Genetic variation in IL28B predicts hepatitis C treatment-induced viral clearance

被引:0
|
作者
Dongliang Ge
Jacques Fellay
Alexander J. Thompson
Jason S. Simon
Kevin V. Shianna
Thomas J. Urban
Erin L. Heinzen
Ping Qiu
Arthur H. Bertelsen
Andrew J. Muir
Mark Sulkowski
John G. McHutchison
David B. Goldstein
机构
[1] Institute for Genome Sciences & Policy,Duke Clinical Research Institute and Division of Gastroenterology
[2] Center for Human Genome Variation,undefined
[3] Duke University,undefined
[4] Durham,undefined
[5] North Carolina 27708,undefined
[6] USA ,undefined
[7] School of Medicine,undefined
[8] Duke University,undefined
[9] Durham,undefined
[10] North Carolina 27705,undefined
[11] USA,undefined
[12] Schering-Plough Research Institute,undefined
[13] Kenilworth,undefined
[14] New Jersey 07033,undefined
[15] USA ,undefined
[16] Johns Hopkins University School of Medicine,undefined
[17] Baltimore,undefined
[18] Maryland 21205,undefined
[19] USA ,undefined
来源
Nature | 2009年 / 461卷
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摘要
Hepatitis C is one of the most common infections in the world. Many of its estimated 170 million sufferers live with the disease for years with no serious symptoms, but in about one in four patients it leads to cirrhosis of the liver. The discovery of a biomarker that predicts an individual's response to hepatitis C treatment raises the possibility that clinical outcomes could be improved by raising patient compliance to the often demanding interferon treatment regime. The new marker is a 'single letter' genetic variant — a C (cytosine) replacing a T (thymidine) in a segment of DNA near the IL28B gene that encodes interleukin 28B (interferon-γ-3). This finding goes some way towards explaining the different treatment outcomes between individuals of European (high IL28B frequency), African and Asian ancestry. And importantly, it is of immediate clinical utility.
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页码:399 / 401
页数:2
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