August 26, 2009

Is endotoxin receptor CD14 rs2569190/C-159T gene correlated with chronic hepatitis C?

It is still unknown why the natural history of chronic disease caused by hepatitis C virus (HCV), which currently infects 3% of the world's population, varies from mild in some patients to rapidly progressing in others.

Age, sex, alcohol consumption and liver sensitivity to gut-derived bacterial endotoxins, were the early factors defined to enhance the risk of fibrosis progression. Host genetic variations, e.g., the CD14 single nucleotide polymorphism (SNP), rs2569190/C-159T, have been recently intensively investigated and suggested to be prognostic factors for cirrhosis in various liver diseases. Is this endotoxin receptor SNP correlated with liver disease features in patients?

A research article to be published on August 21, 2009 in the addresses this question. The research team lead by Professor Sabine Mihm and her colleagues from the Department of Gastroenterology and Endocrinology, University Medical Center Göttingen, Germany, analyzed the distribution of various epidemiological, biochemical, and histological characteristics in 2 cohorts of Caucasian chronic hepatitis C patients with respect to their genotypes according to the CD14 rs2569190/C-159T SNP.

In one cohort, patients who carried 2 variant alleles (TT) were found to be younger than C allele carriers (CC or CT). Among the histological lesions studied, portal lymphoid aggregates were more frequently observed among TT than among C carriers. The presence of portal lymphoid aggregates was also closely correlated with another 2 lesions, moderate and severe hepatic inflammation and the presence of bile duct damage. However, the degree of fibrosis was not found to be related to the CD14 gene C-159T SNP.

The different situation between chronic liver diseases caused by HCV infection or by in relation to TT status suggests that endotoxin sensitivity depends on both genetic and environmental factors (gene environment interaction). Our analysis suggests, for the first time, a relationship between the CD14 variation and the formation of portal lymphoid aggregates, which was attributed to the host's immunological participation in liver disease pathogenesis.

More information: Askar E, Ramadori G, Mihm S. Endotoxin receptor CD14 genevariants and histological features in chronic HCV infection. World J Gastroenterol 2009; 15(31): 3884-3890 www.wjgnet.com/1007-9327/15/3884.asp

Source: World Journal of Gastroenterology (news : web)

Citation: Is endotoxin receptor CD14 rs2569190/C-159T gene correlated with chronic hepatitis C? (2009, August 26) retrieved 23 April 2024 from https://medicalxpress.com/news/2009-08-endotoxin-receptor-cd14-rs2569190c-159t-gene.html
This document is subject to copyright. Apart from any fair dealing for the purpose of private study or research, no part may be reproduced without the written permission. The content is provided for information purposes only.

Explore further

The risk factors of idiopathic pulmonary fibrosis in HCV patients
 shares

Feedback to editors
Active military service may heighten women's risk of having low birthweight babies

9 hours ago
Significant global variation in COVID-19 guidelines: Most countries recommend at least one treatment that doesn't work

9 hours ago
Study connects enjoyment of nature to lower inflammation levels

10 hours ago
Bacteria in the intestine that change in response to inflammation could have an impact on our immune system

10 hours ago
Researchers develop deep-learning model capable of predicting cardiac arrhythmia 30 minutes before it happens

11 hours ago
Improving cancer immunotherapy by prolonging T-cell survival

11 hours ago
Eye-opener: Pupils enlarge when people focus on tasks

11 hours ago
Study finds COVID-19 pandemic led to some, but not many, developmental milestone delays in infants and young children

11 hours ago
Common antibiotic may be helpful in fighting respiratory viral infections

12 hours ago
In psychedelic therapy, clinician-patient bond may matter most

12 hours ago
Load comments (0)