Department of Gastroenterology, Sanjay Gandhi Postgraduate Institute of Medical Sciences, Lucknow, UP, India.
Biomedical Informatics Centre, Sanjay Gandhi Postgraduate Institute of Medical Sciences, Lucknow, UP, India.
Ann Hepatol. 2018;17(4):561-568. doi: 10.5604/01.3001.0012.0917.
HAVCR1 protein is the cellular receptor for hepatitis A virus (HAV). Genetic polymorphism in this gene may alter the outcome of HAV infection. In a previous study, a 6-amino acid insertion (157insMTTTVP) in HAVCR1 gene was associated with more severe disease. We decided to investigate this association further.
We sequenced exon 4 of the HAVCR1 gene in patients with clinical hepatitis A attending our institution, and a group of healthy controls in a disease-endemic setting in India. Frequencies of different haplotypes of a genomic region with two overlapping insertion-deletion polymorphisms (indels; rs141023871 and rs139041445) were compared between patients and controls, as well as between patients with and without a severe form of disease (liver failure).
The gene had three haplotypes in the region of interest - a short form, an intermediate-form with a 5-amino acid 157insMTTVP insertion and a long-form with a 6-amino acid 157insMTTTVP insertion. The allele frequency (29/150 [19%] vs. 43/146 [29%]; p = ns) and haplotype frequency (29/75 [39%] vs. 39/73 [53%]; p = ns) of the 157insMTTTVP variant were similar in hepatitis A patients and healthy controls (30%). Further, the allele frequency (12/58 [21%] vs. 17/92 [18%]; p = ns) and haplotype frequency (12/29 [41%] vs.17/46 [37%]; p = ns) of the longest variant were also similar in patients with severe and mild disease.
In the study population, the 157insMTTTVP variant of HAVCR1 gene was not associated with more severe outcome of HAV infection. Further studies in other populations around the world are needed to assess the relation of this genetic variation with disease outcome.
HAVCR1 蛋白是甲型肝炎病毒(HAV)的细胞受体。该基因的遗传多态性可能改变 HAV 感染的结果。在之前的研究中,HAVCR1 基因中的 6 个氨基酸插入(157insMTTTVP)与更严重的疾病相关。我们决定进一步研究这种相关性。
我们对我院就诊的临床甲型肝炎患者和印度疾病流行地区的一组健康对照者的 HAVCR1 基因外显子 4 进行了测序。比较了患者和对照组以及有和无严重疾病(肝衰竭)的患者之间两个重叠插入缺失多态性(indels;rs141023871 和 rs139041445)的基因组区域不同单倍型的频率。
该基因在感兴趣的区域有三种单倍型 - 短型、中间型(5 个氨基酸 157insMTTVP 插入)和长型(6 个氨基酸 157insMTTTVP 插入)。甲型肝炎患者和健康对照组的等位基因频率(29/150[19%]与 43/146[29%];p=ns)和单倍型频率(29/75[39%]与 39/73[53%];p=ns)的 157insMTTTVP 变体相似(30%)。此外,严重和轻度疾病患者的最长变体的等位基因频率(12/58[21%]与 17/92[18%];p=ns)和单倍型频率(12/29[41%]与 17/46[37%];p=ns)也相似。
在研究人群中,HAVCR1 基因的 157insMTTTVP 变体与 HAV 感染的更严重结局无关。需要在世界各地的其他人群中进行进一步的研究,以评估这种遗传变异与疾病结局的关系。