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KIR content genotypes associate with carriage of hepatitis B surface antigen, e antigen and HBV viral load in Gambians

机译:KIR含量基因型与冈比亚乙型肝炎表面抗原,e抗原和HBV病毒载量的运输有关

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摘要

Hepatocellular carcinoma (HCC) causes over 800,000 deaths worldwide annually, mainly in low income countries, and incidence is rising rapidly in the developed world with the spread of hepatitis B (HBV) and C (HCV) viruses. Natural Killer (NK) cells protect against viral infections and tumours by killing abnormal cells recognised by Killer-cell Immunoglobulin-like Receptors (KIR). Thus genes and haplotypes encoding these receptors may be important in determining both outcome of initial hepatitis infection and subsequent chronic liver disease and tumour formation. HBV is highly prevalent in The Gambia and the commonest cause of liver disease. The Gambia Liver Cancer Study was a matched case-control study conducted between September 1997 and January 2001 where cases with liver disease were identified in three tertiary referral hospitals and matched with out-patient controls with no clinical evidence of liver disease.We typed 15 KIR genes using the polymerase chain reaction with sequence specific primers (PCR-SSP) in 279 adult Gambians, 136 with liver disease (HCC or Cirrhosis) and 143 matched controls. We investigated effects of KIR genotypes and haplotypes on HBV infection and associations with cirrhosis and HCC.Homozygosity for KIR group A gene-content haplotype was associated with HBsAg carriage (OR 3.7, 95% CI 1.4–10.0) whilst telomeric A genotype (t-AA) was associated with reduced risk of e antigenaemia (OR 0.2, 95% CI 0.0–0.6) and lower viral loads (mean log viral load 5.2 vs. 6.9, pc = 0.022). One novel telomeric B genotype (t-ABx2) containing KIR3DS1 (which is rare in West Africa) was also linked to e antigenaemia (OR 8.8, 95% CI 1.3–60.5). There were no associations with cirrhosis or HCC.Certain KIR profiles may promote clearance of hepatitis B surface antigen whilst others predispose to e antigen carriage and high viral load. Larger studies are necessary to quantify the effects of individual KIR genes, haplotypes and KIR/HLA combinations on long-term viral carriage and risk of liver cancer. KIR status could potentially inform antiviral therapy and identify those at increased risk of complications for enhanced surveillance.
机译:每年在世界范围内,主要是在低收入国家,肝细胞癌(HCC)导致80万例死亡,并且随着乙型肝炎(HBV)和丙型肝炎(HCV)病毒的传播,在发达国家发病率正在迅速上升。天然杀伤(NK)细胞通过杀死被杀伤细胞免疫球蛋白样受体(KIR)识别的异常细胞来保护免受病毒感染和肿瘤侵害。因此,编码这些受体的基因和单倍型在确定最初的肝炎感染以及随后的慢性肝病和肿瘤形成的结果中可能都是重要的。 HBV在冈比亚非常普遍,也是肝病的最常见原因。冈比亚肝癌研究是一项于1997年9月至2001年1月进行的匹配病例对照研究,在三家三级转诊医院中发现了肝病病例,并与无肝病临床证据的门诊患者相匹配。我们输入了15个KIR聚合酶链反应与序列特异性引物(PCR-SSP)在279名成年冈比亚人,136例患有肝病(HCC或肝硬化)和143个匹配对照中发现了这些基因。我们调查了KIR基因型和单倍型对HBV感染的影响以及与肝硬化和HCC的关系。KIR组A基因含量单倍型与HBsAg转运相关(OR 3.7,95%CI 1.4-10.0),而端粒A基因型(t- AA)与降低e抗原血症的风险(OR 0.2,95%CI 0.0–0.6)和降低病毒载量(平均对数病毒载量5.2 vs. 6.9,pc = 0.022)相关。一种含有KIR3DS1的新型端粒B基因型(t-ABx2)(在西非罕见)也与e抗原血症相关(OR 8.8,95%CI 1.3–60.5)。肝硬化或肝癌没有相关性。某些KIR图谱可能会促进乙型肝炎表面抗原的清除,而另一些则倾向于携带e抗原并携带高病毒量。有必要进行更大的研究来量化单个KIR基因,单倍型和KIR / HLA组合对长期病毒携带和肝癌风险的影响。 KIR状况可能会为抗病毒治疗提供信息,并确定并发症风险增加的患者,以加强监测。

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