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1. A common mechanism of clinical HIV-1 resistance to the CCR5 antagonist maraviroc despite divergent resistance levels and lack of common gp120 resistance mutations

Author

Roche, Michael, Salimi, Hamid, Duncan, Renee, Wilkinson, Brendan L, Chikere, Kelechi, Moore, Miranda S, Webb, Nicholas E, Zappi, Helena, Sterjovski, Jasminka, Flynn, Jacqueline K, Ellett, Anne, Gray, Lachlan R, Lee, Benhur, Jubb, Becky, Westby, Mike, Ramsland, Paul A, Lewin, Sharon R, Payne, Richard J, Churchill, Melissa J, and Gorry, Paul R

Abstract

Abstract Background The CCR5 antagonist maraviroc (MVC) inhibits human immunodeficiency virus type 1 (HIV-1) entry by altering the CCR5 extracellular loops (ECL), such that the gp120 envelope glycoproteins (Env) no longer recognize CCR5. The mechanisms of HIV-1 resistance to MVC, the only CCR5 antagonist licensed for clinical use are poorly understood, with insights into MVC resistance almost exclusively limited to knowledge obtained from in vitro studies or from studies of resistance to other CCR5 antagonists. To more precisely understand mechanisms of resistance to MVC in vivo, we characterized Envs isolated from 2 subjects who experienced virologic failure on MVC. Results Envs were cloned from subjects 17 and 24 before commencement of MVC (17-Sens and 24-Sens) and after virologic failure (17-Res and 24-Res). The Envs cloned during virologic failure showed broad divergence in resistance levels, with 17-Res Env exhibiting a relatively high maximal percent inhibition (MPI) of ~90% in NP2-CD4/CCR5 cells and peripheral blood mononuclear cells (PBMC), and 24-Res Env exhibiting a very low MPI of ~0 to 12% in both cell types, indicating relatively “weak” and “strong” resistance, respectively. Resistance mutations were strain-specific and mapped to the gp120 V3 loop. Affinity profiling by the 293-Affinofile assay and mathematical modeling using VERSA (Viral Entry Receptor Sensitivity Analysis) metrics revealed that 17-Res and 24-Res Envs engaged MVC-bound CCR5 inefficiently or very efficiently, respectively. Despite highly divergent phenotypes, and a lack of common gp120 resistance mutations, both resistant Envs exhibited an almost superimposable pattern of dramatically increased reliance on sulfated tyrosine residues in the CCR5 N-terminus, and on histidine residues in the CCR5 ECLs. This altered mechanism of CCR5 engagement rendered both the resistant Envs susceptible to neutralization by a sulfated peptide fragment of the CCR5 N-terminus. Conclusions Clinical resistance to MVC may involve divergent Env phenotypes and different genetic alterations in gp120, but the molecular mechanism of resistance of the Envs studied here appears to be related. The increased reliance on sulfated CCR5 N-terminus residues suggests a new avenue to block HIV-1 entry by CCR5 N-terminus sulfopeptidomimetic drugs.

Published
2013

2. HIV-1 predisposed to acquiring resistance to maraviroc (MVC) and other CCR5 antagonists in vitro has an inherent, low-level ability to utilize MVC-bound CCR5 for entry

Author

Roche, Michael, Jakobsen, Martin R, Ellett, Anne, Salimiseyedabad, Hamid, Jubb, Becky, Westby, Mike, Lee, Benhur, Lewin, Sharon R, Churchill, Melissa J, and Gorry, Paul R

Abstract

Abstract Background Maraviroc (MVC) and other CCR5 antagonists are HIV-1 entry inhibitors that bind to- and alter the conformation of CCR5, such that CCR5 is no longer recognized by the viral gp120 envelope (Env) glycoproteins. Resistance to CCR5 antagonists results from HIV-1 Env acquiring the ability to utilize the drug-bound conformation of CCR5. Selecting for HIV-1 resistance to CCR5-antagonists in vitro is relatively difficult. However, the CCR5-using CC1/85 strain appears to be uniquely predisposed to acquiring resistance to several CCR5 antagonists in vitro including MVC, vicriviroc and AD101. Findings Here, we show that Env derived from the parental CC1/85 strain is inherently capable of a low affinity interaction with MVC-bound CCR5. However, this phenotype was only revealed in 293-Affinofile cells and NP2-CD4/CCR5 cells that express very high levels of CCR5, and was masked in TZM-bl, JC53 and U87-CD4/CCR5 cells as well as PBMC, which express comparatively lower levels of CCR5 and which are more commonly used to detect resistance to CCR5 antagonists. Conclusions Env derived from the CC1/85 strain of HIV-1 is inherently capable of a low-affinity interaction with MVC-bound CCR5, which helps explain the relative ease in which CC1/85 can acquire resistance to CCR5 antagonists in vitro. The detection of similar phenotypes in patients may identify those who could be at higher risk of virological failure on MVC.

Published
2011

6. Maraviroc

Author

Gorry, Paul, primary, Ellett, Anne, additional, and Lewin, Sharon, additional

Published
2010
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10. HIV latency can be established in proliferating and nonproliferating resting CD4+ T cells in vitro

Author

Moso, Michael A., primary, Anderson, Jenny L., additional, Adikari, Samantha, additional, Gray, Lachlan R., additional, Khoury, Georges, additional, Chang, Judy J., additional, Jacobson, Jonathan C., additional, Ellett, Anne M., additional, Cheng, Wan-Jung, additional, Saleh, Suha, additional, Zaunders, John J., additional, Purcell, Damian F.J., additional, Cameron, Paul U., additional, Churchill, Melissa J., additional, Lewin, Sharon R., additional, and Lu, Hao K., additional

Published
2019
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11. HIV-1 predisposed to acquiring resistance to maraviroc (MVC) and other CCR5 antagonists in vitro has an inherent, low-level ability to utilize MVC-bound CCR5 for entry

Author

Westby Mike, Jubb Becky, Salimiseyedabad Hamid, Ellett Anne, Jakobsen Martin R, Roche Michael, Lee Benhur, Lewin Sharon R, Churchill Melissa J, and Gorry Paul R

Subjects
Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Background Maraviroc (MVC) and other CCR5 antagonists are HIV-1 entry inhibitors that bind to- and alter the conformation of CCR5, such that CCR5 is no longer recognized by the viral gp120 envelope (Env) glycoproteins. Resistance to CCR5 antagonists results from HIV-1 Env acquiring the ability to utilize the drug-bound conformation of CCR5. Selecting for HIV-1 resistance to CCR5-antagonists in vitro is relatively difficult. However, the CCR5-using CC1/85 strain appears to be uniquely predisposed to acquiring resistance to several CCR5 antagonists in vitro including MVC, vicriviroc and AD101. Findings Here, we show that Env derived from the parental CC1/85 strain is inherently capable of a low affinity interaction with MVC-bound CCR5. However, this phenotype was only revealed in 293-Affinofile cells and NP2-CD4/CCR5 cells that express very high levels of CCR5, and was masked in TZM-bl, JC53 and U87-CD4/CCR5 cells as well as PBMC, which express comparatively lower levels of CCR5 and which are more commonly used to detect resistance to CCR5 antagonists. Conclusions Env derived from the CC1/85 strain of HIV-1 is inherently capable of a low-affinity interaction with MVC-bound CCR5, which helps explain the relative ease in which CC1/85 can acquire resistance to CCR5 antagonists in vitro. The detection of similar phenotypes in patients may identify those who could be at higher risk of virological failure on MVC.

Published
2011
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12. Asn 362 in gp120 contributes to enhanced fusogenicity by CCR5-restricted HIV-1 envelope glycoprotein variants from patients with AIDS

Author

Wang Bin, Saksena Nitin, Purcell Damian FJ, Dunfee Rebecca L, Roche Michael J, Gray Lachlan R, Ellett Anne, Churchill Melissa J, Sterjovski Jasminka, Sonza Secondo, Wesselingh Steven L, Karlsson Ingrid, Fenyo Eva-Maria, Gabuzda Dana, Cunningham Anthony L, and Gorry Paul R

Subjects
Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Background CCR5-restricted (R5) human immunodeficiency virus type 1 (HIV-1) variants cause CD4+ T-cell loss in the majority of individuals who progress to AIDS, but mechanisms underlying the pathogenicity of R5 strains are poorly understood. To better understand envelope glycoprotein (Env) determinants contributing to pathogenicity of R5 viruses, we characterized 37 full-length R5 Envs from cross-sectional and longitudinal R5 viruses isolated from blood of patients with asymptomatic infection or AIDS, referred to as pre-AIDS (PA) and AIDS (A) R5 Envs, respectively. Results Compared to PA-R5 Envs, A-R5 Envs had enhanced fusogenicity in quantitative cell-cell fusion assays, and reduced sensitivity to inhibition by the fusion inhibitor T-20. Sequence analysis identified the presence of Asn 362 (N362), a potential N-linked glycosylation site immediately N-terminal to CD4-binding site (CD4bs) residues in the C3 region of gp120, more frequently in A-R5 Envs than PA-R5 Envs. N362 was associated with enhanced fusogenicity, faster entry kinetics, and increased sensitivity of Env-pseudotyped reporter viruses to neutralization by the CD4bs-directed Env mAb IgG1b12. Mutagenesis studies showed N362 contributes to enhanced fusogenicity of most A-R5 Envs. Molecular models indicate N362 is located adjacent to the CD4 binding loop of gp120, and suggest N362 may enhance fusogenicity by promoting greater exposure of the CD4bs and/or stabilizing the CD4-bound Env structure. Conclusion Enhanced fusogenicity is a phenotype of the A-R5 Envs studied, which was associated with the presence of N362, enhanced HIV-1 entry kinetics and increased CD4bs exposure in gp120. N362 contributes to fusogenicity of R5 Envs in a strain dependent manner. Our studies suggest enhanced fusogenicity of A-R5 Envs may contribute to CD4+ T-cell loss in subjects who progress to AIDS whilst harbouring R5 HIV-1 variants. N362 may contribute to this effect in some individuals.

Published
2007
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13. Analysis of Clinical HIV-1 Strains with Resistance to Maraviroc Reveals Strain-Specific Resistance Mutations, Variable Degrees of Resistance, and Minimal Cross-Resistance to Other CCR5 Antagonists

Author

Flynn, Jacqueline K., primary, Ellenberg, Paula, additional, Duncan, Renee, additional, Ellett, Anne, additional, Zhou, Jingling, additional, Sterjovski, Jasminka, additional, Cashin, Kieran, additional, Borm, Katharina, additional, Gray, Lachlan R, additional, Lewis, Marilyn, additional, Jubb, Becky, additional, Westby, Mike, additional, Lee, Benhur, additional, Lewin, Sharon R, additional, Churchill, Melissa, additional, Roche, Michael, additional, and Gorry, Paul R., additional

Published
2017
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14. CD4 and MHC class I down-modulation activities of nef alleles from brain- and lymphoid tissue-derived primary HIV-1 isolates

Author

Gray, Lachlan R., Gabuzda, Dana, Cowley, Daniel, Ellett, Anne, Chiavaroli, Lisa, Wesselingh, Steven L., Churchill, Melissa J., and Gorry, Paul R.

Subjects
Central Nervous System, Male, AIDS Dementia Complex, Lymphoid Tissue, viruses, Molecular Sequence Data, virus diseases, Brain, Down-Regulation, Genes, MHC Class I, HIV Infections, Virus Replication, Article, Cell Line, Genes, nef, CD4 Antigens, HIV-1, Humans, Amino Acid Sequence, nef Gene Products, Human Immunodeficiency Virus, Alleles, Phylogeny
Abstract

Human immunodeficiency virus type 1 (HIV-1) nef undergoes adaptive evolution in the central nervous system (CNS), reflecting altered requirements for HIV-1 replication in macrophages/microglia and brain-specific immune selection pressures. The role of Nef in HIV-1 neurotropism and pathogenesis of HIV-associated dementia (HAD) is unclear. In this study, we characterized 82 nef alleles cloned from brain, cerebral spinal fluid, spinal cord, and blood/lymphoid tissue-derived HIV-1 isolates from seven subjects with HAD. CNS isolate-derived nef alleles were genetically compartmentalized and had reduced sequence diversity compared to those from lymphoid tissue isolates. Defective nef alleles predominated in a brain-derived isolate from one of the seven subjects (MACS2-br). The ability of Nef to down-modulate CD4 and MHC class 1 (MHC-1) was generally conserved among nef alleles from both CNS and lymphoid tissues. However, the potency of CD4 and MHC-1 down-modulation was variable, which was associated with sequence alterations known to influence these Nef functions. These results suggest that CD4 and MHC-1 down-modulations are highly conserved functions among nef alleles from CNS- and lymphoid tissue-derived HIV-1 isolates that may contribute to viral replication and escape from immune surveillance in the CNS.

Published
2010

16. HIV-1 Entry and Trans-Infection of Astrocytes Involves CD81 Vesicles

Author

Gray, Lachlan R., primary, Turville, Stuart G., additional, HItchen, Tina L., additional, Cheng, Wan-Jung, additional, Ellett, Anne M., additional, Salimi, Hamid, additional, Roche, Michael J., additional, Wesselingh, Steve L., additional, Gorry, Paul R., additional, and Churchill, Melissa J., additional

Published
2014
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18. Longitudinal Analysis of CCR5 and CXCR4 Usage in a Cohort of Antiretroviral Therapy-Naïve Subjects with Progressive HIV-1 Subtype C Infection

Author

Jakobsen, Martin R, Cashin, Kieran, Roche, Michael, Sterjovski, Jasminka, Ellett, Anne, Borm, Katharina, Flynn, Jacqueline, Erikstrup, Christian, Gouillou, Maelenn, Gray, Lachlan R, Saksena, Nitin K, Wang, Bin, Purcell, Damian F J, Kallestrup, Per, Zinyama-Gutsire, Rutendo B, Gomo, Exnevia, Ullum, Henrik, Ostergaard, Lars, Lee, Benhur, Ramsland, Paul A, Churchill, Melissa J, Gorry, Paul R, Jakobsen, Martin R, Cashin, Kieran, Roche, Michael, Sterjovski, Jasminka, Ellett, Anne, Borm, Katharina, Flynn, Jacqueline, Erikstrup, Christian, Gouillou, Maelenn, Gray, Lachlan R, Saksena, Nitin K, Wang, Bin, Purcell, Damian F J, Kallestrup, Per, Zinyama-Gutsire, Rutendo B, Gomo, Exnevia, Ullum, Henrik, Ostergaard, Lars, Lee, Benhur, Ramsland, Paul A, Churchill, Melissa J, and Gorry, Paul R

Abstract

HIV-1 subtype C (C-HIV) is responsible for most HIV-1 cases worldwide. Although the pathogenesis of C-HIV is thought to predominantly involve CCR5-restricted (R5) strains, we do not have a firm understanding of how frequently CXCR4-using (X4 and R5X4) variants emerge in subjects with progressive C-HIV infection. Nor do we completely understand the molecular determinants of coreceptor switching by C-HIV variants. Here, we characterized a panel of HIV-1 envelope glycoproteins (Envs) (n = 300) cloned sequentially from plasma of 21 antiretroviral therapy (ART)-naïve subjects who experienced progression from chronic to advanced stages of C-HIV infection, and show that CXCR4-using C-HIV variants emerged in only one individual. Mutagenesis studies and structural models suggest that the evolution of R5 to X4 variants in this subject principally involved acquisition of an "Ile-Gly" insertion in the gp120 V3 loop and replacement of the V3 "Gly-Pro-Gly" crown with a "Gly-Arg-Gly" motif, but that the accumulation of additional gp120 "scaffold" mutations was required for these V3 loop changes to confer functional effects. In this context, either of the V3 loop changes could confer possible transitional R5X4 phenotypes, but when present together they completely abolished CCR5 usage and conferred the X4 phenotype. Our results show that the emergence of CXCR4-using strains is rare in this cohort of untreated individuals with advanced C-HIV infection. In the subject where X4 variants did emerge, alterations in the gp120 V3 loop were necessary but not sufficient to confer CXCR4 usage.

Published
2013

20. The magnitude of HIV-1 resistance to the CCR5 antagonist maraviroc may impart a differential alteration in HIV-1 tropism for macrophages and T-cell subsets

Author

Flynn, Jacqueline K., primary, Paukovics, Geza, additional, Moore, Miranda S., additional, Ellett, Anne, additional, Gray, Lachlan R., additional, Duncan, Renee, additional, Salimi, Hamid, additional, Jubb, Becky, additional, Westby, Mike, additional, Purcell, Damian F.J., additional, Lewin, Sharon R., additional, Lee, Benhur, additional, Churchill, Melissa J., additional, Gorry, Paul R, additional, and Roche, Michael, additional

Published
2013
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21. Longitudinal Analysis of CCR5 and CXCR4 Usage in a Cohort of Antiretroviral Therapy-Naïve Subjects with Progressive HIV-1 Subtype C Infection

Author

Jakobsen, Martin R., primary, Cashin, Kieran, additional, Roche, Michael, additional, Sterjovski, Jasminka, additional, Ellett, Anne, additional, Borm, Katharina, additional, Flynn, Jacqueline, additional, Erikstrup, Christian, additional, Gouillou, Maelenn, additional, Gray, Lachlan R., additional, Saksena, Nitin K., additional, Wang, Bin, additional, Purcell, Damian F. J., additional, Kallestrup, Per, additional, Zinyama-Gutsire, Rutendo, additional, Gomo, Exnevia, additional, Ullum, Henrik, additional, Østergaard, Lars, additional, Lee, Benhur, additional, Ramsland, Paul A., additional, Churchill, Melissa J., additional, and Gorry, Paul R., additional

Published
2013
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23. Macrophage-tropic HIV-1 variants from brain demonstrate alterations in the way gp120 engages both CD4 and CCR5

Author

Salimi, Hamid, primary, Roche, Michael, additional, Webb, Nicholas, additional, Gray, Lachlan R, additional, Chikere, Kelechi, additional, Sterjovski, Jasminka, additional, Ellett, Anne, additional, Wesselingh, Steve L, additional, Ramsland, Paul A, additional, Lee, Benhur, additional, Churchill, Melissa J, additional, and Gorry, Paul R, additional

Published
2013
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26. HIV-1 Escape from the CCR5 Antagonist Maraviroc Associated with an Altered and Less-Efficient Mechanism of gp120-CCR5 Engagement That Attenuates Macrophage Tropism

Author

Roche, Michael, primary, Jakobsen, Martin R., additional, Sterjovski, Jasminka, additional, Ellett, Anne, additional, Posta, Filippo, additional, Lee, Benhur, additional, Jubb, Becky, additional, Westby, Mike, additional, Lewin, Sharon R., additional, Ramsland, Paul A., additional, Churchill, Melissa J., additional, and Gorry, Paul R., additional

Published
2011
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29. Extremely prolonged HIV seroconversion associated with an MHC haplotype carrying disease susceptibility genes for antibody deficiency disorders

Author

Padiglione, Alex, primary, Aleksic, Eman, additional, French, Martyn, additional, Arnott, Alicia, additional, Wilson, Kim M., additional, Tippett, Emma, additional, Kaye, Matthew, additional, Gray, Lachlan, additional, Ellett, Anne, additional, Crane, Megan, additional, Leslie, David E., additional, Lewin, Sharon R., additional, Breschkin, Alan, additional, Birch, Chris, additional, Gorry, Paul R., additional, McPhee, Dale A., additional, and Crowe, Suzanne M., additional

Published
2010
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30. An altered and more efficient mechanism of CCR5 engagement contributes to macrophage tropism of CCR5-using HIV-1 envelopes

Author

Sterjovski, Jasminka, primary, Roche, Michael, additional, Churchill, Melissa J., additional, Ellett, Anne, additional, Farrugia, William, additional, Gray, Lachlan R., additional, Cowley, Daniel, additional, Poumbourios, Pantelis, additional, Lee, Benhur, additional, Wesselingh, Steven L., additional, Cunningham, Anthony L., additional, Ramsland, Paul A., additional, and Gorry, Paul R., additional

Published
2010
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31. Enhanced CD4+ cellular apoptosis by CCR5-restricted HIV-1 envelope glycoprotein variants from patients with progressive HIV-1 infection

Author

Wade, Jessica, primary, Sterjovski, Jasminka, additional, Gray, Lachlan, additional, Roche, Michael, additional, Chiavaroli, Lisa, additional, Ellett, Anne, additional, Jakobsen, Martin R., additional, Cowley, Daniel, additional, da Fonseca Pereira, Candida, additional, Saksena, Nitin, additional, Wang, Bin, additional, Purcell, Damian F.J., additional, Karlsson, Ingrid, additional, Fenyö, Eva-Maria, additional, Churchill, Melissa, additional, and Gorry, Paul R., additional

Published
2010
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32. Tissue-Specific Sequence Alterations in the Human Immunodeficiency Virus Type 1 Envelope Favoring CCR5 Usage Contribute to Persistence of Dual-Tropic Virus in the Brain

Author

Gray, Lachlan, primary, Roche, Michael, additional, Churchill, Melissa J., additional, Sterjovski, Jasminka, additional, Ellett, Anne, additional, Poumbourios, Pantelis, additional, Sherieff, Shameem, additional, Wang, Bin, additional, Saksena, Nitin, additional, Purcell, Damian F. J., additional, Wesselingh, Steven, additional, Cunningham, Anthony L., additional, Brew, Bruce J., additional, Gabuzda, Dana, additional, and Gorry, Paul R., additional

Published
2009
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33. Asn 362 in gp120 contributes to enhanced fusogenicity by CCR5-restricted HIV-1 envelope glycoprotein variants from patients with AIDS

Author

Sterjovski, Jasminka, primary, Churchill, Melissa J, additional, Ellett, Anne, additional, Gray, Lachlan R, additional, Roche, Michael J, additional, Dunfee, Rebecca L, additional, Purcell, Damian FJ, additional, Saksena, Nitin, additional, Wang, Bin, additional, Sonza, Secondo, additional, Wesselingh, Steven L, additional, Karlsson, Ingrid, additional, Fenyo, Eva-Maria, additional, Gabuzda, Dana, additional, Cunningham, Anthony L, additional, and Gorry, Paul R, additional

Published
2007
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34. Genetic and Functional Analysis of R5X4 Human Immunodeficiency Virus Type 1 Envelope Glycoproteins Derived from Two Individuals Homozygous for the CCR5Δ32 Allele

Author

Gray, Lachlan, primary, Churchill, Melissa J., additional, Keane, Niamh, additional, Sterjovski, Jasminka, additional, Ellett, Anne M., additional, Purcell, Damian F. J., additional, Poumbourios, Pantelis, additional, Kol, Chenda, additional, Wang, Bin, additional, Saksena, Nitin K., additional, Wesselingh, Steven L., additional, Price, Patricia, additional, French, Martyn, additional, Gabuzda, Dana, additional, and Gorry, Paul R., additional

Published
2006
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35. HIV-1 Entry and Trans-Infection of Astrocytes Involves CD81 Vesicles.

Author

Gray, Lachlan R., Turville, Stuart G., HItchen, Tina L., Cheng, Wan-Jung, Ellett, Anne M., Salimi, Hamid, Roche, Michael J., Wesselingh, Steve L., Gorry, Paul R., and Churchill, Melissa J.

Subjects
HIV, ASTROCYTES, CD81 antigen, COGNITIVE ability, TRYPSIN, VIRUS diseases, VIROLOGY
Abstract

Astrocytes are extensively infected with HIV-1 in vivo and play a significant role in the development of HIV-1-associated neurocognitive disorders. Despite their extensive infection, little is known about how astrocytes become infected, since they lack cell surface CD4 expression. In the present study, we investigated the fate of HIV-1 upon infection of astrocytes. Astrocytes were found to bind and harbor virus followed by biphasic decay, with HIV-1 detectable out to 72 hours. HIV-1 was observed to associate with CD81-lined vesicle structures. shRNA silencing of CD81 resulted in less cell-associated virus but no loss of co-localization between HIV-1 and CD81. Astrocytes supported trans-infection of HIV-1 to T-cells without de novo virus production, and the virus-containing compartment required 37°C to form, and was trypsin-resistant. The CD81 compartment observed herein, has been shown in other cell types to be a relatively protective compartment. Within astrocytes, this compartment may be actively involved in virus entry and/or spread. The ability of astrocytes to transfer virus, without de novo viral synthesis suggests they are capable of sequestering and protecting virus and thus, they could potentially facilitate viral dissemination in the CNS. [ABSTRACT FROM AUTHOR]

Published
2014
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36. Quantifying Susceptibility of CD4+ Stem Memory T-Cells to Infection by Laboratory Adapted and Clinical HIV-1 Strains.

Author

Flynn, Jacqueline K., Paukovics, Geza, Cashin, Kieran, Borm, Katharina, Ellett, Anne, Roche, Michael, Jakobsen, Martin R., Churchill, Melissa J., and Gorry, Paul R.

Subjects
HIV-1 glycoprotein 120, HIV infections, T cells, CD4 antigen, CHIASMUS, PLANT resistance to viruses, DISEASES
Abstract

CD4+ T cells are principal targets for human immunodeficiency virus type 1 (HIV-1) infection. CD4+ T cell subsets are heterogeneous cell populations, divided by functional and phenotypic differences into naïve and memory T cells. The memory CD4+ T cells are further segregated into central, effector and transitional memory cell subsets by functional, phenotypic and homeostatic characteristics. Defining the distribution of HIV-1 infection in different T cell subsets is important, as this can play a role in determining the size and composition of the viral reservoir. Both central memory and transitional memory CD4+ T cells have been described as long-lived viral reservoirs for HIV. Recently, the newly described stem memory T cell subset has also been implicated as a long-lived HIV reservoir. Using green fluorescent protein (GFP) reporter strains of HIV-1 and multi parameter flow cytometry, we developed an assay to simultaneously quantify the susceptibility of stem memory (TSCM), central memory, effector memory, transitional memory and naïve CD4+ T cell subsets, to HIV-1 infection in vitro. We show that TSCM are susceptible to infection with laboratory adapted and clinical HIV-1 strains. Our system facilitates the quantitation of HIV-1 infection in alternative T cell subsets by CCR5- and CXCR4-using viruses across different HIV-1 subtypes, and will be useful for studies of HIV-1 pathogenesis and viral reservoirs. [ABSTRACT FROM AUTHOR]

Published
2014
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38. Linkages between HIV-1 specificity for CCR5 or CXCR4 and in vitro usage of alternative coreceptors during progressive HIV-1 subtype C infection.

Author

Cashin, Kieran, Jakobsen, Martin R., Sterjovski, Jasminka, Roche, Michael, Ellett, Anne, Flynn, Jacqueline K., Borm, Katharina, Gouillou, Maelenn, Churchill, Melissa J., and Gorry, Paul R.

Subjects
HIV infections, GLYCOPROTEINS, LUCIFERASES, HIGHLY active antiretroviral therapy, PAPILLOMAVIRUS pathogenicity
Abstract

Background: Human immunodeficiency virus type 1 (HIV-1) subtype C (C-HIV) is spreading rapidly and is now responsible for >50% of HIV-1 infections worldwide, and >95% of infections in southern Africa and central Asia. These regions are burdened with the overwhelming majority of HIV-1 infections, yet we know very little about the pathogenesis of C-HIV. In addition to CCR5 and CXCR4, the HIV-1 envelope glycoproteins (Env) may engage a variety of alternative coreceptors for entry into transfected cells. Whilst alternative coreceptors do not appear to have a broad role in mediating the entry of HIV-1 into primary cells, characterizing patterns of alternative coreceptor usage in vitro can provide valuable insights into mechanisms of Env-coreceptor engagement that may be important for HIV-1 pathogenesis. Results: Here, we characterized the ability of luciferase reporter viruses pseudotyped with HIV-1 Envs (n = 300) cloned sequentially from plasma of 21 antiretroviral therapy (ART)-naïve subjects experiencing progression from chronic to advanced C-HIV infection over an approximately 3-year period, who either exclusively maintained CCR5- using (R5) variants (n = 20 subjects) or who experienced a coreceptor switch to CXCR4-using (X4) variants (n = 1 subject), to utilize alternative coreceptors for entry. At a population level, CCR5 usage by R5 C-HIV Envs was strongly linked to usage of FPRL1, CCR3 and CCR8 as alternative coreceptors, with the linkages to FPRL1 and CCR3 usage becoming statistically more robust as infection progressed from chronic to advanced stages of disease. In contrast, acquisition of an X4 Env phenotype at advanced infection was accompanied by a dramatic loss of FPRL1 usage. Env mutagenesis studies confirmed a direct link between CCR5 and FPRL1 usage, and showed that the V3 loop crown, but not other V3 determinants of CCR5-specificity, was the principal Env determinant governing the ability of R5 C-HIV Envs from one particular subject to engage FPRL1. Conclusions: Our results suggest that, in the absence of coreceptor switching, the ability of R5 C-HIV viruses to engage certain alternative coreceptors in vitro, in particular FPRL1, may reflect an altered use of CCR5 that is selected for during progressive C-HIV infection, and which may contribute to C-HIV pathogenicity. [ABSTRACT FROM AUTHOR]

Published
2013
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