Your search keyword '"HIV control"' showing total 31 results

1. Identification of a Clade-Specific HLA-C*03:02 CTL Epitope GY9 Derived from the HIV-1 p17 Matrix Protein.

Author

Kyobe, Samuel, Mwesigwa, Savannah, Nkurunungi, Gyaviira, Retshabile, Gaone, Egesa, Moses, Katagirya, Eric, Amujal, Marion, Mlotshwa, Busisiwe C., Williams, Lesedi, Sendagire, Hakim, Kiragga, Dithan, Mardon, Graeme, Matshaba, Mogomotsi, Hanchard, Neil A., Kyosiimire-Lugemwa, Jacqueline, and Robinson, David

Subjects

*EXTRACELLULAR matrix proteins, *HIV, *HISTOCOMPATIBILITY class I antigens, *VACCINE effectiveness, *EPITOPES, *T cells

Abstract

Efforts towards an effective HIV-1 vaccine have remained mainly unsuccessful. There is increasing evidence for a potential role of HLA-C-restricted CD8+ T cell responses in HIV-1 control, including our recent report of HLA-C*03:02 among African children. However, there are no documented optimal HIV-1 CD8+ T cell epitopes restricted by HLA-C*03:02; additionally, the structural influence of HLA-C*03:02 on epitope binding is undetermined. Immunoinformatics approaches provide a fast and inexpensive method to discover HLA-restricted epitopes. Here, we employed immunopeptidomics to identify HLA-C*03:02 CD8+ T cell epitopes. We identified a clade-specific Gag-derived GY9 (GTEELRSLY) HIV-1 p17 matrix epitope potentially restricted to HLA-C*03:02. Residues E62, T142, and E151 in the HLA-C*03:02 binding groove and positions p3, p6, and p9 on the GY9 epitope are crucial in shaping and stabilizing the epitope binding. Our findings support the growing evidence of the contribution of HLA-C molecules to HIV-1 control and provide a prospect for vaccine strategies. [ABSTRACT FROM AUTHOR]

Published

2024

2. T Cell Homeostasis Disturbances in a Cohort of Long-Term Elite Controllers of HIV Infection.

Author

Benito, José M., Jiménez-Carretero, Daniel, Restrepo, Clara, Ligos, José M., Valentín-Quiroga, Jaime, Mahillo, Ignacio, Cabello, Alfonso, López-Collazo, Eduardo, Sánchez-Cabo, Fátima, Górgolas, Miguel, Estrada, Vicente, and Rallón, Norma

Subjects

*T cells, *LONG-term non-progressors, *HIV infections, *IMMUNOSENESCENCE, *HOMEOSTASIS, *HIV-positive persons, *ANTIRETROVIRAL agents

Abstract

Elite controllers (ECs) are people living with HIV (PLWH) able to control HIV replication without antiretroviral therapy and have been proposed as a model of a functional HIV cure. Much evidence suggests that this spontaneous control of HIV has a cost in terms of T cell homeostasis alterations. We performed a deep phenotypic study to obtain insight into T cell homeostasis disturbances in ECs maintaining long-term virologic and immunologic control of HIV (long-term elite controllers; LTECs). Forty-seven PLWH were included: 22 LTECs, 15 non-controllers under successful antiretroviral therapy (onART), and 10 non-controllers not receiving ART (offART). Twenty uninfected participants (UCs) were included as a reference. T cell homeostasis was analyzed by spectral flow cytometry and data were analyzed using dimensionality reduction and clustering using R software v3.3.2. Dimensionality reduction and clustering yielded 57 and 54 different CD4 and CD8 T cell clusters, respectively. The offART group showed the highest perturbation of T cell homeostasis, with 18 CD4 clusters and 15 CD8 clusters significantly different from those of UCs. Most of these alterations were reverted in the onART group. Interestingly, LTECs presented several disturbances of T cell homeostasis with 15 CD4 clusters and 13 CD8 clusters different from UC. Moreover, there was a specific profile of T cell homeostasis alterations associated with LTECs, characterized by increases in clusters of naïve T cells, increases in clusters of non-senescent effector CD8 cells, and increases in clusters of central memory CD4 cells. These results demonstrate that, compared to ART-mediated control of HIV, the spontaneous control of HIV is associated with several disturbances in CD4 and CD8 T cell homeostasis. These alterations could be related to the existence of a potent and efficient virus-specific T cell response, and to the ability to halt disease progression by maintaining an adequate pool of CD4 T cells. [ABSTRACT FROM AUTHOR]

Published

2024

3. Mathematical study of a fractional order HIV model of CD4+ T-cells with recovery

Author

Sardar, Purnendu, Das, Krishna Pada, and Biswas, Santosh

Published

2024

4. Identification of a Clade-Specific HLA-C*03:02 CTL Epitope GY9 Derived from the HIV-1 p17 Matrix Protein

Author

Samuel Kyobe, Savannah Mwesigwa, Gyaviira Nkurunungi, Gaone Retshabile, Moses Egesa, Eric Katagirya, Marion Amujal, Busisiwe C. Mlotshwa, Lesedi Williams, Hakim Sendagire, on behalf of the CAfGEN Consortium, Dithan Kiragga, Graeme Mardon, Mogomotsi Matshaba, Neil A. Hanchard, Jacqueline Kyosiimire-Lugemwa, and David Robinson

Subjects

HIV control, HLA-C*03:02, immunoinformatics, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Efforts towards an effective HIV-1 vaccine have remained mainly unsuccessful. There is increasing evidence for a potential role of HLA-C-restricted CD8+ T cell responses in HIV-1 control, including our recent report of HLA-C*03:02 among African children. However, there are no documented optimal HIV-1 CD8+ T cell epitopes restricted by HLA-C*03:02; additionally, the structural influence of HLA-C*03:02 on epitope binding is undetermined. Immunoinformatics approaches provide a fast and inexpensive method to discover HLA-restricted epitopes. Here, we employed immunopeptidomics to identify HLA-C*03:02 CD8+ T cell epitopes. We identified a clade-specific Gag-derived GY9 (GTEELRSLY) HIV-1 p17 matrix epitope potentially restricted to HLA-C*03:02. Residues E62, T142, and E151 in the HLA-C*03:02 binding groove and positions p3, p6, and p9 on the GY9 epitope are crucial in shaping and stabilizing the epitope binding. Our findings support the growing evidence of the contribution of HLA-C molecules to HIV-1 control and provide a prospect for vaccine strategies.

Published

2024

5. HIV programme sustainability in Southern and Eastern Africa and the changing role of external assistance for health.

Author

Neel, Abigail H, Rodríguez, Daniela C, Sikazwe, Izukanji, Pillay, Yogan, Barron, Peter, Pereira, Shreya K, Makakole-Nene, Sesupo, and Bennett, Sara C

Subjects

HIV, SUSTAINABILITY

Abstract

High human immunodeficiency virus (HIV)–prevalence countries in Southern and Eastern Africa continue to receive substantial external assistance (EA) for HIV programming, yet countries are at risk of transitioning out of HIV aid without achieving epidemic control. We sought to address two questions: (1) to what extent has HIV EA in the region been programmed and delivered in a way that supports long-term sustainability and (2) how should development agencies change operational approaches to support long-term, sustainable HIV control? We conducted 20 semi-structured key informant interviews with global and country-level respondents coupled with an analysis of Global Fund budget data for Malawi, Uganda, and Zambia (from 2017 until the present). We assessed EA practice along six dimensions of sustainability, namely financial, epidemiological, programmatic, rights-based, structural and political sustainability. Our respondents described HIV systems' vulnerability to donor departure, as well as how development partner priorities and practices have created challenges to promoting long-term HIV control. The challenges exacerbated by EA patterns include an emphasis on treatment over prevention, limiting effects on new infection rates; resistance to service integration driven in part by 'winners' under current EA patterns and challenges in ensuring coverage for marginalized populations; persistent structural barriers to effectively serving key populations and limited capacity among organizations best positioned to respond to community needs; and the need for advocacy given the erosion of political commitment by the long-term and substantive nature of HIV EA. Our recommendations include developing a robust investment case for primary prevention, providing operational support for integration processes, investing in local organizations and addressing issues of political will. While strategies must be locally crafted, our paper provides initial suggestions for how EA partners could change operational approaches to support long-term HIV control and the achievement of universal health coverage. [ABSTRACT FROM AUTHOR]

Published

2024

6. Functional impairment of HIV-specific CD8+ T cells precedes aborted spontaneous control of viremia

Author

Collins, David R, Urbach, Jonathan M, Racenet, Zachary J, Arshad, Umar, Power, Karen A, Newman, Ruchi M, Mylvaganam, Geetha H, Ly, Ngoc L, Lian, Xiaodong, Rull, Anna, Rassadkina, Yelizaveta, Yanez, Adrienne G, Peluso, Michael J, Deeks, Steven G, Vidal, Francesc, Lichterfeld, Mathias, Yu, Xu G, Gaiha, Gaurav D, Allen, Todd M, and Walker, Bruce D

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Prevention, Genetics, Sexually Transmitted Infections, Infectious Diseases, Clinical Research, HIV/AIDS, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Adult, CD8-Positive T-Lymphocytes, Female, HIV Infections, Humans, Male, Middle Aged, Recurrence, Viremia, CD8(+) T cell dysfunction, HIV control, human immunology

Abstract

Spontaneous control of HIV infection has been repeatedly linked to antiviral CD8+ T cells but is not always permanent. To address mechanisms of durable and aborted control of viremia, we evaluated immunologic and virologic parameters longitudinally among 34 HIV-infected subjects with differential outcomes. Despite sustained recognition of autologous virus, HIV-specific proliferative and cytolytic T cell effector functions became selectively and intrinsically impaired prior to aborted control. Longitudinal transcriptomic profiling of functionally impaired HIV-specific CD8+ T cells revealed altered expression of genes related to activation, cytokine-mediated signaling, and cell cycle regulation, including increased expression of the antiproliferative transcription factor KLF2 but not of genes associated with canonical exhaustion. Lymphoid HIV-specific CD8+ T cells also exhibited poor functionality during aborted control relative to durable control. Our results identify selective functional impairment of HIV-specific CD8+ T cells as prognostic of impending aborted HIV control, with implications for clinical monitoring and immunotherapeutic strategies.

Published

2021

7. Reasons People Living with HIV Might Prefer Oral Daily Antiretroviral Therapy, Long-Acting Formulations, or Future HIV Remission Options

Author

Dubé, Karine, Campbell, Danielle M, Perry, Kelly E, Kanazawa, John T, Saberi, Parya, Sauceda, John A, Poteat, Tonia, and Evans, David

Subjects

Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Infectious Diseases, Clinical Research, Anti-Retroviral Agents, Cross-Sectional Studies, HIV Infections, Humans, Research Personnel, Surveys and Questionnaires, HIV control, antiretroviral treatment, long-acting ART, HIV remission, HIV cure research, people living with HIV, Clinical Sciences, Virology, Clinical sciences

Abstract

A growing body of research is beginning to elucidate reasons people living with HIV (PLWHIV) might prefer oral daily antiretroviral treatment (ART) compared with emerging long-acting ART (LA-ART) or HIV remission strategies under investigation. Our objective is to provide qualitative insights into the reasons why PLWHIV might prefer one of these HIV control therapies over others. From May to August 2018, we implemented a semistructured cross-sectional survey of PLWHIV in the United States to better understand patient preferences around various HIV treatment and remission options. Using free text, respondents were asked to explain why they preferred one HIV control option over the other two. We analyzed responses to the open-ended survey questions on reasons for preferring oral daily ART versus LA-ART versus HIV remission strategies using conventional content analysis. The results showed that PLWHIV preferred oral daily ART because of its familiarity and known safety and efficacy profile, whereas those who preferred LA-ART would value the convenience it offers. Finally, HIV remission strategies would be preferred to avoid taking ART altogether. The qualitative results provide insights into reasons why PLWHIV in the United States might prefer oral daily ART versus novel therapies. More importantly, they provide information to better align HIV virological control strategies with end-user perspectives. To make informed choices around evolving HIV therapeutics, PLWHIV and HIV care providers would benefit from decision tools to better assess options and trade-offs. More research is needed on how best to effectively support PLWHIV and HIV care providers in shared decision-making.

Published

2020

8. T Cell Homeostasis Disturbances in a Cohort of Long-Term Elite Controllers of HIV Infection

Author

José M. Benito, Daniel Jiménez-Carretero, Clara Restrepo, José M. Ligos, Jaime Valentín-Quiroga, Ignacio Mahillo, Alfonso Cabello, Eduardo López-Collazo, Fátima Sánchez-Cabo, Miguel Górgolas, Vicente Estrada, and Norma Rallón

Subjects

HIV control, long-term elite controllers (LTECs), T cell homeostasis, immunology, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Elite controllers (ECs) are people living with HIV (PLWH) able to control HIV replication without antiretroviral therapy and have been proposed as a model of a functional HIV cure. Much evidence suggests that this spontaneous control of HIV has a cost in terms of T cell homeostasis alterations. We performed a deep phenotypic study to obtain insight into T cell homeostasis disturbances in ECs maintaining long-term virologic and immunologic control of HIV (long-term elite controllers; LTECs). Forty-seven PLWH were included: 22 LTECs, 15 non-controllers under successful antiretroviral therapy (onART), and 10 non-controllers not receiving ART (offART). Twenty uninfected participants (UCs) were included as a reference. T cell homeostasis was analyzed by spectral flow cytometry and data were analyzed using dimensionality reduction and clustering using R software v3.3.2. Dimensionality reduction and clustering yielded 57 and 54 different CD4 and CD8 T cell clusters, respectively. The offART group showed the highest perturbation of T cell homeostasis, with 18 CD4 clusters and 15 CD8 clusters significantly different from those of UCs. Most of these alterations were reverted in the onART group. Interestingly, LTECs presented several disturbances of T cell homeostasis with 15 CD4 clusters and 13 CD8 clusters different from UC. Moreover, there was a specific profile of T cell homeostasis alterations associated with LTECs, characterized by increases in clusters of naïve T cells, increases in clusters of non-senescent effector CD8 cells, and increases in clusters of central memory CD4 cells. These results demonstrate that, compared to ART-mediated control of HIV, the spontaneous control of HIV is associated with several disturbances in CD4 and CD8 T cell homeostasis. These alterations could be related to the existence of a potent and efficient virus-specific T cell response, and to the ability to halt disease progression by maintaining an adequate pool of CD4 T cells.

Published

2024

9. Patient and health provider costs of integrated HIV, diabetes and hypertension ambulatory health services in low-income settings — an empirical socio-economic cohort study in Tanzania and Uganda

Author

Tinevimbo Shiri, Josephine Birungi, Anupam V. Garrib, Sokoine L. Kivuyo, Ivan Namakoola, Janneth Mghamba, Joshua Musinguzi, Godfather Kimaro, Gerald Mutungi, Moffat J. Nyirenda, Joseph Okebe, Kaushik Ramaiya, M. Bachmann, Nelson K. Sewankambo, Sayoki Mfinanga, Shabbar Jaffar, and Louis W. Niessen

Subjects

HIV control, Diabetes, Hypertension, Integrated care, Primary level, Economics, Medicine

Abstract

Abstract Background Integration of health services might be an efficient strategy for managing multiple chronic conditions in sub-Saharan Africa, considering the scope of treatments and synergies in service delivery. Proven to promote compliance, integration may lead to increased economies-of-scale. However, evidence on the socio-economic consequences of integration for providers and patients is lacking. We assessed the clinical resource use, staff time, relative service efficiency and overall societal costs associated with integrating HIV, diabetes and hypertension services in single one-stop clinics where persons with one or more of these conditions were managed. Methods 2273 participants living with HIV infection, diabetes, or hypertension or combinations of these conditions were enrolled in 10 primary health facilities in Tanzania and Uganda and followed-up for up to 12 months. We collected data on resources used from all participants and on out-of-pocket costs in a sub-sample of 1531 participants, while a facility-level costing study was conducted at each facility. Health worker time per participant was assessed in a time-motion morbidity-stratified study among 228 participants. The mean health service cost per month and out-of-pocket costs per participant visit were calculated in 2020 US$ prices. Nested bootstrapping from these samples accounted for uncertainties. A data envelopment approach was used to benchmark the efficiency of the integrated services. Last, we estimated the budgetary consequences of integration, based on prevalence-based projections until 2025, for both country populations. Results Their average retention after 1 year service follow-up was 1911/2273 (84.1%). Five hundred and eighty-two of 2273 (25.6%) participants had two or all three chronic conditions and 1691/2273 (74.4%) had a single condition. During the study, 84/2239 (3.8%) participants acquired a second or third condition. The mean service costs per month of managing two conditions in a single participant were $39.11 (95% CI 33.99, 44.33), $32.18 (95% CI 30.35, 34.07) and $22.65 (95% CI 21.86, 23.43) for the combinations of HIV and diabetes and of HIV and hypertension, diabetes and hypertension, respectively. These costs were 34.4% (95% CI 17.9%, 41.9%) lower as compared to managing any two conditions separately in two different participants. The cost of managing an individual with all three conditions was 48.8% (95% CI 42.1%, 55.3%) lower as compared to managing these conditions separately. Out-of-pocket healthcare expenditure per participant per visit was $7.33 (95% CI 3.70, 15.86). This constituted 23.4% (95% CI 9.9, 54.3) of the total monthly service expenditure per patient and 11.7% (95% CI 7.3, 22.1) of their individual total household income. The integrated clinics’ mean efficiency benchmark score was 0.86 (range 0.30–1.00) suggesting undercapacity that could serve more participants without compromising quality of care. The estimated budgetary consequences of managing multi-morbidity in these types of integrated clinics is likely to increase by 21.5% (range 19.2–23.4%) in the next 5 years, including substantial savings of 21.6% on the provision of integrated care for vulnerable patients with multi-morbidities. Conclusion Integration of HIV services with diabetes and hypertension control reduces both health service and household costs, substantially. It is likely an efficient and equitable way to address the increasing burden of financially vulnerable households among Africa’s ageing populations. Additional economic evidence is needed from longer-term larger-scale implementation studies to compare extended integrated care packages directly simultaneously with evidence on sustained clinical outcomes.

Published

2021

10. Patient and health provider costs of integrated HIV, diabetes and hypertension ambulatory health services in low-income settings - an empirical socio-economic cohort study in Tanzania and Uganda.

Author

Shiri, Tinevimbo, Birungi, Josephine, Garrib, Anupam V., Kivuyo, Sokoine L., Namakoola, Ivan, Mghamba, Janneth, Musinguzi, Joshua, Kimaro, Godfather, Mutungi, Gerald, Nyirenda, Moffat J., Okebe, Joseph, Ramaiya, Kaushik, Bachmann, M., Sewankambo, Nelson K., Mfinanga, Sayoki, Jaffar, Shabbar, and Niessen, Louis W.

Subjects

*HYPERTENSION, *DIABETES, *MEDICAL care, *HEALTH facilities, *HIV, *HIV infection epidemiology, *HYPERTENSION epidemiology, *HIV infections, *RESEARCH, *RESEARCH methodology, *CLINICS, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *RESEARCH funding, *POVERTY, *LONGITUDINAL method

Abstract

Background: Integration of health services might be an efficient strategy for managing multiple chronic conditions in sub-Saharan Africa, considering the scope of treatments and synergies in service delivery. Proven to promote compliance, integration may lead to increased economies-of-scale. However, evidence on the socio-economic consequences of integration for providers and patients is lacking. We assessed the clinical resource use, staff time, relative service efficiency and overall societal costs associated with integrating HIV, diabetes and hypertension services in single one-stop clinics where persons with one or more of these conditions were managed.Methods: 2273 participants living with HIV infection, diabetes, or hypertension or combinations of these conditions were enrolled in 10 primary health facilities in Tanzania and Uganda and followed-up for up to 12 months. We collected data on resources used from all participants and on out-of-pocket costs in a sub-sample of 1531 participants, while a facility-level costing study was conducted at each facility. Health worker time per participant was assessed in a time-motion morbidity-stratified study among 228 participants. The mean health service cost per month and out-of-pocket costs per participant visit were calculated in 2020 US$ prices. Nested bootstrapping from these samples accounted for uncertainties. A data envelopment approach was used to benchmark the efficiency of the integrated services. Last, we estimated the budgetary consequences of integration, based on prevalence-based projections until 2025, for both country populations.Results: Their average retention after 1 year service follow-up was 1911/2273 (84.1%). Five hundred and eighty-two of 2273 (25.6%) participants had two or all three chronic conditions and 1691/2273 (74.4%) had a single condition. During the study, 84/2239 (3.8%) participants acquired a second or third condition. The mean service costs per month of managing two conditions in a single participant were $39.11 (95% CI 33.99, 44.33), $32.18 (95% CI 30.35, 34.07) and $22.65 (95% CI 21.86, 23.43) for the combinations of HIV and diabetes and of HIV and hypertension, diabetes and hypertension, respectively. These costs were 34.4% (95% CI 17.9%, 41.9%) lower as compared to managing any two conditions separately in two different participants. The cost of managing an individual with all three conditions was 48.8% (95% CI 42.1%, 55.3%) lower as compared to managing these conditions separately. Out-of-pocket healthcare expenditure per participant per visit was $7.33 (95% CI 3.70, 15.86). This constituted 23.4% (95% CI 9.9, 54.3) of the total monthly service expenditure per patient and 11.7% (95% CI 7.3, 22.1) of their individual total household income. The integrated clinics' mean efficiency benchmark score was 0.86 (range 0.30-1.00) suggesting undercapacity that could serve more participants without compromising quality of care. The estimated budgetary consequences of managing multi-morbidity in these types of integrated clinics is likely to increase by 21.5% (range 19.2-23.4%) in the next 5 years, including substantial savings of 21.6% on the provision of integrated care for vulnerable patients with multi-morbidities.Conclusion: Integration of HIV services with diabetes and hypertension control reduces both health service and household costs, substantially. It is likely an efficient and equitable way to address the increasing burden of financially vulnerable households among Africa's ageing populations. Additional economic evidence is needed from longer-term larger-scale implementation studies to compare extended integrated care packages directly simultaneously with evidence on sustained clinical outcomes. [ABSTRACT FROM AUTHOR]

Published

2021

11. HIV Antibody Profiles in HIV Controllers and Persons With Treatment-Induced Viral Suppression

Author

Kai Kammers, Athena Chen, Daniel R. Monaco, Sarah E. Hudelson, Wendy Grant-McAuley, Richard D. Moore, Galit Alter, Steven G. Deeks, Charles S. Morrison, Leigh A. Eller, Joel N. Blankson, Oliver Laeyendecker, Ingo Ruczinski, Susan H. Eshleman, and H. Benjamin Larman

Subjects

HIV control, viral load set point, antibody profiling, phage display, VirScan, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionLow HIV viral load is associated with delayed disease progression and reduced HIV transmission. HIV controllers suppress viral load to low levels in the absence of antiretroviral treatment (ART). We used an antibody profiling system, VirScan, to compare antibody reactivity and specificity in HIV controllers, non-controllers with treatment-induced viral suppression, and viremic non-controllers.MethodsThe VirScan library contains 3,384 phage-displayed peptides spanning the HIV proteome. Antibody reactivity to these peptides was measured in plasma from a Discovery Cohort that included 13 elite controllers, 27 viremic controllers, 12 viremic non-controllers, and 21 non-controllers who were virally suppressed on ART. Antibody reactivity to selected peptides was also assessed in an independent cohort of 29 elite controllers and 37 non-controllers who were virally suppressed on ART (Validation Cohort) and in a longitudinal cohort of non-controllers.ResultsIn the Discovery Cohort, 62 peptides were preferentially targeted in HIV controllers compared to non-controllers who were virally suppressed on ART. These specificities were not significantly different when comparing controllers versus viremic non-controllers. Aggregate reactivity to these peptides was also high in elite controllers from the independent Validation Cohort. The 62 peptides formed seven clusters of homologous epitopes in env, gag, integrase, and vpu. Reactivity to one of these clusters located in gag p17 was inversely correlated with viral load set point in an independent cohort of non-controllers.ConclusionsAntibody reactivity was low in non-controllers suppressed on ART, but remained high in viremic controllers despite viral suppression. Antibodies in controllers and viremic non-controllers were directed against epitopes in diverse HIV proteins; higher reactivity against p17 peptides was associated with lower viral load set point. Further studies are needed to determine if these antibodies play a role in regulation of HIV viral load.

Published

2021

12. HIV Antibody Profiles in HIV Controllers and Persons With Treatment-Induced Viral Suppression.

Author

Kammers, Kai, Chen, Athena, Monaco, Daniel R., Hudelson, Sarah E., Grant-McAuley, Wendy, Moore, Richard D., Alter, Galit, Deeks, Steven G., Morrison, Charles S., Eller, Leigh A., Blankson, Joel N., Laeyendecker, Oliver, Ruczinski, Ingo, Eshleman, Susan H., and Larman, H. Benjamin

Subjects

HIV antibodies, VIRAL load, ANTIRETROVIRAL agents, HIV infection transmission, PEPTIDES

Abstract

Introduction: Low HIV viral load is associated with delayed disease progression and reduced HIV transmission. HIV controllers suppress viral load to low levels in the absence of antiretroviral treatment (ART). We used an antibody profiling system, VirScan, to compare antibody reactivity and specificity in HIV controllers, non-controllers with treatment-induced viral suppression, and viremic non-controllers. Methods: The VirScan library contains 3,384 phage-displayed peptides spanning the HIV proteome. Antibody reactivity to these peptides was measured in plasma from a Discovery Cohort that included 13 elite controllers, 27 viremic controllers, 12 viremic non-controllers, and 21 non-controllers who were virally suppressed on ART. Antibody reactivity to selected peptides was also assessed in an independent cohort of 29 elite controllers and 37 non-controllers who were virally suppressed on ART (Validation Cohort) and in a longitudinal cohort of non-controllers. Results: In the Discovery Cohort, 62 peptides were preferentially targeted in HIV controllers compared to non-controllers who were virally suppressed on ART. These specificities were not significantly different when comparing controllers versus viremic non-controllers. Aggregate reactivity to these peptides was also high in elite controllers from the independent Validation Cohort. The 62 peptides formed seven clusters of homologous epitopes in env, gag, integrase, and vpu. Reactivity to one of these clusters located in gag p17 was inversely correlated with viral load set point in an independent cohort of non-controllers. Conclusions: Antibody reactivity was low in non-controllers suppressed on ART, but remained high in viremic controllers despite viral suppression. Antibodies in controllers and viremic non-controllers were directed against epitopes in diverse HIV proteins; higher reactivity against p17 peptides was associated with lower viral load set point. Further studies are needed to determine if these antibodies play a role in regulation of HIV viral load. [ABSTRACT FROM AUTHOR]

Published

2021

13. Human leukocyte antigen B*57 does not fully explain hepatitis C clearance in HIV controllers

Author

Asher, Alice K, Santos, Glenn-Milo, Evans, Jennifer, Dokubo, Emily K, Lee, Tzong-Hae, Martin, Jeffrey N, Deeks, Steven G, Tobler, Leslie H, Busch, Michael, Hunt, Peter W, and Page, Kimberly

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Hepatitis, Chronic Liver Disease and Cirrhosis, Emerging Infectious Diseases, Hepatitis - C, Infectious Diseases, HIV/AIDS, Prevention, Sexually Transmitted Infections, Genetics, Digestive Diseases, Clinical Research, Liver Disease, Infection, Good Health and Well Being, Adult, Cohort Studies, Female, Gene Frequency, HIV Infections, HIV Long-Term Survivors, HLA-B Antigens, Hepatitis C, Hepatitis C Antibodies, Humans, Male, Middle Aged, Prospective Studies, RNA, Viral, hepatitis C virus, HIV control, human leukocyte antigen type, spontaneous clearance, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Virology, Biomedical and clinical sciences, Health sciences

Abstract

ObjectiveHIV controllers demonstrate high rates of spontaneous clearance of hepatitis C virus (HCV) infection. The objective of this study was to evaluate the role of human leukocyte antigen (HLA) B*57 and other genetic polymorphisms on HCV clearance in HIV controllers.DesignThis is a prospective cohort study.MethodsPatients in the Study of the Consequences of Protease Inhibitor Era (SCOPE) were tested for anti-HCV using enzyme immunoassay (EIA3) and HCV RNA using discriminatory HCV transcription-mediated amplification assay (Norvatis). We compared the proportion of HIV controllers and noncontrollers demonstrating HCV clearance and fitted multivariable Poisson regression models with robust standard errors to estimate adjusted prevalence ratios (APRs) and assessed genetic and immunologic predictors of HCV clearance.ResultsOf 279 HIV/HCV seropositive individuals, 48 were HIV controllers. HIV controllers compared to HIV noncontrollers, were significantly more likely to have HLA B*57 (33 vs. 10%, P

Published

2013

14. Erratum to: Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner?

Author

Harper J, Betts MR, Lichterfeld M, Müller-Trutwin M, Margolis D, Bar KJ, Li JZ, McCune JM, Lewin SR, Kulpa D, Ávila-Ríos S, Diallo DD, Lederman MM, and Paiardini M

Abstract

[This corrects the article DOI: 10.20411/pai.v8i2.665.]., Competing Interests: JH and MP have active collaborations with Merck & Co., Inc., and routinely receive antiretroviral compounds for nonhuman primate studies from ViiV Healthcare and Gilead Sciences, but the authors declare no financial stake. MML has received competitive grant funding from Gilead., (Copyright © 2024 Pathogens and Immunity.)

Published

2024

15. Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner?

Author

Harper J, Betts MR, Lichterfeld M, Müller-Trutwin M, Margolis D, Bar KJ, Li JZ, McCune JM, Lewin SR, Kulpa D, Diallo DD, Lederman MM, and Paiardini M

Abstract

Once a death sentence, HIV is now considered a manageable chronic disease due to the development of antiretroviral therapy (ART) regimens with minimal toxicity and a high barrier for genetic resistance. While highly effective in arresting AIDS progression and rendering the virus untransmissible in people living with HIV (PLWH) with undetectable viremia (U=U) [1, 2]), ART alone is incapable of eradicating the "reservoir" of resting, latently infected CD4 + T cells from which virus recrudesces upon treatment cessation. As of 2022 estimates, there are 39 million PLWH, of whom 86% are aware of their status and 76% are receiving ART [3]. As of 2017, ART-treated PLWH exhibit near normalized life expectancies without adjustment for socioeconomic differences [4]. Furthermore, there is a global deceleration in the rate of new infections [3] driven by expanded access to pre-exposure prophylaxis (PrEP), HIV testing in vulnerable populations, and by ART treatment [5]. Therefore, despite outstanding issues pertaining to cost and access in developing countries, there is strong enthusiasm that aggressive testing, treatment, and effective viral suppression may be able to halt the ongoing HIV epidemic (ie, UNAIDS' 95-95-95 targets) [6-8]; especially as evidenced by recent encouraging observations in Sydney [9]. Despite these promising efforts to limit further viral transmission, for PLWH, a "cure" remains elusive; whether it be to completely eradicate the viral reservoir (ie, cure) or to induce long-term viral remission in the absence of ART (ie, control; Figure 1). In a previous salon hosted by Pathogens and Immunity in 2016 [10], some researchers were optimistic that a cure was a feasible, scalable goal, albeit with no clear consensus on the best route. So, how are these cure strategies panning out? In this commentary, 8 years later, we will provide a brief overview on recent advances and failures towards identifying determinants of viral persistence and developing a scalable cure for HIV. Based on these observations, and as in the earlier salon, we have asked several prominent HIV cure researchers for their perspectives., Competing Interests: JH and MP have active collaborations with Merck & Co., Inc., and routinely receive antiretroviral compounds for nonhuman primate studies from ViiV Healthcare and Gilead Sciences, but the authors declare no financial stake. MML has received competitive grant funding from Gilead., (Copyright © 2024 Pathogens and Immunity.)

Published

2024

16. HLA allele-specific expression : Methods, disease associations, and relevance in hematopoietic stem cell transplantation

Author

Johansson, Tiira, Partanen, Jukka, Saavalainen, Päivi, Immunomics, TRIMM - Translational Immunology Research Program, Research Programs Unit, and University of Helsinki

Subjects

next generation sequencing, BLOOD, LEVEL, HUMAN-LEUKOCYTE ANTIGEN, DP EXPRESSION, RNA sequencing, allele-specific expression, SEQUENCE, DR EXPRESSION, MHC CLASS-I, C EXPRESSION, disease associations, 3121 General medicine, internal medicine and other clinical medicine, HIV CONTROL, human leucocyte antigen, GENE-EXPRESSION

Abstract

Varying HLA allele-specific expression levels are associated with human diseases, such as graft versus host disease (GvHD) in hematopoietic stem cell transplantation (HSCT), cytotoxic T cell response and viral load in HIV infection, and the risk of Crohn's disease. Only recently, RNA-based next generation sequencing (NGS) methodologies with accompanying bioinformatics tools have emerged to quantify HLA allele-specific expression replacing the quantitative PCR (qPCR) -based methods. These novel NGS approaches enable the systematic analysis of the HLA allele-specific expression changes between individuals and between normal and disease phenotypes. Additionally, analyzing HLA allele-specific expression and allele-specific expression loss provide important information for predicting efficacies of novel immune cell therapies. Here, we review available RNA sequencing-based approaches and computational tools for NGS to quantify HLA allele-specific expression. Moreover, we explore recent studies reporting disease associations with differential HLA expression. Finally, we discuss the role of allele-specific expression in HSCT and how considering the expression quantification in recipient-donor matching could improve the outcome of HSCT.

Published

2022

17. The network structure of sex partner meeting places reported by HIV-infected MSM: Opportunities for HIV targeted control.

Author

Brantley, Meredith, Schumacher, Christina, Fields, Errol L., Perin, Jamie, Safi, Amelia Greiner, Ellen, Jonathan M., Muvva, Ravikiran, Chaulk, Patrick, and Jennings, Jacky M.

Subjects

*HIV prevention, *HIV infection transmission, *HIV-positive persons, *MEDICAL screening, *VIRAL load, *MEN who have sex with men, *SEXUAL partners

Abstract

Baltimore, Maryland ranks among U.S. cities with the highest incidence of HIV infection among men who have sex with men (MSM). HIV screening at sex partner meeting places or venues frequented by MSM with new diagnoses and/or high HIV viral load may reduce transmission by identifying and linking infected individuals to care. We investigated venue-based clustering of newly diagnosed MSM to identify high HIV transmission venues. HIV surveillance data from MSM diagnosed between October 2012–June 2014 and reporting ≥1 sex partner meeting place were examined. Venue viral load was defined according to the geometric mean viral load of the cluster of cases that reported the venue and classified as high (>50,000 copies/mL), moderate (1500–50,000 copies/mL), and low (<1500 copies/mL). 143 MSM provided information on ≥1 sex partner meeting place, accounting for 132 unique venues. Twenty-six venues were reported by > 1 MSM; of these, a tightly connected cluster of six moderate viral load sex partner meeting places emerged, representing 66% of reports. Small, dense networks of moderate to high viral load venues may be important for targeted HIV control among MSM. [ABSTRACT FROM AUTHOR]

Published

2017

18. Patient and health provider costs of integrated HIV, diabetes and hypertension ambulatory health services in low-income settings — an empirical socio-economic cohort study in Tanzania and Uganda

Author

Louis W. Niessen, Joshua Musinguzi, Max O Bachmann, Kaushik Ramaiya, Shabbar Jaffar, Anupam Garrib, Tinevimbo Shiri, Godfather Kimaro, Josephine Birungi, Joseph Okebe, Moffat J. Nyirenda, Sayoki Mfinanga, Nelson K. Sewankambo, Sokoine Kivuyo, Janneth Mghamba, Gerald Mutungi, and Ivan Namakoola

Subjects

Multi-morbidity, wk_810, Service delivery framework, Economics, Vulnerable populations, HIV Infections, wa_395, wc_503, Efficiency, 41b6e438, Ambulatory Care Facilities, Tanzania, Cohort Studies, Environmental health, Health care, Diabetes Mellitus, Medicine, Humans, Uganda, Activity-based costing, Poverty, HIV control, Service (business), biology, business.industry, Diabetes, Integrated care, General Medicine, Health Services, biology.organism_classification, wg_200, wg_100, Hypertension, Household income, business, Primary level, Cohort study, Research Article

Abstract

Background Integration of health services might be an efficient strategy for managing multiple chronic conditions in sub-Saharan Africa, considering the scope of treatments and synergies in service delivery. Proven to promote compliance, integration may lead to increased economies-of-scale. However, evidence on the socio-economic consequences of integration for providers and patients is lacking. We assessed the clinical resource use, staff time, relative service efficiency and overall societal costs associated with integrating HIV, diabetes and hypertension services in single one-stop clinics where persons with one or more of these conditions were managed. Methods 2273 participants living with HIV infection, diabetes, or hypertension or combinations of these conditions were enrolled in 10 primary health facilities in Tanzania and Uganda and followed-up for up to 12 months. We collected data on resources used from all participants and on out-of-pocket costs in a sub-sample of 1531 participants, while a facility-level costing study was conducted at each facility. Health worker time per participant was assessed in a time-motion morbidity-stratified study among 228 participants. The mean health service cost per month and out-of-pocket costs per participant visit were calculated in 2020 US$ prices. Nested bootstrapping from these samples accounted for uncertainties. A data envelopment approach was used to benchmark the efficiency of the integrated services. Last, we estimated the budgetary consequences of integration, based on prevalence-based projections until 2025, for both country populations. Results Their average retention after 1 year service follow-up was 1911/2273 (84.1%). Five hundred and eighty-two of 2273 (25.6%) participants had two or all three chronic conditions and 1691/2273 (74.4%) had a single condition. During the study, 84/2239 (3.8%) participants acquired a second or third condition. The mean service costs per month of managing two conditions in a single participant were $39.11 (95% CI 33.99, 44.33), $32.18 (95% CI 30.35, 34.07) and $22.65 (95% CI 21.86, 23.43) for the combinations of HIV and diabetes and of HIV and hypertension, diabetes and hypertension, respectively. These costs were 34.4% (95% CI 17.9%, 41.9%) lower as compared to managing any two conditions separately in two different participants. The cost of managing an individual with all three conditions was 48.8% (95% CI 42.1%, 55.3%) lower as compared to managing these conditions separately. Out-of-pocket healthcare expenditure per participant per visit was $7.33 (95% CI 3.70, 15.86). This constituted 23.4% (95% CI 9.9, 54.3) of the total monthly service expenditure per patient and 11.7% (95% CI 7.3, 22.1) of their individual total household income. The integrated clinics’ mean efficiency benchmark score was 0.86 (range 0.30–1.00) suggesting undercapacity that could serve more participants without compromising quality of care. The estimated budgetary consequences of managing multi-morbidity in these types of integrated clinics is likely to increase by 21.5% (range 19.2–23.4%) in the next 5 years, including substantial savings of 21.6% on the provision of integrated care for vulnerable patients with multi-morbidities. Conclusion Integration of HIV services with diabetes and hypertension control reduces both health service and household costs, substantially. It is likely an efficient and equitable way to address the increasing burden of financially vulnerable households among Africa’s ageing populations. Additional economic evidence is needed from longer-term larger-scale implementation studies to compare extended integrated care packages directly simultaneously with evidence on sustained clinical outcomes.

Published

2021

19. Functional impairment of HIV-specific CD8+ T cells precedes aborted spontaneous control of viremia

Author

Medicina i Cirurgia, Bioquímica i Biotecnologia, Universitat Rovira i Virgili, Collins DR; Urbach JM; Racenet ZJ; Arshad U; Power KA; Newman RM; Mylvaganam GH; Ly NL; Lian X; Rull A; Rassadkina Y; Yanez AG; Peluso MJ; Deeks SG; Vidal F; Lichterfeld M; Yu XG; Gaiha GD; Allen TM; Walker BD, Medicina i Cirurgia, Bioquímica i Biotecnologia, Universitat Rovira i Virgili, and Collins DR; Urbach JM; Racenet ZJ; Arshad U; Power KA; Newman RM; Mylvaganam GH; Ly NL; Lian X; Rull A; Rassadkina Y; Yanez AG; Peluso MJ; Deeks SG; Vidal F; Lichterfeld M; Yu XG; Gaiha GD; Allen TM; Walker BD

Abstract

Spontaneous control of HIV infection has been repeatedly linked to antiviral CD8+ T cells but is not always permanent. To address mechanisms of durable and aborted control of viremia, we evaluated immunologic and virologic parameters longitudinally among 34 HIV-infected subjects with differential outcomes. Despite sustained recognition of autologous virus, HIV-specific proliferative and cytolytic T cell effector functions became selectively and intrinsically impaired prior to aborted control. Longitudinal transcriptomic profiling of functionally impaired HIV-specific CD8+ T cells revealed altered expression of genes related to activation, cytokine-mediated signaling, and cell cycle regulation, including increased expression of the antiproliferative transcription factor KLF2 but not of genes associated with canonical exhaustion. Lymphoid HIV-specific CD8+ T cells also exhibited poor functionality during aborted control relative to durable control. Our results identify selective functional impairment of HIV-specific CD8+ T cells as prognostic of impending aborted HIV control, with implications for clinical monitoring and immunotherapeutic strategies.

Published

2021

20. HIV Antibody Profiles in HIV Controllers and Persons With Treatment-Induced Viral Suppression

Author

Ingo Ruczinski, Wendy Grant-McAuley, Daniel R. Monaco, Galit Alter, Leigh Anne Eller, Richard D. Moore, Charles S. Morrison, H. Benjamin Larman, Kai Kammers, Steven G. Deeks, Susan H. Eshleman, Oliver Laeyendecker, Joel N. Blankson, Athena Chen, and Sarah E. Hudelson

Subjects

Adult, Male, viral load set point, Phage display, HIV Antigens, viruses, Immunology, HIV Infections, HIV Antibodies, Biology, gag Gene Products, Human Immunodeficiency Virus, Epitope, Epitopes, Young Adult, Peptide Library, HIV Non-Progressors, Humans, antibody profiling, Immunology and Allergy, Viral suppression, HIV control, Original Research, RC581-607, Viral Load, Virology, Integrase, Anti-Retroviral Agents, Cohort, Proteome, HIV-1, VirScan, biology.protein, Female, Immunologic diseases. Allergy, phage display, Antibody, Viral load, Epitope Mapping

Abstract

IntroductionLow HIV viral load is associated with delayed disease progression and reduced HIV transmission. HIV controllers suppress viral load to low levels in the absence of antiretroviral treatment (ART). We used an antibody profiling system, VirScan, to compare antibody reactivity and specificity in HIV controllers, non-controllers with treatment-induced viral suppression, and viremic non-controllers.MethodsThe VirScan library contains 3,384 phage-displayed peptides spanning the HIV proteome. Antibody reactivity to these peptides was measured in plasma from a Discovery Cohort that included 13 elite controllers, 27 viremic controllers, 12 viremic non-controllers, and 21 non-controllers who were virally suppressed on ART. Antibody reactivity to selected peptides was also assessed in an independent cohort of 29 elite controllers and 37 non-controllers who were virally suppressed on ART (Validation Cohort) and in a longitudinal cohort of non-controllers.ResultsIn the Discovery Cohort, 62 peptides were preferentially targeted in HIV controllers compared to non-controllers who were virally suppressed on ART. These specificities were not significantly different when comparing controllers versus viremic non-controllers. Aggregate reactivity to these peptides was also high in elite controllers from the independent Validation Cohort. The 62 peptides formed seven clusters of homologous epitopes in env, gag, integrase, and vpu. Reactivity to one of these clusters located in gag p17 was inversely correlated with viral load set point in an independent cohort of non-controllers.ConclusionsAntibody reactivity was low in non-controllers suppressed on ART, but remained high in viremic controllers despite viral suppression. Antibodies in controllers and viremic non-controllers were directed against epitopes in diverse HIV proteins; higher reactivity against p17 peptides was associated with lower viral load set point. Further studies are needed to determine if these antibodies play a role in regulation of HIV viral load.

Published

2021

21. Short Communication: Is It Possible to Control HIV Infection in a Middle-Income Country Through a Multidisciplinary Approach?

Author

Casseb, Jorge, Fonseca, Luiz A.M., Duarte, Alberto J.S., and ADEE3002 Group

Abstract

Despite the difficulties to follow and retain patients for a long time in the public health service, special programs may bring about increased chances of survival and better quality of life, as well as higher rates of retention in care; this is also true for middle-income developing countries such as Brazil. Our relatively small outpatient service (∼500 HIV-infected patients) may not mirror the reality encountered in other settings, including São Paulo city, but retention and high quality of care may improve rates of virological success, even in poorer settings. Furthermore, prevention of depression or anxiety, with discussion in groups of patients with the presence of a therapist, regular HIV RNA viral and CD4 cells counts, genotyping tests pre-HAART, and vigilance for drug failure, may explain this successful experience. We should also take into consideration that our cohort consists mostly of asymptomatic at-entry patients referred by the Blood Bank of São Paulo, located at the same hospital, implying that they had a better immunological status at start than the more usual HIV population. Besides that, the degree of adherence to treatment in our service, in general, is quite high and the patients have a higher mean educational level: >90% of the patients a high school or college education. Such features make this cohort a very specific and differentiated sample. To extend our findings, we intend to conduct similar studies in other HIV treatment centers, enabling comparisons of populations with different profiles. [ABSTRACT FROM AUTHOR]

Published

2018

22. HIV Controllers Are Distinguished by Chemokine Expression Profile and HIV-Specific T-Cell Proliferative Potential.

Author

Card, Catherine M., Keynan, Yoav, Lajoie, Julie, Bell, Courtney P., Dawood, Magdy, Becker, Marissa, Kasper, Ken, and Fowke, Keith R.

Abstract

HIV controllers demonstrate a natural ability to control HIV replication in the absence of antiretroviral therapy. We performed a comprehensive evaluation of inflammation and T-cell activation in a demographically unique cohort of HIV controllers and noncontrollers.Plasma concentrations of 22 cytokines and chemokines were evaluated using a multiplex bead array approach. Multicolor flow cytometry was used to measure baseline levels of T-cell activation and regulatory T cells (Tregs) and HIV-specific T-cell cytokine (interferon γ, interleukin 2) and proliferation responses.HIV controllers were characterized by elevated macrophage inflammatory protein 1α and low levels of interferon γ-induced protein 10, monocyte chemotactic protein 1, and Transforming growth factor beta. Activated (CD38+ HLA DR+) CD4+ and CD8+ T cells were reduced in HIV controllers relative to noncontrollers. HIV controllers and noncontrollers had comparable proportions of Tregs within the CD4+ T-cell compartment, but absolute Treg counts were depleted in noncontrollers. Absolute Treg counts correlated inversely with T-cell activation. Proliferative CD4+ and CD8+ T-cell responses directed against HIV gag epitopes were found most frequently among HIV controllers with the lowest viral loads (elite controllers) and were rarely detected among noncontrollers, supporting a relationship between HIV-specific T-cell proliferation and viral control.Collectively, these data suggest a model in which HIV controllers maintain low levels of viral replication through robust HIV-specific T-cell responses in an environment of low inflammation and reduced availability of activated target cells. [ABSTRACT FROM AUTHOR]

Published

2012

23. Transactional sex in the fishing communities along Lake Victoria, Kenya: a catalyst for the spread of HIV.

Author

Kwena, Zachary A., Bukusi, Elizabeth, Omondi, Enos, Ng'ayo, Musa, and Holmes, King K.

Subjects

*HIV infection risk factors, *HIV infection transmission, *COMMUNITIES, *FISHING, *FOCUS groups, *INTERPERSONAL relations, *RESEARCH funding, *RISK-taking behavior, *SEXUAL intercourse, *SOCIOECONOMIC factors, *DATA analysis software, *DESCRIPTIVE statistics

Abstract

The study describes the nature, context and implications of a unique form of transactional sexual relationships in the fishing communities along Lake Victoria in Kisumu County, Kenya. We conducted 12 focus group discussions and 17 key informant interviews among fishermen, fishmongers and fish transporters in Kisumu. Women fishmongers in the fishing communities commonly form relationships with fishermen, which are often sexual, as part of the jaboya system, wherein women who wish to sell fish in the market secure the rights to purchase the fish caught by the fishermen. Due to the nature and context of the sexual intercourse, sex typically occurs in a hurried manner, often without preparation or protection. Thus, by engaging in a web of these relationships, conducted in contexts that compromise their ability to practice safer sex, men and women in these fishing communities are at increased risk of HIV. [ABSTRACT FROM AUTHOR]

Published

2012

24. Successful Sex Pre-selection using Natural Family Planning.

Author

McSweeney, Léonie

Subjects

BIRTH control, SEX preselection, LONGITUDINAL method, HEALTH outcome assessment, OVULATION detection, SEXUAL intercourse, TREATMENT effectiveness

Abstract

Copyright of African Journal of Reproductive Health is the property of Women's Health & Action Research Centre and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2011

25. Virological, immune and host genetics markers in the control of HIV infection.

Author

Mothe, Beatriz, Ibarrondo, Javier, Llano, Anuska, and Brander, Christian

Subjects

*AIDS vaccines, *AIDS, *HIV, *GENETIC markers, *OPPORTUNISTIC infections

Abstract

HIV infection, if left untreated, leads in most cases to the development of wide immune deterioration, opportunistic infections and eventually AIDS and death. The identification of individuals who despite persisting infection show no or few signs of HIV disease progression has spurred hopes that an effective HIV vaccine could be attainable. The design of such a vaccine will greatly depend on the precise definition of disease markers, host genetic and immune characteristics that mediate relative in vivo control of this virus. Accordingly, a number of viral factors and host genetic characteristics have been shown to play a crucial role in the control of HIV disease by delaying progression to AIDS or even preventing infection. There is also an improved understanding of humoral and cellular immune responses in terms of specificity, functional repertoire, longevity and tissue distribution and their ability to contain HIV replication. However, the definition of good immune correlates unequivocally and causally associated with protection or disease progression remains elusive. Here we review work on viral factors, host genetic markers and immunological determinants that have been identified in individuals with superior control of HIV infection or in subjects who remain uninfected despite frequent exposure to the viral pathogen. [ABSTRACT FROM AUTHOR]

Published

2009

26. A role for antibodies in natural HIV control

Author

Arnaud Moris, Lisa A. Chakrabarti, Mathias Pereira, Centre d'Immunologie et de Maladies Infectieuses (CIMI), Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Institut de Biologie Intégrative de la Cellule (I2BC), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS), Département Virologie (Dpt Viro), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS), Virulence et Latence des Herpesvirus (HERPES), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Institut de Biologie Intégrative de la Cellule (I2BC), Virus et Immunité - Virus and immunity, Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS), ANRS, Sidaction, and ANR, ANR-14-CE16-0029,PD1VAX,Une nouvelle stratégie de vaccination par vecteur ADN PD1 pour mimer les réponses spécifiques de Gag trouvées chez les contrôleurs spontanés du VIH(2014), Centre d'Immunologie et des Maladies Infectieuses (CIMI), Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), SERRE, Marie-Claude, Appel à projets générique - Une nouvelle stratégie de vaccination par vecteur ADN PD1 pour mimer les réponses spécifiques de Gag trouvées chez les contrôleurs spontanés du VIH - - PD1VAX2014 - ANR-14-CE16-0029 - Appel à projets générique - VALID, and Virus et Immunité - Virus and immunity (CNRS-UMR3569)

Subjects

0301 basic medicine, CD4+ T cell help, [SDV]Life Sciences [q-bio], Immunology, HIV Infections, HIV Antibodies, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Virology, memory B cells, Animals, Humans, neutralizing antibodies, 030212 general & internal medicine, Neutralizing antibody, HIV control, Antibody-dependent cell-mediated cytotoxicity, [SDV.MP.VIR] Life Sciences [q-bio]/Microbiology and Parasitology/Virology, B-Lymphocytes, biology, Oncology (nursing), Effector, T-Lymphocytes, Helper-Inducer, Hematology, Isotype, 3. Good health, [SDV] Life Sciences [q-bio], 030104 developmental biology, Infectious Diseases, Oncology, [SDV.IMM.IA]Life Sciences [q-bio]/Immunology/Adaptive immunology, [SDV.IMM.IA] Life Sciences [q-bio]/Immunology/Adaptive immunology, Humoral immunity, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, biology.protein, Antibody, ADCC, Immunologic Memory

Abstract

International audience; PURPOSE OF REVIEW: Rare patients naturally control HIV replication without antiretroviral therapy. Understanding the mechanisms implicated in natural HIV control will inform the development of immunotherapies against HIV. Elite controllers are known for developing efficient antiviral T-cell responses, but recent findings suggest that antibody responses also play a significant role in HIV control. We review the key studies that uncovered a potent memory B-cell response and highly functional anti-HIV antibodies in elite controllers, and explore the mechanisms that may account for the distinct properties of their humoral response. RECENT FINDINGS: Elite controllers maintain a large HIV-specific memory B-cell pool that is sustained by efficient T follicular helper function. Neutralizing antibody rarely show high titers in controllers, but seem capable, at least in certain cases, of neutralizing contemporaneous viral strains. In addition, elite controllers display a unique HIV-specific antibody profile in terms of isotype, antigen specificity, and glycosylation pattern, resulting in polyfunctional antibody effector functions that may promote infected cell lysis and prime effectors of the antiviral immune response. SUMMARY: Lessons from elite controller studies argue for the importance of integrating the many parameters defining a polyfunctional antibody response when evaluating candidate vaccines and immunotherapeutic approaches directed at HIV.

Published

2019

27. Functional impairment of HIV-specific CD8 + T cells precedes aborted spontaneous control of viremia.

Author

Collins DR, Urbach JM, Racenet ZJ, Arshad U, Power KA, Newman RM, Mylvaganam GH, Ly NL, Lian X, Rull A, Rassadkina Y, Yanez AG, Peluso MJ, Deeks SG, Vidal F, Lichterfeld M, Yu XG, Gaiha GD, Allen TM, and Walker BD

Subjects

Adult, Female, Humans, Male, Middle Aged, Recurrence, CD8-Positive T-Lymphocytes immunology, HIV Infections immunology, HIV Infections virology, Viremia immunology, Viremia virology

Abstract

Spontaneous control of HIV infection has been repeatedly linked to antiviral CD8 + T cells but is not always permanent. To address mechanisms of durable and aborted control of viremia, we evaluated immunologic and virologic parameters longitudinally among 34 HIV-infected subjects with differential outcomes. Despite sustained recognition of autologous virus, HIV-specific proliferative and cytolytic T cell effector functions became selectively and intrinsically impaired prior to aborted control. Longitudinal transcriptomic profiling of functionally impaired HIV-specific CD8 + T cells revealed altered expression of genes related to activation, cytokine-mediated signaling, and cell cycle regulation, including increased expression of the antiproliferative transcription factor KLF2 but not of genes associated with canonical exhaustion. Lymphoid HIV-specific CD8 + T cells also exhibited poor functionality during aborted control relative to durable control. Our results identify selective functional impairment of HIV-specific CD8 + T cells as prognostic of impending aborted HIV control, with implications for clinical monitoring and immunotherapeutic strategies., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

28. Human genetic variation in HIV disease: beyond genome-wide association studies

Author

Jacques Fellay and Paul J. McLaren

Subjects

Genetics, Candidate gene, Oncology (nursing), Immunology, Genetic Variation, HIV Infections, Genomics, Genome-wide association study, HIV acquisition, Hematology, Human genetic variation, Computational biology, Disease, Biology, Genome, 3. Good health, Infectious Diseases, Oncology, Virology, Genetic variation, Humans, genetics, HIV control, Genetic association

Abstract

PURPOSE OF REVIEW: Rapid expansion of genomic technologies has resulted in an unprecedented ability to interrogate the impact of human genetic variation on disease. HIV-1 infection is a unique model for studying this impact because host genetic variation influences both clinical outcome and the genetic sequence and evolution of the pathogen itself. RECENT FINDINGS: Several candidate gene studies have proposed novel associations with HIV acquisition and/or disease progression; however, many of these are not supported by larger genome-wide association studies. Thus, controversy remains as to which host and viral genetic factors truly impact HIV infection. Novel methods for assessing the genetic (viral and host) component of disease progression are becoming important areas of investigation. SUMMARY: To fully understand the impact of human genetic variation in HIV disease, the field will need to come together to set a standard for discovery of new genes. Additionally, novel avenues of investigation such as sequencing studies (to define the role of rare variants), studies of epistasis and host/viral genome interaction will be of great value

Published

2015

29. Role of Different Subpopulations of CD8+ T Cells during HIV Exposure and Infection

Author

Sandra Milena Gonzalez, Natalia Andrea Taborda, and María Teresa Rugeles

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, Immunology, Context (language use), Review, natural resistance to HIV, Biology, CD38, CD8+ T cells, Jurkat cells, 03 medical and health sciences, Interleukin 21, Immune system, spontaneous control of HIV replication, Human immunodeficiency viruses, Immunology and Allergy, Cytotoxic T cell, HIV control, Antiviral immune response, Effector, HIV infection, Virology, 030104 developmental biology, CD8+ T cells subpopulations, antiviral immune response, lcsh:RC581-607, CD8, Resistance to HIV

Abstract

ABSTARCT: During HIV infection, specific responses exhibited by CD8+ T cells are crucial to establish an early, effective, and sustained viral control, preventing severe immune alterations and organ dysfunction. Several CD8+ T cells subsets have been identified, exhibiting differences in terms of activation, functional profile, and ability to limit HIV replication. Some of the most important CD8+ T cells subsets associated with viral control, production of potent antiviral molecules, and strong polyfunctional responses include Th1-like cytokine pattern and Tc17 cells. In addition, the expression of specific activation markers has been also associated with a more effective response of CD8+ T cells, as evidenced in HLA-DR+ CD38- cells. CD8+ T cells in both, peripheral blood and gut mucosa, are particularly important in individuals with a resistant phenotype, including HIV-exposed seronegative individuals (HESNs), long-term non-progressors (LTNPs) and HIV-controllers. Although the role of CD8+ T cells has been extensively explored in the context of an established HIV-1 infection, the presence of HIV-specific cells with effector abilities and a defined functional profile in HESNs, remain poorly understood. Here, we reviewed studies carried out on different subpopulations of CD8+ T cells in relation with natural resistance to HIV infection and progression. Keywords: CD8+ T cells subpopulations, HIV infection, Natural resistance to HIV, spontaneous control of HIV replication, antiviral immune response

Published

2017

30. Human leukocyte antigen B*57 does not fully explain hepatitis C clearance in HIV controllers

Author

Michael P. Busch, Tzong-Hae Lee, Jeffrey N. Martin, Steven G. Deeks, Alice Asher, Kimberly Page, Jennifer L. Evans, Peter W. Hunt, Glenn-Milo Santos, Leslie H. Tobler, and Emily K Dokubo

Subjects

Male, hepatitis C virus, HIV Infections, medicine.disease_cause, Medical and Health Sciences, Hepatitis, Cohort Studies, Gene Frequency, Genotype, Immunology and Allergy, Viral, Prospective Studies, Liver Disease, human leukocyte antigen type, virus diseases, Hepatitis C, Middle Aged, Biological Sciences, HLA-B, spontaneous clearance, Infectious Diseases, HIV/AIDS, Female, Infection, Adult, Hepatitis C virus, Immunology, Chronic Liver Disease and Cirrhosis, Human leukocyte antigen, Biology, Virus, HIV Long-Term Survivors, Hepatitis - C, Clinical Research, Virology, medicine, HLA-B Antigens, Genetics, Humans, HIV control, Psychology and Cognitive Sciences, Hepatitis C Antibodies, medicine.disease, Emerging Infectious Diseases, Good Health and Well Being, RNA, Digestive Diseases

Abstract

A small percentage (1-5%) of people living with HIV are able to intrinsically control their HIV infection over long periods of time without the use of antiviral therapy (ART) [1]. Two groups of “HIV controllers” have been described: (1) Elite controllers, who have HIV antibodies (anti-HIV), but plasma HIV RNA levels below the detection limits of commercially available assays, and; (2) Viremic controllers, who have measurable, but very low levels of HIV RNA (< 2000 copies/mL). HIV controllers represent “outliers” in the clinical HIV spectrum, and are considered very important for studies of host immunological and genetic factors that control viral replication, with the expectation that they will inform vaccine and drug development, or perhaps identify strategies to achieve a “functional cure [1, 2].” Interestingly, HIV controllers may also be more likely to spontaneously clear hepatitis C virus (HCV) infection. While not observed in all studies [3, 4], most studies suggest a significantly higher rate of spontaneous HCV clearance in HIV controllers (23-39%) [5, 6] than in monoinfected groups (25%) [7] and HIV non-controllers (6.6%-10%) [1, 5]. This has led several groups to examine host genetic factors that might contribute to the control of both virus infections. For example, HLA B*57, the major histocompatibility class I allele, is highly enriched in HIV controllers and is also associated with spontaneous HCV clearance [8-10]. In contrast, HLA Cw*04 has been associated with faster progression of both HIV disease and chronic HCV infection [11, 12]. The IL28B CC genotype has been shown to be significantly associated with spontaneous control of HCV [13-16], conferring as much as 3.1 higher odds of clearance compared to CT and TT genotypes [17, 18]. Whether the CC genotype of IL28B is also enriched in HIV controllers remains controversial. A relatively small Spanish study found that the CC genotype of IL28B was enriched in Caucasian HIV controllers relative to non-controllers [4], while other studies in primarily African-American cohorts have not observed this [6, 19]. Furthermore, none of the much larger genome-wide association studies have found an association between the IL28B (CC) genotype and HIV control, at least at the genome-wide level of significance [20-23]. In one study the IL28B CC genotype has been associated with higher all-cause mortality among all people living with HIV [24]. In this study, we investigated the degree to which spontaneous clearance of HCV could be explained by HLA B*57 and/or IL28B CC genotype in a well characterized cohort of HIV controllers.

Published

2013

31. Elite controller CD8+ T cells exhibit comparable viral inhibition capacity, but better sustained effector properties compared to chronic progressors.

Author

Shasha D, Karel D, Angiuli O, Greenblatt A, Ghebremichael M, Yu X, Porichis F, and Walker BD

Subjects

Antiretroviral Therapy, Highly Active, Apoptosis, Cells, Cultured, Cryopreservation, Cytotoxicity, Immunologic, Disease Progression, HIV physiology, HIV Infections drug therapy, Humans, Interleukin-15 pharmacology, T-Cell Antigen Receptor Specificity, Virus Replication, CD8-Positive T-Lymphocytes immunology, HIV immunology, HIV Infections immunology, T-Lymphocyte Subsets immunology

Abstract

Mechanisms modulating HIV-specific CD8+ T cell-mediated viral inhibition are not well defined. To delineate features of effective control, we compared the ability of CD8 + T cells from HIV ECs and CPs to inhibit HIV ex vivo. ECs showed superior inhibition compared to HAART-treated or untreated CPs in a typical VIA in which CD8+ T cells are rested 3 d before use (P = 0.025). In contrast, comparable antiviral activity was observed in freshly thawed cells. Rested CD8 + T cells underwent apoptosis with preferential loss of HIV-specific cells. EC CD8 + T cells showed greater capacity to sustain polyfunctionality ex vivo compared with those of CPs, and incubation of CD8 + T cells with IL-15 augmented inhibition. These results indicate that superior ex vivo inhibition of viral replication by CD8 + T cells from ECs is associated with enhanced retention of functional qualities and that in vitro antiviral function is enhanced by IL-15., (© Society for Leukocyte Biology.)

Published

2016