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一名慢性感染患者中前核心突变型乙型肝炎病毒的潜伏与再激活

Latency and reactivation of a precore mutant hepatitis B virus in a chronically infected patient.

作者信息

Raimondo G, Stemler M, Schneider R, Wildner G, Squadrito G, Will H

机构信息

Max-Planck-Institut für Biochemie, Martinsried, Federal Republic of Germany.

出版信息

J Hepatol. 1990 Nov;11(3):374-80. doi: 10.1016/0168-8278(90)90224-f.

Abstract

In human patients infected with hepatitis B virus (HBV) seroconversion from HBe to anti-HBe often signals virus elimination. Occasionally, a second viremic phase is observed which may be due to superinfection with a variant or reactivation of a latent virus. To differentiate between these two possibilities we investigated the nucleotide sequences of virus populations from sera of a chronically infected patient who had two distinct viremic phases, one e-antigen positive and one anti-HBe antibody positive. By direct sequencing of amplified HBV C- and pre-S gene sequences we found that the viruses in the two populations differed by only two point mutations, one of which prevents expression of precore derived e-antigen. In the nonviremic phase viral DNA and antigen were found in the liver but nucleocapsid protein expression appeared drastically downregulated. These data demonstrate that HBV can enter a latent phase with low expression of core protein and selection for HBV variants which cannot synthesize e-antigen. This suggests that e-antigen expression can be a critical target for virus elimination and that loss of its expression can prolong chronicity and provoke latency of HBV infection.

摘要

在感染乙型肝炎病毒(HBV)的人类患者中,从HBe到抗-HBe的血清学转换通常标志着病毒清除。偶尔会观察到第二个病毒血症期,这可能是由于变异株的重叠感染或潜伏病毒的重新激活所致。为了区分这两种可能性,我们研究了一名慢性感染患者血清中病毒群体的核苷酸序列,该患者有两个不同的病毒血症期,一个是e抗原阳性,另一个是抗-HBe抗体阳性。通过对扩增的HBV C基因和前S基因序列进行直接测序,我们发现这两个群体中的病毒仅存在两个点突变差异,其中一个突变阻止了前核心衍生的e抗原的表达。在非病毒血症期,在肝脏中发现了病毒DNA和抗原,但核衣壳蛋白表达明显下调。这些数据表明,HBV可以进入核心蛋白低表达的潜伏阶段,并选择不能合成e抗原的HBV变异株。这表明e抗原表达可能是病毒清除的关键靶点,其表达缺失可延长慢性期并引发HBV感染的潜伏。

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