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A comparative review of HLA associations with hepatitis B and C viral infections across global populations

机译:全球人群HLA与乙型和丙型肝炎病毒感染的关联性比较研究

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摘要

Hepatitis B (HBV) and hepatitis C (HCV) viral infection or co-infection leads to risk of development of chronic infection, cirrhosis and hepatocellular carcinoma (HCC). Immigration and globalization have added to the challenges of public health concerns regarding chronic HBV and HCV infections worldwide. The aim of this study is to review existing global literature across ethnic populations on HBV and HCV related human leukocyte antigen (HLA) associations in relation to susceptibility, viral persistence and treatment. Extensive literature search was conducted to explore the HLA associations in HBV and HCV infections reported across global populations over the past decade to understand the knowledge status, weaknesses and strengths of this information in different ethnic populations. HLA DR13 is consistently associated with HBV clearance globally. HLADRB1*11/*12 alleles and DQB1*0301 are associated with HBV persistence but with HCV clearance worldwide. Consistent association of DRB1*03 and *07 is observed with HCV susceptibility and non-responsiveness to HBV vaccination across the population. HLA DR13 is protective for vertical HBV and HCV transmission in Chinese and Italian neonates, but different alleles are associated with their susceptibility in these populations. HLA class Imolecule interactions with Killer cell immunoglobulin like receptors (KIR) of natural killer (NK) cells modulate HCV infection outcome via regulating immune regulatory cells and molecules. HLA associations with HBV vaccination, interferon therapy in HBV and HCV, and with extra hepatic manifestations of viral hepatitis are also discussed. Systematic studies in compliance with global regulatory standards are required to identify the HLA specific viral epitope, stage specific T cell populations interacting with different HLA alleles during disease progression and viral clearance of chronic HBV or HCV infections among different ethnic populations. These studies would facilitate stage specific therapeutic strategies for clearance of HBV and HCV infections or co-infections across global populations and aid in identification of HBV-HCV combined vaccine. HLA associations of chronic HBV or HCV development with confounding host factors including alcohol, drug abuse, insulin resistance, age and gender are lacking and warrant detailed investigation across global populations.
机译:乙型肝炎(HBV)和丙型肝炎(HCV)病毒感染或合并感染会导致发生慢性感染,肝硬化和肝细胞癌(HCC)的风险。移民和全球化增加了有关全球慢性HBV和HCV感染的公共卫生问题的挑战。这项研究的目的是回顾全球人群中有关易感性,病毒持久性和治疗的HBV和HCV相关人类白细胞抗原(HLA)关联的全球文献。进行了广泛的文献搜索,以探讨过去十年来全球人群中报告的HBV和HCV感染中的HLA关联,以了解不同种族人群中该信息的知识状况,弱点和优势。 HLA DR13在全球始终与HBV清除率相关。 HLADRB1 * 11 / * 12等位基因和DQB1 * 0301与HBV持续性相关,但与全世界的HCV清除率相关。在人群中,观察到DRB1 * 03和* 07的一致性与HCV敏感性和对HBV疫苗的无反应性有关。 HLA DR13可保护中国和意大利新生儿的垂直HBV和HCV传播,但在这些人群中,不同的等位基因与其易感性有关。 HLA类分子与自然杀伤(NK)细胞的杀伤细胞免疫球蛋白样受体(KIR)相互作用通过调节免疫调节细胞和分子来调节HCV感染的结果。还讨论了HLA与HBV疫苗接种,干扰素治疗HBV和HCV以及肝炎的肝外表现。需要进行符合全球法规标准的系统研究,以鉴定HLA特异性病毒表位,疾病发展过程中的HLA特异性病毒表位以及与不同HLA等位基因相互作用的阶段性T细胞群体,以及不同种族人群之间慢性HBV或HCV感染的病毒清除率。这些研究将有助于在全球人群中清除HBV和HCV感染或合并感染的特定阶段治疗策略,并有助于鉴定HBV-HCV联合疫苗。缺乏慢性HBV或HCV发生与包括酒精,药物滥用,胰岛素抵抗,年龄和性别在内的混杂宿主因素的HLA关联,需要对全球人群进行详细调查。

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