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细胞色素P4502E1基因多态性是否为中国人群酒精性终末期器官损伤易感性遗传标志物的研究。

An investigation of whether polymorphisms of cytochrome P4502E1 are genetic markers of susceptibility to alcoholic end-stage organ damage in a Chinese population.

作者信息

Chao Y C, Young T H, Chang W K, Tang H S, Hsu C T

机构信息

Department of Internal Medicine, Tri-Service General Hospital, National Defense Medical Center, Taipei, Taiwan, Republic of China.

出版信息

Hepatology. 1995 Nov;22(5):1409-14.

PMID:7590656
Abstract

The human cytochrome P4502E1 gene (P4502E1), coding for an ethanol-inducible nitrosamine-metabolizing P-450, is involved in the metabolism of ethanol and many known carcinogens. Recently, restriction fragment length polymorphisms (RFLPs) within the P4502E1 have been suggested as genetic markers of susceptibility to alcohol-induced liver disease but the previous studies disagree whether alcoholics with c1 or c2 allele are more susceptible to alcohol-induced liver diseases. Using a polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) method, we determined the RsaI and PstI polymorphism of P4502E1 in 77 Chinese alcoholic patients (54 with alcohol-induced cirrhosis and 23 with acute alcohol-induced pancreatitis) and 164 non-alcoholics and compared them with previously published data. The PCR-RFLPs showed three P4502E1 genotypes: type A, homozygote c1/c1; type B, heterozygote c1/c2; and type C, homozygote c2/c2. The RsaI and PstI polymorphism of P4502E1 were completely linked in both Chinese alcoholics and nonalcoholic controls. The rare allele (c2) occurs at similar frequency of 0.232 and 0.234 (P > .05) in nonalcoholic controls and alcoholics, respectively. The genotype distributions of P4502E1 between Chinese alcoholics and nonalcoholics are not significantly different. The genotype and allele frequencies of P4502E1 for Chinese are significantly different from those of Swedes, European-Americans, and African-Americans, respectively (P < .00001), but very similar to Japanese (P > .05). In conclusion, ethnic variations exist between Asians and Caucasians and between Asians and African-Americans. No allelic variants at loci associated with RsaI/PstI RFLPs result in phenotypes displaying greater susceptibility to alcohol-induced cirrhosis or alcoholism in Chinese populations, which contradicts previous reports from Japanese groups.

摘要

人类细胞色素P4502E1基因(P4502E1)编码一种乙醇诱导的亚硝胺代谢P-450,参与乙醇和许多已知致癌物的代谢。最近,有人提出P4502E1内的限制性片段长度多态性(RFLP)作为酒精性肝病易感性的遗传标记,但先前的研究对于携带c1或c2等位基因的酗酒者是否更易患酒精性肝病存在分歧。我们采用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)方法,测定了77例中国酗酒患者(54例酒精性肝硬化患者和23例急性酒精性胰腺炎患者)及164例非酗酒者中P4502E1的RsaI和PstI多态性,并与先前发表的数据进行比较。PCR-RFLP显示出三种P4502E1基因型:A型,纯合子c1/c1;B型,杂合子c1/c2;C型,纯合子c2/c2。P4502E1的RsaI和PstI多态性在中国酗酒者和非酗酒对照者中完全连锁。非酗酒对照者和酗酒者中罕见等位基因(c2)的出现频率分别为0.232和0.234(P>.05)。中国酗酒者和非酗酒者之间P4502E1的基因型分布无显著差异。中国人P4502E1的基因型和等位基因频率分别与瑞典人、欧裔美国人和非裔美国人有显著差异(P<.00001),但与日本人非常相似(P>.05)。总之,亚洲人和高加索人之间以及亚洲人和非裔美国人之间存在种族差异。在中国人群中,与RsaI/PstI RFLP相关位点的等位基因变异不会导致对酒精性肝硬化或酗酒表现出更高易感性的表型,这与日本人群先前的报道相矛盾。

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