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黑猩猩8.2年感染丙型肝炎病毒期间的基因漂移:变异性与稳定性

Genetic drift of hepatitis C virus during an 8.2-year infection in a chimpanzee: variability and stability.

作者信息

Okamoto H, Kojima M, Okada S, Yoshizawa H, Iizuka H, Tanaka T, Muchmore E E, Peterson D A, Ito Y, Mishiro S

机构信息

Immunology Division, Jichi Medical School, Tochigi-ken, Japan.

出版信息

Virology. 1992 Oct;190(2):894-9. doi: 10.1016/0042-6822(92)90933-g.

Abstract

Extensive variability in genomic sequence, especially at "hypervariable regions" within the NS1/E2 region of the long open reading frame, has been reported for RNA cloned from hepatitis C virus (HCV)-infected humans and chimpanzees. However, genetic changes of HCV occurring during the course of chronic infections in humans and animals have been evaluated only for partial sequences of the HCV genome. We compared two full-length cDNA sequences of HCV obtained from a chimpanzee that was experimentally infected with the HC-J4 strain of HCV: one during the early acute phase and another during a chronic phase 8.2 years afterward. Both isolates had 9412 nucleotides plus the 3' poly(U) tail with varying length organized as follows: 5'UTR (1-341); C (342-914); E (915-1490); NS1/E2 (1491-2528); NS2 (2529-3359); NS3 (3360-5186); NS4 (5187-6380); NS5 (6381-9371); and 3'UTR (9372-9412). We found that 111 (1.18%) of the 9412 nucleotides differed between the two isolates and estimated the mutation rate as approximately 1.44 x 10(-3) base substitutions per site per year. Changes in amino acid coding were associated with 42 mutations, 8 of which were clustered at 5' end of NS1/E2 coding region, so-called "HVR-1." We analyzed the HVR-1 and HVR-2 sequences during the course of infection and found that homologous populations were present at the beginning of infection, and sequence heterogeneity within the region had developed 3.5 years later. Two regions of the HCV genome were characterized by a high degree of conservation of nucleotide sequence: 5'UTR and the 3' half of the NS4 region. The possible secondary structure of the 5'UTR suggests a region for internal ribosomal entry. The 3' half of the NS4 region may also have some specific function which depends upon a strict conservation of nucleotide sequence.

摘要

据报道,从丙型肝炎病毒(HCV)感染的人类和黑猩猩中克隆的RNA,其基因组序列存在广泛变异,尤其是在长开放阅读框的NS1/E2区域内的“高变区”。然而,仅针对HCV基因组的部分序列评估了人类和动物慢性感染过程中发生的HCV基因变化。我们比较了从一只实验感染HC-J4株HCV的黑猩猩获得的两个HCV全长cDNA序列:一个在急性早期阶段,另一个在8.2年后的慢性期。两个分离株均有9412个核苷酸加上长度各异的3'聚(U)尾,其组织方式如下:5'非翻译区(1-341);C区(342-914);E区(915-1490);NS1/E2区(1491-2528);NS2区(2529-3359);NS3区(3360-5186);NS4区(5187-6380);NS5区(6381-9371);以及3'非翻译区(9372-9412)。我们发现,两个分离株之间的9412个核苷酸中有111个(1.18%)不同,并估计突变率约为每年每个位点1.44×10⁻³个碱基替换。氨基酸编码的变化与42个突变相关,其中8个聚集在NS1/E2编码区的5'端,即所谓的“高变区-1”。我们分析了感染过程中的高变区-1和高变区-2序列,发现感染开始时存在同源群体,该区域内的序列异质性在3.5年后出现。HCV基因组的两个区域具有核苷酸序列高度保守的特征:5'非翻译区和NS4区域的3'半部分。5'非翻译区可能的二级结构提示了一个内部核糖体进入区域。NS4区域的3'半部分可能也有一些特定功能,这取决于核苷酸序列的严格保守。

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