Increased Virus Replication and Cytotoxicity of Non-pathogenic Simian Human Immuno Deficiency Viruses-NM-3rN After Serial Passage in a Monkey-Derived Cell Line

Increased Virus Replication and Cytotoxicity of Non-pathogenic Simian Human Immuno Deficiency Viruses-NM-3rN After Serial Passage in a Monkey-Derived Cell Line

Background: Infection and disease induction of variants of HIV type 1 (HIV-1) in vivo, especially their persistence, replication and rate of disease progression, have been found to depend on phenotypic characteristics. However, the mechanism (s) underlying these diverse phenotypic characteristics re...

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Bibliographic Details
Published in:Annals of medical and health sciences research Vol. 3; no. 1; pp. 55 - 61
Main Authors: Kwofie, T, Miura, T
Format: Journal Article
Language:English
Published: India Medknow Publications Pvt Ltd 01-01-2013
Medknow Publications and Media Pvt. Ltd
Medknow Publications & Media Pvt Ltd
Subjects:
Analysis
Development and progression
Enzyme-linked immunosorbent assay
Health aspects
Infection
Original
Cell culture
Evolution
Replication
HIV/SIV
Monkey
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Summary:Background: Infection and disease induction of variants of HIV type 1 (HIV-1) in vivo, especially their persistence, replication and rate of disease progression, have been found to depend on phenotypic characteristics. However, the mechanism (s) underlying these diverse phenotypic characteristics remain poorly understood. Aim: It was aimed at determining whether a SHIV that had been adapted to a monkey-derived cell line could be used to explain the mechanism that underlies adaptive evolution of a virus to its host cell environment. Materials and Methods: Standard procedures in virology such as cell culturing, FACS analysis and ELISA were employed to measure virus replication and growth kinetics, cell viability, reverse transcriptase (RT) activity assay and CD4 cells down-regulation. Results: After about 20 passages, LT efficiently adapted to the monkey-derived cell line and replicated much better than the parent virus. LT accumulated a number of mutations in its entire genome with a majority of them being monkey cell-specific. Conclusion: Thus we think we have obtained a virus that may enable studies to determine which of these mutations are specifically related to in vitro viral replication and which are specifically related to cytotoxicity so as to explain the mechanism associated with viral cytotoxicity and host cell specificity.
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ISSN:2141-9248
2277-9205
DOI:10.4103/2141-9248.109490