摘要
目的应用HRM技术检测炎症性肠病(IBD)患者TPMT基因多态性,进而探索IBD患者TPMT基因型与硫唑嘌呤(AZA)致骨髓抑制的关系。方法采用聚合酶链反应-高分辨熔解曲线(PCR-HRM)与Sanger法序列测定相结合的方法,对82例IBD患者和53名健康志愿者TPMT基因第7、10外显子进行检测。结果 IBD患者中TPMT*1/*3C杂合子4例,健康对照者中TPMT*1/*3C杂合子2例。未检测出TPMT*3A和TPMT*3B型突变。IBD患者4例出现骨髓抑制的患者中,1例是TPMT*1/*3C杂合子;其余3例为TPMT野生型。结论 TPMT*3C(A719G)基因突变在中国的IBD患者中较TPMT*3A(G460A/A719G)、TPMT*3B(G460A)发生率高,而存在此基因突变的IBD患者对硫唑嘌呤不能耐受,导致骨髓抑制。然而TPMT基因突变只能解释部分AZA治疗IBD导致骨髓抑制的病例。
Objective To detect the gene polymorphism of the inflammatory bowel disease ~ ll^LJ) patients, Iartner more, to discuss the relationship between the genotype of TPMT and AZA induced myelotoxicity in the patients with IBD. Methods Three commom mutation alleles of TPMT [ TPMT * 3A (G460A/A719G), TPMT * 3B (G460A), TPMT * 3C (ATIgG:) ] were detected by polymerasechain reacti0n:high resolutidn melting and sequencing in 82 IBD patients and 53' healthy :Chin^e peopte; Resuits) F8ur eases of heterozygote TPMT * 1/* 3C were found in IBD pa- tients. No TPMT* 3A or TPMT* 3B was found;. =Bone marrow supDression occurred in four of the patients who received AZA, but only one of them had the TPMT * 1/* 3C mutation, others were wild-type homozygote. Conclusion The fre- quency of TPMT * 3C(A719G) mutation is more than TPMT * 3A(G460A/A719G) and TPMT * 3B(G460A) mutation in Chinese IBD patients. Patient who has the TPMT * 3C(A719G)mutation is very likely to have the bone marrow sup- pression. But mutantion of TPMT gene could just partially explain the AZA induced myelotoxicity.
出处
《胃肠病学和肝病学杂志》
CAS
2014年第1期66-69,共4页
Chinese Journal of Gastroenterology and Hepatology
关键词
炎症性肠病
甲基转移酶类
基因型
硫唑嘌呤
Inflammatory bowel disease
Methyltransferase
Genotype
Azathioprine
