Literature DB >> 12186410

N-acetyltransferase 2 genotype-related sulfapyridine acetylation and its adverse events.

Yusuke Tanigawara1, Tomoko Kita, Nobuo Aoyama, Manabu Gobara, Fusao Komada, Toshiyuki Sakai, Masato Kasuga, Hisakatsu Hatanaka, Toshiyuki Sakaeda, Katsuhiko Okumura.   

Abstract

Sulfapyridine (SP), one of the metabolites of sulfasalazine (SASP), is further metabolized into N-acetylsulfapyridine (AcSP) by polymorphic N-acetyltransferase 2 (NAT2). NAT2 activity has been diagnosed by phenotyping, that is, evaluating plasma concentrations or urinary excretions of tentatively administered test drugs for dose individualization and avoidance of serious adverse events. Herein, we investigated the relationship between NAT2 genotypes and the pharmacokinetics of SP in healthy Japanese subjects, as well as the adverse events of SASP in patients with inflammatory bowel disease (IBD). Eight healthy subjects and 13 IBD patients were classified into three groups by NAT2 genotyping; the homozygote for the wild-type allele (Rapid Types), the compound heterozygote for the wild-type and mutant alleles (Intermediate Types), and the homozygote for mutant alleles (Slow Types). A single oral dose of 40 mg/kg SASP was administered to each healthy subject, and plasma and urine samples were taken until 51 and 72 h after administration, respectively. Both the SP and AcSP concentrations in each sample were determined by the HPLC method. The NAT2 genotypes were well-correlated with the plasma concentrations or urinary excretions of SP and AcSP in 8 healthy subjects, except for one Slow Type. In patients with IBD, skin rash was seen in 3 of 6 Rapid Types and 1 of 6 Intermediate Types, consistent with the concept that hypersensitive reactions are independent of serum SP concentrations. In contrast, SASP dosing-related acute pancreatitis was found in the Slow Type patient. In this case, the NAT2 activity was diagnosed by genotyping in advance, and the medical staff could pay scrupulous attention, resulting in no serious subjective symptoms such as abdominal pain, anorexia or fever. Further investigations on the relationship between the NAT2 genotype and adverse events are required, although genotyping appeared to be a promising method to avoid such serious adverse events.

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Year:  2002        PMID: 12186410     DOI: 10.1248/bpb.25.1058

Source DB:  PubMed          Journal:  Biol Pharm Bull        ISSN: 0918-6158            Impact factor:   2.233


  10 in total

1.  N-acetyltransferase 2 slow acetylator genotype associated with adverse effects of sulphasalazine in the treatment of inflammatory bowel disease.

Authors:  Min Chen; Bing Xia; Bixiao Chen; Qiusha Guo; Jin Li; Mei Ye; Zhengguo Hu
Journal:  Can J Gastroenterol       Date:  2007-03       Impact factor: 3.522

2.  Study of NAT2 gene polymorphisms in an Indian population: association with plasma isoniazid concentration in a cohort of tuberculosis patients.

Authors:  Neera Singh; Sudhisha Dubey; Saravanan Chinnaraj; Anil Golani; Anurupa Maitra
Journal:  Mol Diagn Ther       Date:  2009       Impact factor: 4.074

3.  N-acetyltransferase 2 genotype-related efficacy of sulfasalazine in patients with rheumatoid arthritis.

Authors:  Shunichi Kumagai; Fusao Komada; Tomoko Kita; Akio Morinobu; Shoichi Ozaki; Hiroshi Ishida; Hajime Sano; Tsukasa Matsubara; Katsuhiko Okumura
Journal:  Pharm Res       Date:  2004-02       Impact factor: 4.200

4.  A cross-sectional study of self-reported chemical-related sensitivity is associated with gene variants of drug-metabolizing enzymes.

Authors:  Eckart Schnakenberg; Karl-Rainer Fabig; Martin Stanulla; Nils Strobl; Michael Lustig; Nathalie Fabig; Werner Schloot
Journal:  Environ Health       Date:  2007-02-10       Impact factor: 5.984

5.  Hepatotoxicity associated with sulfasalazine in inflammatory arthritis: A case series from a local surveillance of serious adverse events.

Authors:  Paresh Jobanputra; Roshan Amarasena; Fiona Maggs; Dawn Homer; Simon Bowman; Elizabeth Rankin; Andrew Filer; Karim Raza; Ronald Jubb
Journal:  BMC Musculoskelet Disord       Date:  2008-04-11       Impact factor: 2.362

6.  Arylamine N-acetyltransferase polymorphisms in Han Chinese patients with ankylosing spondylitis and their correlation to the adverse drug reactions to sulfasalazine.

Authors:  Zhi-duo Hou; Zheng-yu Xiao; Yao Gong; Yu-ping Zhang; Qing Yu Zeng
Journal:  BMC Pharmacol Toxicol       Date:  2014-11-21       Impact factor: 2.483

7.  Genetic variation in aryl N-acetyltransferase results in significant differences in the pharmacokinetic and safety profiles of amifampridine (3,4-diaminopyridine) phosphate.

Authors:  Peter E Haroldsen; Marvin R Garovoy; Donald G Musson; Huiyu Zhou; Laurie Tsuruda; Boyd Hanson; Charles A O'Neill
Journal:  Pharmacol Res Perspect       Date:  2014-12-09

8.  Unusual Case of an Alcoholic with Liver Injury from Sulfasalazine Use.

Authors:  Umair Masood; Anuj Sharma; Sonny Nijjar; Barbara Krenzer
Journal:  J Basic Clin Pharm       Date:  2016-12

9.  The association between NAT2 acetylator status and adverse drug reactions of sulfasalazine: a systematic review and meta-analysis.

Authors:  Jeong Yee; So Min Kim; Ji Min Han; Nari Lee; Ha Young Yoon; Hye Sun Gwak
Journal:  Sci Rep       Date:  2020-02-27       Impact factor: 4.379

10.  Characterization of N-acetyltransferase 1 and 2 polymorphisms and haplotype analysis for inflammatory bowel disease and sporadic colorectal carcinoma.

Authors:  Suhal S Mahid; Daniel W Colliver; Nigel P S Crawford; Benjamin D Martini; Mark A Doll; David W Hein; Gary A Cobbs; Robert E Petras; Susan Galandiuk
Journal:  BMC Med Genet       Date:  2007-05-30       Impact factor: 2.103
  10 in total

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