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优化算法诊断新诊断 HIV 感染患者的慢性乙型肝炎标志物。

Optimization of the algorithm diagnosis chronic hepatitis B markers in patients with newly diagnosed HIV infection.

机构信息

Saint-Petersburg Pasteur Institute.

Saint-Petersburg State Medical University n.a. acad. I.P. Pavlov.

出版信息

Klin Lab Diagn. 2020 Sep 16;65(9):574-579. doi: 10.18821/0869-2084-2020-65-9-574-579.

Abstract

The possibility of modifying the algorithms for chronic viral hepatitis B laboratory diagnosis in individuals with newly diagnosed HIV infection is analyzed. Plasma samples were used from 196 patients residing in the Northwestern Federal District. Serological HBV markers were found in 79.6% of cases. However, HBsAg was detected in 5.6% of patients. Anti-HBcore IgG antibodies are found in 62.24% of cases, anti-HBe IgG antibodies in 27.55%, anti-HBs IgG antibodies in 52.55% of cases. Using a commercial kit with a 100 IU / ml sensitivity, HBV DNA was detected in 4.6% of patients, that is, 81.8% of HBsAg-positive individuals. Using the method developed by us, HBV DNA was found in 18.36% of HIV-infected individuals, including 12.75% of cases was HBsAg-negative (latent) disease form. In the examined group, HBV of genotype D prevailed (91.7%), genotype A was detected in 8.3% of cases. The distribution of subgenotypes is presented in the following ratios: D2 - 55.6%, D1 - 22.2%, D3 - 13.9%, A2 - 8.3%. Mutations were detected in the reverse transcriptase (RT) region in 91.6% of patients, in the SHB region in 83.3%, in the Core and Precore regions in 72.2% and in 27.7% of patients, respectively. Three HBV isolates (8.3%) were identified with drug resistance mutations to lamivudine, entericavir, telbivudine and tenofovir, which are amino acid substitutions in the HBV polymerase gene at positions L180M, T184A, M204V. Vaccine escape mutations were detected in 61.1% of patients. In all samples with drug resistance mutations, escape-mutants were simultaneously present. When analyzing the basal nucleus promoter, Precore and Core regions, 22.2% of patients with the double mutation A1762T / G1764A, 25% with the mutation G1896A were identified. In one person, all three substitutions were found. In the Core region, 77.7% of patients showed mutations in one of the hot spots (codons 87, 97, 112, and 130 substitution), which can play a role in immunomodulation in CHB. Analysis of the HBV genetic structure, mutations detection early in the virus in patients with HBV can help predict the clinical course and disease progression, and ART complications. To reduce the HIV HBV co-infection burden and to appointer anti-HBV therapy, it is necessary to introduce detection the occult HBV to modify the algorithm for CHB laboratory diagnosis.

摘要

分析了为新诊断出 HIV 感染的个体修改慢性乙型肝炎病毒实验室诊断算法的可能性。使用了来自居住在西北联邦区的 196 名患者的血浆样本。在 79.6%的病例中发现了乙型肝炎病毒血清学标志物。然而,仅在 5.6%的患者中检测到 HBsAg。在 62.24%的病例中发现了抗-HBcore IgG 抗体,在 27.55%的病例中发现了抗-HBe IgG 抗体,在 52.55%的病例中发现了抗-HBs IgG 抗体。使用灵敏度为 100 IU/ml 的商业试剂盒,在 4.6%的患者中检测到了 HBV DNA,即 81.8%的 HBsAg 阳性个体。使用我们开发的方法,在 18.36%的 HIV 感染个体中发现了 HBV DNA,其中 12.75%的病例为 HBsAg 阴性(潜伏)疾病形式。在检查的组中,D 型 HBV 占优势(91.7%),A 型在 8.3%的病例中检测到。亚基因型的分布如下:D2-55.6%,D1-22.2%,D3-13.9%,A2-8.3%。在 91.6%的患者中检测到逆转录酶(RT)区域的突变,在 83.3%的患者中检测到 SHB 区域的突变,在 Core 和 Precore 区域的突变分别为 72.2%和 27.7%。在 8.3%的患者中鉴定出三种具有对拉米夫定、恩替卡韦、替比夫定和替诺福韦耐药性的 HBV 分离株,这是 HBV 聚合酶基因中位置 L180M、T184A、M204V 的氨基酸取代。在 61.1%的患者中检测到疫苗逃逸突变。在所有具有耐药突变的样本中,同时存在逃逸突变。在分析基本核启动子、前核心和核心区域时,鉴定出 22.2%的患者同时存在 A1762T/G1764A 双突变,25%的患者存在 G1896A 突变。在 1 名患者中发现了所有三种取代。在核心区域,77.7%的患者显示出一个热点(密码子 87、97、112 和 130 取代)中的一个突变,这可能在乙型肝炎病毒慢性感染的免疫调节中发挥作用。分析乙型肝炎病毒的遗传结构,早期检测病毒中的突变,可以帮助预测乙型肝炎病毒的临床病程和疾病进展以及抗逆转录病毒治疗的并发症。为了降低 HIV 和乙型肝炎病毒合并感染的负担,并制定乙型肝炎病毒的治疗方案,有必要引入乙型肝炎病毒的隐匿性检测,以修改慢性乙型肝炎病毒的实验室诊断算法。

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