLFIRI-treated metastatic colorectal cancer in two prospective studies in Japan.

Shoichi Hazama¹, Hideyuki Mishima, Ryouichi Tsunedomi, Yusuke Okuyama, Takeshi Kato, Ken-ichi Takahashi, Hiroshi Nozawa, Hideaki Ando, Michiya Kobayashi, Hiroyoshi Takemoto, Naoki Nagata, Shinsuke Kanekiyo, Yuka Inoue, Yoshihiko Hamamoto, Yusuke Fujita, Yuji Hinoda, Naoko Okayama, Koji Oba, Jun-ichi Sakamoto, Masaaki Oka.

Abstract

UNLABELLED: Retrospective studies have suggested that UDP-glucuronosyltransferase (UGT)1A1, UGT1A7, and UGT1A9 predict severe toxicity and efficacy of irinotecan-containing regimens. We prospectively evaluated the impact of UGT1A genotypes and haplotypes on severe toxicity and efficacy in patients treated with fluorouracil, leucovorin, and irinotecan combination chemotherapy (FOLFIRI) for metastatic colorectal cancer (mCRC) from the two prospective multicenter phase II studies in Japan. The FLIGHT1 study was a first-line FOLFIRI trial, and FLIGHT2 was a FOLFOX-refractory, second-line FOLFIRI trial. A total of 73 patients agreed to additional analysis, and were genotyped for UGT1A polymorphisms, UGT1A1*28 (TA6>TA7), UGT1A1*6 (211G>A), UGT1A1*27 (686C>A), UGT1A1*60 (-3279T>G), UGT1A1*93 (-3156G>A), UGT1A7 (-57T>G), UGT1A7*3 (387T>G, 622T>C), and UGT1A9*22 (T9>T10). Of 73 patients, 34 developed G3/4 severe hematological toxicities. The toxicities were significantly more frequent in patients with UGT1A1*6 (211A), UGT1A7 (387G), and UGT1A9*22 reference alleles (T9). Haplotype I, which consists of all favorable alleles, was associated with a significant reduction in hematologic toxicity (P = 0.031). In contrast, haplotype II, which contains four high-risk alleles, showed significantly higher hematologic toxicity than the other haplotypes (P = 0.010). Six out of seven patients who were homozygous for UGT1A1*28 or *6 experienced severe hematological toxicity despite the fact that their response rate was not impaired (42.9%). We concluded that UGT1A polymorphisms, especially UGT1A1*6, are important for the prediction of severe toxicity of FOLFIRI in northeast Asian populations. In this regard, haplotype analyses should substantially impact the prediction of severe hematological toxicities of FOLFIRI. ( CLINICAL TRIAL REGISTRATION: UMIN000002388 and UMIN000002476).

Entities: Chemical Disease Gene Mutation Species

Mesh：

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Year: 2013 PMID： 24033692 PMCID： PMC7653527 DOI： 10.1111/cas.12283

Source DB: PubMed Journal: Cancer Sci ISSN： 1347-9032 Impact factor: 6.716

28 in total

1. Genetic testing for UGT1A128 and 6 in Japanese patients who receive irinotecan chemotherapy.

Authors: Y Akiyama; K Fujita; F Nagashima; W Yamamoto; H Endo; Y Sunakawa; K Yamashita; H Ishida; K Mizuno; K Araki; W Ichikawa; T Miya; M Narabayashi; K Kawara; M Sugiyama; T Hirose; Y Ando; Y Sasaki
Journal: Ann Oncol Date: 2008-10-26 Impact factor: 32.976

2. Is there diversity among UGT1A1 polymorphism in Japan?

Authors: Michiya Kobayashi; Shoichi Hazama; Kenichi Takahashi; Koji Oba; Naoko Okayama; Mitsuaki Nishioka; Yuji Hinoda; Masaaki Oka; Ken Okamoto; Hiromichi Maeda; Daisuke Nakamura; Junichi Sakamoto; Hideyuki Mishima
Journal: World J Gastrointest Oncol Date: 2012-07-15

3. Irinotecan combined with fluorouracil compared with fluorouracil alone as first-line treatment for metastatic colorectal cancer: a multicentre randomised trial.

Authors: J Y Douillard; D Cunningham; A D Roth; M Navarro; R D James; P Karasek; P Jandik; T Iveson; J Carmichael; M Alakl; G Gruia; L Awad; P Rougier
Journal: Lancet Date: 2000-03-25 Impact factor: 79.321

4. Phase I study of irinotecan and doxifluridine for metastatic colorectal cancer focusing on the UGT1A1*28 polymorphism.

Authors: Shoichi Hazama; Atsushi Nagashima; Hiroshi Kondo; Shin Yoshida; Ryoichi Shimizu; Atsuhiro Araki; Shigefumi Yoshino; Naoko Okayama; Yuji Hinoda; Masaaki Oka
Journal: Cancer Sci Date: 2009-11-07 Impact factor: 6.716

5. FOLFIRI followed by FOLFOX6 or the reverse sequence in advanced colorectal cancer: a randomized GERCOR study.

Authors: Christophe Tournigand; Thierry André; Emmanuel Achille; Gérard Lledo; Michel Flesh; Dominique Mery-Mignard; Emmanuel Quinaux; Corinne Couteau; Marc Buyse; Gérard Ganem; Bruno Landi; Philippe Colin; Christophe Louvet; Aimery de Gramont
Journal: J Clin Oncol Date: 2003-12-02 Impact factor: 44.544

6. A novel polymorphism in the promoter region of human UGT1A9 gene (UGT1A9*22) and its effects on the transcriptional activity.

Authors: Hiroyuki Yamanaka; Miki Nakajima; Miki Katoh; Yusuke Hara; Osamu Tachibana; Junkoh Yamashita; Howard L McLeod; Tsuyoshi Yokoi
Journal: Pharmacogenetics Date: 2004-05

7. Intracellular roles of SN-38, a metabolite of the camptothecin derivative CPT-11, in the antitumor effect of CPT-11.

Authors: Y Kawato; M Aonuma; Y Hirota; H Kuga; K Sato
Journal: Cancer Res Date: 1991-08-15 Impact factor: 12.701

8. UGT1A16, 1A73, and 1A9*22 genotypes predict severe neutropenia in FOLFIRI-treated metastatic colorectal cancer in two prospective studies in Japan.

Authors: Shoichi Hazama; Hideyuki Mishima; Ryouichi Tsunedomi; Yusuke Okuyama; Takeshi Kato; Ken-ichi Takahashi; Hiroshi Nozawa; Hideaki Ando; Michiya Kobayashi; Hiroyoshi Takemoto; Naoki Nagata; Shinsuke Kanekiyo; Yuka Inoue; Yoshihiko Hamamoto; Yusuke Fujita; Yuji Hinoda; Naoko Okayama; Koji Oba; Jun-ichi Sakamoto; Masaaki Oka
Journal: Cancer Sci Date: 2013-10-27 Impact factor: 6.716

9. UGT1A and TYMS genetic variants predict toxicity and response of colorectal cancer patients treated with first-line irinotecan and fluorouracil combination therapy.

Authors: E Martinez-Balibrea; A Abad; A Martínez-Cardús; A Ginés; M Valladares; M Navarro; E Aranda; E Marcuello; M Benavides; B Massutí; A Carrato; L Layos; J L Manzano; V Moreno
Journal: Br J Cancer Date: 2010-07-13 Impact factor: 7.640

10. Genetic polymorphisms of the UDP-glucuronosyltransferase 1A7 gene and irinotecan toxicity in Japanese cancer patients.

Authors: Maki Ando; Yuichi Ando; Yoshitaka Sekido; Masahiko Ando; Kaoru Shimokata; Yoshinori Hasegawa
Journal: Jpn J Cancer Res Date: 2002-05

12 in total

1. UGT1A16, UGT1A73 and UGT1A9*1b polymorphisms are predictive markers for severe toxicity in patients with metastatic gastrointestinal cancer treated with irinotecan-based regimens.

Authors: Chengxu Cui; Chang Shu; Dandan Cao; Yi Yang; Junbao Liu; Shuping Shi; Zhujun Shao; Nan Wang; Ting Yang; Hao Liang; Shanshan Zou; Songnian Hu
Journal: Oncol Lett Date: 2016-09-14 Impact factor: 2.967

2. The UGT1A9*22 genotype identifies a high-risk group for irinotecan toxicity among gastric cancer patients.

Authors: Choong-Kun Lee; Hong Jae Chon; Woo Sun Kwon; Hyo-Jeong Ban; Sang Cheol Kim; Hyunwook Kim; Hei-Cheul Jeung; Jimyung Chung; Sun Young Rha
Journal: Genomics Inform Date: 2022-09-30

3. UGT1A16, 1A73, and 1A9*22 genotypes predict severe neutropenia in FOLFIRI-treated metastatic colorectal cancer in two prospective studies in Japan.

4. Comparison of effects of UGT1A16 and UGT1A128 on irinotecan-induced adverse reactions in the Japanese population: analysis of the Biobank Japan Project.

Authors: Keiko Hikino; Takeshi Ozeki; Masaru Koido; Chikashi Terao; Yoichiro Kamatani; Yoshinori Murakami; Michiaki Kubo; Taisei Mushiroda
Journal: J Hum Genet Date: 2019-10-04 Impact factor: 3.172

5. An internally and externally validated nomogram for predicting the risk of irinotecan-induced severe neutropenia in advanced colorectal cancer patients.

Authors: W Ichikawa; K Uehara; K Minamimura; C Tanaka; Y Takii; H Miyauchi; S Sadahiro; K Fujita; T Moriwaki; M Nakamura; T Takahashi; A Tsuji; K Shinozaki; S Morita; Y Ando; Y Okutani; M Sugihara; T Sugiyama; Y Ohashi; Y Sakata
Journal: Br J Cancer Date: 2015-04-16 Impact factor: 7.640

6. Differences in UGT1A1, UGT1A7, and UGT1A9 polymorphisms between Uzbek and Japanese populations.

Authors: Hiromichi Maeda; Shoichi Hazama; Abdiev Shavkat; Ken Okamoto; Koji Oba; Junichi Sakamoto; Kenichi Takahashi; Masaki Oka; Daisuke Nakamura; Ryouichi Tsunedomi; Naoko Okayama; Hideyuki Mishima; Michiya Kobayashi
Journal: Mol Diagn Ther Date: 2014-06 Impact factor: 4.074

7. Clinical Implication of UGT1A1 Promoter Polymorphism for Irinotecan Dose Escalation in Metastatic Colorectal Cancer Patients Treated with Bevacizumab Combined with FOLFIRI in the First-line Setting.

Authors: Chien-Yu Lu; Ching-Wen Huang; I-Chen Wu; Hsiang-Lin Tsai; Cheng-Jen Ma; Yung-Sung Yeh; Se-Fen Chang; Meng-Lin Huang; Jaw-Yuan Wang
Journal: Transl Oncol Date: 2015-12 Impact factor: 4.243

8. Rapid and sensitive detection of UGT1A1 polymorphisms associated with irinotecan toxicity by a novel DNA microarray.

Authors: Ryouichi Tsunedomi; Shoichi Hazama; Naoko Okayama; Masaaki Oka; Hiroaki Nagano
Journal: Cancer Sci Date: 2017-06-05 Impact factor: 6.716

9. Examination of multiple UGT1A and DPYD polymorphisms has limited ability to predict the toxicity and efficacy of metastatic colorectal cancer treated with irinotecan-based chemotherapy: a retrospective analysis.

Authors: Dan Liu; Jian Li; Jing Gao; Yanyan Li; Rui Yang; Lin Shen
Journal: BMC Cancer Date: 2017-06-20 Impact factor: 4.430

10. A novel system for predicting the toxicity of irinotecan based on statistical pattern recognition with UGT1A genotypes.

Authors: Ryouichi Tsunedomi; Shoichi Hazama; Yusuke Fujita; Naoko Okayama; Shinsuke Kanekiyo; Yuka Inoue; Shigefumi Yoshino; Takahiro Yamasaki; Yutaka Suehiro; Koji Oba; Hideyuki Mishima; Junichi Sakamoto; Yoshihiko Hamamoto; Masaaki Oka
Journal: Int J Oncol Date: 2014-07-22 Impact factor: 5.650