Cyanovirin-N Inhibits AIDS Virus Infections in Vaginal Transmission Models

Tsai, Che-Chung; Emau, Peter; Jiang, Yuanchun; Agy, Michael B.; Shattock, Robin J.; Schmidt, Ann Marie; Morton, William R.; Gustafson, Kirk R.; Boyd, Michael R.

doi:10.1089/088922204322749459

Cited by 208 publications

(177 citation statements)

References 27 publications

(39 reference statements)

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“…An example of the successful use of an NHP model in HIV prevention is the study of Parikh, et al, which used SHIV SF162P3 and pig-tailed macaques to predict that tenofovir gel could block vaginal HIV transmission as was subsequently determined in the CAPRISA 004 clinical trial (1,38). Yet because many new-generation microbicides being considered contain antiretrovirals that often exhibit exquisite specificity for HIV, multiple SIV/SHIV macaque models need to be developed for efficacy testing in vivo (20,27,28,38,46,50,52). Furthermore, within different NHP models there are differences in viral (i.e., HIV versus SHIV envelope variable region 3) and host (i.e., human versus macaque CCR5) sequences, resulting in distinctions that preclude the use of certain HIV-specific inhibitors and can confound the interpretation of the data obtained (4,33,42,49).…”

Section: Vol 85 2011mentioning

confidence: 99%

One Percent Tenofovir Applied Topically to Humanized BLT Mice and Used According to the CAPRISA 004 Experimental Design Demonstrates Partial Protection from Vaginal HIV Infection, Validating the BLT Model for Evaluation of New Microbicide Candidates

Denton

Othieno

Martinez-Torres

et al. 2011

J Virol

130

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Section: Vol 85 2011mentioning

confidence: 99%

One Percent Tenofovir Applied Topically to Humanized BLT Mice and Used According to the CAPRISA 004 Experimental Design Demonstrates Partial Protection from Vaginal HIV Infection, Validating the BLT Model for Evaluation of New Microbicide Candidates

Denton

Othieno

Martinez-Torres

et al. 2011

J Virol

130

150

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“…Another group of four macaques were not pretreated with DMPA prior to virus challenge. Two macaques in each group were inoculated intravaginally with 500 TCID 50 of RT-SHIV; the remaining two macaques in each group received 1,000 TCID 50 as previously described [13,14]. Briefly, 0.5 ml of virus preparation was atraumatically introduced to the vaginal mucosa using a stainless steel animal feeding tube.…”

Section: Methodsmentioning

confidence: 99%

“…SIVmac239 gag -specific primers were used to amplify virus DNA by PCR as described previously [13,14,46]. …”

Section: Methodsmentioning

confidence: 99%

RT-SHIV, an infectious CCR5-tropic chimeric virus suitable for evaluating HIV reverse transcriptase inhibitors in macaque models

et al. 2009

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BackgroundNon-nucleoside reverse transcriptase inhibitors (NNRTIs) are an important category of drugs for both chemotherapy and prevention of human immunodeficiency virus type 1 (HIV-1) infection. However, current non-human primate (NHP) models utilizing simian immunodeficiency virus (SIV) or commonly used chimeric SHIV (SIV expressing HIV-1 envelope) are inadequate due to the insensitivity to NNRTIs. To develop a NHP model for evaluation of NNRTI compounds, we characterized a RT-SHIV virus that was assembled by replacing the SIVmac239 reverse transcriptase (RT) with that of HIV-1HXB2. Since RT-SHIV exhibited in vitro characteristics of high infectivity, CCR5-usage, and sensitivity to HIV-1 specific NNRTIs, this virus was thought to be suitable for mucosal transmission and then was used to carry out a vaginal transmission study in pigtail macaques (Macaca nemestrina).ResultsRT-SHIV exhibited in vitro characteristics of an infectious CCR5-tropic chimeric virus. This virus was not only highly sensitive to HIV-1 RT specific NNRTIs; its replication was also inhibited by a variety of NRTIs and protease inhibitors. For in vivo vaginal transmission studies, macaques were either pretreated with a single dose of DMPA (depot medroxyprogesterone acetate) or left untreated before intravaginal inoculation with 500 or 1,000 TCID50 of RT-SHIV. All macaques became systemically infected by 2 or 3 weeks post-inoculation exhibiting persistent high viremia, marked CD4+T cell depletion, and antiviral antibody response. DMPA-pretreated macaques showed a higher mean plasma viral load after the acute infection stage, highly variable antiviral antibody response, and a higher incidence of AIDS-like disease as compared with macaques without DMPA pretreatment.ConclusionThis chimeric RT-SHIV has exhibited productive replication in both macaque and human PBMCs, predominantly CCR5-coreceptor usage for viral entry, and sensitivity to NNRTIs as well as other anti-HIV compounds. This study demonstrates rapid systemic infection in macaques following intravaginal exposure to RT-SHIV. This RT-SHIV/macaque model could be useful for evaluation of NNRTI-based therapies, microbicides, or other preventive strategies.

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“…This binding then inhibits the conformational change required for virus-target cell attachment and subsequent fusion. Previous in vivo studies, with CV-N formulated as a gel, have shown promising efficacy when the compound was used topically as a rectal or vaginal microbicide in macaques challenged with the highly pathogenic SHIV89.6P virus (Tsai et al, 2003(Tsai et al, , 2004.…”

Section: Introductionmentioning

confidence: 99%

“…These studies expand and build on our early demonstration of compound efficacy in tissue and animal models (Tsai et al, 2004). In this study, we have evaluated multiple aspects of CV-N activity including: the ability to block cell-free and cell-to-cell HIV-1 transmission; its activity in the presence of semen; efficacy in the presence of Candida albicans; and activity in human cervical explant cultures (Fletcher et al, 2005;Greenhead et al, 2000;Hu et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

Cyanovirin-N potently inhibits human immunodeficiency virus type 1 infection in cellular and cervical explant models

Buffa

Stieh

Mamhood

et al. 2009

Journal of General Virology

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Cyanovirin-N Inhibits AIDS Virus Infections in Vaginal Transmission Models

Cited by 208 publications

References 27 publications

One Percent Tenofovir Applied Topically to Humanized BLT Mice and Used According to the CAPRISA 004 Experimental Design Demonstrates Partial Protection from Vaginal HIV Infection, Validating the BLT Model for Evaluation of New Microbicide Candidates

One Percent Tenofovir Applied Topically to Humanized BLT Mice and Used According to the CAPRISA 004 Experimental Design Demonstrates Partial Protection from Vaginal HIV Infection, Validating the BLT Model for Evaluation of New Microbicide Candidates

RT-SHIV, an infectious CCR5-tropic chimeric virus suitable for evaluating HIV reverse transcriptase inhibitors in macaque models

Cyanovirin-N potently inhibits human immunodeficiency virus type 1 infection in cellular and cervical explant models

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