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Emergence of and takeover by hepatitis B virus (HBV) with rearrangements in the pre-S/S and pre-C/C genes during chronic HBV infection.

机译：在慢性HBV感染期间乙型肝炎病毒（HBV）的出现和被乙型肝炎病毒（HBV）接管并且前S / S和前C / C基因重排。

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We have shown, by analyzing serial serum samples from a chronic hepatitis B virus (HBV) carrier, the emergence of HBV DNA molecules with nucleotide rearrangements in the pre-S/S and pre-C/C genes. Serum samples were obtained at four different times (1983, 1985, 1988, and 1989) from an HBsAg- and HBeAg-positive carrier with chronic hepatitis. The polymerase chain reaction was used to amplify the pre-S/S and pre-C/C genes. The amplified products were cloned, and 8 to 10 independent clones were sequenced. In 1983 and 1985 only one type of HBV DNA molecule was observed. Nucleotide divergence relative to the adw2 subtype was 4.7, 7.2, and 1.6%, for the pre-S1, pre-S2, and S regions, respectively, and 2.2 and 3.9% for the pre-C and C regions, respectively. In 1988 and 1989, HBV DNA forms with marked rearrangements of both the pre-S/S and pre-C/C regions were evidenced. In the pre-S/S region, they comprised two distinct HBV DNA molecules. The first showed nucleotide divergence of 20.4, 14.8, and 3.3% for the pre-S1, pre-S2, and S regions when compared with the adw2 sequence. In addition, nucleotide deletions in the pre-S1 region led to the appearance of a stop codon. The second was created by recombination between the original and mutated HBV DNA. In the pre-C/C region, the mutated viral DNA showed 11.7% divergence when compared with the adw2 sequence. A point mutation led to the creation of a stop codon in the pre-C region, together with an insertion of 36 nucleic acids in the core gene. Most of this DNA insertion was identical to that reported in an independent HBV isolate but showed no significant homology with known sequences. Semiquantitative estimation of the proportion of wild-type and mutated HBV DNA molecules showed a marked increase in the mutated forms during the period of follow-up. Sucrose gradient analysis indicated that the defective HBV DNA molecules were present in circulating virions. Western immunoblot analysis showed the appearance of modified translation products. Our findings thus indicate the emergence of and gradual takeover by mutated HBV DNA forms during the HBV chronic carrier state. The rearrangements we observed in the pre-S/S and pre-C/C genes might lead to changes in the immunogenicity of the viral particles and thus affect the clearance of the virus by the immune system.

机译：通过分析来自慢性乙型肝炎病毒（HBV）载体的连续血清样品，我们已经显示了在前S / S和前C / C基因中具有核苷酸重排的HBV DNA分子的出现。在四个不同的时间（1983、1985、1988和1989）从患有慢性肝炎的HBsAg和HBeAg阳性携带者那里获得血清样本。聚合酶链反应用于扩增pre-S / S和pre-C / C基因。克隆扩增产物，并测序8至10个独立克隆。在1983年和1985年，仅观察到一种类型的HBV DNA分子。相对于adw2亚型的核苷酸差异，前S1，前S2和S区分别为4.7％，7.2％和1.6％，而前C和C区分别为2.2％和3.9％。在1988年和1989年，已证明HBV DNA形式在S / S之前和C / C之前的区域均发生了明显的重排。在前S / S区，它们包含两个不同的HBV DNA分子。当与adw2序列比较时，第一个显示出pre-S1，pre-S2和S区域的核苷酸差异分别为20.4、14.8和3.3％。另外，前S1区域中的核苷酸缺失导致终止密码子的出现。第二个是通过原始和突变的HBV DNA重组产生的。在C / C前区，与adw2序列相比，突变的病毒DNA表现出11.7％的差异。点突变导致在前C区中产生终止密码子，并在核心基因中插入了36个核酸。这种DNA插入的大部分与独立HBV分离株报道的相同，但与已知序列没有显着同源性。对野生型和突变HBV DNA分子比例的半定量估计显示，在随访期间，突变形式明显增加。蔗糖梯度分析表明循环病毒粒子中存在缺陷的HBV DNA分子。 Western免疫印迹分析显示修饰的翻译产物的外观。因此，我们的发现表明，在HBV慢性携带者状态期间，突变的HBV DNA形式的出现和逐渐被其接管。我们在前S / S和前C / C基因中观察到的重排可能导致病毒颗粒的免疫原性发生变化，从而影响免疫系统对病毒的清除。

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期刊名称 Journal of Virology
作者
A Tran; D Kremsdorf; F Capel; C Housset; C Dauguet; M A Petit; C Brechot;
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年(卷),期 1991(65),7
年度 1991
页码 3566–3574
总页数 9
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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1. Sequence analysis of pre-S/surface and pre-core/core promoter genes of hepatitis B virus in chronic hepatitis C patients with occult HBV infection. [J] . Kao JH, Chen PJ, Lai MY, Journal of Medical Virology . 2002,第2期

机译：慢性丙型肝炎合并隐匿性HBV感染的乙肝病毒前S /表面和前核心/核心/核心启动子基因的序列分析。
2. Complete genome sequence and phylogenetic analysis of hepatitis B virus (HBV) isolated from Mongolian patients with chronic HBV infection. [J] . Odgerel Z, Choi IK, Byun KS, Virus Genes . 2006,第3期

机译：从蒙古族慢性HBV感染患者中分离出的乙型肝炎病毒（HBV）的完整基因组序列和系统发育分析。
3. Characteristics of Circulating T Cell Receptor gammadelta T Cells from Individuals Chronically Infected with Hepatitis B Virus (HBV): An Association between V(delta)2 Subtype and Chronic HBV Infection. [J] . Chen M, Zhen W, Liu Y, The Journal of Infectious Diseases . 2008,第11期

机译：慢性乙型肝炎病毒（HBV）感染者的循环T细胞受体gammadelta T细胞特征：Vδ2亚型与慢性HBV感染之间的关联。
4. Negative Effect of IFN-onα2b against HBV-DNA in PBMC, Serum and Inducement to CD25 in the Patients with Chronic Hepatitis B [C] . WANG Jian, SUN Lin, XIANG Gui-ju, 2009 IEEE International Symposium on IT in Medicine Education( IEEE 教育与医药信息化国际会议）论文集 . 2009

机译：慢性乙型肝炎患者IFN-α2b对PBMC HBV-DNA，血清和CD25诱导的负面影响
5. Generation, characterization, and use of the HBV baculovirus-HepG2 system: A novel in vitro model system for studying hepatitis B virus. [D] . Delaney, William Ellis, IV. 1998

机译：HBV杆状病毒-HepG2系统的产生，表征和使用：用于研究乙型肝炎病毒的新型体外模型系统。
6. Hepatitis B virus (HBV) sequence variation of cytotoxic T lymphocyte epitopes is not common in patients with chronic HBV infection. [O] . B Rehermann, C Pasquinelli, S M Mosier, 1995

机译：在慢性HBV感染患者中细胞毒性T淋巴细胞表位的乙肝病毒（HBV）序列变异并不常见。
7. Emergence of and takeover by hepatitis B virus (HBV) with rearrangements in the pre-S/S and pre-C/C genes during chronic HBV infection [O] . A Tran, D Kremsdorf, F Capel, 1991

机译：在慢性HBV感染期间，乙型肝炎病毒（HBV）的出现和服用乙型肝炎病毒（HBV）和C / C前C / C基因的重排

Emergence of and takeover by hepatitis B virus (HBV) with rearrangements in the pre-S/S and pre-C/C genes during chronic HBV infection.

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