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   Identification of sequence polymorphism in the D-Loop region of mitochondrial DNA as a risk factor for hepatocellular carcinoma with distinct etiology  
   
نویسنده zhang r. ,zhang f. ,wang c. ,wang s. ,shiao y.-h. ,guo z.
منبع journal of experimental and clinical cancer research - 2010 - دوره : 29 - شماره : 1
چکیده    Background. hepatocellular carcinoma (hcc) is frequently preceded by hepatitis virus infection or alcohol abuse. genetic backgrounds may increase susceptibility to hcc from these exposures. methods. mitochondrial dna (mtdna) of peripheral blood,tumor,and/or adjacent non-tumor tissue from 49 hepatitis b virus-related and 11 alcohol-related hcc patients,and from 38 controls without hcc were examined for single nucleotide polymorphisms (snps) and mutations in the d-loop region. results. single nucleotide polymorphisms (snps) in the d-loop region of mt dna were examined in hcc patients. individual snps,namely the 16266c/t,16293a/g,16299a/g,16303g/a,242c/t,368a/g,and 462c/t minor alleles,were associated with increased risk for alcohol- hcc,and the 523a/del was associated with increased risks of both hcc types. the mitochondrial haplotypes under the m haplogroup with a defining 489c polymorphism were detected in 27 (55.1%) of hbv-hccand 8 (72.7%) of alcohol- hcc patients,and in 15 (39.5%) of controls. frequencies of the 489t/152t,489t/523a,and 489t/525c haplotypes were significantly reduced in hbv-hcc patients compared with controls. in contrast,the haplotypes of 489c with 152t,249a,309c,523del,or 525del associated significantly with increase of alcohol-hcc risk. mutations in the d-loop region were detected in 5 adjacent non-tumor tissues and increased in cancer stage (21 of 49 hbv-hcc and 4 of 11 alcohol- hcc,p < 0.002). conclusions. in sum,mitochondrial haplotypes may differentially predispose patients to hbv-hcc and alcohol-hcc. mutations of the mitochondrial d-loop sequence may relate to hcc development. © 2010 zhang et al; licensee biomed central ltd.
آدرس department of gastroenterology and hepatology,fourth hospital of hebei medical university,shijiazhuang, China, department of gastroenterology and hepatology,fourth hospital of hebei medical university,shijiazhuang, China, department of gynecology ultrasound,fourth hospital of hebei medical university,shijiazhuang, China, department of hepatobiliary surgery,fourth hospital of hebei medical university,shijiazhuang, China, laboratory of comparative carcinogenesis,national cancer institute at frederick,frederick,md 21702, United States, department of gastroenterology and hepatology,fourth hospital of hebei medical university,shijiazhuang, China
 
     
   
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