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Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug

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dc.contributor.author Baron, MK
dc.contributor.author Kinsley, N
dc.contributor.author Sewell, BT
dc.contributor.author Jaffer, MA
dc.contributor.author Capovilla, A
dc.contributor.author James, W
dc.contributor.author Khati, M
dc.date.accessioned 2008-12-01T11:06:48Z
dc.date.available 2008-12-01T11:06:48Z
dc.date.issued 2008-11
dc.identifier.citation Baron, MK, Kinsley, N, Sewell, BT et al. 2008. Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug. Science real and relevant: 2nd CSIR Biennial Conference, CSIR International Convention Centre Pretoria, 17 & 18 November 2008, pp 1 en
dc.identifier.uri http://hdl.handle.net/10204/2643
dc.description Science real and relevant: 2nd CSIR Biennial Conference, CSIR International Convention Centre Pretoria, 17 & 18 November 2008, pp 12 en
dc.description.abstract HIV-1 infection and its concomitant disease – Aids, remain major public health problems in southern Africa. While current antiretroviral drugs have prolonged the quality of life for many HIV-positive individuals, they do not eliminate the virus (2, 5). This is compounded by the rapid emergence of drug resistant HIV-1 strains. For these reasons, a search for novel antiretroviral agents with modalities different from those currently in use remains a high priority. As a novel strategy to combat the HIV/Aids epidemic, we have recently discovered and described small nucleic acid ligands called aptamers with antiviral activity (1, 4). These aptamers prevent HIV-1 infection by binding to gp120, which is the viral surface envelope glycoprotein necessary for the earliest stage of infection called entry. In this study we used in silico molecular modelling coupled with biochemical experiments to delineate the interaction of one of the aptamers called B40 and gp120; with a view of using the information to develop the aptamer as a novel HIV-1 entry inhibitor drug en
dc.language.iso en en
dc.publisher CSIR en
dc.subject Molecules en
dc.subject HIV en
dc.subject Aptamer en
dc.subject Drug en
dc.subject HIV/Aids epidemic en
dc.subject HIV-1 entry inhibitor drug en
dc.title Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug en
dc.type Conference Presentation en
dc.identifier.apacitation Baron, M., Kinsley, N., Sewell, B., Jaffer, M., Capovilla, A., James, W., & Khati, M. (2008). Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug. CSIR. http://hdl.handle.net/10204/2643 en_ZA
dc.identifier.chicagocitation Baron, MK, N Kinsley, BT Sewell, MA Jaffer, A Capovilla, W James, and M Khati. "Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug." (2008): http://hdl.handle.net/10204/2643 en_ZA
dc.identifier.vancouvercitation Baron M, Kinsley N, Sewell B, Jaffer M, Capovilla A, James W, et al, Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug; CSIR; 2008. http://hdl.handle.net/10204/2643 . en_ZA
dc.identifier.ris TY - Conference Presentation AU - Baron, MK AU - Kinsley, N AU - Sewell, BT AU - Jaffer, MA AU - Capovilla, A AU - James, W AU - Khati, M AB - HIV-1 infection and its concomitant disease – Aids, remain major public health problems in southern Africa. While current antiretroviral drugs have prolonged the quality of life for many HIV-positive individuals, they do not eliminate the virus (2, 5). This is compounded by the rapid emergence of drug resistant HIV-1 strains. For these reasons, a search for novel antiretroviral agents with modalities different from those currently in use remains a high priority. As a novel strategy to combat the HIV/Aids epidemic, we have recently discovered and described small nucleic acid ligands called aptamers with antiviral activity (1, 4). These aptamers prevent HIV-1 infection by binding to gp120, which is the viral surface envelope glycoprotein necessary for the earliest stage of infection called entry. In this study we used in silico molecular modelling coupled with biochemical experiments to delineate the interaction of one of the aptamers called B40 and gp120; with a view of using the information to develop the aptamer as a novel HIV-1 entry inhibitor drug DA - 2008-11 DB - ResearchSpace DP - CSIR KW - Molecules KW - HIV KW - Aptamer KW - Drug KW - HIV/Aids epidemic KW - HIV-1 entry inhibitor drug LK - https://researchspace.csir.co.za PY - 2008 T1 - Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug TI - Molecular interaction of gp120 and B40 aptamer: A potential new HIV-1 entry inhibitor drug UR - http://hdl.handle.net/10204/2643 ER - en_ZA


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