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1. Impact of early antiretroviral treatment on sexual behaviour:A randomised comparison

Author

Lampe, Fiona C., Rodger, Alison J., Burman, William, Grulich, Andrew, Friedland, Gerald, Sadr, Wafaa El, Neaton, James, Corbelli, Giulio M., Emery, Sean, Molina, Jean Michel, Orkin, Chloe, Gatell, Jose, Gerstoft, Jan, Ruxrungtham, Kiat, Barbosa De Souza, Monica, Phillips, Andrew N., Lampe, Fiona C., Rodger, Alison J., Burman, William, Grulich, Andrew, Friedland, Gerald, Sadr, Wafaa El, Neaton, James, Corbelli, Giulio M., Emery, Sean, Molina, Jean Michel, Orkin, Chloe, Gatell, Jose, Gerstoft, Jan, Ruxrungtham, Kiat, Barbosa De Souza, Monica, and Phillips, Andrew N.

Published
2019

2. Strategies used by gay male HIV serodiscordant couples to reduce the risk of HIV transmission from anal intercourse in three countries

Author

Bavinton, BR ; https://orcid.org/0000-0001-5834-8278, Prestage, GP ; https://orcid.org/0000-0003-3917-8992, Jin, F ; https://orcid.org/0000-0002-8573-637X, Phanuphak, N, Grinsztejn, B, Fairley, CK, Baker, D, Hoy, J, Templeton, DJ ; https://orcid.org/0000-0003-2157-9587, Tee, BK, Kelleher, A ; https://orcid.org/0000-0002-0009-3337, Grulich, AE, Zablotska-Manos, Iryna, Cooper, David ; https://orcid.org/0000-0002-6031-6678, Triffitt, Kathy, Bloch, Mark ; https://orcid.org/0000-0002-1143-5013, McNulty, Anna, Pell, Catherine, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Bavinton, BR ; https://orcid.org/0000-0001-5834-8278, Prestage, GP ; https://orcid.org/0000-0003-3917-8992, Jin, F ; https://orcid.org/0000-0002-8573-637X, Phanuphak, N, Grinsztejn, B, Fairley, CK, Baker, D, Hoy, J, Templeton, DJ ; https://orcid.org/0000-0003-2157-9587, Tee, BK, Kelleher, A ; https://orcid.org/0000-0002-0009-3337, Grulich, AE, Zablotska-Manos, Iryna, Cooper, David ; https://orcid.org/0000-0002-6031-6678, Triffitt, Kathy, Bloch, Mark ; https://orcid.org/0000-0002-1143-5013, McNulty, Anna, Pell, Catherine, and Emery, Sean ; https://orcid.org/0000-0001-6072-8309

Abstract

Introduction: There are few data about the range of strategies used to prevent sexual HIV transmission within gay male serodiscordant couples. We examined HIV prevention strategies used by such couples and compared differences between countries. Methods: Opposites Attract was a cohort study of male serodiscordant couples in Australia, Brazil and Thailand, from May 2014 (Australia) or May 2016 (Brazil/Thailand) to December 2016. At visits, HIV-positive partners had viral load (VL) tested; HIV-negative partners reported sexual behaviour and perceptions of their HIV-positive partner's VL results. Within-couple acts of condomless anal intercourse (CLAI) were categorized by strategy: condom-protected, biomedically protected (undetectable VL and/or pre-exposure prophylaxis [PrEP]), or not protected by either (HIV-negative partners engaging in insertive CLAI, receptive CLAI with withdrawal, or receptive CLAI with ejaculation). Results: A total of 343 couples were included in this analysis (153 in Australia, 93 in Brazil and 97 in Thailand). Three-quarters of HIV-positive partners were consistently virally suppressed (<200 copies/mL) during follow-up, and HIV-negative partners had correct perceptions of their partner's VL result for 76.5% of tests. One-third of HIV-negative partners used daily PrEP during follow-up. Over follow-up, 73.8% of couples had CLAI. HIV-negative partners reported 31,532 acts of anal intercourse with their HIV-positive partner. Of these, 46.7% were protected by condoms, 48.6% by a biomedical strategy and 4.7% of acts were not protected by these strategies. Australian couples had fewer condom-protected acts and a higher proportion of biomedically protected acts than Brazilian and Thai couples. Of the 1473 CLAI acts where the perceived VL was detectable/unknown and were not protected by PrEP (4.7% of all acts), two-thirds (n = 983) were when the HIV-negative partner was insertive (strategic positioning). Of the 490 acts when the HIV-negative partner w

Published
2019

3. Using clinical research networks to assess severity of an emerging influenza pandemic

Author

Simonsen, L, Higgs, E, Taylor, RJ, Wentworth, D, Cozzi-Lepri, A, Pett, S, Dwyer, DE, Davey, R, Lynfield, R, Losso, M, Morales, K, Glesby, MJ, Weckx, J, Carey, D ; https://orcid.org/0000-0003-0156-8143, Lane, C, Lundgren, J, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Simonsen, L, Higgs, E, Taylor, RJ, Wentworth, D, Cozzi-Lepri, A, Pett, S, Dwyer, DE, Davey, R, Lynfield, R, Losso, M, Morales, K, Glesby, MJ, Weckx, J, Carey, D ; https://orcid.org/0000-0003-0156-8143, Lane, C, Lundgren, J, and Emery, Sean ; https://orcid.org/0000-0001-6072-8309

Abstract

Background Early clinical severity assessments during the 2009 influenza A H1N1 pandemic (pH1N1) overestimated clinical severity due to selection bias and other factors. We retrospectively investigated how to use data from the International Network for Strategic Initiatives in Global HIV Trials, a global clinical influenza research network, to make more accurate case fatality ratio (CFR) estimates early in a future pandemic, an essential part of pandemic response. Methods We estimated the CFR of medically attended influenza (CFR MA) as the product of probability of hospitalization given confirmed outpatient influenza and the probability of death given hospitalization with confirmed influenza for the pandemic (2009-2011) and post-pandemic (2012-2015) periods. We used literature survey results on health-seeking behavior to convert that estimate to CFR among all infected persons (CFR AR). Results During the pandemic period, 5.0% (3.1%-6.9%) of 561 pH1N1-positive outpatients were hospitalized. Of 282 pH1N1-positive inpatients, 8.5% (5.7%-12.6%) died. CFR MA for pH1N1 was 0.4% (0.2%-0.6%) in the pandemic period 2009-2011 but declined 5-fold in young adults during the post-pandemic period compared to the level of seasonal influenza in the post-pandemic period 2012-2015. CFR for influenza-negative patients did not change over time. We estimated the 2009 pandemic CFR AR to be 0.025%, 16-fold lower than CFR MA. Conclusions Data from a clinical research network yielded accurate pandemic severity estimates, including increased severity among younger people. Going forward, clinical research networks with a global presence and standardized protocols would substantially aid rapid assessment of clinical severity. Clinical Trials Registration NCT01056354 and NCT010561.

Published
2018

4. In silico thrombin generation:Plasma composition imbalance and mortality in human immunodeficiency virus

Author

Brummel-Ziedins, Kathleen E, Gissel, Matthew, Neuhaus, Jacqueline, Borges, Álvaro H, Chadwick, David R, Emery, Sean, Neaton, James D, Tracy, Russell P, Baker, Jason V, Brummel-Ziedins, Kathleen E, Gissel, Matthew, Neuhaus, Jacqueline, Borges, Álvaro H, Chadwick, David R, Emery, Sean, Neaton, James D, Tracy, Russell P, and Baker, Jason V

Abstract

Background: Effective HIV treatment with antiretroviral therapy has prolonged survival and shifted causes of death to non-AIDS illnesses such as cardiovascular disease. We have shown that inflammation and HIV viral load associate with pro- and anticoagulant factor imbalances resulting in increased thrombin generation when mathematically modeled. We explore the hypothesis that factor compositional imbalance, corresponding to increased in silico thrombin generation, predicts mortality among HIV+ persons.Methods: In a nested case-control study of HIV+ individuals on continuous antiretroviral therapy in two large trials, we evaluated cases (any non-violent mortality, n = 114) and matched controls (n = 318). Thrombin generation in response to a tissue-factor initiator for each individual was calculated by a mathematical model incorporating levels of factors (F)II, V, VII, VIII, IX, X, antithrombin, tissue factor pathway inhibitor, and protein C (PC) measured at study entry to the trials. In silico thrombin generation metrics included clot time, maximum rate (MaxR), maximum level (MaxL), and area under the curve (AUC).Results: Levels of antithrombin and PC decreased, while FV and FVIII were higher in cases vs controls. This resulted in a more procoagulant phenotype with increased MaxR, MaxL, and AUC in cases compared to controls (P < 0.05 for all).Conclusions: Antithrombin, FV, FVIII, and PC were the major contributors to the increased thrombin generation associated with mortality risk. Our results suggest that mortality in HIV is associated with an increase in in silico thrombin generation via altered balance of pro- and anticoagulant factors, likely due to an inflammatory response signal, and resulting coagulopathy.

Published
2018

5. In silico thrombin generation:Plasma composition imbalance and mortality in human immunodeficiency virus

Author

Brummel-Ziedins, Kathleen E, Gissel, Matthew, Neuhaus, Jacqueline, Borges, Álvaro H, Chadwick, David R, Emery, Sean, Neaton, James D, Tracy, Russell P, Baker, Jason V, Brummel-Ziedins, Kathleen E, Gissel, Matthew, Neuhaus, Jacqueline, Borges, Álvaro H, Chadwick, David R, Emery, Sean, Neaton, James D, Tracy, Russell P, and Baker, Jason V

Abstract

Background: Effective HIV treatment with antiretroviral therapy has prolonged survival and shifted causes of death to non-AIDS illnesses such as cardiovascular disease. We have shown that inflammation and HIV viral load associate with pro- and anticoagulant factor imbalances resulting in increased thrombin generation when mathematically modeled. We explore the hypothesis that factor compositional imbalance, corresponding to increased in silico thrombin generation, predicts mortality among HIV+ persons.Methods: In a nested case-control study of HIV+ individuals on continuous antiretroviral therapy in two large trials, we evaluated cases (any non-violent mortality, n = 114) and matched controls (n = 318). Thrombin generation in response to a tissue-factor initiator for each individual was calculated by a mathematical model incorporating levels of factors (F)II, V, VII, VIII, IX, X, antithrombin, tissue factor pathway inhibitor, and protein C (PC) measured at study entry to the trials. In silico thrombin generation metrics included clot time, maximum rate (MaxR), maximum level (MaxL), and area under the curve (AUC).Results: Levels of antithrombin and PC decreased, while FV and FVIII were higher in cases vs controls. This resulted in a more procoagulant phenotype with increased MaxR, MaxL, and AUC in cases compared to controls (P < 0.05 for all).Conclusions: Antithrombin, FV, FVIII, and PC were the major contributors to the increased thrombin generation associated with mortality risk. Our results suggest that mortality in HIV is associated with an increase in in silico thrombin generation via altered balance of pro- and anticoagulant factors, likely due to an inflammatory response signal, and resulting coagulopathy.

Published
2018

6. Anti-HIV-1 ADCC Antibodies following Latency Reversal and Treatment Interruption

Author

Lee, Wen Shi, Kristensen, Anne B., Rasmussen, Thomas A., Tolstrup, Martin, Ostergaard, Lars, Sogaard, Ole S., Wines, Bruce D., Hogarth, P. Mark, Reynaldi, Arnold, Davenport, Miles P., Emery, Sean, Amin, Janaki, Cooper, David A., Kan, Virginia L., Fox, Julie, Gruell, Henning, Parsons, Matthew S., Kent, Stephen J., Lee, Wen Shi, Kristensen, Anne B., Rasmussen, Thomas A., Tolstrup, Martin, Ostergaard, Lars, Sogaard, Ole S., Wines, Bruce D., Hogarth, P. Mark, Reynaldi, Arnold, Davenport, Miles P., Emery, Sean, Amin, Janaki, Cooper, David A., Kan, Virginia L., Fox, Julie, Gruell, Henning, Parsons, Matthew S., and Kent, Stephen J.

Abstract

There is growing interest in utilizing antibody-dependent cellular cytotoxicity (ADCC) to eliminate infected cells following reactivation from HIV-1 latency. A potential barrier is that HIV-1-specific ADCC antibodies decline in patients on long-term antiretroviral therapy (ART) and may not be sufficient to eliminate reactivated latently infected cells. It is not known whether reactivation from latency with latency-reversing agents (LRAs) could provide sufficient antigenic stimulus to boost HIV-1-specific ADCC. We found that treatment with the LRA panobinostat or a short analytical treatment interruption (ATI), 21 to 59 days, was not sufficient to stimulate an increase in ADCC-competent antibodies, despite viral rebound in all subjects who underwent the short ATI. In contrast, a longer ATI, 2 to 12 months, among subjects enrolled in the Strategies for Management of Antiretroviral Therapy (SMART) trial robustly boosted HIV-1 gp120-specific Fc receptor-binding antibodies and ADCC against HIV-1-infected cells in vitro. These results show that there is a lag between viral recrudescence and the boosting of ADCC antibodies, which has implications for strategies toward eliminating latently infected cells. IMPORTANCE The shock and kill HIV-1 cure strategy aims to reactivate HIV-1 expression in latently infected cells and subsequently eliminate the reactivated cells through immune-mediated killing. Several latency reversing agents (LRAs) have been examined in vivo, but LRAs alone have not been able to achieve HIV-1 remission and prevent viral rebound following analytical treatment interruption (ATI). In this study, we examined whether LRA treatment or ATI can provide sufficient antigenic stimulus to boost HIV-1-specific functional antibodies that can eliminate HIV-1-infected cells. Our study has implications for the antigenic stimulus required for antilatency strategies and/or therapeutic vaccines to boost functional antibodies and assist in eliminating the latent reservoir.

Published
2017

7. Anti-HIV-1 ADCC Antibodies following Latency Reversal and Treatment Interruption

Author

Lee, Wen Shi, Kristensen, Anne B., Rasmussen, Thomas A., Tolstrup, Martin, Ostergaard, Lars, Sogaard, Ole S., Wines, Bruce D., Hogarth, P. Mark, Reynaldi, Arnold, Davenport, Miles P., Emery, Sean, Amin, Janaki, Cooper, David A., Kan, Virginia L., Fox, Julie, Gruell, Henning, Parsons, Matthew S., Kent, Stephen J., Lee, Wen Shi, Kristensen, Anne B., Rasmussen, Thomas A., Tolstrup, Martin, Ostergaard, Lars, Sogaard, Ole S., Wines, Bruce D., Hogarth, P. Mark, Reynaldi, Arnold, Davenport, Miles P., Emery, Sean, Amin, Janaki, Cooper, David A., Kan, Virginia L., Fox, Julie, Gruell, Henning, Parsons, Matthew S., and Kent, Stephen J.

Abstract

There is growing interest in utilizing antibody-dependent cellular cytotoxicity (ADCC) to eliminate infected cells following reactivation from HIV-1 latency. A potential barrier is that HIV-1-specific ADCC antibodies decline in patients on long-term antiretroviral therapy (ART) and may not be sufficient to eliminate reactivated latently infected cells. It is not known whether reactivation from latency with latency-reversing agents (LRAs) could provide sufficient antigenic stimulus to boost HIV-1-specific ADCC. We found that treatment with the LRA panobinostat or a short analytical treatment interruption (ATI), 21 to 59 days, was not sufficient to stimulate an increase in ADCC-competent antibodies, despite viral rebound in all subjects who underwent the short ATI. In contrast, a longer ATI, 2 to 12 months, among subjects enrolled in the Strategies for Management of Antiretroviral Therapy (SMART) trial robustly boosted HIV-1 gp120-specific Fc receptor-binding antibodies and ADCC against HIV-1-infected cells in vitro. These results show that there is a lag between viral recrudescence and the boosting of ADCC antibodies, which has implications for strategies toward eliminating latently infected cells. IMPORTANCE The shock and kill HIV-1 cure strategy aims to reactivate HIV-1 expression in latently infected cells and subsequently eliminate the reactivated cells through immune-mediated killing. Several latency reversing agents (LRAs) have been examined in vivo, but LRAs alone have not been able to achieve HIV-1 remission and prevent viral rebound following analytical treatment interruption (ATI). In this study, we examined whether LRA treatment or ATI can provide sufficient antigenic stimulus to boost HIV-1-specific functional antibodies that can eliminate HIV-1-infected cells. Our study has implications for the antigenic stimulus required for antilatency strategies and/or therapeutic vaccines to boost functional antibodies and assist in eliminating the latent reservoir.

Published
2017

8. Comparison of the Outcomes of Individuals With Medically Attended Influenza A and B Virus Infections Enrolled in 2 International Cohort Studies Over a 6-Year Period:2009-2015

Author

Dwyer, Dominic E, Lynfield, Ruth, Losso, Marcelo H, Davey, Richard T, Cozzi-Lepri, Alessandro, Wentworth, Deborah, Uyeki, Timothy M, Gordin, Fred, Angus, Brian, Qvist, Tavs, Emery, Sean, Lundgren, Jens, Neaton, James D, Dwyer, Dominic E, Lynfield, Ruth, Losso, Marcelo H, Davey, Richard T, Cozzi-Lepri, Alessandro, Wentworth, Deborah, Uyeki, Timothy M, Gordin, Fred, Angus, Brian, Qvist, Tavs, Emery, Sean, Lundgren, Jens, and Neaton, James D

Abstract

Background: Outcome data from prospective follow-up studies comparing infections with different influenza virus types/subtypes are limited.Methods: Demographic, clinical characteristics and follow-up outcomes for adults with laboratory-confirmed influenza A(H1N1)pdm09, A(H3N2), or B virus infections were compared in 2 prospective cohorts enrolled globally from 2009 through 2015. Logistic regression was used to compare outcomes among influenza virus type/subtypes.Results: Of 3952 outpatients, 1290 (32.6%) had A(H1N1)pdm09 virus infection, 1857 (47.0%) had A(H3N2), and 805 (20.4%) had influenza B. Of 1398 inpatients, 641 (45.8%) had A(H1N1)pdm09, 532 (38.1%) had A(H3N2), and 225 (16.1%) had influenza B. Outpatients with A(H1N1)pdm09 were younger with fewer comorbidities and were more likely to be hospitalized during the 14-day follow-up (3.3%) than influenza B (2.2%) or A(H3N2) (0.7%; P < .0001). Hospitalized patients with A(H1N1)pdm09 (20.3%) were more likely to be enrolled from intensive care units (ICUs) than those with A(H3N2) (11.3%) or B (9.8%; P < .0001). However, 60-day follow-up of discharged inpatients showed no difference in disease progression (P = .32) or all-cause mortality (P = .30) among influenza types/subtypes. These findings were consistent after covariate adjustment, in sensitivity analyses, and for subgroups defined by age, enrollment location, and comorbidities.Conclusions: Outpatients infected with influenza A(H1N1)pdm09 or influenza B were more likely to be hospitalized than those with A(H3N2). Hospitalized patients infected with A(H1N1)pdm09 were younger and more likely to have severe disease at study entry (measured by ICU enrollment), but did not have worse 60-day outcomes.

Published
2017

9. Systemic Inflammation, Coagulation, and Clinical Risk in the START Trial

Author

Baker, Jason V, Sharma, Shweta, Grund, Birgit, Rupert, Adam, Metcalf, Julia A, Schechter, Mauro, Munderi, Paula, Aho, Inka, Emery, Sean, Babiker, Abdel, Phillips, Andrew, Lundgren, Jens D, Neaton, James D, Lane, H Clifford, Baker, Jason V, Sharma, Shweta, Grund, Birgit, Rupert, Adam, Metcalf, Julia A, Schechter, Mauro, Munderi, Paula, Aho, Inka, Emery, Sean, Babiker, Abdel, Phillips, Andrew, Lundgren, Jens D, Neaton, James D, and Lane, H Clifford

Abstract

Background: The Strategic Timing of AntiRetroviral Treatment (START) trial demonstrated that immediate (at CD4+ >500 cells/µL) vs deferred (to CD4+ <350 cells/µL or AIDS) antiretroviral therapy (ART) initiation reduced risk for AIDS and serious non-AIDS (SNA). We investigated associations of inflammation, coagulation, and vascular injury biomarkers with AIDS, SNA or death, and the effect of immediate ART initiation.Methods: Biomarkers were measured from stored plasma prior to randomization and at month 8. Associations of baseline biomarkers with event risk were estimated with Cox regression, pooled across groups, adjusted for age, gender, and treatment group, and stratified by region. Mean changes over 8 months were estimated and compared between the immediate and deferred ART arms using analysis of covariance models, adjusted for levels at entry.Results: Baseline biomarker levels were available for 4299 START participants (92%). Mean follow-up was 3.2 years. Higher levels of IL-6 and D-dimer were the only biomarkers associated with risk for AIDS, SNA or death, as well as the individual components of SNA and AIDS events (HRs ranged 1.37-1.41 per 2-fold higher level), even after adjustment for baseline CD4+ count, HIV RNA level, and other biomarkers. At month 8, biomarker levels were lower in the immediate arm by 12%-21%.Conclusions: These data, combined with evidence from prior biomarker studies, demonstrate that IL-6 and D-dimer consistently predict clinical risk across a broad spectrum of CD4 counts for those both ART-naïve and treated. Research is needed to identify disease-modifying treatments that target inflammation beyond the effects of ART.

Published
2017

10. Changes in Cardiovascular Disease Risk Factors With Immediate Versus Deferred Antiretroviral Therapy Initiation Among HIV-Positive Participants in the START (Strategic Timing of Antiretroviral Treatment) Trial

Author

Baker, Jason V, Sharma, Shweta, Achhra, Amit C, Bernardino, Jose Ignacio, Bogner, Johannes R, Duprez, Daniel, Emery, Sean, Gazzard, Brian, Gordin, Jonathan, Grandits, Greg, Phillips, Andrew N, Schwarze, Siegfried, Soliman, Elsayed Z, Spector, Stephen A, Tambussi, Giuseppe, Lundgren, Jens, Baker, Jason V, Sharma, Shweta, Achhra, Amit C, Bernardino, Jose Ignacio, Bogner, Johannes R, Duprez, Daniel, Emery, Sean, Gazzard, Brian, Gordin, Jonathan, Grandits, Greg, Phillips, Andrew N, Schwarze, Siegfried, Soliman, Elsayed Z, Spector, Stephen A, Tambussi, Giuseppe, and Lundgren, Jens

Abstract

INTRODUCTION: HIV infection and certain antiretroviral therapy (ART) medications increase atherosclerotic cardiovascular disease risk, mediated, in part, through traditional cardiovascular disease risk factors.METHODS AND RESULTS: We studied cardiovascular disease risk factor changes in the START (Strategic Timing of Antiretroviral Treatment) trial, a randomized study of immediate versus deferred ART initiation among HIV-positive persons with CD4+ cell counts >500 cells/mm3. Mean change from baseline in risk factors and the incidence of comorbid conditions were compared between groups. The characteristics among 4685 HIV-positive START trial participants include a median age of 36 years, a CD4 cell count of 651 cells/mm3, an HIV viral load of 12 759 copies/mL, a current smoking status of 32%, a median systolic/diastolic blood pressure of 120/76 mm Hg, and median levels of total cholesterol of 168 mg/dL, low-density lipoprotein cholesterol of 102 mg/dL, and high-density lipoprotein cholesterol of 41 mg/dL. Mean follow-up was 3.0 years. The immediate and deferred ART groups spent 94% and 28% of follow-up time taking ART, respectively. Compared with patients in the deferral group, patients in the immediate ART group had increased total cholesterol and low-density lipoprotein cholesterol and higher use of lipid-lowering therapy (1.2%; 95% CI, 0.1-2.2). Concurrent increases in high-density lipoprotein cholesterol with immediate ART resulted in a 0.1 lower total cholesterol to high-density lipoprotein cholesterol ratio (95% CI, 0.1-0.2). Immediate ART resulted in 2.3% less BP-lowering therapy use (95% CI, 0.9-3.6), but there were no differences in new-onset hypertension or diabetes mellitus.CONCLUSIONS: Among HIV-positive persons with preserved immunity, immediate ART led to increases in total cholesterol and low-density lipoprotein cholesterol but also concurrent increases in high-density lipoprotein cholesterol and decreased use of blood pressure medi

Published
2017

11. Changes in Cardiovascular Disease Risk Factors With Immediate Versus Deferred Antiretroviral Therapy Initiation Among HIV-Positive Participants in the START (Strategic Timing of Antiretroviral Treatment) Trial

Author

Baker, Jason V, Sharma, Shweta, Achhra, Amit C, Bernardino, Jose Ignacio, Bogner, Johannes R, Duprez, Daniel, Emery, Sean, Gazzard, Brian, Gordin, Jonathan, Grandits, Greg, Phillips, Andrew N, Schwarze, Siegfried, Soliman, Elsayed Z, Spector, Stephen A, Tambussi, Giuseppe, Lundgren, Jens, Baker, Jason V, Sharma, Shweta, Achhra, Amit C, Bernardino, Jose Ignacio, Bogner, Johannes R, Duprez, Daniel, Emery, Sean, Gazzard, Brian, Gordin, Jonathan, Grandits, Greg, Phillips, Andrew N, Schwarze, Siegfried, Soliman, Elsayed Z, Spector, Stephen A, Tambussi, Giuseppe, and Lundgren, Jens

Abstract

INTRODUCTION: HIV infection and certain antiretroviral therapy (ART) medications increase atherosclerotic cardiovascular disease risk, mediated, in part, through traditional cardiovascular disease risk factors.METHODS AND RESULTS: We studied cardiovascular disease risk factor changes in the START (Strategic Timing of Antiretroviral Treatment) trial, a randomized study of immediate versus deferred ART initiation among HIV-positive persons with CD4+ cell counts >500 cells/mm3. Mean change from baseline in risk factors and the incidence of comorbid conditions were compared between groups. The characteristics among 4685 HIV-positive START trial participants include a median age of 36 years, a CD4 cell count of 651 cells/mm3, an HIV viral load of 12 759 copies/mL, a current smoking status of 32%, a median systolic/diastolic blood pressure of 120/76 mm Hg, and median levels of total cholesterol of 168 mg/dL, low-density lipoprotein cholesterol of 102 mg/dL, and high-density lipoprotein cholesterol of 41 mg/dL. Mean follow-up was 3.0 years. The immediate and deferred ART groups spent 94% and 28% of follow-up time taking ART, respectively. Compared with patients in the deferral group, patients in the immediate ART group had increased total cholesterol and low-density lipoprotein cholesterol and higher use of lipid-lowering therapy (1.2%; 95% CI, 0.1-2.2). Concurrent increases in high-density lipoprotein cholesterol with immediate ART resulted in a 0.1 lower total cholesterol to high-density lipoprotein cholesterol ratio (95% CI, 0.1-0.2). Immediate ART resulted in 2.3% less BP-lowering therapy use (95% CI, 0.9-3.6), but there were no differences in new-onset hypertension or diabetes mellitus.CONCLUSIONS: Among HIV-positive persons with preserved immunity, immediate ART led to increases in total cholesterol and low-density lipoprotein cholesterol but also concurrent increases in high-density lipoprotein cholesterol and decreased use of blood pressure medi

Published
2017

12. Systemic Inflammation, Coagulation, and Clinical Risk in the START Trial

Author

Baker, Jason V, Sharma, Shweta, Grund, Birgit, Rupert, Adam, Metcalf, Julia A, Schechter, Mauro, Munderi, Paula, Aho, Inka, Emery, Sean, Babiker, Abdel, Phillips, Andrew, Lundgren, Jens D, Neaton, James D, Lane, H Clifford, Baker, Jason V, Sharma, Shweta, Grund, Birgit, Rupert, Adam, Metcalf, Julia A, Schechter, Mauro, Munderi, Paula, Aho, Inka, Emery, Sean, Babiker, Abdel, Phillips, Andrew, Lundgren, Jens D, Neaton, James D, and Lane, H Clifford

Abstract

Background: The Strategic Timing of AntiRetroviral Treatment (START) trial demonstrated that immediate (at CD4+ >500 cells/µL) vs deferred (to CD4+ <350 cells/µL or AIDS) antiretroviral therapy (ART) initiation reduced risk for AIDS and serious non-AIDS (SNA). We investigated associations of inflammation, coagulation, and vascular injury biomarkers with AIDS, SNA or death, and the effect of immediate ART initiation.Methods: Biomarkers were measured from stored plasma prior to randomization and at month 8. Associations of baseline biomarkers with event risk were estimated with Cox regression, pooled across groups, adjusted for age, gender, and treatment group, and stratified by region. Mean changes over 8 months were estimated and compared between the immediate and deferred ART arms using analysis of covariance models, adjusted for levels at entry.Results: Baseline biomarker levels were available for 4299 START participants (92%). Mean follow-up was 3.2 years. Higher levels of IL-6 and D-dimer were the only biomarkers associated with risk for AIDS, SNA or death, as well as the individual components of SNA and AIDS events (HRs ranged 1.37-1.41 per 2-fold higher level), even after adjustment for baseline CD4+ count, HIV RNA level, and other biomarkers. At month 8, biomarker levels were lower in the immediate arm by 12%-21%.Conclusions: These data, combined with evidence from prior biomarker studies, demonstrate that IL-6 and D-dimer consistently predict clinical risk across a broad spectrum of CD4 counts for those both ART-naïve and treated. Research is needed to identify disease-modifying treatments that target inflammation beyond the effects of ART.

Published
2017

13. Comparison of the Outcomes of Individuals With Medically Attended Influenza A and B Virus Infections Enrolled in 2 International Cohort Studies Over a 6-Year Period:2009-2015

Author

Dwyer, Dominic E, Lynfield, Ruth, Losso, Marcelo H, Davey, Richard T, Cozzi-Lepri, Alessandro, Wentworth, Deborah, Uyeki, Timothy M, Gordin, Fred, Angus, Brian, Qvist, Tavs, Emery, Sean, Lundgren, Jens, Neaton, James D, Dwyer, Dominic E, Lynfield, Ruth, Losso, Marcelo H, Davey, Richard T, Cozzi-Lepri, Alessandro, Wentworth, Deborah, Uyeki, Timothy M, Gordin, Fred, Angus, Brian, Qvist, Tavs, Emery, Sean, Lundgren, Jens, and Neaton, James D

Abstract

Background: Outcome data from prospective follow-up studies comparing infections with different influenza virus types/subtypes are limited.Methods: Demographic, clinical characteristics and follow-up outcomes for adults with laboratory-confirmed influenza A(H1N1)pdm09, A(H3N2), or B virus infections were compared in 2 prospective cohorts enrolled globally from 2009 through 2015. Logistic regression was used to compare outcomes among influenza virus type/subtypes.Results: Of 3952 outpatients, 1290 (32.6%) had A(H1N1)pdm09 virus infection, 1857 (47.0%) had A(H3N2), and 805 (20.4%) had influenza B. Of 1398 inpatients, 641 (45.8%) had A(H1N1)pdm09, 532 (38.1%) had A(H3N2), and 225 (16.1%) had influenza B. Outpatients with A(H1N1)pdm09 were younger with fewer comorbidities and were more likely to be hospitalized during the 14-day follow-up (3.3%) than influenza B (2.2%) or A(H3N2) (0.7%; P < .0001). Hospitalized patients with A(H1N1)pdm09 (20.3%) were more likely to be enrolled from intensive care units (ICUs) than those with A(H3N2) (11.3%) or B (9.8%; P < .0001). However, 60-day follow-up of discharged inpatients showed no difference in disease progression (P = .32) or all-cause mortality (P = .30) among influenza types/subtypes. These findings were consistent after covariate adjustment, in sensitivity analyses, and for subgroups defined by age, enrollment location, and comorbidities.Conclusions: Outpatients infected with influenza A(H1N1)pdm09 or influenza B were more likely to be hospitalized than those with A(H3N2). Hospitalized patients infected with A(H1N1)pdm09 were younger and more likely to have severe disease at study entry (measured by ICU enrollment), but did not have worse 60-day outcomes.

Published
2017

14. Maraviroc, as a Switch Option, in HIV-1-infected Individuals With Stable, Well-controlled HIV Replication and R5-tropic Virus on Their First Nucleoside/Nucleotide Reverse Transcriptase Inhibitor Plus Ritonavir-boosted Protease Inhibitor Regimen: Week 48 Results of the Randomized, Multicenter MARCH Study

Author

Pett, Sarah Lilian, Amin, Janaki, Horban, Andrejz, Andrade-Villanueva, Jaime, Losso, Marcelo, Porteiro, Norma, Sierra Madero, Juan, Belloso, Waldo, Tu, Elise, Silk, David, Kelleher, Anthony, Harrigan, Richard, Clark, Andrew, Sugiura, Wataru, Wolff, Marcelo, Gill, John, Gatell, Jose, Fisher, Martin, Clarke, Amanda, Ruxrungtham, Kiat, Prazuck, Thierry, Kaiser, Rolf, Woolley, Ian, Alberto Arnaiz, Juan, Cooper, David, Rockstroh, Jurgen K., Mallon, Patrick, Emery, Sean, Pett, Sarah Lilian, Amin, Janaki, Horban, Andrejz, Andrade-Villanueva, Jaime, Losso, Marcelo, Porteiro, Norma, Sierra Madero, Juan, Belloso, Waldo, Tu, Elise, Silk, David, Kelleher, Anthony, Harrigan, Richard, Clark, Andrew, Sugiura, Wataru, Wolff, Marcelo, Gill, John, Gatell, Jose, Fisher, Martin, Clarke, Amanda, Ruxrungtham, Kiat, Prazuck, Thierry, Kaiser, Rolf, Woolley, Ian, Alberto Arnaiz, Juan, Cooper, David, Rockstroh, Jurgen K., Mallon, Patrick, and Emery, Sean

Abstract

Background. Alternative combination antiretroviral therapies in virologically suppressed human immunodeficiency virus (HIV)-infected patients experiencing side effects and/or at ongoing risk of important comorbidities from current therapy are needed. Maraviroc (MVC), a chemokine receptor 5 antagonist, is a potential alternative component of therapy in those with R5-tropic virus. Methods. The Maraviroc Switch Study is a randomized, multicenter, 96-week, open-label switch study in HIV type 1-infected adults with R5-tropic virus, virologically suppressed on a ritonavir-boosted protease inhibitor (PI/r) plus double nucleoside/nucleotide reverse transcriptase inhibitor (2 N(t)RTI) backbone. Participants were randomized 1: 2: 2 to current combination antiretroviral therapy (control), or replacing the protease inhibitor (MVC + 2 N(t)RTI arm) or the nucleoside reverse transcriptase inhibitor backbone (MVC + PI/r arm) with twice-daily MVC. The primary endpoint was the difference (switch minus control) in proportion with plasma viral load (VL) <200copies/mL at 48 weeks. The switch arms were judged noninferior if the lower limit of the 95% confidence interval (CI) for the difference in the primary endpoint was <-12% in the intention-to-treat (ITT) population. Results. The ITT population comprised 395 participants (control, n = 82; MVC + 2 N(t) RTI, n = 156; MVC + PI/r, n = 157). Baseline characteristics were well matched. At week 48, noninferior rates of virological suppression were observed in those switching away from a PI/r (93.6% [95% CI, -9.0% to 2.2%] and 91.7% [95% CI, -9.6% to 3.8%] with VL <200 and <50 copies/mL, respectively) compared to the control arm (97.6% and 95.1% with VL <200 and <50 copies/mL, respectively). In contrast, MVC + PI/r did not meet noninferiority bounds and was significantly inferior (84.1% [95% CI, -19.8% to -5.8%] and 77.7% [95% CI, -24.9% to -8.4%] with VL <200 and <50 copies/mL, respectively) to the control arm in the ITT analysis. Conclusion

Published
2016

16. Maraviroc, as a Switch Option, in HIV-1-infected Individuals With Stable, Well-controlled HIV Replication and R5-tropic Virus on Their First Nucleoside/Nucleotide Reverse Transcriptase Inhibitor Plus Ritonavir-boosted Protease Inhibitor Regimen: Week 48 Results of the Randomized, Multicenter MARCH Study

Author

Pett, Sarah Lilian, Amin, Janaki, Horban, Andrejz, Andrade-Villanueva, Jaime, Losso, Marcelo, Porteiro, Norma, Sierra Madero, Juan, Belloso, Waldo, Tu, Elise, Silk, David, Kelleher, Anthony, Harrigan, Richard, Clark, Andrew, Sugiura, Wataru, Wolff, Marcelo, Gill, John, Gatell, Jose, Fisher, Martin, Clarke, Amanda, Ruxrungtham, Kiat, Prazuck, Thierry, Kaiser, Rolf, Woolley, Ian, Alberto Arnaiz, Juan, Cooper, David, Rockstroh, Jurgen K., Mallon, Patrick, Emery, Sean, Pett, Sarah Lilian, Amin, Janaki, Horban, Andrejz, Andrade-Villanueva, Jaime, Losso, Marcelo, Porteiro, Norma, Sierra Madero, Juan, Belloso, Waldo, Tu, Elise, Silk, David, Kelleher, Anthony, Harrigan, Richard, Clark, Andrew, Sugiura, Wataru, Wolff, Marcelo, Gill, John, Gatell, Jose, Fisher, Martin, Clarke, Amanda, Ruxrungtham, Kiat, Prazuck, Thierry, Kaiser, Rolf, Woolley, Ian, Alberto Arnaiz, Juan, Cooper, David, Rockstroh, Jurgen K., Mallon, Patrick, and Emery, Sean

Abstract

Background. Alternative combination antiretroviral therapies in virologically suppressed human immunodeficiency virus (HIV)-infected patients experiencing side effects and/or at ongoing risk of important comorbidities from current therapy are needed. Maraviroc (MVC), a chemokine receptor 5 antagonist, is a potential alternative component of therapy in those with R5-tropic virus. Methods. The Maraviroc Switch Study is a randomized, multicenter, 96-week, open-label switch study in HIV type 1-infected adults with R5-tropic virus, virologically suppressed on a ritonavir-boosted protease inhibitor (PI/r) plus double nucleoside/nucleotide reverse transcriptase inhibitor (2 N(t)RTI) backbone. Participants were randomized 1: 2: 2 to current combination antiretroviral therapy (control), or replacing the protease inhibitor (MVC + 2 N(t)RTI arm) or the nucleoside reverse transcriptase inhibitor backbone (MVC + PI/r arm) with twice-daily MVC. The primary endpoint was the difference (switch minus control) in proportion with plasma viral load (VL) <200copies/mL at 48 weeks. The switch arms were judged noninferior if the lower limit of the 95% confidence interval (CI) for the difference in the primary endpoint was <-12% in the intention-to-treat (ITT) population. Results. The ITT population comprised 395 participants (control, n = 82; MVC + 2 N(t) RTI, n = 156; MVC + PI/r, n = 157). Baseline characteristics were well matched. At week 48, noninferior rates of virological suppression were observed in those switching away from a PI/r (93.6% [95% CI, -9.0% to 2.2%] and 91.7% [95% CI, -9.6% to 3.8%] with VL <200 and <50 copies/mL, respectively) compared to the control arm (97.6% and 95.1% with VL <200 and <50 copies/mL, respectively). In contrast, MVC + PI/r did not meet noninferiority bounds and was significantly inferior (84.1% [95% CI, -19.8% to -5.8%] and 77.7% [95% CI, -24.9% to -8.4%] with VL <200 and <50 copies/mL, respectively) to the control arm in the ITT analysis. Conclusion

Published
2016

17. Circulating microRNAs in Sera Correlate with Soluble Biomarkers of Immune Activation but Do Not Predict Mortality in ART Treated Individuals with HIV-1 Infection: A Case Control Study.

Author

Murray, Daniel D, Murray, Daniel D, Suzuki, Kazuo, Law, Matthew, Trebicka, Jonel, Neuhaus, Jacquie, Wentworth, Deborah, Johnson, Margaret, Vjecha, Michael J, Kelleher, Anthony D, Emery, Sean, INSIGHT ESPRIT and SMART Study Groups, Murray, Daniel D, Murray, Daniel D, Suzuki, Kazuo, Law, Matthew, Trebicka, Jonel, Neuhaus, Jacquie, Wentworth, Deborah, Johnson, Margaret, Vjecha, Michael J, Kelleher, Anthony D, Emery, Sean, and INSIGHT ESPRIT and SMART Study Groups

Abstract

IntroductionThe use of anti-retroviral therapy (ART) has dramatically reduced HIV-1 associated morbidity and mortality. However, HIV-1 infected individuals have increased rates of morbidity and mortality compared to the non-HIV-1 infected population and this appears to be related to end-organ diseases collectively referred to as Serious Non-AIDS Events (SNAEs). Circulating miRNAs are reported as promising biomarkers for a number of human disease conditions including those that constitute SNAEs. Our study sought to investigate the potential of selected miRNAs in predicting mortality in HIV-1 infected ART treated individuals.Materials and methodsA set of miRNAs was chosen based on published associations with human disease conditions that constitute SNAEs. This case: control study compared 126 cases (individuals who died whilst on therapy), and 247 matched controls (individuals who remained alive). Cases and controls were ART treated participants of two pivotal HIV-1 trials. The relative abundance of each miRNA in serum was measured, by RTqPCR. Associations with mortality (all-cause, cardiovascular and malignancy) were assessed by logistic regression analysis. Correlations between miRNAs and CD4+ T cell count, hs-CRP, IL-6 and D-dimer were also assessed.ResultsNone of the selected miRNAs was associated with all-cause, cardiovascular or malignancy mortality. The levels of three miRNAs (miRs -21, -122 and -200a) correlated with IL-6 while miR-21 also correlated with D-dimer. Additionally, the abundance of miRs -31, -150 and -223, correlated with baseline CD4+ T cell count while the same three miRNAs plus miR-145 correlated with nadir CD4+ T cell count.DiscussionNo associations with mortality were found with any circulating miRNA studied. These results cast doubt onto the effectiveness of circulating miRNA as early predictors of mortality or the major underlying diseases that contribute to mortality in participants treated for HIV-1 infection.

Published
2015

18. Efficacy and safety of efavirenz 400 mg daily versus 600 mg daily: 96-week data from the randomised, double-blind, placebo-controlled, non-inferiority ENCORE1 study

Author

Amin, J ; https://orcid.org/0000-0003-2161-9366, Becker, S, Belloso, W, Boffito, M, Cooper, D ; https://orcid.org/0000-0002-6031-6678, Crabtree-Ramirez, B, Duncombe, C, Foulkes, S, Hill, A, Jessen, H, Kumar, S, Lee, MP, Nwizu, C, Read, T, Rooney, J, Schaffer, K, Shahar, E, Winston, A, Wolff, M, Young, B, Abela, C, Avihingsanon, A, Boyd, M ; https://orcid.org/0000-0002-6848-3307, Carey, D ; https://orcid.org/0000-0003-0156-8143, Clarke, A, Courtney-Vega, K, Delfino, M, Donaldson, A, Emery, S, Espinosa, N, Johannesen, T, Lin, E, Losso, M, Moricz, A, Pett, S, Phanupak, P, Puls, R, Pussadee, K, Sutheerasak, P, Tomlins, L, Ubolyam, S, bin Raja Azwa, RIS, Bissio, E, Calanni, L, Chetchotisakd, P, Doong, N, Elliott, J, Gazzard, B, Kelly, M, Laplume, H, del Carmen Luna, N, Lupo, S, Messina, OG, Mohapi, L, Moore, R, Nolan, D, Orrell, C, Perez, C, Phanuphak, P, Rockstroh, J, Rowling, D, Supparatpinyo, K, Smith, D ; https://orcid.org/0000-0002-1308-4595, Villanueva, JA, Vlahakis, E, Kelleher, T, Cunningham, P ; https://orcid.org/0000-0003-2613-6910, Merlin, K, Yeung, J, Shaik, A, Fsadni, B, Carrera, A, Lograsso, M, Gulick, R, Dunn, D, Dolan, M, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Kelleher, Anthony ; https://orcid.org/0000-0002-0009-3337, Amin, J ; https://orcid.org/0000-0003-2161-9366, Becker, S, Belloso, W, Boffito, M, Cooper, D ; https://orcid.org/0000-0002-6031-6678, Crabtree-Ramirez, B, Duncombe, C, Foulkes, S, Hill, A, Jessen, H, Kumar, S, Lee, MP, Nwizu, C, Read, T, Rooney, J, Schaffer, K, Shahar, E, Winston, A, Wolff, M, Young, B, Abela, C, Avihingsanon, A, Boyd, M ; https://orcid.org/0000-0002-6848-3307, Carey, D ; https://orcid.org/0000-0003-0156-8143, Clarke, A, Courtney-Vega, K, Delfino, M, Donaldson, A, Emery, S, Espinosa, N, Johannesen, T, Lin, E, Losso, M, Moricz, A, Pett, S, Phanupak, P, Puls, R, Pussadee, K, Sutheerasak, P, Tomlins, L, Ubolyam, S, bin Raja Azwa, RIS, Bissio, E, Calanni, L, Chetchotisakd, P, Doong, N, Elliott, J, Gazzard, B, Kelly, M, Laplume, H, del Carmen Luna, N, Lupo, S, Messina, OG, Mohapi, L, Moore, R, Nolan, D, Orrell, C, Perez, C, Phanuphak, P, Rockstroh, J, Rowling, D, Supparatpinyo, K, Smith, D ; https://orcid.org/0000-0002-1308-4595, Villanueva, JA, Vlahakis, E, Kelleher, T, Cunningham, P ; https://orcid.org/0000-0003-2613-6910, Merlin, K, Yeung, J, Shaik, A, Fsadni, B, Carrera, A, Lograsso, M, Gulick, R, Dunn, D, Dolan, M, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, and Kelleher, Anthony ; https://orcid.org/0000-0002-0009-3337

Published
2015

21. Initiation of Antiretroviral Therapy in Early Asymptomatic HIV Infection

Author

Lundgren, Jens D., Babiker, Abdel G., Gordin, Fred, Emery, Sean, Sharma, Shweta, Avihingsanon, An-Chalee, Cooper, David A., Faetkenheuer, Gerd, Llibre, Josep M., Moli-Na, Jean-Michel, Munderi, Paula, Schechter, Mauro, Wood, Robin, Klingman, Karin L., Collins, Simon, Lane, H. Clifford, Phillips, Andrew N., Neaton, James D., Lundgren, Jens D., Babiker, Abdel G., Gordin, Fred, Emery, Sean, Sharma, Shweta, Avihingsanon, An-Chalee, Cooper, David A., Faetkenheuer, Gerd, Llibre, Josep M., Moli-Na, Jean-Michel, Munderi, Paula, Schechter, Mauro, Wood, Robin, Klingman, Karin L., Collins, Simon, Lane, H. Clifford, Phillips, Andrew N., and Neaton, James D.

Abstract

BACKGROUND Data from randomized trials are lacking on the benefits and risks of initiating antiretroviral therapy in patients with asymptomatic human immunodeficiency virus (HIV) infection who have a CD4+ count of more than 350 cells per cubic millimeter. METHODS We randomly assigned HIV-positive adults who had a CD4+ count of more than 500 cells per cubic millimeter to start antiretroviral therapy immediately (immediate-initiation group) or to defer it until the CD4+ count decreased to 350 cells per cubic millimeter or until the development of the acquired immunodeficiency syndrome (AIDS) or another condition that dictated the use of antiretroviral therapy (deferred-initiation group). The primary composite end point was any serious AIDS-related event, serious non-AIDS-related event, or death from any cause. RESULTS A total of 4685 patients were followed for a mean of 3.0 years. At study entry, the median HIV viral load was 12,759 copies per milliliter, and the median CD4+ count was 651 cells per cubic millimeter. On May 15, 2015, on the basis of an interim analysis, the data and safety monitoring board determined that the study question had been answered and recommended that patients in the deferred-initiation group be offered antiretroviral therapy. The primary end point occurred in 42 patients in the immediate-initiation group (1.8%; 0.60 events per 100 person-years), as compared with 96 patients in the deferred-initiation group (4.1%; 1.38 events per 100 person-years), for a hazard ratio of 0.43 (95% confidence interval [CI], 0.30 to 0.62; P<0.001). Hazard ratios for serious AIDS-related and serious non-AIDS-related events were 0.28 (95% CI, 0.15 to 0.50; P<0.001) and 0.61 (95% CI, 0.38 to 0.97; P = 0.04), respectively. More than two thirds of the primary end points (68%) occurred in patients with a CD4+ count of more than 500 cells per cubic millimeter. The risks of a grade 4 event were similar in the two groups, as were the risks of unscheduled hospital admiss

Published
2015

22. Circulating microRNAs in sera correlate with soluble biomarkers of immune activation but do not predict mortality in ART treated individuals with HIV-1 infection: A case control study

Author

Murray, Daniel D., Suzuki, Kazuo, Law, Matthew, Trebicka, Jonel, Neuhaus, Jacquie, Wentworth, Deborah, Johnson, Margaret, Vjecha, Michael J., Kelleher, Anthony D., Emery, Sean, Lundgren, J., Angus, B., Larson, G., Beral, V., Chaisson, R, Fleming, T., Hill, C., Rogers, Gary, SMART STUDY GROUP, ESPIRIT STUDY GROUP, Murray, Daniel D., Suzuki, Kazuo, Law, Matthew, Trebicka, Jonel, Neuhaus, Jacquie, Wentworth, Deborah, Johnson, Margaret, Vjecha, Michael J., Kelleher, Anthony D., Emery, Sean, Lundgren, J., Angus, B., Larson, G., Beral, V., Chaisson, R, Fleming, T., Hill, C., Rogers, Gary, SMART STUDY GROUP, and ESPIRIT STUDY GROUP

Published
2015

23. Circulating microRNAs in Sera Correlate with Soluble Biomarkers of Immune Activation but Do Not Predict Mortality in ART Treated Individuals with HIV-1 Infection: A Case Control Study.

Author

Murray, Daniel D, Pacheco, Antonio Guilherme1, Murray, Daniel D, Suzuki, Kazuo, Law, Matthew, Trebicka, Jonel, Neuhaus, Jacquie, Wentworth, Deborah, Johnson, Margaret, Vjecha, Michael J, Kelleher, Anthony D, Emery, Sean, INSIGHT ESPRIT and SMART Study Groups, Murray, Daniel D, Pacheco, Antonio Guilherme1, Murray, Daniel D, Suzuki, Kazuo, Law, Matthew, Trebicka, Jonel, Neuhaus, Jacquie, Wentworth, Deborah, Johnson, Margaret, Vjecha, Michael J, Kelleher, Anthony D, Emery, Sean, and INSIGHT ESPRIT and SMART Study Groups

Abstract

IntroductionThe use of anti-retroviral therapy (ART) has dramatically reduced HIV-1 associated morbidity and mortality. However, HIV-1 infected individuals have increased rates of morbidity and mortality compared to the non-HIV-1 infected population and this appears to be related to end-organ diseases collectively referred to as Serious Non-AIDS Events (SNAEs). Circulating miRNAs are reported as promising biomarkers for a number of human disease conditions including those that constitute SNAEs. Our study sought to investigate the potential of selected miRNAs in predicting mortality in HIV-1 infected ART treated individuals.Materials and methodsA set of miRNAs was chosen based on published associations with human disease conditions that constitute SNAEs. This case: control study compared 126 cases (individuals who died whilst on therapy), and 247 matched controls (individuals who remained alive). Cases and controls were ART treated participants of two pivotal HIV-1 trials. The relative abundance of each miRNA in serum was measured, by RTqPCR. Associations with mortality (all-cause, cardiovascular and malignancy) were assessed by logistic regression analysis. Correlations between miRNAs and CD4+ T cell count, hs-CRP, IL-6 and D-dimer were also assessed.ResultsNone of the selected miRNAs was associated with all-cause, cardiovascular or malignancy mortality. The levels of three miRNAs (miRs -21, -122 and -200a) correlated with IL-6 while miR-21 also correlated with D-dimer. Additionally, the abundance of miRs -31, -150 and -223, correlated with baseline CD4+ T cell count while the same three miRNAs plus miR-145 correlated with nadir CD4+ T cell count.DiscussionNo associations with mortality were found with any circulating miRNA studied. These results cast doubt onto the effectiveness of circulating miRNA as early predictors of mortality or the major underlying diseases that contribute to mortality in participants treated for HIV-1 infection.

Published
2015

26. Initiation of Antiretroviral Therapy in Early Asymptomatic HIV Infection

Author

Lundgren, Jens D., Babiker, Abdel G., Gordin, Fred, Emery, Sean, Sharma, Shweta, Avihingsanon, An-Chalee, Cooper, David A., Faetkenheuer, Gerd, Llibre, Josep M., Moli-Na, Jean-Michel, Munderi, Paula, Schechter, Mauro, Wood, Robin, Klingman, Karin L., Collins, Simon, Lane, H. Clifford, Phillips, Andrew N., Neaton, James D., Lundgren, Jens D., Babiker, Abdel G., Gordin, Fred, Emery, Sean, Sharma, Shweta, Avihingsanon, An-Chalee, Cooper, David A., Faetkenheuer, Gerd, Llibre, Josep M., Moli-Na, Jean-Michel, Munderi, Paula, Schechter, Mauro, Wood, Robin, Klingman, Karin L., Collins, Simon, Lane, H. Clifford, Phillips, Andrew N., and Neaton, James D.

Abstract

BACKGROUND Data from randomized trials are lacking on the benefits and risks of initiating antiretroviral therapy in patients with asymptomatic human immunodeficiency virus (HIV) infection who have a CD4+ count of more than 350 cells per cubic millimeter. METHODS We randomly assigned HIV-positive adults who had a CD4+ count of more than 500 cells per cubic millimeter to start antiretroviral therapy immediately (immediate-initiation group) or to defer it until the CD4+ count decreased to 350 cells per cubic millimeter or until the development of the acquired immunodeficiency syndrome (AIDS) or another condition that dictated the use of antiretroviral therapy (deferred-initiation group). The primary composite end point was any serious AIDS-related event, serious non-AIDS-related event, or death from any cause. RESULTS A total of 4685 patients were followed for a mean of 3.0 years. At study entry, the median HIV viral load was 12,759 copies per milliliter, and the median CD4+ count was 651 cells per cubic millimeter. On May 15, 2015, on the basis of an interim analysis, the data and safety monitoring board determined that the study question had been answered and recommended that patients in the deferred-initiation group be offered antiretroviral therapy. The primary end point occurred in 42 patients in the immediate-initiation group (1.8%; 0.60 events per 100 person-years), as compared with 96 patients in the deferred-initiation group (4.1%; 1.38 events per 100 person-years), for a hazard ratio of 0.43 (95% confidence interval [CI], 0.30 to 0.62; P<0.001). Hazard ratios for serious AIDS-related and serious non-AIDS-related events were 0.28 (95% CI, 0.15 to 0.50; P<0.001) and 0.61 (95% CI, 0.38 to 0.97; P = 0.04), respectively. More than two thirds of the primary end points (68%) occurred in patients with a CD4+ count of more than 500 cells per cubic millimeter. The risks of a grade 4 event were similar in the two groups, as were the risks of unscheduled hospital admiss

Published
2015

27. Initiation of Antiretroviral Therapy in Early Asymptomatic HIV Infection

Author

Lundgren, Jens D, Babiker, Abdel G, Gordin, Fred, Emery, Sean, Grund, Birgit, Sharma, Shweta, Avihingsanon, Anchalee, Cooper, David A, Fätkenheuer, Gerd, Llibre, Josep M, Molina, Jean-Michel, Munderi, Paula, Schechter, Mauro, Wood, Robin, Klingman, Karin L, Collins, Simon, Lane, H Clifford, Phillips, Andrew N, Neaton, James D, Lundgren, Jens D, Babiker, Abdel G, Gordin, Fred, Emery, Sean, Grund, Birgit, Sharma, Shweta, Avihingsanon, Anchalee, Cooper, David A, Fätkenheuer, Gerd, Llibre, Josep M, Molina, Jean-Michel, Munderi, Paula, Schechter, Mauro, Wood, Robin, Klingman, Karin L, Collins, Simon, Lane, H Clifford, Phillips, Andrew N, and Neaton, James D

Abstract

BACKGROUND: Data from randomized trials are lacking on the benefits and risks of initiating antiretroviral therapy in patients with asymptomatic human immunodeficiency virus (HIV) infection who have a CD4+ count of more than 350 cells per cubic millimeter.METHODS: We randomly assigned HIV-positive adults who had a CD4+ count of more than 500 cells per cubic millimeter to start antiretroviral therapy immediately (immediate-initiation group) or to defer it until the CD4+ count decreased to 350 cells per cubic millimeter or until the development of the acquired immunodeficiency syndrome (AIDS) or another condition that dictated the use of antiretroviral therapy (deferred-initiation group). The primary composite end point was any serious AIDS-related event, serious non-AIDS-related event, or death from any cause.RESULTS: A total of 4685 patients were followed for a mean of 3.0 years. At study entry, the median HIV viral load was 12,759 copies per milliliter, and the median CD4+ count was 651 cells per cubic millimeter. On May 15, 2015, on the basis of an interim analysis, the data and safety monitoring board determined that the study question had been answered and recommended that patients in the deferred-initiation group be offered antiretroviral therapy. The primary end point occurred in 42 patients in the immediate-initiation group (1.8%; 0.60 events per 100 person-years), as compared with 96 patients in the deferred-initiation group (4.1%; 1.38 events per 100 person-years), for a hazard ratio of 0.43 (95% confidence interval [CI], 0.30 to 0.62; P<0.001). Hazard ratios for serious AIDS-related and serious non-AIDS-related events were 0.28 (95% CI, 0.15 to 0.50; P<0.001) and 0.61 (95% CI, 0.38 to 0.97; P=0.04), respectively. More than two thirds of the primary end points (68%) occurred in patients with a CD4+ count of more than 500 cells per cubic millimeter. The risks of a grade 4 event were similar in the two groups, as were the risks of unsch

Published
2015

29. Pre-therapy inflammation and coagulation activation and long-term CD4 count responses to the initiation of antiretroviral therapy

Author

Achhra, Amit C., Phillips, Andrew, Emery, Sean, MacArthur, R D, Furrer, Hansjakob, De Wit, Stéphane, Losso, Marcelo, Law, Mathew M.G., International Network for Strategic Initiatives in Global HIV Trials (INSIGHT) Strategic Management of Antiretroviral Therapy (SMART) and Flexible Initial Retrovirus Suppressive Therapies (FIRST) study groups, Achhra, Amit C., Phillips, Andrew, Emery, Sean, MacArthur, R D, Furrer, Hansjakob, De Wit, Stéphane, Losso, Marcelo, Law, Mathew M.G., and International Network for Strategic Initiatives in Global HIV Trials (INSIGHT) Strategic Management of Antiretroviral Therapy (SMART) and Flexible Initial Retrovirus Suppressive Therapies (FIRST) study groups

Abstract

Pre-antiretroviral therapy (ART) inflammation and coagulation activation predict clinical outcomes in HIV-positive individuals. We assessed whether pre-ART inflammatory marker levels predicted the CD4 count response to ART., SCOPUS: ar.j, FLWIN, info:eu-repo/semantics/published

Published
2015

30. Pre-therapy inflammation and coagulation activation and long-term CD4 count responses to the initiation of antiretroviral therapy

Author

Conference on Retroviruses and Opportunistic Infections - CROI 2015 (22: February 23-26, 2015: Seattle, USA), Achhra, Amit C., Phillips, Andrew N., Emery, Sean, MacArthur, R D, Furrer, Hansjakob, De Wit, Stéphane, Losso, Marcello, Law, Mathew M.G., Conference on Retroviruses and Opportunistic Infections - CROI 2015 (22: February 23-26, 2015: Seattle, USA), Achhra, Amit C., Phillips, Andrew N., Emery, Sean, MacArthur, R D, Furrer, Hansjakob, De Wit, Stéphane, Losso, Marcello, and Law, Mathew M.G.

Abstract

For the International Network for Strategic Initiatives in Global HIV Trials (INSIGHT) Strategic Management of Antiretroviral Therapy (SMART) and Flexible Initial Retrovirus Suppressive Therapies (FIRST) study groups, info:eu-repo/semantics/nonPublished

Published
2015

31. Involvement of the Endocannabinoid System in the Development and Treatment of Breast Cancer

Author

VIRGINIA COMMONWEALTH UNIV RICHMOND, Emery, Sean M, Lichtman, Aron H, Gewirtz, David A, VIRGINIA COMMONWEALTH UNIV RICHMOND, Emery, Sean M, Lichtman, Aron H, and Gewirtz, David A

Abstract

Studies to evaluate the interaction of the synthetic cannabinoid WIN55,212-2 (WIN2) and ionizing radiation have led to preliminary results implicating a novel site of action of WIN2 in the MCF-7 breast cancer model. In previous reports, WIN2 was found to stereoselectively inhibit the growth of breast cancer cells in a dose-dependent but cannabinoid receptor-independent mechanism. Experiments described in this report evaluated antiproliferative mechanisms of WIN2 treatment both alone and in combination with ionizing radiation (IR). Evaluation of autophagy, apoptosis and necrotic mechanism failed to indicate that WIN2 promoted death of the tumor cells. Autophagy was induced both for radiation alone, WIN2 alone and WIN2 + radiation, but did not appear to be involved in the antiproliferative mechanisms of either treatment. Senescence, quantified by β-galactosidase staining, and DNA damage, quantified by γH2AX formation, confirmed that radiation treatment induced senescent growth arrest both alone and in combination with WIN2; however, WIN2 was unable to alter the magnitude of senescent growth arrest induced by IR. Comparison of γH2AX levels at 1 and 24 h also showed that WIN2 did not alter the rate of DNA repair after radiation treatment. These data assessing cell death and senescence combined with additional temporal cell count studies indicated that WIN2 induces growth arrest but not cell death. It was further concluded that augmentation of IR induced antiproliferative effects by WIN2 occur from the parallel induction of both senescent and classical growth arrest responses in the breast tumor cells.

Published
2014

32. Biomarkers of inflammation, coagulation and microbial translocation in HIV/HCV co-infected patients in the SMART study

Author

Peters, L, Neuhaus, J, Duprez, D, Neaton, JD, Tracy, R, Klein, MB, Mocroft, A, Rockstroh, J, Dore, G ; https://orcid.org/0000-0002-4741-2622, Lundgren, JD, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Peters, L, Neuhaus, J, Duprez, D, Neaton, JD, Tracy, R, Klein, MB, Mocroft, A, Rockstroh, J, Dore, G ; https://orcid.org/0000-0002-4741-2622, Lundgren, JD, and Emery, Sean ; https://orcid.org/0000-0001-6072-8309

Abstract

Background: Previous results from the SMART study showed that HIV/viral hepatitis co-infected persons with impaired liver function are at increased risk of death following interruption of antiretroviral therapy (ART). Objectives: To investigate the influence of fibrosis and ART interruption on levels of biomarkers of inflammation, coagulation and microbial translocation in HIV/HCV co-infected persons in the SMART study. Study design: All HIV/HCV co-infected persons with stored plasma at study entry and at six months of follow-up were included (N= 362). D-dimer, IL-6, sCD14 and hepatic synthesized coagulation markers were measured and compared according to the liver fibrosis marker hyaluronic acid (HA) at study entry. Percent difference in changes in biomarker levels from study entry to month 6 was compared between randomization groups and according to study entry HA levels. Results: At study entry, persons with elevated HA (>75. ng/mL vs. ≤75. ng/mL) had higher median (IQR) levels of IL-6 [4.14. pg/mL (2.60-6.32) vs. 2.74. pg/mL (1.88-3.97)] and soluble CD14 [2163. ng/mL (1952-2916) vs. 1979. ng/mL (1742-2310)] (p<. 0.001). Elevated HA was also associated with alterations of both pro- and anti-coagulation markers but the overall coagulation profile was not affected. Interruption of ART lead to a particularly pronounced increase in IL-6 levels in persons with elevated HA levels (p= 0.01 for interaction between randomization group and continuous HA level). Conclusions: HIV/HCV co-infected persons with impaired liver function are in an enhanced pro-inflammatory state which is further exacerbated upon interruption of ART. © 2014 Elsevier B.V.

Published
2014

33. The Opposites Attract Study of viral load, HIV treatment and HIV transmission in serodiscordant homosexual male couples: Design and methods

Author

Bavinton, BR ; https://orcid.org/0000-0001-5834-8278, Jin, F ; https://orcid.org/0000-0002-8573-637X, Prestage, G ; https://orcid.org/0000-0003-3917-8992, Zablotska, I, Koelsch, KK, Phanuphak, N, Grinsztejn, B, Cooper, DA ; https://orcid.org/0000-0002-6031-6678, Fairley, C, Kelleher, A ; https://orcid.org/0000-0002-0009-3337, Triffitt, K, Grulich, AE, Templeton, David ; https://orcid.org/0000-0003-2157-9587, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Bavinton, BR ; https://orcid.org/0000-0001-5834-8278, Jin, F ; https://orcid.org/0000-0002-8573-637X, Prestage, G ; https://orcid.org/0000-0003-3917-8992, Zablotska, I, Koelsch, KK, Phanuphak, N, Grinsztejn, B, Cooper, DA ; https://orcid.org/0000-0002-6031-6678, Fairley, C, Kelleher, A ; https://orcid.org/0000-0002-0009-3337, Triffitt, K, Grulich, AE, Templeton, David ; https://orcid.org/0000-0003-2157-9587, and Emery, Sean ; https://orcid.org/0000-0001-6072-8309

Abstract

Background: Studies in heterosexual HIV serodiscordant couples have provided critical evidence on the role of HIV treatments and undetectable viral load in reducing the risk of HIV transmission. There is very limited data on the risk of transmission from anal sex in homosexual male serodiscordant couples.

Published
2014

34. Adjudicated morbidity and mortality outcomes by age among individuals with HIV infection on suppressive antiretroviral therapy

Author

Landay, Alan, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Miller, CJ, Baker, JV, Bormann, AM, Erlandson, KM, Hullsiek, KH, Justice, AC, Neuhaus, J, Paredes, R, Petoumenos, K ; https://orcid.org/0000-0001-7534-7154, Wentworth, D, Winston, A, Wolfson, J, Neaton, JD, Landay, Alan, Emery, Sean ; https://orcid.org/0000-0001-6072-8309, Miller, CJ, Baker, JV, Bormann, AM, Erlandson, KM, Hullsiek, KH, Justice, AC, Neuhaus, J, Paredes, R, Petoumenos, K ; https://orcid.org/0000-0001-7534-7154, Wentworth, D, Winston, A, Wolfson, J, and Neaton, JD

Abstract

Background: Non-AIDS conditions such as cardiovascular disease and non-AIDS defining cancers dominate causes of morbidity and mortality among persons with HIV on suppressive combination antiretroviral therapy. Accurate estimates of disease incidence and of risk factors for these conditions are important in planning preventative efforts. Methods: With use of medical records, serious non-AIDS events, AIDS events, and causes of death were adjudicated using pre-specified criteria by an Endpoint Review Committee in two large international trials. Rates of serious non-AIDS which include cardiovascular disease, end-stage renal disease, decompensated liver disease, and non-AIDS cancer, and other serious (grade 4) adverse events were determined, overall and by age, over a median follow-up of 4.3 years for 3,570 participants with CD4cell count 300 cells/mm3 who were taking antiretroviral therapy and had an HIV RNA level ≤500 copies/mL. Cox models were used to examine the effect of age and other baseline factors on risk of a composite outcome of all-cause mortality, AIDS, or serious non-AIDS. Results: Five-year Kaplan-Meier estimates of the composite outcome, overall and by age were 8.3% (overall), 3.6% (<40), 8.7% (40-49) and 16.1% (≥50), respectively (p<0.001). In addition to age, smoking and higher levels of interleukin-6 and Ddimer were significant predictors of the composite outcome. The composite outcome was dominated by serious non-AIDS events (overall 65% of 277 participants with a composite event). Most serious non-AIDS events were due to cardiovascular disease and non-AIDS cancers. Conclusions: To date, few large studies have carefully collected data on serious non-AIDS outcomes. Thus, reliable estimates of event rates are scarce. Data cited here, from a geographically diverse cohort, will be useful for planning studies of interventions aimed at reducing rates of serious non-AIDS events among people with HIV. © 2014 Miller et al.

Published
2014

35. Involvement of the Endocannabinoid System in the Development and Treatment of Breast Cancer

Author

VIRGINIA COMMONWEALTH UNIV RICHMOND, Emery, Sean M, Lichtman, Aron H, Gewirtz, David A, VIRGINIA COMMONWEALTH UNIV RICHMOND, Emery, Sean M, Lichtman, Aron H, and Gewirtz, David A

Abstract

Work looking at the interaction of the synthetic cannabinoid WIN55,212-2 and ionizing radiation has led to preliminary results implicating a novel site of action in the MCF-7 breast cancer model. WIN55,212-2 has been shown previously to dose dependently, and potentially more importantly stereoselectively, inhibit the growth of breast cancer cells. Interestingly, when selective cannabinoid receptor antagonists AM251 and AM630 were administered, we see a failure to antagonize WIN55,212-2 s antiproliferative effects. This despite the observation the MCF-7 cells express mRNA for the cannabinoid receptor CB2, which WIN55,212-2 has been shown to act on in other breast cancer cell lines. Further studies were conducted that pharmacologically excluded the involvement of members of the PPAR receptor system, known to be reactive to WIN55,212-2. TRPV1 is reported to be sensitive to some cannabinoids as well, and subsequently was evaluated and then excluded based on similar pharmacological experiments. Studies from a colleague have implicated the involvement of sphingosine-1-phosphate receptors as a potential site of action for WIN55,212-2 in the brain. Our work has since shown WIN55,212-2 to be able to antagonize this sphingosine-1-phosphate receptor system, and it s known importance to MCF-7 cell growth gives a potential mechanism of action. This interaction has not previously been reported and suggests a novel site of action that could be exploited with future research., The original document contains color images.

Published
2013

36. Issues on Results of the External Quality Assessment for Proviral DNA Testing of HIV-1 Tropism in the Maraviroc Switch Collaborative Study Reply to Issues on Results of the External Quality Assessment for Proviral DNA Testing of HIV-1 Tropism in the Maraviroc Switch Collaborative Study

Author

Tu, Elise, Swenson, Luke C., Land, Sally, Pett, Sarah, Emery, Sean, Marks, Kat, Kelleher, Anthony D., Kaye, Steve, Kaiser, Rolf, Schuelter, Eugene, Harrigan, Richard, Tu, Elise, Swenson, Luke C., Land, Sally, Pett, Sarah, Emery, Sean, Marks, Kat, Kelleher, Anthony D., Kaye, Steve, Kaiser, Rolf, Schuelter, Eugene, and Harrigan, Richard

Published
2013

37. Bone mineral density in HIV participants randomized to raltegravir and lopinavir/ritonavir compared with standard second line therapy

Author

Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, Boyd, Mark A, Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, and Boyd, Mark A

Abstract

Objective: To compare changes over 48 weeks in bone mineral density (BMD) between participants randomized to lopinavir/ritonavir (LPV/r) + raltegravir (RAL) or LPV/r + 2-3 nucleoside/nucleotide reverse transcriptase inhibitors (N(t)RTIs) as second line therapy. Design: 48-week open-label sub-study of the Second Line trial conducted in South Africa, India, Thailand, Malaysia and Argentina. Methods: Dual energy X-ray absorptiometry scans of proximal femur and lumbar spine were performed at baseline and week 48. Linear regression was used to compare means of differences between arms. McNemars test compared osteopenia and osteoporosis. Associations between percentage BMD changes and baseline variables were assessed by multivariate linear regression. Results: Two hundred and ten participants were randomized. Analyses were adjusted for sex, BMI and smoking status. Mean (95% CI) proximal femur BMD% reduced over 48 weeks by -5.2% (-6.7 to -3.8%) in the LPV/r+2-3N(t)RTIs arm and by -2.9% (-4.3 to -1.5%) in the LPV/r+RAL arm (P = 0.0001). Lumbar spine BMD reduced by -4.2% (-5.7 to -2.7%) in the LPV/r+2-3N(t)RTIs arm and by -2.0% (-3.5 to -0.6%) in the LPV/r+RAL arm (P = 0.0006). The incidence of osteopenia (7.6%) and osteoporosis (2.0%) assessed over 48 weeks were similar between arms. Reduced BMD over 48 weeks was significantly associated with longer duration of tenofovir on study [% change (SE) -1.58 (0.38) femur, -1.65 (0.38) spine, P = 0.0001] and low baseline BMI [% change (SE) 0.5 (0.13) femur, 0.17 (0.07) spine; P < 0.01]. Conclusion: An N(t)RTI-sparing antiretroviral regimen of LPV/r and raltegravir as second line therapy is associated with less bone loss than a LPV/r regimen containing N(t)RTIs.

Published
2013

38. Issues on Results of the External Quality Assessment for Proviral DNA Testing of HIV-1 Tropism in the Maraviroc Switch Collaborative Study Reply to Issues on Results of the External Quality Assessment for Proviral DNA Testing of HIV-1 Tropism in the Maraviroc Switch Collaborative Study

Author

Tu, Elise, Swenson, Luke C., Land, Sally, Pett, Sarah, Emery, Sean, Marks, Kat, Kelleher, Anthony D., Kaye, Steve, Kaiser, Rolf, Schuelter, Eugene, Harrigan, Richard, Tu, Elise, Swenson, Luke C., Land, Sally, Pett, Sarah, Emery, Sean, Marks, Kat, Kelleher, Anthony D., Kaye, Steve, Kaiser, Rolf, Schuelter, Eugene, and Harrigan, Richard

Published
2013

39. Biomarkers and bacterial pneumonia risk in patients with treated HIV infection: a case-control study

Author

Bjerk, Sonja M., Baker, Jason V., Emery, Sean, Neuhaus, Jacqueline, Angus, Brian, Gordin, Fred M., Pett, Sarah L., Stephan, Christoph, Kunisaki, Ken M., Bjerk, Sonja M., Baker, Jason V., Emery, Sean, Neuhaus, Jacqueline, Angus, Brian, Gordin, Fred M., Pett, Sarah L., Stephan, Christoph, and Kunisaki, Ken M.

Abstract

Background: Despite advances in HIV treatment, bacterial pneumonia continues to cause considerable morbidity and mortality in patients with HIV infection. Studies of biomarker associations with bacterial pneumonia risk in treated HIV-infected patients do not currently exist. Methods: We performed a nested, matched, case-control study among participants randomized to continuous combination antiretroviral therapy (cART) in the Strategies for Management of Antiretroviral Therapy trial. Patients who developed bacterial pneumonia (cases) and patients without bacterial pneumonia (controls) were matched 1:1 on clinical center, smoking status, age, and baseline cART use. Baseline levels of Club Cell Secretory Protein 16 (CC16), Surfactant Protein D (SP-D), C-reactive protein (hsCRP), interleukin-6 (IL-6), and d-dimer were compared between cases and controls. Results: Cases (n = 72) and controls (n = 72) were 25.7% female, 51.4% black, 65.3% current smokers, 9.7% diabetic, 36.1% co-infected with Hepatitis B/C, and 75.0% were on cART at baseline. Median (IQR) age was 45 (41, 51) years with CD4+ count of 553 (436, 690) cells/mm3. Baseline CC16 and SP-D were similar between cases and controls, but hsCRP was significantly higher in cases than controls (2.94 µg/mL in cases vs. 1.93 µg/mL in controls; p = 0.02). IL-6 and d-dimer levels were also higher in cases compared to controls, though differences were not statistically significant (p-value 0.06 and 0.10, respectively). Conclusions: In patients with cART-treated HIV infection, higher levels of systemic inflammatory markers were associated with increased bacterial pneumonia risk, while two pulmonary-specific inflammatory biomarkers, CC16 and SP-D, were not associated with bacterial pneumonia risk.

Published
2013

40. Considerations in the rationale, design and methods of the Strategic Timing of AntiRetroviral Treatment (START) study

Author

Babiker, Abdel G, Emery, Sean, Fätkenheuer, Gerd, Gordin, Fred M, Grund, Birgit, Lundgren, Jens D, Neaton, James D, Pett, Sarah L, Phillips, Andrew, Touloumi, Giota, Vjechaj, Michael J, Babiker, Abdel G, Emery, Sean, Fätkenheuer, Gerd, Gordin, Fred M, Grund, Birgit, Lundgren, Jens D, Neaton, James D, Pett, Sarah L, Phillips, Andrew, Touloumi, Giota, and Vjechaj, Michael J

Abstract

Untreated human immunodeficiency virus (HIV) infection is characterized by progressive depletion of CD4+ T lymphocyte (CD4) count leading to the development of opportunistic diseases (acquired immunodeficiency syndrome (AIDS)), and more recent data suggest that HIV is also associated with an increased risk of serious non-AIDS (SNA) diseases including cardiovascular, renal, and liver diseases and non-AIDS-defining cancers. Although combination antiretroviral treatment (ART) has resulted in a substantial decrease in morbidity and mortality in persons with HIV infection, viral eradication is not feasible with currently available drugs. The optimal time to start ART for asymptomatic HIV infection is controversial and remains one of the key unanswered questions in the clinical management of HIV-infected individuals.

Published
2013

41. HIV Lipodystrophy in Participants Randomised to Lopinavir/Ritonavir (LPV/r) +2-3 Nucleoside/Nucleotide Reverse Transcriptase Inhibitors (N(t)RTI) or LPV/r + Raltegravir as Second-Line Antiretroviral Therapy

Author

Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, Boyd, Mark A, Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, and Boyd, Mark A

Abstract

Objective To compare changes over 48 weeks in body fat, lipids, Metabolic Syndrome and cardiovascular disease risk between patients randomised 1:1 to lopinavir/ritonavir (r/LPV) plus raltegravir (RAL) compared to r/LPV plus 2-3 nucleoside/nucleotide reverse transcriptase inhibitors (N(t)RTIs) as second-line therapy. Methods Participants were HIV-1 positive (>16 years) failing first-line treatment (2 consecutive HIV RNA >500 copies/mL) of NNRTI +2N(t)RTI. Whole body dual energy x-ray absorptiometry was performed at baseline and week 48. Data were obtained to calculate the Metabolic Syndrome and Framingham cardiovascular disease (CVD) risk score. Linear regression was used to compare mean differences between arms. Logistic regression compared incidence of metabolic syndrome. Associations between percent limb fat changes at 48 weeks with baseline variables were assessed by backward stepwise multivariate linear regression. Analyses were adjusted for gender, body mass index and smoking status. Results 210 participants were randomised. The mean (95% CI) increase in limb fat over 48 weeks was 15.7% (5.3, 25.9) or 0.9 kg (0.2, 1.5) in the r/LPV+N(t)RTI arm and 21.1% (11.1, 31,1) or 1.3 kg (0.7, 1.9) in the r/LPV+RAL arm, with no significant difference between treatment arms (−5.4% [−0.4 kg], p>0.1). Increases in total body fat mass (kg) and trunk fat mass (kg) were also similar between groups. Total:HDL cholesterol ratio was significantly higher in the RAL arm (mean difference −0.4 (1.4); p = 0.03), there were no other differences in lipid parameters between treatment arms. There were no statistically significant differences in CVD risk or incidence of Metabolic Syndrome between the two treatment arms. The baseline predictors of increased limb fat were high viral load, high insulin and participant's not taking lipid lowering treatment. Conclusion In patients switching to second line therapy, r/LPV combined with RAL demonstrated similar improvements in limb fat as an N(t)RTI

Published
2013

42. Ritonavir-boosted lopinavir plus nucleoside or nucleotide reverse transcriptase inhibitors versus ritonavir-boosted lopinavir plus raltegravir for treatment of HIV-1 infection in adults with virological failure of a standard first-line ART regimen (SECOND-LINE): a randomised, open-label, non-inferiority study

Author

SECOND-LINE Study Group, Boyd, Mark A, Kumarasamy, N, Moore, Cecilia L, Nwizu, C, Losso, M H, Mohapi, L, Martin, Allison, Kerr, S, Sohn, A H, Teppler, H, Van De Steen, O, Molina, J-M, Emery, Sean, Cooper, David A, SECOND-LINE Study Group, Boyd, Mark A, Kumarasamy, N, Moore, Cecilia L, Nwizu, C, Losso, M H, Mohapi, L, Martin, Allison, Kerr, S, Sohn, A H, Teppler, H, Van De Steen, O, Molina, J-M, Emery, Sean, and Cooper, David A

Abstract

Background Uncertainty exists about the best treatment for people with HIV-1 who have virological failure with first-line combination antiretroviral therapy of a non-nucleoside analogue (NNRTI) plus two nucleoside or nucleotide analogue reverse transcriptase inhibitors (NtRTI). We compared a second-line regimen combining two new classes of drug with a WHO-recommended regimen. Methods We did this 96-week, phase 3b/4, randomised, open-label non-inferiority trial at 37 sites worldwide. Adults with HIV-1 who had confirmed virological failure (plasma viral load >500 copies per mL) after 24 weeks or more of first-line treatment were randomly assigned (1:1) to receive ritonavir-boosted lopinavir plus two or three NtRTIs (control group) or ritonavir-boosted lopinavir plus raltegravir (raltegravir group). The randomisation sequence was computer generated with block randomisation (block size four). Neither participants nor investigators were masked to allocation. The primary endpoint was the proportion of participants with plasma viral load less than 200 copies per mL at 48 weeks in the modified intention-to-treat population, with a non-inferiority margin of 12%. This study is registered with ClinicalTrials.gov, number NCT00931463. Findings We enrolled 558 patients, of whom 541 (271 in the control group, 270 in the raltegravir group) were included in the primary analysis. At 48 weeks, 219 (81%) patients in the control group compared with 223 (83%) in the raltegravir group met the primary endpoint (difference 1·8%, 95% CI −4·7 to 8·3), fulfilling the criterion for non-inferiority. 993 adverse events occurred in 271 participants in the control group versus 895 in 270 participants in the raltegravir group, the most common being gastrointestinal. Interpretation The raltegravir regimen was no less efficacious than the standard of care and was safe and well tolerated. This simple NtRTI-free treatment strategy might extend the successful public health approach to management of HIV b

Published
2013

43. HIV Lipodystrophy in Participants Randomised to Lopinavir/Ritonavir (LPV/r) +2-3 Nucleoside/Nucleotide Reverse Transcriptase Inhibitors (N(t)RTI) or LPV/r + Raltegravir as Second-Line Antiretroviral Therapy

Author

Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, Boyd, Mark A, Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, and Boyd, Mark A

Abstract

Objective To compare changes over 48 weeks in body fat, lipids, Metabolic Syndrome and cardiovascular disease risk between patients randomised 1:1 to lopinavir/ritonavir (r/LPV) plus raltegravir (RAL) compared to r/LPV plus 2-3 nucleoside/nucleotide reverse transcriptase inhibitors (N(t)RTIs) as second-line therapy. Methods Participants were HIV-1 positive (>16 years) failing first-line treatment (2 consecutive HIV RNA >500 copies/mL) of NNRTI +2N(t)RTI. Whole body dual energy x-ray absorptiometry was performed at baseline and week 48. Data were obtained to calculate the Metabolic Syndrome and Framingham cardiovascular disease (CVD) risk score. Linear regression was used to compare mean differences between arms. Logistic regression compared incidence of metabolic syndrome. Associations between percent limb fat changes at 48 weeks with baseline variables were assessed by backward stepwise multivariate linear regression. Analyses were adjusted for gender, body mass index and smoking status. Results 210 participants were randomised. The mean (95% CI) increase in limb fat over 48 weeks was 15.7% (5.3, 25.9) or 0.9 kg (0.2, 1.5) in the r/LPV+N(t)RTI arm and 21.1% (11.1, 31,1) or 1.3 kg (0.7, 1.9) in the r/LPV+RAL arm, with no significant difference between treatment arms (−5.4% [−0.4 kg], p>0.1). Increases in total body fat mass (kg) and trunk fat mass (kg) were also similar between groups. Total:HDL cholesterol ratio was significantly higher in the RAL arm (mean difference −0.4 (1.4); p = 0.03), there were no other differences in lipid parameters between treatment arms. There were no statistically significant differences in CVD risk or incidence of Metabolic Syndrome between the two treatment arms. The baseline predictors of increased limb fat were high viral load, high insulin and participant's not taking lipid lowering treatment. Conclusion In patients switching to second line therapy, r/LPV combined with RAL demonstrated similar improvements in limb fat as an N(t)RTI

Published
2013

44. Ritonavir-boosted lopinavir plus nucleoside or nucleotide reverse transcriptase inhibitors versus ritonavir-boosted lopinavir plus raltegravir for treatment of HIV-1 infection in adults with virological failure of a standard first-line ART regimen (SECOND-LINE): a randomised, open-label, non-inferiority study

Author

SECOND-LINE Study Group, Boyd, Mark A, Kumarasamy, N, Moore, Cecilia L, Nwizu, C, Losso, M H, Mohapi, L, Martin, Allison, Kerr, S, Sohn, A H, Teppler, H, Van De Steen, O, Molina, J-M, Emery, Sean, Cooper, David A, SECOND-LINE Study Group, Boyd, Mark A, Kumarasamy, N, Moore, Cecilia L, Nwizu, C, Losso, M H, Mohapi, L, Martin, Allison, Kerr, S, Sohn, A H, Teppler, H, Van De Steen, O, Molina, J-M, Emery, Sean, and Cooper, David A

Abstract

Background Uncertainty exists about the best treatment for people with HIV-1 who have virological failure with first-line combination antiretroviral therapy of a non-nucleoside analogue (NNRTI) plus two nucleoside or nucleotide analogue reverse transcriptase inhibitors (NtRTI). We compared a second-line regimen combining two new classes of drug with a WHO-recommended regimen. Methods We did this 96-week, phase 3b/4, randomised, open-label non-inferiority trial at 37 sites worldwide. Adults with HIV-1 who had confirmed virological failure (plasma viral load >500 copies per mL) after 24 weeks or more of first-line treatment were randomly assigned (1:1) to receive ritonavir-boosted lopinavir plus two or three NtRTIs (control group) or ritonavir-boosted lopinavir plus raltegravir (raltegravir group). The randomisation sequence was computer generated with block randomisation (block size four). Neither participants nor investigators were masked to allocation. The primary endpoint was the proportion of participants with plasma viral load less than 200 copies per mL at 48 weeks in the modified intention-to-treat population, with a non-inferiority margin of 12%. This study is registered with ClinicalTrials.gov, number NCT00931463. Findings We enrolled 558 patients, of whom 541 (271 in the control group, 270 in the raltegravir group) were included in the primary analysis. At 48 weeks, 219 (81%) patients in the control group compared with 223 (83%) in the raltegravir group met the primary endpoint (difference 1·8%, 95% CI −4·7 to 8·3), fulfilling the criterion for non-inferiority. 993 adverse events occurred in 271 participants in the control group versus 895 in 270 participants in the raltegravir group, the most common being gastrointestinal. Interpretation The raltegravir regimen was no less efficacious than the standard of care and was safe and well tolerated. This simple NtRTI-free treatment strategy might extend the successful public health approach to management of HIV b

Published
2013

45. Bone mineral density in HIV participants randomized to raltegravir and lopinavir/ritonavir compared with standard second line therapy

Author

Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, Boyd, Mark A, Martin, Allison, Moore, Cecilia L, Mallon, Patrick W. G, Hoy, Jennifer F, Emery, Sean, Belloso, Waldo H, Phanuphak, Praphan, Ferret, Samuel, Cooper, David A, and Boyd, Mark A

Abstract

Objective: To compare changes over 48 weeks in bone mineral density (BMD) between participants randomized to lopinavir/ritonavir (LPV/r) + raltegravir (RAL) or LPV/r + 2-3 nucleoside/nucleotide reverse transcriptase inhibitors (N(t)RTIs) as second line therapy. Design: 48-week open-label sub-study of the Second Line trial conducted in South Africa, India, Thailand, Malaysia and Argentina. Methods: Dual energy X-ray absorptiometry scans of proximal femur and lumbar spine were performed at baseline and week 48. Linear regression was used to compare means of differences between arms. McNemars test compared osteopenia and osteoporosis. Associations between percentage BMD changes and baseline variables were assessed by multivariate linear regression. Results: Two hundred and ten participants were randomized. Analyses were adjusted for sex, BMI and smoking status. Mean (95% CI) proximal femur BMD% reduced over 48 weeks by -5.2% (-6.7 to -3.8%) in the LPV/r+2-3N(t)RTIs arm and by -2.9% (-4.3 to -1.5%) in the LPV/r+RAL arm (P = 0.0001). Lumbar spine BMD reduced by -4.2% (-5.7 to -2.7%) in the LPV/r+2-3N(t)RTIs arm and by -2.0% (-3.5 to -0.6%) in the LPV/r+RAL arm (P = 0.0006). The incidence of osteopenia (7.6%) and osteoporosis (2.0%) assessed over 48 weeks were similar between arms. Reduced BMD over 48 weeks was significantly associated with longer duration of tenofovir on study [% change (SE) -1.58 (0.38) femur, -1.65 (0.38) spine, P = 0.0001] and low baseline BMI [% change (SE) 0.5 (0.13) femur, 0.17 (0.07) spine; P < 0.01]. Conclusion: An N(t)RTI-sparing antiretroviral regimen of LPV/r and raltegravir as second line therapy is associated with less bone loss than a LPV/r regimen containing N(t)RTIs.

Published
2013

46. Considerations in the rationale, design and methods of the Strategic Timing of AntiRetroviral Treatment (START) study

Author

Babiker, Abdel G, Emery, Sean, Fätkenheuer, Gerd, Gordin, Fred M, Grund, Birgit, Lundgren, Jens D, Neaton, James D, Pett, Sarah L, Phillips, Andrew, Touloumi, Giota, Vjechaj, Michael J, Babiker, Abdel G, Emery, Sean, Fätkenheuer, Gerd, Gordin, Fred M, Grund, Birgit, Lundgren, Jens D, Neaton, James D, Pett, Sarah L, Phillips, Andrew, Touloumi, Giota, and Vjechaj, Michael J

Abstract

Untreated human immunodeficiency virus (HIV) infection is characterized by progressive depletion of CD4+ T lymphocyte (CD4) count leading to the development of opportunistic diseases (acquired immunodeficiency syndrome (AIDS)), and more recent data suggest that HIV is also associated with an increased risk of serious non-AIDS (SNA) diseases including cardiovascular, renal, and liver diseases and non-AIDS-defining cancers. Although combination antiretroviral treatment (ART) has resulted in a substantial decrease in morbidity and mortality in persons with HIV infection, viral eradication is not feasible with currently available drugs. The optimal time to start ART for asymptomatic HIV infection is controversial and remains one of the key unanswered questions in the clinical management of HIV-infected individuals.

Published
2013

47. Involvement of the Endocannabinoid System in the Development and Treatment of Breast Cancer

Author

VIRGINIA COMMONWEALTH UNIV RICHMOND, Emery, Sean, VIRGINIA COMMONWEALTH UNIV RICHMOND, and Emery, Sean

Abstract

The synthetic cannabinoids, Win55,212-2 (Win2), enhanced the growth-inhibitory response to ionizing radiation in three different (MCF7, MDA-MB-231 and 4T1) experimental breast tumor cell lines. Studies using an inactive analog of Win-2 demonstrated that this effect was structure-specific. This finding was confirmed in an immune-competent (4T1) rodent model of tumor growth. Unexpectedly, Win2 failed to improve the response to a variety of cancer chemotherapeutic agents such as Adriamycin and Paclitaxel; studies in vivo also failed to demonstrate that the combination of Win-2 + Adriamycin was more effective than Adriamycin alone. However, in view of the fact that cannabinoids are currently used to improve the quality of life for cancer chemotherapy patients, the absence of antagonistic effects suggests that Win2 could be used in combination with radiation and chemotherapy without interfering with the effectiveness of chemotherapeutic agents as antitumor drugs., The original document contains color images.

Published
2012

48. The influence of HLA supertype on thymidine analogue associated with low peripheral fat in HIV

Author

Cordery, Damien V, Martin, Allison, Amin, Janaki, Kelleher, Anthony D, Emery, Sean, Cooper, David A, Cordery, Damien V, Martin, Allison, Amin, Janaki, Kelleher, Anthony D, Emery, Sean, and Cooper, David A

Abstract

Objectives: To examine the relationship between human leukocyte antigen (HLA) genotype and body composition changes induced by thymidine analogue nucleoside reverse transcriptase inhibitor (NtRTI) use in HIV-positive individuals. Design: Data collected during the Simplification with Tenofovir-Emtricitabine (TDF-FTC) or Abacavir-Lamivudine (ABC-3TC) (STEAL) study were analysed to examine the potential association of HLA genotypes with changes in body composition in treatment-experienced HIV-positive individuals. Methods: Demographic, HIV-related, body composition and HLA genotyping data from the STEAL study were used in this analysis. The mean percentage peripheral fat at study baseline was compared in participants with and without prior NtRTI use. Analyses were also carried out for each HLA supertype strata, for five HLA genes, within the thymidine-exposed group. These comparisons were made using Mann-Whitney rank-sum tests. Results: Participants with prior NtRTI use had a significantly lower baseline mean peripheral fat percentage compared to those without NtRTI use (31.9 vs. 34.7%; P = 0.0045). However, participants carrying one or more of the three particular HLA supertype alleles, A01, B08 and DQ2, showed no significant difference in mean peripheral fat percentage at baseline by NtRTI use. Among participants with prior NtRTI exposure, there were significant differences in mean peripheral fat by HLA A01, B08 and DQ2 allele expression compared to those without expression of these alleles (A01: 34.91% vs. no A01: 30.3%; P = 0.0087; B08: 36.2% vs. no B08: 31.1%; P = 0.0317; DQ2: 35.16% vs. no DQ2: 30.06%; P = 0.0081). Conclusion: This analysis suggests that HIV-infected individuals carrying HLA A01, B08 or DQ2 supertype alleles may be resistant to NtRTI-induced peripheral fat loss.

Published
2012

49. The influence of HLA supertype on thymidine analogue associated with low peripheral fat in HIV

Author

Cordery, Damien V, Martin, Allison, Amin, Janaki, Kelleher, Anthony D, Emery, Sean, Cooper, David A, Cordery, Damien V, Martin, Allison, Amin, Janaki, Kelleher, Anthony D, Emery, Sean, and Cooper, David A

Abstract

Objectives: To examine the relationship between human leukocyte antigen (HLA) genotype and body composition changes induced by thymidine analogue nucleoside reverse transcriptase inhibitor (NtRTI) use in HIV-positive individuals. Design: Data collected during the Simplification with Tenofovir-Emtricitabine (TDF-FTC) or Abacavir-Lamivudine (ABC-3TC) (STEAL) study were analysed to examine the potential association of HLA genotypes with changes in body composition in treatment-experienced HIV-positive individuals. Methods: Demographic, HIV-related, body composition and HLA genotyping data from the STEAL study were used in this analysis. The mean percentage peripheral fat at study baseline was compared in participants with and without prior NtRTI use. Analyses were also carried out for each HLA supertype strata, for five HLA genes, within the thymidine-exposed group. These comparisons were made using Mann-Whitney rank-sum tests. Results: Participants with prior NtRTI use had a significantly lower baseline mean peripheral fat percentage compared to those without NtRTI use (31.9 vs. 34.7%; P = 0.0045). However, participants carrying one or more of the three particular HLA supertype alleles, A01, B08 and DQ2, showed no significant difference in mean peripheral fat percentage at baseline by NtRTI use. Among participants with prior NtRTI exposure, there were significant differences in mean peripheral fat by HLA A01, B08 and DQ2 allele expression compared to those without expression of these alleles (A01: 34.91% vs. no A01: 30.3%; P = 0.0087; B08: 36.2% vs. no B08: 31.1%; P = 0.0317; DQ2: 35.16% vs. no DQ2: 30.06%; P = 0.0081). Conclusion: This analysis suggests that HIV-infected individuals carrying HLA A01, B08 or DQ2 supertype alleles may be resistant to NtRTI-induced peripheral fat loss.

Published
2012

50. Predictors of limb fat gain in HIV positive patients following a change to tenofovir-emtricitabine or Abacavir-Lamivudine

Author

Martin, Allison, Amin, Janaki, Emery, Sean, Baker, David, Carr, Andrew, Cooper, David A, Bloch, Mark, Martin, Allison, Amin, Janaki, Emery, Sean, Baker, David, Carr, Andrew, Cooper, David A, and Bloch, Mark

Abstract

Background Antiretroviral treatment (cART) in HIV causes lipoatrophy. We examined predictors of anthropometric outcomes over 96 weeks in HIV-infected, lipoatrophic adults receiving stable cART randomised to tenofovir-emtricitabine (TDF-FTC) or abacavir-lamivudine (ABC-3TC) fixed dose combinations. Methodology/Principal Findings The STEAL study was a prospective trial of virologically suppressed participants randomised to either TDF-FTC (n = 178) or ABC-3TC (n = 179). Anthropometric assessment was conducted at baseline, weeks 48 and 96. The analysis population included those with baseline and week 96 data remaining on randomised therapy. Distribution of limb fat change was divided into four categories (≤0%, >0-10%, >10-20%, >20%). Baseline characteristics [demographics, medical history, metabolic and cardiovascular biomarkers] were assessed as potential predictors of change in percent subcutaneous limb fat using linear regression. 303 participants (85% of STEAL population) were included. Baseline characteristics were: mean (±SD) age 45 (±8) years; thymidine analogue nucleoside reverse transcriptase inhibitor (tNRTI) duration 4 (±3) years; limb fat 5.4 (±3.0)kg; body mass index 24.7 (±3.5) kg/m2. Mean (SD) limb fat gain to week 48 and 96 was 7.6% (±22.4) and 13.2% (±27.3), respectively, with no significant difference between groups. 51.5% of all participants had >10% gain in limb fat. Predictors of greater limb fat gain at week 96 were baseline tNRTI (10.3, p = 0.001), glucose >6 mmol/L (16.1, p = 0.04), higher interleukin 6 (IL-6) (2.8, p = 0.004) and lower baseline limb fat (3.8-6.4 kg - 11.2; >6.4 kg - 15.7, p trend<0.001). Conclusions/Significance Modest peripheral fat gain occurred with both TDF-FTC and ABC-3TC. Baseline factors associated with more severe lipodystrophy (lipoatrophy, baseline tNRTI, raised IL6, and glucose) predicted greater limb fat recovery at 96 weeks.

Published
2011

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