Tumour necrosis factor‐alpha, interleukin‐10, interferon‐gamma and vitamin D receptor gene polymorphisms in patients with chronic hepatitis delta

Summary No data exist to assess certain polymorphisms that have a potential effect on the immune response in patients with chronic hepatitis delta ( CHD ). The aim of this study was to investigate polymorphisms in 6 polymorphic sites: IL ‐10 ‐1082 (rs1800896), IL ‐10 ‐627 (rs1800872), IFN ‐γ +874 (rs62559044), TNF ‐α ‐308 (rs1800629), vitamin D receptor ( VDR ) Fok I (rs2228570) and VDR Taq I (rs731236). The genotypes of 67 patients with CHD and 119 patients with chronic hepatitis B ( CHB ) were compared. In addition, 56 individuals with resolved hepatitis B virus ( HBV ) infection were used as a control group for patients with CHB . Polymorphisms in TNF ‐α, IL ‐10, and VDR genes were analysed using polymerase chain reaction/restriction fragment length polymorphism methods. The IFN ‐γ gene polymorphism was detected by allele‐specific polymerase chain reaction ( PCR ). Patients with CDH were more likely to have advanced liver disease compared with patients with CHB ( P  < 0.0001). IL ‐10 ‐1082 and VDR Taq I polymorphisms showed significant differences between patients with CHD and CHB . The high secretory IL ‐10 ‐1082 genotype GG was less frequent in CHD compared with patients with CHB and resolved HBV (17.7%, 37.4% and 47.1%, respectively ( P  < 0.05 for CHD vs CHB and resolved HBV ). The frequency of the high secretory VDR Taq I TT genotype was 86.6% in patients with CHD , 62.7% in patients with CHB and 62.5% in resolved HBV individuals ( CHD vs CHB : P  < 0.05). None of the polymorphisms analysed had an effect on HBV persistence. IL ‐10 ‐1082 and VDR Taq I polymorphisms may contribute to the more severe liver disease associated with CHD compared with CHB .