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Characterization of differential antibody production against hepatitis C virus in different HCV infection status

机译:不同HCV感染状态下抗丙型肝炎病毒的差异抗体产生的特征

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Background The Centers for Disease Control and Prevention (CDC) issued an update on hepatitis C virus (HCV) testing approach, in which it omitted the use of recombinant immunoblot assay (RIBA) in the diagnostic algorithm and recommended that future studies are needed to evaluate the performance of HCV testing without RIBA. As Egypt has the highest prevalence of HCV worldwide, we aimed to evaluate the value of RIBA in HCV testing in a high prevalence population. Our objective was to clarify whether enzyme linked immunosorbent assay (ELISA) anti-HCV signal-to-cutoff (S/CO) ratios were able to discriminate true positive from false positive anti-HCV antibody status and to evaluate the role of RIBA in solving this problem which may lead to a redefined strategy for diagnosis of HCV infection. Our second objective was to elucidate the effects of different HCV peptides of both structural and non-structural proteins on the humoral immune response to HCV infection. Methods The current study drew results from 167 individuals divided into three groups: Group I: included 77 HCV antibody positive (ELISA) high risk health care workers (HCW), Group II: included 56 presumably uninfected individuals who showed normal liver enzymes, negative HCV RNA and were asymptomatic. Their ELISA HCV antibody S/C ratio ranged from 0.9 to rd generation ELISA which was confirmed by RIBA. Results Interpreting the results of both ELISA and RIBA together, false positive results were highly significantly increased in HCW when compared with the other two groups. Indeterminate and false negative results were only found in the presumably uninfected group. For differentiated antibody responses by RIBA, chronic HCV cases had the highest frequency of positive antibody response to core peptides while the presumably uninfected group had the lowest. Antibody response to E2 was found less frequently in chronic cases than Core 1, Core 2 and NS3. The specific antibody response to the different HCV peptides showed the same distribution of frequencies in both chronic HCV cases and the presumably uninfected individuals with the chronic cases having the highest frequencies. This distribution was different from the HCW. The most evident difference was the reaction towards NS3 which was the highest antibody producing peptide in chronic HCV and presumably uninfected individuals whereas in HCW Core1 was the highest. Conclusion The HCV antibody immunoblot assay (RIBA) is still necessary for the detection of false positive cases which can occur quite frequently in countries of high prevalence as Egypt. Indeterminate RIBA results indicate a waning antibody response in elderly individuals who recovered from previous or distant HCV infection.
机译:背景疾病控制与预防中心(CDC)发布了有关丙型肝炎病毒(HCV)测试方法的最新信息,该方法在该算法中省略了在诊断算法中使用重组免疫印迹测定(RIBA)的建议,并建议需要进行进一步的研究以评估无需RIBA的HCV测试性能。由于埃及是全世界HCV患病率最高的国家,因此我们旨在评估RIBA在高流行人群HCV检测中的价值。我们的目的是阐明酶联免疫吸附测定(ELISA)抗HCV信号截止(S / CO)比率是否能够区分真阳性与假阳性抗HCV抗体状态,并评估RIBA在解决方案中的作用这个问题可能导致重新定义诊断HCV感染的策略。我们的第二个目标是阐明结构蛋白和非结构蛋白的不同HCV肽对HCV感染的体液免疫反应的影响。方法本研究从167名个人中分为三组:第一组:包括77名HCV抗体阳性(ELISA)高危医护人员(HCW),第二组:包括56名未感染的,肝酶正常,HCV阴性的人RNA和无症状。 ELISA结果表明,HCV抗体的S / C比值在0.9-rdsup ELISA之间。结果ELISA和RIBA的结果一起解释,与其他两组相比,HCW的假阳性结果显着增加。不确定和假阴性结果仅在大概未感染的人群中发现。对于通过RIBA进行的差异化抗体反应,慢性HCV病例对核心肽的阳性抗体反应频率最高,而未感染人群则最低。在慢性病例中发现对E2的抗体应答的频率低于Core 1,Core 2和NS3。对不同HCV肽的特异性抗体反应在慢性HCV病例和可能未感染的慢性病例中发病率最高的个体均显示相同的频率分布。此分布与HCW不同。最明显的差异是对NS3的反应,这是慢性HCV和可能未感染的个体中产生抗体最多的肽,而在HCW Core1中是最高的。结论HCV抗体免疫印迹试验(RIBA)对于检测假阳性病例仍然是必需的,假阳性病例在埃及等高流行国家可能经常发生。不确定的RIBA结果表明,从先前或远处的HCV感染中恢复过来的老年人中抗体反应减弱。

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