Article ID Journal Published Year Pages File Type
2795464 Cytokine 2008 6 Pages PDF
Abstract

Background and Aims: Transforming growth factor β1 (TGFβ1) acts as an important profibrogenic cytokine in liver fibrogenesis. The aim of this study was to explore the association between TGFβ1 gene polymorphisms and liver cirrhosis. Methods: Totally 118 Chinese suffering from liver cirrhosis induced by HBV infection and 104 healthy controls were recruited. The polymorphisms at positions −988, −800, −509 and codon10, codon25, codon263 of the TGFβ1 gene were genotyped by ARMS-PCR or LightCycler. Enzyme immunoassay was used for TGFβ1 measurement. The promoter activities and DNA-binding capacities containing −509C>T were analyzed by reporter gene and EMSA. Results: The allele frequencies of CAT −509 and of T at codon10 were elevated in patients at severe Child-Pugh grade. Elevated concentrations of TGFβ1 were observed in patients, especially in those with −509CC/CT and codon10 TT/TC. Flanking sequences containing −509C showed higher promoter activities than −509T. EMSA showed one nucleotide change at −509C>T influenced nuclear protein binding to the putative binding site. Conclusions: The C allele at −509 and the T allele at codon10 could play important roles in progression of liver cirrhosis. The C allele at −509 mediates higher transcriptional activity than the T allele providing a potential explanation for the clinical findings.

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