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RANTES启动子变体与CCR5Delta32之间的相互作用有利于乙型肝炎的康复。

Interaction between RANTES promoter variant and CCR5Delta32 favors recovery from hepatitis B.

作者信息

Thio Chloe L, Astemborski Jacquie, Thomas Rasmi, Mosbruger Timothy, Witt Mallory D, Goedert James J, Hoots Keith, Winkler Cherie, Thomas David L, Carrington Mary

机构信息

Department of Medicine, Johns Hopkins University, Baltimore, MD 21205, USA.

出版信息

J Immunol. 2008 Dec 1;181(11):7944-7. doi: 10.4049/jimmunol.181.11.7944.

Abstract

Recovery from acute hepatitis B virus (HBV) infection occurs in 95% of adult-acquired infections. A 32-bp deletion in CCR5 (CCR5Delta32), which encodes for a nonfunctional receptor, increases the likelihood of recovery. Using 181 subjects with persistent HBV infection and 316 who had recovered, we tested the hypothesis that an epistatic interaction between functional polymorphisms in RANTES (a CCR5 ligand) and CCR5 impacts recovery. Specific models designed to assess individual contributions of compound genotypes demonstrated that the only combination associated with recovery from an HBV infection was RANTES -403A with CCR5Delta32 (odds ratio 0.36, p = 0.02). Because the phenotypic consequence of -403A is reported to be higher levels of RANTES, we propose a model in which excess RANTES in combination with low CCR5 favors recovery from an HBV infection, which will require validation through functional testing.

摘要

95%的成人获得性急性乙型肝炎病毒(HBV)感染可实现康复。编码无功能受体的CCR5基因中一个32碱基对的缺失(CCR5Delta32)会增加康复的可能性。我们以181名持续性HBV感染患者和316名已康复患者为研究对象,检验了以下假设:调节激活正常T细胞表达和分泌因子(RANTES,一种CCR5配体)与CCR5功能多态性之间的上位相互作用会影响康复情况。旨在评估复合基因型个体贡献的特定模型表明,与HBV感染康复相关的唯一组合是RANTES -403A与CCR5Delta32(优势比0.36,p = 0.02)。由于据报道-403A的表型结果是RANTES水平升高,我们提出了一个模型,即过量的RANTES与低水平的CCR5共同作用有利于从HBV感染中康复,这需要通过功能测试进行验证。

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