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Literature DB >> 9261369

Identification of GB virus C variants by phylogenetic analysis of 5'-untranslated and coding region sequences.

A S Muerhoff¹, D B Smith, T P Leary, J C Erker, S M Desai, I K Mushahwar.

Abstract

Phylogenetic analysis of 44 GB virus C (GBV-C) 5'-untranslated region (5'-UTR) sequences from 37 individuals suggested the presence of GBV-C genotypes (A. S. Muerhoff, J. N. Simons, T. P. Leary, J. C. Erker, M. L. Chalmers, T. J. Pilot-Matias, G. J. Dawson, S. M. Desai, and I. K. Mushahwar, J. Hepatol. 25:379-384, 1996) that correlated with geographic origin: type 1, 2a and 2b, and 3 isolates are found predominantly in West Africa, the United States and Europe, and Japan, respectively. We have extended our analysis to include 5'-UTR sequences from 129 globally distributed GBV-C isolates and sequences from the second envelope protein (E2) gene and nonstructural (NS) regions 3 and 5b from a subset of these isolates. Bootstrap analysis of a 157-nucleotide segment of the 5'-UTR from 129 sequences provided weak support for the existence of the four major groups of GBV-C isolates previously described, although phylogenetic analysis of a 374-nucleotide segment of the 5'-UTR from 83 isolates provided stronger support. Thus, the groups of GBV-C variants previously identified upon analysis of the entire 5'-UTR can be distinguished by analysis of the shorter, 374-nucleotide region from the 5'-UTR. In contrast, independent analysis of the E2, NS3, or NS5b region sequences does not identify groups of GBV-C variants that correlate with geographic origin. However, bootstrap analysis of these coding sequences, when linked to form colinear sequences, demonstrates that longer coding regions can produce GBV-C groupings that are similar to that determined from 5'-UTR sequence analysis. The inability to distinguish between GBV-C variants by using small segments of coding sequence suggests that the GBV-C genome is constrained. As a result of these constraints, there is a high degree of nucleotide and amino acid sequence conservation between isolates from widely separated geographic areas. Hence, substitutions at many nucleotide positions are not tolerated, so that substitutions at the positions which can change are saturated, thereby obscuring the evolutionary relationships.

Entities: Disease Species

Mesh：

Substances：
DNA, Viral

Year: 1997 PMID： 9261369 PMCID： PMC191925

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

33 in total

1. Consensus oligonucleotide primers for the detection of GB virus C in human cryptogenic hepatitis.

Authors: T P Leary; A S Muerhoff; J N Simons; T J Pilot-Matias; J C Erker; M L Chalmers; G G Schlauder; G J Dawson; S M Desai; I K Mushahwar
Journal: J Virol Methods Date: 1996-01 Impact factor: 2.014

2. Phylogenetic analysis of GB virus C: comparison of isolates from Africa, North America, and Taiwan.

Authors: J H Kao; P J Chen; S C Hsiang; W Chen; D S Chen
Journal: J Infect Dis Date: 1996-08 Impact factor: 5.226

3. Translation initiation in GB viruses A and C: evidence for internal ribosome entry and implications for genome organization.

Authors: J N Simons; S M Desai; D E Schultz; S M Lemon; I K Mushahwar
Journal: J Virol Date: 1996-09 Impact factor: 5.103

4. Mechanism of vertical transmission of hepatitis G.

Authors: H H Lin; J H Kao; P J Chen; D S Chen
Journal: Lancet Date: 1996-04-20 Impact factor: 79.321

5. Vertical transmission of hepatitis G.

Authors: H H Feucht; B Zollner; S Polywka; R Laufs
Journal: Lancet Date: 1996-03-02 Impact factor: 79.321

6. Nucleotide sequence of the 5' noncoding region of hepatitis G virus isolated from Japanese patients: comparison with reported isolates.

Authors: S Fukushi; C Kurihara; N Ishiyama; H Okamura; F B Hoshino; A Oya; K Katayama
Journal: Biochem Biophys Res Commun Date: 1996-09-13 Impact factor: 3.575

7. Infection with GB virus C (GBV-C) in patients with chronic liver disease or on maintenance hemodialysis in Indonesia.

Authors: F Tsuda; S Hadiwandowo; N Sawada; M Fukuda; T Tanaka; H Okamoto; Y Miyakawa; M Mayumi
Journal: J Med Virol Date: 1996-07 Impact factor: 2.327

8. Sequence and genomic organization of GBV-C: a novel member of the flaviviridae associated with human non-A-E hepatitis.

Authors: T P Leary; A S Muerhoff; J N Simons; T J Pilot-Matias; J C Erker; M L Chalmers; G G Schlauder; G J Dawson; S M Desai; I K Mushahwar
Journal: J Med Virol Date: 1996-01 Impact factor: 2.327

9. Isolation of novel virus-like sequences associated with human hepatitis.

Authors: J N Simons; T P Leary; G J Dawson; T J Pilot-Matias; A S Muerhoff; G G Schlauder; S M Desai; I K Mushahwar
Journal: Nat Med Date: 1995-06 Impact factor: 53.440

10. Molecular cloning and disease association of hepatitis G virus: a transfusion-transmissible agent.

Authors: J Linnen; J Wages; Z Y Zhang-Keck; K E Fry; K Z Krawczynski; H Alter; E Koonin; M Gallagher; M Alter; S Hadziyannis; P Karayiannis; K Fung; Y Nakatsuji; J W Shih; L Young; M Piatak; C Hoover; J Fernandez; S Chen; J C Zou; T Morris; K C Hyams; S Ismay; J D Lifson; G Hess; S K Foung; H Thomas; D Bradley; H Margolis; J P Kim
Journal: Science Date: 1996-01-26 Impact factor: 47.728

21 in total

1. GB virus C/hepatitis G virus groups and subgroups: classification by a restriction fragment length polymorphism method based on phylogenetic analysis of the 5' untranslated region.

Authors: J F Quarleri; V L Mathet; M Feld; D Ferrario; M P della Latta; R Verdun; D O Sánchez; J R Oubiña
Journal: J Clin Microbiol Date: 1999-05 Impact factor: 5.948

2. A high frequency of GBV-C/HGV coinfection in hepatitis C patients in Germany.

Authors: Jie Yan; Reinhard H Dennin
Journal: World J Gastroenterol Date: 2000-12 Impact factor: 5.742

3. Prevalence of GB virus C/Hepatitis G virus infection among various populations in Surabaya, Indonesia, and identification of novel groups of sequence variants.

Authors: R Handajani; M I Lusida; P Suryohudoyo; P Adi; P B Setiawan; C A Nidom; R Soemarto; Y Katayama; M Fujii; H Hotta
Journal: J Clin Microbiol Date: 2000-02 Impact factor: 5.948

Identification of GB virus C variants by phylogenetic analysis of 5'-untranslated and coding region sequences.

1. Consensus oligonucleotide primers for the detection of GB virus C in human cryptogenic hepatitis.

2. Phylogenetic analysis of GB virus C: comparison of isolates from Africa, North America, and Taiwan.

3. Translation initiation in GB viruses A and C: evidence for internal ribosome entry and implications for genome organization.

4. Mechanism of vertical transmission of hepatitis G.

5. Vertical transmission of hepatitis G.

6. Nucleotide sequence of the 5' noncoding region of hepatitis G virus isolated from Japanese patients: comparison with reported isolates.

7. Infection with GB virus C (GBV-C) in patients with chronic liver disease or on maintenance hemodialysis in Indonesia.

8. Sequence and genomic organization of GBV-C: a novel member of the flaviviridae associated with human non-A-E hepatitis.

9. Isolation of novel virus-like sequences associated with human hepatitis.

10. Molecular cloning and disease association of hepatitis G virus: a transfusion-transmissible agent.

1. GB virus C/hepatitis G virus groups and subgroups: classification by a restriction fragment length polymorphism method based on phylogenetic analysis of the 5' untranslated region.

2. A high frequency of GBV-C/HGV coinfection in hepatitis C patients in Germany.

3. Prevalence of GB virus C/Hepatitis G virus infection among various populations in Surabaya, Indonesia, and identification of novel groups of sequence variants.

4. Sequence heterogeneity of TT virus and closely related viruses.

5. Large scale screening of human sera for HCV RNA and GBV-C RNA.

6. Hepatitis G virus infection in Amerindians and other Venezuelan high-risk groups.

7. High prevalence of GB virus C in Brazil and molecular evidence for intrafamilial transmission.

8. Structural constraints on RNA virus evolution.

9. Identification of a novel genotype of hepatitis G virus in Southeast Asia.

10. Diversity of hepatitis G virus within a single infected individual.