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Analysis of carriers of hepatitis B virus from a tertiary referral hospital: does the viral load change during the natural course of infection?

机译:三级转诊医院的乙肝病毒携带者分析:在自然感染过程中病毒载量是否发生变化?

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This study was designed to determine the prevalence, forms of transmission, mutational profile and viral load at baseline of hepatitis B virus (HBV) carriers in Delhi. HBV surface antigen (HBsAg)-positive patients were enrolled and evaluated clinically for liver function, serological markers for hepatitis B and HBV DNA quantitation. Tests were carried out again 1 year later and the results were compared. Liver biopsy was carried out on all carriers with active viral replication. HBV DNA-positive samples were subjected to polymerase chain reaction single-stranded conformation polymorphism (PCR-SSCP) to screen mutations in the Precore, core, and the X-gene prior to sequencing analysis. Among the 100 patients examined, HBeAg was detected in 23% and 40% were HBV DNA-positive. Of the 40 HBV DNA-positive cases, 8 had precore/core mutations, [G1896A (10%), T2066A (12.5%), T2050C (10%), and G1888A (7.5%)]. No X gene mutants were detected. Reduction in viral load was higher in HBeAg-positive patients, as compared to HBeAg-negative patients, over 1 year. At follow-up, 2/8 HBV mutants corresponded with altered liver function and morphological changes suggestive of chronic hepatitis. One patient was re-designated as DNA-negative on follow-up and had wild-type virus infection with a relatively low viral load. The predominant route for HBV transmission was determined to be parenteral. Twenty percent of the HBV carriers were infected with precore and core mutant HBV. Although the clinical and biochemical profiles of these HBV carriers remained largely stable on follow-up, there was evidence of spontaneous reduction in the mean viral load over the 1-year study period.
机译:本研究旨在确定德里的乙型肝炎病毒(HBV)携带者基线时的患病率,传播形式,突变谱和病毒载量。招募了HBV表面抗原(HBsAg)阳性的患者,并对其肝功能,乙型肝炎的血清学标志物和HBV DNA定量进行了临床评估。一年后再次进行测试,并比较结果。对所有具有活跃病毒复制的载体进行肝活检。在测序分析之前,对HBV DNA阳性样品进行聚合酶链反应单链构象多态性(PCR-SSCP),以筛选Precore,核心和X基因中的突变。在接受检查的100例患者中,HBeAg检出率为23%,HBV DNA阳性检出率为40%。在40例HBV DNA阳性病例中,有8例发生了前核/核心突变,[G1896A(10%),T2066A(12.5%),T2050C(10%)和G1888A(7.5%)]。没有检测到X基因突变体。与HBeAg阴性患者相比,HBeAg阳性患者的病毒载量减少超过一年。在随访中,有2/8 HBV突变体与肝功能改变和形态变化有关,提示慢性肝炎。一名患者在随访中被重新指定为DNA阴性,并且感染了野生型病毒,病毒载量相对较低。 HBV传播的主要途径被确定为肠胃外。百分之二十的HBV携带者感染了前核心和核心突变体HBV。尽管这些HBV携带者的临床和生化特征在随访中基本保持稳定,但有证据表明在1年的研究期内平均病毒载量自发减少。

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