Predominant amino acid substitutions in NS5B gene of hepatitis C virus in blood donors and treatment-naïve hepatitis and HIV patients in Nigeria

G. Odaibo, D. Olaleye, Prof. S. S. Taiwo, J. A. Shenge
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Abstract

Background: Hepatitis C virus (HCV) genome undergoes high rate of mutation, which results in generation of genetically diverse HCV isolates. There is paucity of data on mutations in the nonstructural 5b (NS5b) gene of circulating HCV and their implications in the Nigerian population. Here, we identified clinically-important mutations in HCV isolates, which may influence response to therapy and disease prognosis. Methodology: HCV RNA was extracted from a total of 301 blood samples collected from 99 symptomatic treatment-naïve hepatitis patients, 125 HIV-infected individuals and 77 asymptomatic blood donors in Ibadan, Nigeria. The RNA was reverse–transcribed to complimentary DNA and HCV NS5B gene amplified by nested PCR. The amplified products of 42 HCV were sequenced and sequences were aligned with those from GenBank and HCV databases in MEGA 7.0. Nucleotide sequences were translated to amino acids while substitutions in the amino acids were analyzed with reference to H77 prototype strain of HCV. Results: A total of 10 amino acid polymorphisms were observed from the 42 sequenced NS5B gene, with the major clinically-important amino acid mutations being S15G in 28 (66.7%) participants, T7N (24, 57.1%), G61R (23, 54.8%), S54L (22, 52.4%), G89E (14, 33.3%), T79M (12, 28.6%), and T711 (11, 26.2%). Others were Q67R (7, 16.7%), Q47H (7, 16.7%) and S84F (2, 4.8%). S15G/A/V mutations were more predominant in patients with HIV (76.9%, 10/13) followed by patients with clinical hepatitis (75.0%, 12/16) and blood donors (46.1%, 6/13). Q67R and T71I mutations were not predominant in patients with clinical hepatitis as they were detected in only 31.3% (5/16) and 43.8% (7/16) participants respectively, compared to S15G (75.0%, 12/16), S54L (68.8%, 11/16), G61R/E (68.8%, 11/16) and T7N/S (56.3%, 9/16). There was no statistically significant difference in the distribution of each of the 10 amino acid polymorphisms detected within patients with symptomatic clinical hepatitis (x2=9.311, p=0.409), HIV-infected patients (x2=13.431, p=0.1440) and asymp- tomatic blood donors (x2=3.775, p=0.9256). Similarly, there was no significant difference in the distribution between the 3 categories of the study participants except for T79M mutation, which was significantly higher in HIV-infected patients (61.5%, 8/13) compared to patients with clinical hepatitis (18.8%, 3/16) and asymp- tomatic blood donors (7.7%, 1/13) (x2=10.456, p=0.0054). Conclusion: Mutations in the NS5B gene could be associated with worse prognosis of the disease or antiviral failure due to viral resistance in patients undergoing therapy. The absence of Q47H mutations in majority of the study participants in our study implies that they will not respond well to daprevir and mericitabine. Screening of patients for pre-existing resistant mutations before commencement of therapy and monitoring during and after therapy are recommended.
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尼日利亚献血者以及治疗无效的肝炎和艾滋病患者中丙型肝炎病毒 NS5B 基因的主要氨基酸替换
背景:丙型肝炎病毒(HCV)基因组的突变率很高,从而产生了基因多样的 HCV 分离株。有关循环型 HCV 的非结构 5b (NS5b) 基因突变及其对尼日利亚人群的影响的数据很少。在此,我们确定了 HCV 分离物中具有临床重要性的突变,这些突变可能会影响治疗反应和疾病预后。方法:我们从尼日利亚伊巴丹市 99 名无症状、未经治疗的肝炎患者、125 名艾滋病病毒感染者和 77 名无症状献血者的 301 份血液样本中提取了 HCV RNA。RNA 经反向转录后可得到免费 DNA,并通过巢式 PCR 扩增 HCV NS5B 基因。对 42 种 HCV 的扩增产物进行了测序,并在 MEGA 7.0 中与 GenBank 和 HCV 数据库中的序列进行了比对。核苷酸序列被翻译成氨基酸,而氨基酸中的取代则参照 HCV 的 H77 原型菌株进行分析。结果:在 42 个已测序的 NS5B 基因中,共观察到 10 个氨基酸多态性,其中对临床有重要意义的主要氨基酸突变为 S15G(28 人,占 66.7%)、T7N(24 人,占 57.1%)、G61R(23 人,占 54.8%)、S54L(22 人,占 52.4%)、G89E(14 人,占 33.3%)、T79M(12 人,占 28.6%)和 T711(11 人,占 26.2%)。其他还有 Q67R(7 例,占 16.7%)、Q47H(7 例,占 16.7%)和 S84F(2 例,占 4.8%)。S15G/A/V突变主要发生在艾滋病病毒感染者(76.9%,10/13),其次是临床肝炎患者(75.0%,12/16)和献血者(46.1%,6/13)。Q67R和T71I突变在临床肝炎患者中并不占主导地位,因为分别只有31.3%(5/16)和43.8%(7/16)的参与者检测到这两种突变,相比之下,S15G(75.0%,12/16)、S54L(68.8%,11/16)、G61R/E(68.8%,11/16)和T7N/S(56.3%,9/16)在临床肝炎患者中并不占主导地位。在有症状的临床肝炎患者(x2=9.311,p=0.409)、HIV 感染者(x2=13.431,p=0.1440)和非临床献血者(x2=3.775,p=0.9256)中,检测到的 10 种氨基酸多态性的分布差异无统计学意义。同样,除 T79M 突变外,三类研究参与者的分布无明显差异,与临床肝炎患者(18.8%,3/16)和非临床献血者(7.7%,1/13)相比,HIV 感染者(61.5%,8/13)的 T79M 突变明显较高(x2=10.456,p=0.0054)。结论NS5B基因突变可能与疾病预后恶化或正在接受治疗的患者因病毒耐药而导致抗病毒失败有关。在我们的研究中,大多数参与者体内都没有 Q47H 基因突变,这意味着他们对达普瑞韦和美利曲他滨的反应不会很好。建议在开始治疗前筛查患者是否存在耐药突变,并在治疗期间和治疗后进行监测。
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