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DETECTION OF HCV-SPECIFIC IFN-γ RESPONSES IN HCV ANTIBODY AND HCV RNA NEGATIVE INJECTING DRUG USERS

机译:HCV抗体和HCV RNA阴性注射药物使用者中HCV特异性IFN-γ反应的检测

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Background: Detectable HCV-specific cellular immune responses in HCV antibody and RNA negative people who inject drugs (PWID) raise the question of whether some are resistant to HCV infection. Immune responses from people who have been exposed to hepatitis C virus (HCV) and remain anti-HCV negative are of interest for HCV vaccine development, however, limited research addresses this area.Objectives: In a cohort of HCV antibody and RNA negative PWID, we assessed whether the presence of HCV-specific IFN- g responses or genetic associations provide any evidence of protection from HCV infection.Patients and Methods: One hundred and ninety-eight participants were examined longitudinally for clinical, behavioral, social, environmental and genetic characteristics (IFNL3 genotype [formally IL-28B] and HLA type). Sixty-one of the 198 participants were HCV antibody and RNA negative, with 53 able to be examined longitudinally for HCV-specific IFN- g ELISpot T cell responses.Results: Ten of the 53 HCV antibody and RNA negative participants had detectable HCV-specific IFN- g responses at baseline (18%). The magnitude of IFN- g responses averaged 131+/-96 SFC/106 PBMC and the breadth was mean 1+/-1 pool positive. The specificity of responses were mainly directed to E2, NS4b and NS5b. Participants with (10) and without (43) HCV-specific IFN- g responses did not differ in behavioral, clinical or genetic characteristics (P>0.05). There was a larger proportion sharing needles (with 70%, without 49%, P=0.320) and a higher incidence of HCV (with 35.1 per 100 py, 95% CI 14.6, 84.4, without 16.0 per 100 py, 95% CI 7.2, 35.6, P=0.212) in those with IFN- g responses, although not statistically significant. Half the participants with baseline IFN- g responses became HCV RNA positive (5.10), with one of these participants spontaneously clearing HCV. The spontaneous clearer had high magnitude and broad Th1 responses, favorable IFNL3 genotype and favorable HLA types.Conclusions: This study demonstrated the detection of HCV-specific IFN-γ responses in HCV antibody and RNA negative individuals, with a tendency for HCV-specific IFN- g responses to be associated with HCV exposure. The potential role of HCV-specific IFN- g responses in those who remained HCV RNA negative is of value for the development of novel HCV therapeutics.
机译:背景:在注射药物(PWID)的HCV抗体和RNA阴性人群中可检测到的HCV特异性细胞免疫应答提出了一个问题,即某些药物是否对HCV感染具有抗性。接触丙型肝炎病毒(HCV)且仍抗HCV阴性的人的免疫反应是HCV疫苗开发的关注点,但是,针对这一领域的研究有限。目标:在HCV抗体和RNA阴性PWID队列中,我们评估了是否存在HCV特异性IFN-g应答或遗传关联是否提供任何保护免受HCV感染的证据。患者和方法:198名参与者被纵向检查了临床,行为,社会,环境和遗传特征(IFNL3基因型[正式为IL-28B]和HLA类型)。 198名参与者中有61名是HCV抗体和RNA阴性,其中53名能够纵向检查HCV特异性IFN-g ELISpot T细胞反应。结果:53名HCV抗体和RNA阴性参与者中有10名具有可检测到的HCV特异性基线时IFN-g应答(18%)。 IFN-g反应的强度平均为131 +/- 96 SFC / 106 PBMC,广度为平均1 +/- 1池阳性。反应的特异性主要针对E2,NS4b和NS5b。有(10)和没有(43)HCV特异性IFN-g反应的参与者在行为,临床或遗传特征方面没有差异(P> 0.05)。共用针头的比例更大(70%,没有49%,P = 0.320),HCV发生率更高(每100 y 35.1,95%CI 14.6,84.4,每100 py 16.0,95%CI 7.2 (35.6,P = 0.212),但无统计学意义。一半有基线IFN-g应答的受试者变为HCV RNA阳性(5.10),其中一名受试者自发清除HCV。结论:本研究证明在HCV抗体和RNA阴性个体中检测到HCV特异性IFN-γ反应,并具有HCV特异性IFN的趋势。 -与HCV暴露有关的反应。在仍保持HCV RNA阴性的人群中,HCV特异性IFN-g应答的潜在作用对于开发新型HCV治疗剂具有价值。

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