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962 results on '"Plummer, Francis A."'

201. A novel HIV vaccine targeting the protease cleavage sites.

Author

Hongzhao Li, Omange, Robert W., Plummer, Francis A., and Ma Luo

Subjects
SEX work, AIDS vaccines, BIOLOGICAL models, IMMUNITY, MOLECULAR structure, PROTEOLYTIC enzymes, T cells
Abstract

HIV preferentially infects activated CD4+ T cells and mutates rapidly. The classical vaccine approach aimed to generate broad immune responses to full HIV proteins largely failed to address the potential adverse impact of increased number of activated CD4+ T cells as viral targets. Learning from natural immunity observed in a group of HIV resistant Kenyan female sex workers, we are testing a novel vaccine approach. It focuses immune response to the highly conserved sequences surrounding the HIV protease cleavage sites (PCS) to disrupt viral maturation, while limiting excessive immune activation. Our pilot studies using nonhuman primate SIV infection models suggest that this approach is feasible and promising. [ABSTRACT FROM AUTHOR]

Published
2017
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206. Systematic Analysis of HIV-1 Env Epitopes of Two HLA Class I Alleles Associate with Different Rates of HIV Infection in the Pumwani Sex Worker Cohort

Author

Richmond, Meika EI, primary, Daniuk, Christina A., additional, Capina, Rupert E., additional, Kimani, Joshua, additional, Wachihi, Charles, additional, Kimani, Makubo, additional, Bielawny, Thomas, additional, Mendoza, Mark G., additional, Ball, T. Blake, additional, Plummer, Francis A., additional, and Luo, Ma, additional

Published
2014
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207. Longitudinal Analysis of SIVmac239 Mutations around the 12 Protease Cleavage Sites and their Correlations with Viral Load Reduction and CD4 counts

Author

Luo, Ma, primary, Tang, David, additional, La, David, additional, Capina, Rupert, additional, Yuan, Xin-Yang, additional, Correia-Pinto, Jorge, additional, Prego, Cecilia, additional, Alonso, Maria, additional, Barry, Christina, additional, Pilon, Richard, additional, Daniuk, Christina, additional, Nykoluk, Mikaela, additional, Pillet, Stephane, additional, Bielawny, Tomasz, additional, Tuff, Jeffrey, additional, Czarnecki, Chris, additional, Lacap, Philip, additional, Wong, Gary, additional, Tyler, Shaun, additional, Liang, Ben, additional, Yuan, Zhe, additional, Li, Qingsheng, additional, Ball, Terry Blake, additional, Sandstrom, Paul, additional, Kobinger, Gary, additional, and Plummer, Francis, additional

Published
2014
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209. Sequences Surrounding the 12 Protease Cleavage Sites are Good Targets for Both Prophylactic and Therapeutic HIV Vaccines

Author

Tang, David, primary, La, David, additional, Capina, Rupert, additional, Yuan, Xin-Yang, additional, Correia-Pinto, Jorge, additional, Prego, Cecilia, additional, Alonso, Maria, additional, Barry, Christina, additional, Pilon, Richard, additional, Daniuk, Christina, additional, Nykoluk, Mikaela, additional, Pillet, Stephane, additional, Bielawny, Tomasz, additional, Tuff, Jeffrey, additional, Czarnecki, Chris, additional, Lacap, Philip, additional, Wong, Gary, additional, Tyler, Shaun, additional, Liang, Ben, additional, Yuan, Zhe, additional, Li, Qingsheng, additional, Ball, Terry Blake, additional, Sandstrom, Paul, additional, Kobinger, Gary, additional, Plummer, Francis, additional, and Luo, Ma, additional

Published
2014
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213. The frequencies of naturally occurring protease inhibitor resistance mutations in HIV proviral sequences of drug naïve sex workers in Nairobi, Kenya and their correlation with host immune response driven positively selected mutations in HIV-1

Author

Sampathkumar, Raghavan, primary, Shadabi, Elnaz, additional, La, David, additional, Ho, John, additional, Liang, Binhua, additional, Kimani, Joshua, additional, Plummer, Francis A, additional, and Luo, Ma, additional

Published
2014
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214. Presence of CD8+ T Cells in the Ectocervical Mucosa Correlates with Genital Viral Shedding in HIV-Infected Women despite a Low Prevalence of HIV RNA–Expressing Cells in the Tissue

Author

Gibbs, Anna, primary, Hirbod, Taha, additional, Li, Qingsheng, additional, Bohman, Karin, additional, Ball, Terry B., additional, Plummer, Francis A., additional, Kaul, Rupert, additional, Kimani, Joshua, additional, Broliden, Kristina, additional, and Tjernlund, Annelie, additional

Published
2014
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217. Diversity and Frequencies of HLA Class I and Class II Genes of an East African Population

Author

Peterson, Trevor A., primary, Bielawny, Thomas, additional, Lacap, Philip, additional, Hardie, Rae-Anne, additional, Daniuk, Christina, additional, Mendoza, Lillian, additional, Thavaneswaran, Subotheni, additional, Kariri, Tony, additional, Kimani, Joshua, additional, Wachihi, Charles, additional, Kimani, Maboku, additional, Ball, Terry Blake, additional, Plummer, Francis A., additional, and Luo, Ma, additional

Published
2014
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218. Female to male transmission of human immunodeficiency virus type 1: risk factors for seroconversion in men

Author

Cameron, D. William, D'Costa, Lourdes J., Maitha, Gregory M., Cheang, Mary, Piot, Peter, Plummer, Francis A., Simonsen, J. Neil, Ronald, Allan R., Gakinya, Michael N., Ndinya-Achola, J.O., and Brunham, Robert C.

Subjects
AIDS virus carriers -- Health aspects, Circumcision -- Health aspects, Genitourinary organs, HIV (Viruses), AIDS (Disease) -- Demographic aspects, Sexually transmitted diseases -- Complications, Nairobi, Kenya -- Health aspects
Published
1989

219. Human immunodeficiency virus infection among men with sexually transmitted diseases; experience from a center in Africa

Author

Simonsen, J. Neil, Cameron, William, Gakinya, Michael N., Ndinya-Achola, Jackoniah O., D'Costa, Lourdes J., Karasira, Peter, Cheang, Mary, Ronald, Allan R., Piot, Peter, and Plummer, Francis A.

Subjects
Heterosexuals -- Sexual behavior, Sexually transmitted diseases -- Case studies, Regression analysis -- Usage, Reproductive organs, AIDS (Disease) -- Demographic aspects, HIV (Viruses)
Published
1988

221. Association study of common genetic variants and HIV-1 acquisition in 6,300 infected cases and 7,200 controls

Author

McLaren, Paul J, Coulonges, Cédric, Ripke, Stephan, van den Berg, Leonard, Buchbinder, Susan, Carrington, Mary, Cossarizza, Andrea, Dalmau, Judith, Deeks, Steven G, Delaneau, Olivier, De Luca, Andrea, Goedert, James J, Haas, David, Herbeck, Joshua T, Kathiresan, Sekar, Kirk, Gregory D, Lambotte, Olivier, Luo, Ma, Mallal, Simon, van Manen, Daniëlle, Martinez-Picado, Javier, Meyer, Laurence, Miro, José M, Mullins, James I, Obel, Niels, O'Brien, Stephen J, Pereyra, Florencia, Plummer, Francis A, Poli, Guido, Qi, Ying, Rucart, Pierre, Sandhu, Manj S, Shea, Patrick R, Schuitemaker, Hanneke, Theodorou, Ioannis, Vannberg, Fredrik, Veldink, Jan, Walker, Bruce D, Weintrob, Amy, Winkler, Cheryl A, Wolinsky, Steven, Telenti, Amalio, Goldstein, David B, de Bakker, Paul I W, Zagury, Jean-François, Fellay, Jacques, McLaren, Paul J, Coulonges, Cédric, Ripke, Stephan, van den Berg, Leonard, Buchbinder, Susan, Carrington, Mary, Cossarizza, Andrea, Dalmau, Judith, Deeks, Steven G, Delaneau, Olivier, De Luca, Andrea, Goedert, James J, Haas, David, Herbeck, Joshua T, Kathiresan, Sekar, Kirk, Gregory D, Lambotte, Olivier, Luo, Ma, Mallal, Simon, van Manen, Daniëlle, Martinez-Picado, Javier, Meyer, Laurence, Miro, José M, Mullins, James I, Obel, Niels, O'Brien, Stephen J, Pereyra, Florencia, Plummer, Francis A, Poli, Guido, Qi, Ying, Rucart, Pierre, Sandhu, Manj S, Shea, Patrick R, Schuitemaker, Hanneke, Theodorou, Ioannis, Vannberg, Fredrik, Veldink, Jan, Walker, Bruce D, Weintrob, Amy, Winkler, Cheryl A, Wolinsky, Steven, Telenti, Amalio, Goldstein, David B, de Bakker, Paul I W, Zagury, Jean-François, and Fellay, Jacques

Published
2013

222. From bench to almost bedside: the long road to a licensed Ebola virus vaccine

Author

Wong, Gary, Mendoza, Emelissa J., Plummer, Francis A., Gao, George F., Kobinger, Gary P., and Qiu, Xiangguo

Abstract

ABSTRACTIntroduction: The Ebola virus (EBOV) disease epidemic during 2014–16 in West Africa has accelerated the clinical development of several vaccine candidates that have demonstrated efficacy in the gold standard nonhuman primate (NHP) model, namely cynomolgus macaques.Areas covered: This review discusses the pre-clinical research and if available, clinical evaluation of the currently available EBOV vaccine candidates, while emphasizing the translatability of pre-clinical data generated in the NHP model to clinical data in humans.Expert opinion: Despite the existence of many successful EBOV vaccine candidates in the pre-clinical stages, only two platforms became the focus of Phase 2/3 efficacy trials in Liberia, Sierra Leone, and Guinea near the peak of the epidemic: the Vesicular stomatitis virus (VSV)-vectored vaccine and the chimpanzee adenovirus type 3 (ChAd3)-vectored vaccine. The results of three distinct clinical trials involving these candidates may soon pave the way for a licensed, safe and efficacious EBOV vaccine to help combat future epidemics.

Published
2018
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223. The mapping and characterization of a novel binding site on HIV-1 gp120 for the broadly neutralizing monoclonal antibody IgG1 b12

Author

Fowke, Keith (Medical Microbiology) Berry, Jody (Medical Microbiology) Coombs, Kevin (Medical Microbiology) Wilkins, John (Internal Medicine) Shattock, Robin (Cell and Molecular Infection), Plummer, Francis (Medical Microbiology), Waruk, Jillian, Fowke, Keith (Medical Microbiology) Berry, Jody (Medical Microbiology) Coombs, Kevin (Medical Microbiology) Wilkins, John (Internal Medicine) Shattock, Robin (Cell and Molecular Infection), Plummer, Francis (Medical Microbiology), and Waruk, Jillian

Abstract

HIV infects target cells via fusion events following surface envelope glycoprotein binding to the CD4 receptor and a chemokine co-receptor. Despite the high sequence variability of envelope across and within HIV-1 subtypes, this process requires conserved sequences and structures on gp120, which also represent good targets for HIV-1 neutralizing antibodies. Few examples of HIV-1 broadly neutralizing antibodies exist, but these antibodies may hold the key to a protective HIV-1 vaccine. One such antibody, IgG1 b12 (b12), binds the CD4 binding site on the HIV-1 envelope glycoprotein gp120. To date, no vaccine preparations have been able to elicit a b12-like response. A complete understanding of the mechanism of b12 binding to gp120 is essential to successful design of an b12-like immune response. Until now, strategies to map the b12 binding site on gp120 have utilized indirect techniques and/or core gp120 and have shown that b12 binds to a site on gp120 that overlaps the CD4 binding site. To more directly map the b12 epitope on intact gp120, epitope excision mass spectrometry mapping was carried out in the MALDI QqTOF platform. The putative epitope sequence was confirmed by tandem mass spectrometry sequencing. Epitope mapping revealed a novel binding site for IgG1 b12 at the gp120 amino terminus called Nterm. b12 bound a synthesized peptide of the epitope and the nature of the epitope was explored by ELISA. Although the Nterm epitope is involved in b12-gp120 interactions, ELISAs also show that the epitope does not make up the entire binding site on gp120. Rabbits immunized with a peptide version of the Nterm epitope do express antibodies that bind monomeric gp120, but these antibody responses do not neutralize HIV-1 in vitro. These data indicate that the b12 binding site on gp120 is much more complex than previously thought. The b12 binds the Nterm sequence of gp120, perhaps in conjunction with the CD4 binding site. It has been shown that another HIV-1-neutralizing ant

Published
2011

224. Role of polyfunctional and proliferative CD8+ T cell responses in HIV-1 infection

Author

Fowke, Keith (Medical Microbiology) Uzonna, Jude (Immunology) Ho, Emmanuel (Pharmacy) Grant, Micheal (Memorial University), Ball, Blake (Medical Microbiology) Plummer, Francis A (Medical Microbiology), Richmond, Meika, Fowke, Keith (Medical Microbiology) Uzonna, Jude (Immunology) Ho, Emmanuel (Pharmacy) Grant, Micheal (Memorial University), Ball, Blake (Medical Microbiology) Plummer, Francis A (Medical Microbiology), and Richmond, Meika

Abstract

The limited success of HIV vaccine candidates to date highlights our need to better characterize protective cell-mediated immunity. Understanding correlates CD8+ T cell protection against HIV infection and progressive disease is essential for informing effective vaccine development, design and evaluation. CD8+ T cell responses with a robust polyfunctional and proliferative component are strongly linked to better disease outcomes. However, the specificity of polyfunctional and proliferative CD8+ T cell responses has not been thoroughly investigated. Additionally, the specificity of memory subsets and their connection to polyfunctionality and proliferation responses has not been adequately assessed. We address these gaps in knowledge and provide a better understanding of the fine specificity of HIV-specific CD8+ T cell responses. We hypothesize that the epitopes recognized by central memory (TCM) and effector memory (TEM) CD8+ T cells, defined by functional attributes, differ in chronic HIV-1 infection. Additionally, we hypothesize that polyfunctional and proliferative responses will better correlate with protection in HIV disease progression. The qualities of CD8+ T cell responses were evaluated using polyfunctional flow cytometry measuring both functional and phenotypic attributes of both TEM and TCM subsets in HIV infected individuals. We evaluated the quality and evolution of CD8+ T cell responses in HIV infected individuals shortly after seroconversion through to the chronic phase of infection, finding that early polyfunctional responses may result in better HIV disease outcomes. Additionally, we show that epitope-specificity differs between short-term cytokine/chemokine secretion and long-term proliferative assays. Importantly, we show that, at a cohort level, particular epitopes preferentially elicit specific qualities of CD8+ T cell responses in preference to others. This research improves our understanding of HIV pathogenesis and indicates that we can identif

Published
2011

225. Cloning and characterization of novel IgA antibody variable heavy and light chains from HIV-1 resistant sex workers from Nairobi, Kenya

Author

Fowke, Keith R. (Medical Microbiology) Berry, Jody D. (Immunology), Plummer, Francis A. (Medical Microbiology), Sarna, Caitlin S., Fowke, Keith R. (Medical Microbiology) Berry, Jody D. (Immunology), Plummer, Francis A. (Medical Microbiology), and Sarna, Caitlin S.

Abstract

Heterosexual intercourse now accounts for the majority of HIV transmission within sub-Saharan Africa. The generation of microbicides and vaccines, therefore, requires a better understanding of the mucosal correlates of protection, including the role of HIV-specific IgA. It is now accepted that not all individuals are equally susceptible to HIV-1 infection, as exemplified by the HIV Exposed Seronegative (HESN) women of the Pumwani Cohort in Nairobi, Kenya. To assess whether mucosal IgA responses contribute to this protection, 3 novel IgA variable genes were cloned from HESN cervical B-cell cDNA. Nine monoclonal IgA Abs were produced, two of which were properly produced from cell culture. The HESN-derived A6/30L and A9/30L variants had a greater specificity for gp120IIIB than their A6/4L and A9/4L counterparts, while the A6 variant recognizes a distinct gp120 epitope compared to the broadly neutralizing antibody IgGb12. Further characterization of these IgA chains may suggest their suitability for use in microbicides or mucosal vaccines.

Published
2011

226. Examination of HIV-1 diversity and evolution by a bioinformatics approach

Author

Yang, Xi (Medical Microbiology) Ball, Blake T. (Medical Microbiology) Fristensky, Brian W. (Plant Science)Van Domselaar, Gary (Pharmacy) Yao, Xiaojian (Medical Microbiology), Plummer, Francis A. (Medical Microbiology) Jones, Steven J.M. (Medical Microbiology), Liang, Binhua, Yang, Xi (Medical Microbiology) Ball, Blake T. (Medical Microbiology) Fristensky, Brian W. (Plant Science)Van Domselaar, Gary (Pharmacy) Yao, Xiaojian (Medical Microbiology), Plummer, Francis A. (Medical Microbiology) Jones, Steven J.M. (Medical Microbiology), and Liang, Binhua

Abstract

HIV-1 genetic diversity is a major obstacle for developing an effective vaccine. My hypothesis is that HIV-1 genetic diversity can be characterized and that cross-clade immunogens can be predicted at the population level. I systematically investigated positive selection (PS) pressures on HIV-1 Env and Gag proteins based on the analysis of the sequences collected from the Los Alamos Sequence Database. I identified PS sites, investigated PS patterns, correlated PS with the known functional sites of the two proteins, calculated frequencies of HLA alleles targeting CTL epitopes, and compared PS patterns among major subtypes. The results showed that PS pressure was widely dispersed across the entire regions of both HIV-1 Env and Gag proteins, suggesting the conserved regions are under host immune response pressure. The neutralizing antibody, non-neutralizing antibody, and CTL responses were found to be the major forces driving genetic diversity of HIV-1 env and gag genes at population level. However, PS pressures on both Env and Gag proteins remain stable over time, suggesting genetic diversity of HIV-1 driven by host immune responses changed very little over the last 29 years. Furthermore, the results also demonstrated that up to 70% PS sites were shared among the major HIV-1 clades, implying the existence of cross-clade immunogenicity. A number of potential cross-clades immunogens were predicted to elicit CTL or neutralizing antibody responses from Env and Gag proteins. I also detected a significant correlation between HLA allele frequencies and host CTL responses elicited by Accessory/Regulator’s proteins at population level. Moreover, I detected an association between the frequency of HLA-B7 supertype and the number of identified optimal CTL epitopes. The results suggest HLA class I allele frequencies in a population influence the evolution of HIV-1. I also systematically evaluated the utility of ultra-deep pyrosequencing to characterize genetic diversity of HIV-1 ga

Published
2010

227. The role of Trappin-2 and RANTES in mediating resistance to HIV-1 infection

Author

Embree, Joanne (Medical Microbiology) Kung, Sam (Immunology), Plummer, Francis Allan (Medical Microbiology), Mlinar, Diana, Embree, Joanne (Medical Microbiology) Kung, Sam (Immunology), Plummer, Francis Allan (Medical Microbiology), and Mlinar, Diana

Abstract

There are currently more than 33 million people worldwide who are infected with HIV-1 despite development of novel treatments and knowledge of prevention strategies. Within the Pumwani area of Nairobi, Kenya there is a group of commercial sex workers who are highly exposed to HIV-1. A small subset of these women have been classified as resistant to HIV-1 infection as they remain HIV un-infected despite as many as 60 unprotected sexual exposures to HIV each year. A better understanding of such a natural model of HIV resistance would be invaluable to inform the development of a protective HIV vaccine or microbicide. Globally, heterosexual transmission of HIV across mucosal surfaces is responsible for the bulk of new infections and thus it is important to examine both the macro and the micro environments of the vaginal mucosa in efforts to determine what enhances and what thwarts HIV-infection. Previous studies have shown elevated levels of RANTES, a natural ligand for the dominant HIV co-receptor CCR5, in cervicovaginal secretions of HIV-resistant women. Additionally, a novel HIV-inhibitor, Trappin-2 was previously shown to be elevated in cervicovaginal secretions of HIV-resistant women. To test the hypothesis that RANTES and Trappin-2 in cervicovaginal fluid are important mediators of HIV resistance we will: 1) measure RANTES in a much larger group of women from the Pumwani cohort, and 2) measure Trappin-2 levels in samples taken at different time points, and 3) correlate Trappin-2 levels in cervicovaginal fluid with biological confounding variables, and 4) investigate whether SDF-1 plays a role in HIV-disease progression in HIV-positive women.

Published
2009

232. Association Study of Common Genetic Variants and HIV-1 Acquisition in 6,300 Infected Cases and 7,200 Controls

Author

McLaren, Paul J., primary, Coulonges, Cédric, additional, Ripke, Stephan, additional, van den Berg, Leonard, additional, Buchbinder, Susan, additional, Carrington, Mary, additional, Cossarizza, Andrea, additional, Dalmau, Judith, additional, Deeks, Steven G., additional, Delaneau, Olivier, additional, De Luca, Andrea, additional, Goedert, James J., additional, Haas, David, additional, Herbeck, Joshua T., additional, Kathiresan, Sekar, additional, Kirk, Gregory D., additional, Lambotte, Olivier, additional, Luo, Ma, additional, Mallal, Simon, additional, van Manen, Daniëlle, additional, Martinez-Picado, Javier, additional, Meyer, Laurence, additional, Miro, José M., additional, Mullins, James I., additional, Obel, Niels, additional, O'Brien, Stephen J., additional, Pereyra, Florencia, additional, Plummer, Francis A., additional, Poli, Guido, additional, Qi, Ying, additional, Rucart, Pierre, additional, Sandhu, Manj S., additional, Shea, Patrick R., additional, Schuitemaker, Hanneke, additional, Theodorou, Ioannis, additional, Vannberg, Fredrik, additional, Veldink, Jan, additional, Walker, Bruce D., additional, Weintrob, Amy, additional, Winkler, Cheryl A., additional, Wolinsky, Steven, additional, Telenti, Amalio, additional, Goldstein, David B., additional, de Bakker, Paul I. W., additional, Zagury, Jean-François, additional, and Fellay, Jacques, additional

Published
2013
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234. Genetic correlates of HIV resistance

Author

Evans, Jane (Biochemistry and Medical Genetics), Alfa, Michelle (Medical Microbiology), Plummer, Francis A. (Medical Microbiology), Marlin, Crystal Lynn, Evans, Jane (Biochemistry and Medical Genetics), Alfa, Michelle (Medical Microbiology), Plummer, Francis A. (Medical Microbiology), and Marlin, Crystal Lynn

Abstract

The Human Immunodeficiency Virus 1 (HIV-1) epidemic continues to claim millions of lives, despite intense research and public health programs. A natural model of resistance is crucial for the development of an effective vaccine. We have identified a group of sex workers in Nairobi, Kenya, who appear to be resistant to infection with HIV. Research on this cohort has identified numerous immunological and genetic correlates to HIV resistance, but has failed to completely explain the phenomenon. Genetic studies have shown that HIV resistance occurs in families, with both sex worker and non-sex worker relatives of HIV resistant women less likely to be HIV infected. In addition, HIV resistance has been associated with altered innate immune responses, as measured by cytokine production to toll-like receptor stimuli. To test the hypothesis that there is a genetic component to HIV resistance, we will address two specific objectives within this thesis: 1) identify known polymorphisms associated with HIV resistance in the kindred of these women; more specifically interferon regulatory factor 1 (IRF-1) polymorphisms, and 2) identify polymorphisms within toll-like receptors (TLRs) that may be responsible for the altered and apparently successful immune responses in HIV resistant women. Our findings show an association between HIV resistant kindred and an IRF-1 microsatellite, as well as, with an IRF-1 single nucleotide polymorphism. No associations were found between HIV resistance and the investigated TLR2 and TLR4 polymorphisms. These results also suggest a genetic component to HIV resistance, but do not fully explain the altered immune responses observed within these women.

Published
2007

237. HIV-1 Clade D Is Associated with Increased Rates of CD4 Decline in a Kenyan Cohort

Author

McKinnon, Lyle R., primary, Nagelkerke, Nico J., additional, Kaul, Rupert, additional, Shaw, Souradet Y., additional, Capina, Rupert, additional, Luo, Ma, additional, Kariri, Anthony, additional, Apidi, Winnie, additional, Kimani, Makobu, additional, Wachihi, Charles, additional, Jaoko, Walter, additional, Anzala, A. Omu, additional, Kimani, Joshua, additional, Ball, T. Blake, additional, and Plummer, Francis A., additional

Published
2012
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238. A Genetic Polymorphism of FREM1 Is Associated with Resistance against HIV Infection in the Pumwani Sex Worker Cohort

Author

Luo, Ma, primary, Sainsbury, James, additional, Tuff, Jeffrey, additional, Lacap, Philip A., additional, Yuan, Xin-Yong, additional, Hirbod, Taha, additional, Kimani, Joshua, additional, Wachihi, Charles, additional, Ramdahin, Sue, additional, Bielawny, Thomas, additional, Embree, Joanne, additional, Broliden, Kristina, additional, Ball, T. Blake, additional, and Plummer, Francis A., additional

Published
2012
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241. Blunted IL17/IL22 and Pro-Inflammatory Cytokine Responses in the Genital Tract and Blood of HIV-Exposed, Seronegative Female Sex Workers in Kenya

Author

Chege, Duncan, primary, Chai, Yijie, additional, Huibner, Sanja, additional, Kain, Taylor, additional, Wachihi, Charles, additional, Kimani, Makubo, additional, Barasa, Samson, additional, McKinnon, Lyle R., additional, Muriuki, Festus K., additional, Kariri, Anthony, additional, Jaoko, Walter, additional, Anzala, Omu, additional, Kimani, Joshua, additional, Ball, T. Blake, additional, Plummer, Francis A., additional, and Kaul, Rupert, additional

Published
2012
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242. Selection, Phenotyping and Identification of Acid and Hydrogen Peroxide Producing Bacteria from Vaginal Samples of Canadian and East African Women

Author

Schellenberg, John J., primary, Dumonceaux, Tim J., additional, Hill, Janet E., additional, Kimani, Joshua, additional, Jaoko, Walter, additional, Wachihi, Charles, additional, Mungai, Jane Njeri, additional, Lane, Margo, additional, Fowke, Keith R., additional, Ball, T. Blake, additional, and Plummer, Francis A., additional

Published
2012
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244. Microarray Analysis of HIV Resistant Female Sex Workers Reveal a Gene Expression Signature Pattern Reminiscent of a Lowered Immune Activation State

Author

Songok, Elijah M., primary, Luo, Ma, additional, Liang, Ben, additional, Mclaren, Paul, additional, Kaefer, Nadine, additional, Apidi, Winnie, additional, Boucher, Genevieve, additional, Kimani, Joshua, additional, Wachihi, Charles, additional, Sekaly, Rafick, additional, Fowke, Keith, additional, Ball, Blake T., additional, and Plummer, Francis A., additional

Published
2012
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245. For Protection from HIV-1 Infection, More Might Not Be Better: a Systematic Analysis of HIV Gag Epitopes of Two Alleles Associated with Different Outcomes of HIV-1 Infection

Author

Luo, Ma, primary, Daniuk, Christina A., additional, Diallo, Tamsir O., additional, Capina, Rupert E., additional, Kimani, Joshua, additional, Wachihi, Charles, additional, Kimani, Makubo, additional, Bielawny, Thomas, additional, Peterson, Trevor, additional, Mendoza, Mark G. R., additional, Kiazyk, Sandra, additional, Ball, T. Blake, additional, and Plummer, Francis A., additional

Published
2012
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246. The role of G protein gene GNB3 C825TPolymorphism in HIV-1 acquisition, progression and immune activation

Author

Juno, Jennifer, primary, Tuff, Jeffrey, additional, Choi, Robert, additional, Card, Catherine, additional, Kimani, Joshua, additional, Wachihi, Charles, additional, Koesters-Kiazyk, Sandra, additional, Ball, T Blake, additional, Farquhar, Carey, additional, Plummer, Francis A, additional, John-Stewart, Grace, additional, Luo, Ma, additional, and Fowke, Keith R, additional

Published
2012
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247. Does antiretroviral therapy initiation increase sexual risk taking in Kenyan female sex workers? A retrospective case–control study

Author

Mawji, Elysha, primary, McKinnon, Lyle, additional, Wachihi, Charles, additional, Chege, Duncan, additional, Thottingal, Paul, additional, Kariri, Anthony, additional, Plummer, Francis, additional, Ball, T Blake, additional, Jaoko, Walter, additional, Ngugi, Elizabeth, additional, Kimani, Joshua, additional, Gelmon, Lawrence, additional, Nagelkerke, Nico, additional, and Kaul, Rupert, additional

Published
2012
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