2,268 results on '"Sabin, Caroline A."'
Search Results
2. Associations between multimorbidity burden and objective and patient-reported sleep outcomes among people living with HIV
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Sukumaran, Luxsena, Sabin, Caroline A., Kunisaki, Ken M., Doyle, Nicki, Post, Frank A., Vera, Jaime, Mallon, Patrick WG, Sachikonye, Memory, Boffito, Marta, Anderson, Jane, and Winston, Alan
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- 2024
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3. Exploring the concept of unmet need within sexual and reproductive health in England: A qualitative Delphi exercise
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Solomon, Danielle, Gibbs, Jo, Burns, Fiona, and Sabin, Caroline A
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- 2024
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4. Experiences of mpox illness and case management among cis and trans gay, bisexual and other men who have sex with men in England: a qualitative study
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Witzel, T Charles, Ghobrial, Andrew, Palich, Romain, Charles, Hannah, Rodger, Alison J., Sabin, Caroline, Sparrowhawk, Alex, Pool, Erica R.M., Prochazka, Mateo, Vivancos, Roberto, Sinka, Katy, Folkard, Kate, Burns, Fiona M., and Saunders, John
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- 2024
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5. A scoping review of media campaign strategies used to reach populations living with or at high risk for Hepatitis C in high income countries to inform future national campaigns in the United Kingdom
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Etoori, David, Desai, Monica, Mandal, Sema, Rosenberg, William, and Sabin, Caroline A
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- 2023
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6. Facilitators and barriers to community pharmacy PrEP delivery: a scoping review
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Harrison, China, Family, Hannah, Kesten, Joanna, Denford, Sarah, Scott, Anne, Dawson, Sarah, Scott, Jenny, Sabin, Caroline, Copping, Joanna, Harryman, Lindsey, Cochrane, Sarah, and Horwood, Jeremy
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Secondary data analysis -- Management ,Drugstores -- Services ,HIV infection -- Prevention ,Company business management ,Health - Abstract
: Introduction: Pre‐exposure prophylaxis (PrEP) is an effective medication to reduce the risk of acquiring HIV. PrEP is available free of charge in the UK from sexual health clinics. Expanding PrEP delivery to community pharmacies holds promise and aligns with UK government goals to eliminate new cases of HIV by 2030. The aim of this scoping review was to describe the existing evidence about the barriers to and facilitators of community pharmacy oral PrEP delivery, for pharmacists and pharmacy clients, as aligned with the Capacity Opportunity, Motivation Behaviour (COM‐B) Model. Methods: Five bibliographic and five review databases were searched from inception to August 2023. Literature of any study design was included if it discussed barriers and facilitators of community pharmacy PrEP delivery. Trial registrations, protocols and news articles were excluded. Results: A total of 649 records were identified, 73 full texts were reviewed and 56 met the inclusion criteria, predominantly from high‐income/westernized settings. Most of the included literature was original research (55%), from the United States (77%) conducted during or after the year 2020 (63%). Barriers to PrEP delivery for pharmacists included lack of knowledge, training and skills (capability), not having the necessary facilities (opportunity), concern about the costs of PrEP and believing that PrEP use could lead to risk behaviours and sexually transmitted infections (motivation). Facilitators included staff training (capability), time, the right facilities (opportunity), believing PrEP could be a source of profit and could reduce new HIV acquisitions (motivation). For clients, barriers included a lack of PrEP awareness (capability), pharmacy facilities (opportunity) and not considering pharmacists as healthcare providers (motivation). Facilitators included awareness of PrEP and pharmacist's training to deliver it (capability), the accessibility of pharmacies (opportunity) and having an interest in PrEP (motivation). Discussion: To effectively enhance oral PrEP delivery in UK community pharmacies, the identified barriers and facilitators should be explored for UK relevance, addressed and leveraged at the pharmacy team, client and care pathway level. Conclusions: By comprehensively considering all aspects of the COM‐B framework, community pharmacies could become crucial providers in expanding PrEP accessibility, contributing significantly to HIV prevention efforts., INTRODUCTION The human immunodeficiency virus (HIV) epidemic remains a significant public health concern worldwide. In 2021, it was estimated that there were 105,200 people living with HIV in the UK, [...]
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- 2024
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7. HIV pre-exposure prophylaxis and its implementation in the PrEP Impact Trial in England: a pragmatic health technology assessment
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Sullivan, Ann K, Saunders, John, Desai, Monica, Cartier, Andrea, Mitchell, Holly D, Jaffer, Sajjida, Ogaz, Dana, Chiavenna, Chiara, Charlett, Andre, Diamente, Victor, Golombek, Rainer, Manavi, Kaveh, Priestley, Cecilia, Waters, Laura J, Milinkovic, Ana, McOwan, Alan, Estcourt, Claudia, Sabin, Caroline A, Rodger, Alison, Gold, Deborah, Gazzard, Brian G, McCormack, Sheena, and Gill, O Noel
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- 2023
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8. Anti-Hepatitis C (HCV) test positivity and new HCV diagnoses among women tested in antenatal services in England between 2015-2019
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Hibbert, Matthew, Simmons, Ruth, Mandal, Sema, Sabin, Caroline A, and Desai, Monica
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- 2023
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9. Integrase strand-transfer inhibitor use and cardiovascular events in adults with HIV: an emulation of target trials in the HIV-CAUSAL Collaboration and the Antiretroviral Therapy Cohort Collaboration
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Rein, Sophia M, Lodi, Sara, Logan, Roger W, Touloumi, Giota, Antoniadou, Anastasia, Wittkop, Linda, Bonnet, Fabrice, van Sighem, Ard, van der Valk, Marc, Reiss, Peter, Klein, Marina B, Young, James, Jarrin, Inmaculada, d'Arminio Monforte, Antonella, Tavelli, Alessandro, Meyer, Laurence, Tran, Laurent, Gill, Michael J, Lang, Raynell, Surial, Bernard, Haas, Andreas D, Justice, Amy C, Rentsch, Christopher T, Phillips, Andrew, Sabin, Caroline A, Miro, Jose M, Trickey, Adam, Ingle, Suzanne M, Sterne, Jonathan A C, and Hernán, Miguel A
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- 2023
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10. HIV-1 drug resistance in people on dolutegravir-based antiretroviral therapy: a collaborative cohort analysis
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Loosli, Tom, Hossmann, Stefanie, Ingle, Suzanne M, Okhai, Hajra, Kusejko, Katharina, Mouton, Johannes, Bellecave, Pantxika, van Sighem, Ard, Stecher, Melanie, d'Arminio Monforte, Antonella, Gill, M John, Sabin, Caroline A, Maartens, Gary, Günthard, Huldrych F, Sterne, Jonathan A C, Lessells, Richard, Egger, Matthias, and Kouyos, Roger D
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- 2023
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11. Genetic Variants of APOL1 Are Major Determinants of Kidney Failure in People of African Ancestry With HIV
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Booth, John, Waters, Anele, Hand, James, Clarke, Chris, Murphy, Sarah, Murphy, Maurice, Campbell, Marion, Clarke, Amanda, Richardson, Celia, Knott, Alyson, Weir, Gemma, Cleig, Rebecca, Soviarova, Helena, Barbour, Lisa, Adams, Tanya, Kennard, Vicky, Trevitt, Vittorio, Jones, Rachael, Levy, Jeremy, Schoolmeester, Alexandra, Duro, Serah, Hilton, Rachel, Fox, Julie, Rabuya, May, Hamzah, Lisa, Jordan, Deborah, Solano, Teresa, Uzu, Hiromi, Williams, Karen, Lwanga, Julianne, Reid-Amoruso, Linda Ekaette, Gamlen, Hannah, Stocker, Robert J., Ryan, Fiona, Mahiouz, Karina, Cheetham, Tess, Williams, Claire, Nori, Achyuta, Thomas, Caroline, Venkateshwaran, Sivaraj, Doctor, Jessica, Berlanga, Andrea, Post, Frank, Santana-Suarez, Beatriz, McQueen, Leigh, Bhagwandin, Priya, Campbell, Lucy, Barbini, Bee, Wandolo, Emily, Appleby, Tim, Driver, Lois, Parr, Sophy, Deng, Hongbo, Barber, Julie, Crowe, Andrew, Taylor, Chris, Poulton, Mary, Boateng, Vida, Klein, Marie-Pierre, O'Brien, Caitlin, Ohene-Adomako, Samuel, Buckingham, Christian, Trotman, Daniel, Quinn, Killian, Flanagan, Kate, Sullivan, Verity, Middleditch, Holly, Samuel, Itty, Hamlyn, Elizabeth, McDonald, Candice, Canoso, Ana, Agbasi, Emeka, Liskova, Maria, Barber, Sarah, Samarawickrama, Amanda, Ottaway, Zoe, Norcross, Claire, Oliveira, Amelia, Bramham, Kate, Minton, Jane, Lamont, Gary, Cross, Ruby, Saiyad, Gaushiya, Ahmed, Shadia, Ashworth, Rebecca, Window, Nicola, Murira, J., Phyu, Khine, Ustianowski, Andrew, Lindergard, Gabriella, Shaw, Jonathan, Holland, Sarah, Fox, Claire, Flaherty, Jan, Bevan, Margaret-Anne, George, Valerie, Chadwick, David, Branch, Marie, Lambert, Pauline, Craggs, Adele, Pett, Sarah, Lukha, Hinal, Vora, Nina, Fiorino, Marzia, Nunez, Maria Muller, Sally, Deirdre, Burns, James E., Pool, Erica, Matthews, Rebecca, Price, David Ashley, Stothard, Tara, Patel, Bijal, McVittie, Ian, Kennedy, Ciara, Shwab, Uli, Payne, Brendan, Duncan, Sarah, Dixon, Jill, Schmid, Mathias, Evans, Adam, Duncan, Christopher, Hunter, Ewan, Taha, Yusri, Astill, Natasha, Winkler, Cheryl, Binns-Roemer, Elizabeth, David, Victor, Ainsworth, Jonathan, Vincent, Rachel, Kegg, Stephen, Saad, Chloe, Skinner, Sarah, Azzoug, Hocine, Russell, Judith, Moussaoui, Tarik, Mabonga, Emily, Ward, Donna, Francoise, J., Larbi, W., Mitchell, Sue, Manning, A., Russell, V., Burns, Fiona, Harber, Mark, Ngwu, Nnenna, Edwards, Jonathan, Hemat, Nargis, Fernandez, Tom, Ferro, Filippo, Ferreira, Jorge, Nightingale, Alice, Oakes-Monger, Tasha, Matila, Darwin, Nogueira, Pedro, Mutagwanya, Victoria, Cosgrove, Catherine, Isitt, Catherine Emily, Webb, Helen, Popoola, Joyce, Korley, Kate, Mencias, Mark, Ribeiro, Patricia, Ramkhelawn, Rajeshwar, Lara, Sandra Oliva, Sajijad, Sara, Winston, Alan, Shaw, Amber, Petersen, Claire, Ring, Kyle, Rosenvinge, Melanie, Moyo, Thembi, Odong, Faith, Gantert, Katherine, Ibe, Tina, Onyango, Denis, Sabin, Caroline, Hill, Teresa, Hung, Rachel K.Y., Booth, John W., Price, David A., Sabin, Caroline A., Winkler, Cheryl A., and Post, Frank A.
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- 2022
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12. Sickle Cell Trait and Kidney Disease in People of African Ancestry With HIV
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Booth, John, Waters, Anele, Hand, James, Clarke, Chris, Murphy, Sarah, Murphy, Maurice, Campbell, Marion, Clarke, Amanda, Richardson, Celia, Knott, Alyson, Weir, Gemma, Cleig, Rebecca, Soviarova, Helena, Barbour, Lisa, Adams, Tanya, Kennard, Vicky, Trevitt, Vittorio, Jones, Rachael, Levy, Jeremy, Schoolmeester, Alexandra, Duro, Serah, Hilton, Rachel, Fox, Julie, Rabuya, May, Hamzah, Lisa, Jordan, Deborah, Solano, Teresa, Uzu, Hiromi, Williams, Karen, Lwanga, Julianne, Reid-Amoruso, Linda Ekaette, Gamlen, Hannah, Stocker, Robert J., Ryan, Fiona, Mahiouz, Karina, Cheetham, Tess, Williams, Claire, Nori, Achyuta, Thomas, Caroline, Venkateshwaran, Sivaraj, Doctor, Jessica, Berlanga, Andrea, Post, Frank, Santana-Suarez, Beatriz, McQueen, Leigh, Bhagwandin, Priya, Campbell, Lucy, Barbini, Bee, Wandolo, Emily, Appleby, Tim, Driver, Lois, Parr, Sophy, Deng, Hongbo, Barber, Julie, Crowe, Andrew, Taylor, Chris, Poulton, Mary, Boateng, Vida, Klein, Marie-Pierre, O’Brien, Caitlin, Ohene-Adomako, Samuel, Buckingham, Christian, Trotman, Daniel, Quinn, Killian, Flanagan, Kate, Sullivan, Verity, Middleditch, Holly, Samuel, Itty, Hamlyn, Elizabeth, McDonald, Candice, Canoso, Ana, Agbasi, Emeka, Liskova, Maria, Barber, Sarah, Samarawickrama, Amanda, Ottaway, Zoe, Norcross, Claire, Oliveira, Amelia, Bramham, Kate, Minton, Jane, Lamont, Gary, Cross, Ruby, Saiyad, Gaushiya, Ahmed, Shadia, Ashworth, Rebecca, Window, Nicola, Murira, J., Phyu, Khine, Ustianowski, Andrew, Lindergard, Gabriella, Shaw, Jonathan, Holland, Sarah, Fox, Claire, Flaherty, Jan, Bevan, Margaret-Anne, George, Valerie, Chadwick, David, Branch, Marie, Lambert, Pauline, Craggs, Adele, Pett, Sarah, Lukha, Hinal, Vora, Nina, Fiorino, Marzia, Nunez, Maria Muller, Sally, Deirdre, Burns, James E., Pool, Erica, Matthews, Rebecca, Price, David Ashley, Stothard, Tara, Patel, Bijal, McVittie, Ian, Kennedy, Ciara, Shwab, Uli, Payne, Brendan, Duncan, Sarah, Dixon, Jill, Schmid, Mathias, Evans, Adam, Duncan, Christopher, Hunter, Ewan, Taha, Yusri, Astill, Natasha, Winkler, Cheryl, Binns-Roemer, Elizabeth, David, Victor, Ainsworth, Jonathan, Vincent, Rachel, Kegg, Stephen, Saad, Chloe, Skinner, Sarah, Azzoug, Hocine, Russell, Judith, Moussaoui, Tarik, Mabonga, Emily, Ward, Donna, Francoise, J., Larbi, W., Mitchell, Sue, Manning, A., Russell, V., Burns, Fiona, Harber, Mark, Ngwu, Nnenna, Edwards, Jonathan, Hemat, Nargis, Fernandez, Tom, Ferro, Filippo, Ferreira, Jorge, Nightingale, Alice, Oakes-Monger, Tasha, Matila, Darwin, Nogueira, Pedro, Mutagwanya, Victoria, Cosgrove, Catherine, Isitt, Catherine Emily, Webb, Helen, Popoola, Joyce, Korley, Kate, Mencias, Mark, Ribeiro, Patricia, Ramkhelawn, Rajeshwar, Lara, Sandra Oliva, Sajijad, Sara, Winston, Alan, Shaw, Amber, Petersen, Claire, Ring, Kyle, Rosenvinge, Melanie, Moyo, Thembi, Odong, Faith, Gantert, Katherine, Ibe, Tina, Onyango, Denis, Sabin, Caroline, Hill, Teresa, Hung, Rachel K.Y., Booth, John W., Price, David A., Sharpe, Claire C., Sabin, Caroline A., Winkler, Cheryl A., and Post, Frank A.
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- 2022
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13. Humoral and cellular immune responses eleven months after the third dose of BNT162b2 an mRNA-based COVID-19 vaccine in people with HIV – a prospective observational cohort study
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Heftdal, Line Dam, Pérez-Alós, Laura, Hasselbalch, Rasmus Bo, Hansen, Cecilie Bo, Hamm, Sebastian Rask, Møller, Dina Leth, Pries-Heje, Mia, Fogh, Kamille, Gerstoft, Jan, Grønbæk, Kirsten, Ostrowski, Sisse Rye, Frikke-Schmidt, Ruth, Sørensen, Erik, Hilsted, Linda, Bundgaard, Henning, Garred, Peter, Iversen, Kasper, Sabin, Caroline, and Nielsen, Susanne Dam
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- 2023
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14. Life expectancy after 2015 of adults with HIV on long-term antiretroviral therapy in Europe and North America: a collaborative analysis of cohort studies
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Trickey, Adam, Sabin, Caroline A, Burkholder, Greer, Crane, Heidi, d'Arminio Monforte, Antonella, Egger, Matthias, Gill, M John, Grabar, Sophie, Guest, Jodie L, Jarrin, Inma, Lampe, Fiona C, Obel, Niels, Reyes, Juliana M, Stephan, Christoph, Sterling, Timothy R, Teira, Ramon, Touloumi, Giota, Wasmuth, Jan-Christian, Wit, Ferdinand, Wittkop, Linda, Zangerle, Robert, Silverberg, Michael J, Justice, Amy, and Sterne, Jonathan A C
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- 2023
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15. Hepatitis B virus infection in general practice across England: An analysis of the Royal College of General Practitioners Research and Surveillance Centre real-world database
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Geretti, Anna Maria, Austin, Harrison, Villa, Giovanni, Smith, Colette, Sabin, Caroline, Tsang, Ruby, Sherlock, Julian, Ferreira, Filipa, Byford, Rachel, Meza-Torres, Bernardo, Whyte, Martin, and de Lusignan, Simon
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- 2023
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16. Association of pregnancy with engagement in HIV care among women with HIV in the UK: a cohort study
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Ainsworth, Jonathan, Allan, Sris, Anderson, Jane, Apoola, Ade, Chadwick, David, Churchill, Duncan, Delpech, Valerie, Dunn, David, Fairley, Ian, Fox, Ashini, Gilson, Richard, Gompels, Mark, Hay, Phillip, Hembrom, Rajesh, Hill, Teresa, Johnson, Margaret, Jose, Sophie, Kegg, Stephen, Leen, Clifford, Mital, Dushyant, Nelson, Mark, Okhai, Hajra, Orkin, Chloe, Palfreeman, Adrian, Phillips, Andrew, Pillay, Deenan, Price, Ashley, Post, Frank, Pritchard, Jillian, Sabin, Caroline, Schwenk, Achim, Tariq, Anjum, Trevelion, Roy, Ustianowski, Andy, Walsh, John, Tariq, Shema, Burns, Fiona, Gilleece, Yvonne, Dhairyawan, Rageshri, Peters, Helen, Thorne, Claire, and Sabin, Caroline A
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- 2021
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17. Changes in short-term (in-ICU and in-hospital) mortality following intensive care unit admission in adults living with HIV: 2000–2019
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Kanitkar, Tanmay, Dissanayake, Oshani, Bakewell, Nicholas, Symonds, Maggie, Rimmer, Stephanie, Adlakha, Amit, Lipman, Marc C.I., Bhagani, Sanjay, Sabin, Caroline A., Agarwal, Banwari, and Miller, Robert F.
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- 2023
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18. Recommendations for defining preventable HIV-related mortality for public health monitoring in the era of Getting to Zero: an expert consensus
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Croxford, Sara E, Martin, Veronique, Lucas, Sebastian B, Miller, Robert F, Post, Frank A, Anderson, Jane, Apea, Vanessa J, Asboe, David, Brough, Garry, Chadwick, David R, Collins, Simon, Corkin, Helen, Dean, Gillian, Delpech, Valerie C, Gogia, Maka, Gold, Deborah, Kafkalias, Anna, Korkodilos, Marilena, Kowalska, Justyna D, Lindo, Jacqueline, Lundgren, Jens D, Lynch, Lucy, Martinez, Esteban, McDougall, Niall, North, Sarah, Rockstroh, Juergen K, Sabin, Caroline, Vidal-Read, Maria, Waters, Laura J, and Sullivan, Ann K
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- 2023
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19. Emulating a trial of joint dynamic strategies: An application to monitoring and treatment of HIV‐positive individuals
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Caniglia, Ellen C, Robins, James M, Cain, Lauren E, Sabin, Caroline, Logan, Roger, Abgrall, Sophie, Mugavero, Michael J, Hernández‐Díaz, Sonia, Meyer, Laurence, Seng, Remonie, Drozd, Daniel R, Seage, George R, Bonnet, Fabrice, Le Marec, Fabien, Moore, Richard D, Reiss, Peter, van Sighem, Ard, Mathews, William C, Jarrín, Inma, Alejos, Belén, Deeks, Steven G, Muga, Roberto, Boswell, Stephen L, Ferrer, Elena, Eron, Joseph J, Gill, John, Pacheco, Antonio, Grinsztejn, Beatriz, Napravnik, Sonia, Jose, Sophie, Phillips, Andrew, Justice, Amy, Tate, Janet, Bucher, Heiner C, Egger, Matthias, Furrer, Hansjakob, Miro, Jose M, Casabona, Jordi, Porter, Kholoud, Touloumi, Giota, Crane, Heidi, Costagliola, Dominique, Saag, Michael, and Hernán, Miguel A
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Epidemiology ,Statistics ,Health Sciences ,Mathematical Sciences ,Infectious Diseases ,Clinical Research ,Sexually Transmitted Infections ,Clinical Trials and Supportive Activities ,HIV/AIDS ,Infection ,Adult ,Anti-HIV Agents ,CD4 Lymphocyte Count ,Decision Making ,Drug Monitoring ,Female ,HIV Infections ,Humans ,Male ,Middle Aged ,RNA ,Viral ,Research Design ,Survival Analysis ,Viral Load ,causal inference ,dynamic regime ,joint treatment strategies ,marginal structural model ,no direct effect ,Public Health and Health Services ,Statistics & Probability - Abstract
Decisions about when to start or switch a therapy often depend on the frequency with which individuals are monitored or tested. For example, the optimal time to switch antiretroviral therapy depends on the frequency with which HIV-positive individuals have HIV RNA measured. This paper describes an approach to use observational data for the comparison of joint monitoring and treatment strategies and applies the method to a clinically relevant question in HIV research: when can monitoring frequency be decreased and when should individuals switch from a first-line treatment regimen to a new regimen? We outline the target trial that would compare the dynamic strategies of interest and then describe how to emulate it using data from HIV-positive individuals included in the HIV-CAUSAL Collaboration and the Centers for AIDS Research Network of Integrated Clinical Systems. When, as in our example, few individuals follow the dynamic strategies of interest over long periods of follow-up, we describe how to leverage an additional assumption: no direct effect of monitoring on the outcome of interest. We compare our results with and without the "no direct effect" assumption. We found little differences on survival and AIDS-free survival between strategies where monitoring frequency was decreased at a CD4 threshold of 350 cells/μl compared with 500 cells/μl and where treatment was switched at an HIV-RNA threshold of 1000 copies/ml compared with 200 copies/ml. The "no direct effect" assumption resulted in efficiency improvements for the risk difference estimates ranging from an 7- to 53-fold increase in the effective sample size.
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- 2019
20. Associations of modern initial antiretroviral drug regimens with all-cause mortality in adults with HIV in Europe and North America: a cohort study
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Trickey, Adam, Zhang, Lei, Gill, M John, Bonnet, Fabrice, Burkholder, Greer, Castagna, Antonella, Cavassini, Matthias, Cichon, Piotr, Crane, Heidi, Domingo, Pere, Grabar, Sophie, Guest, Jodie, Obel, Niels, Psichogiou, Mina, Rava, Marta, Reiss, Peter, Rentsch, Christopher T, Riera, Melchor, Schuettfort, Gundolf, Silverberg, Michael J, Smith, Colette, Stecher, Melanie, Sterling, Timothy R, Ingle, Suzanne M, Sabin, Caroline A, and Sterne, Jonathan A C
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- 2022
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21. HIV prevention and missed opportunities among people with recently acquired HIV infection: Α protocol for a systematic review.
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Karakosta, Argyro, Ruiz-Burga, Elisa, Tariq, Shema, Touloumi, Giota, Jay Nicholls, Emily, Pantazis, Nikos, Jarrin, Inma, Van der Valk, Marc, Sabin, Caroline, Mussini, Cristina, Meyer, Laurence, Volny Anne, Alain, Carlander, Christina, Grabar, Sophie, Wittkop, Linda, Spire, Bruno, Gill, Jonh, Porter, Kholoud, and Burns, Fiona
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HIV prevention ,HIV infections ,HIV infection transmission ,MEMORY bias ,SCIENCE databases - Abstract
Background: Individuals who have recently acquired HIV represent a unique population because the time frame since HIV acquisition is relatively short and identification of missed HIV prevention opportunities is, therefore, closer to real time and less subject to recall bias. Identifying prevention measures used and missed opportunities for using them, can help stop further HIV transmission. Objectives: This systematic review aims to synthesise current global evidence on uptake of HIV prevention methods among people with recently acquired HIV from 2007, the year that the concept of ART as a prevention method was first introduced. Methods and analysis: MEDLINE/PubMed, EMBASE, PsycINFO, Cochrane and Web of Science databases, will be searched for articles published January 2007—December 2023. Eligible studies will be those that reported on HIV prevention methods among people with recently acquired HIV. Quality assessment of the studies selected will be undertaken, and reporting of the systematic review will be informed by Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines. Results: The systematic review is expected to provide comprehensive insights into the uptake, use and adherence to HIV prevention methods among individuals with recently acquired HIV. Analysis anticipates identifying gaps in prevention coverage, missed opportunities for intervention, and variations in access to and use of prevention strategies. Sociodemographic, personal, and behavioural factors influencing prevention uptake and adherence will also be synthesised. Conclusions: The findings will be of key relevance to researchers, healthcare providers including third sector organisations/ community groups and policymakers, as they will offer insight into better understanding of missed or failed HIV prevention efforts and will help ensure future efforts meet the needs of those in need of them. [ABSTRACT FROM AUTHOR]
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- 2024
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22. Perception of medical care among women living with HIV aged 40 years or older–A European‐wide survey.
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Miron, Victor Daniel, Sabin, Caroline A., Săndulescu, Oana, Lourida, Giota, Kyrychenko, Tetiana, Dragovic, Gordana, Kowalska, Justyna, Mellgren, Åsa, Galindo, M. José, Josh, Jo, and Moseholm, Ellen
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HIV-positive women , *PATIENTS' rights , *HIV infections , *WOMEN'S health services , *RIGHT of privacy - Abstract
Objectives Methods Results Conclusions Our objective was to explore how women living with HIV aged ≥40 years perceive their care in relation to their HIV infection, comorbidities, and menopausal health and to evaluate the extent to which the care they receive meets their expectations, comparatively across World Health Organization (WHO) European regions.We conducted a cross‐sectional survey (May–December 2023) among women living with HIV aged ≥40 years from the WHO European region. Five dimensions of care were assessed: content of care, information, relationship with caregiver, organization of care, and patients' rights and privacy, in addition to management of non‐HIV comorbidities and menopause.In total, 600 women completed the survey; they were predominantly from the Western European region (70.2%), followed by the Eastern (20.2%) and Central (9.6%) regions. The majority of women (46.5%–95.1%) described positive experiences, responding that they were ‘always’ or ‘usually’ satisfied with the five dimensions of HIV care. The concordance between perceptions and experiences of HIV care ranged from 49.4% to 96.1% and was lower in the Eastern region. Among menopausal women, 58.5% were ‘very satisfied’ or ‘satisfied’ with the care they received; satisfaction was significantly lower in Eastern European countries than in Western countries.Our results highlighted a generally high concordance between respondents' expectations and the services provided, including both HIV and non‐HIV care. Women aged ≥40 years living with HIV face several challenges that should be addressed. These findings inform stakeholders and decision‐makers about the need to adopt a more inclusive and sensitive approach in healthcare systems. [ABSTRACT FROM AUTHOR]
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- 2024
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23. HIV, the gut microbiome and clinical outcomes, a systematic review.
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Mac Cann, Rachel, Newman, Ellen, Devane, Declan, Sabin, Caroline, Cotter, Aoife G., Landay, Alan, O'Toole, Paul W., and Mallon, Patrick W.
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SHORT-chain fatty acids ,GUT microbiome ,BACTERIAL diversity ,NON-communicable diseases ,CARDIOVASCULAR diseases ,MICROBIAL metabolites - Abstract
Background: Effective antiretroviral therapy (ART) has improved the life expectancy of people with HIV (PWH). However, this population is now experiencing accelerated age‐related comorbidities, contributed to by chronic immune activation and inflammation, with dysbiosis of the gut microbiome also implicated. Method: We conducted a systematic literature search of PubMed, Embase, Scopus, Cochrane reviews and international conference abstracts for articles that examined for the following non-communicable diseases (NCDs); cardiovascular disease, cancer, frailty, metabolic, bone, renal and neurocognitive disease, in PWH aged >18 years. Studies were included that measured gut microbiome diversity and composition, microbial translocation markers or microbial metabolite markers. Results: In all, 567 articles were identified and screened of which 87 full‐text articles were assessed for eligibility and 56 were included in the final review. The data suggest a high burden NCD, in particular cardiovascular and metabolic disease in PWH. Alterations in bacterial diversity and structure varied by NCD type, but a general trend in reduced diversity was seen together with alterations in bacterial abundances between different NCD. Lipopolysaccharide was the most commonly investigated marker of microbial translocation across NCD followed by soluble CD14. Short-chain fatty acids, tryptophan and choline metabolites were associated with cardiovascular outcomes and also associated with chronic liver disease (CLD). Conclusions: This systematic review is the first to summarise the evidence for the association between gut microbiome dysbiosis and NCDs in PWH. Understanding this interaction will provide insights into the pathogenesis of many NCD and help develop novel diagnostic and therapeutic strategies for PWH. [ABSTRACT FROM AUTHOR]
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- 2024
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24. CROI 2024 BHIVA working group summary.
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Barber, Tristan J., Clarke, Amanda, Fox, Ashini, Mackie, Nicola E., Sabin, Caroline, and Waters, Laura J.
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OPPORTUNISTIC infections ,MEETINGS ,CONFERENCES & conventions ,HIV infections ,RETROVIRUSES ,COVID-19 pandemic - Abstract
The Conference on Retroviruses and Opportunistic Infections (CROI) is usually the most significant HIV conference of the year in terms of basic and clinical scientific output. CROI 2024 in Denver, USA, felt very much back to 'business as usual' following COVID‐19 disruptions that had impacted preceding years, but also felt more global and outward‐ facing. The British HIV Association supports a working group to attend CROI annually and deliver feedback in the UK. This article summarizes the highlights from that meeting. [ABSTRACT FROM AUTHOR]
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- 2024
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25. Correlation between cerebrospinal fluid and plasma neurofilament light protein in treated HIV infection: results from the COBRA study
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Alagaratnam, Jasmini, De Francesco, Davide, Zetterberg, Henrik, Heslegrave, Amanda, Toombs, Jamie, Kootstra, Neeltje A., Underwood, Jonathan, Gisslen, Magnus, Reiss, Peter, Fidler, Sarah, Sabin, Caroline A., and Winston, Alan
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- 2022
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26. The Impact of Time between Booster Doses on Humoral Immune Response in Solid Organ Transplant Recipients Vaccinated with BNT162b2 Vaccines
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Hamm, Sebastian Rask, primary, Loft, Josefine Amalie, additional, Pérez-Alós, Laura, additional, Heftdal, Line Dam, additional, Hansen, Cecilie Bo, additional, Møller, Dina Leth, additional, Pries-Heje, Mia Marie, additional, Hasselbalch, Rasmus Bo, additional, Fogh, Kamille, additional, Hald, Annemette, additional, Ostrowski, Sisse Rye, additional, Frikke-Schmidt, Ruth, additional, Sørensen, Erik, additional, Hilsted, Linda, additional, Bundgaard, Henning, additional, Garred, Peter, additional, Iversen, Kasper, additional, Perch, Michael, additional, Sørensen, Søren Schwartz, additional, Rasmussen, Allan, additional, Sabin, Caroline A., additional, and Nielsen, Susanne Dam, additional
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- 2024
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27. Changes in bodyweight after initiating antiretroviral therapy close to HIV-1 seroconversion: an international cohort collaboration
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Pantazis, Nikos, Sabin, Caroline A, Grabar, Sophie, Van der Valk, Marc, Jarrin, Inma, van Sighem, Ard, Meyer, Laurence, Carlander, Christina, Gill, John, Volny Anne, Alain, Spire, Bruno, Tariq, Shema, Burns, Fiona, Costagliola, Dominique, Ruiz-Burga, Elisa, Touloumi, Giota, Porter, Kholoud, Moreno, Santiago, Burns, Fiona, Campo, Rafael Eduardo, Garges, Harmony, Mussini, Cristina, Pantazis, Nikos, Kamel, Moustafa, Porter, Kholoud, Sabin, Caroline, Tariq, Shema, Touloumi, Giota, Vannappagari, Vani, Anne, Alain Volny, Young, Lital, Gill, John, Carlander, Christina, Grabar, Sophie, Jarrín, Inma, Meyer, Laurence, van der Valk, Marc, Wittkop, Linda, Aisam, Agnes, Barger, Diana, Davidovich, Udi, Dos Santos, Marie, Eriksson, Lars, Fitzgerald, Eli, Karakosta, Argyro, Krentz, Hartmut, Nicholls, Emily Jay, Policek, Nicoletta, Ruiz-Burga, Elisa, Sandford, Chris, Spire, Bruno, Suárez-García, Inés, Abgrall, Sophie, Andriantsoanirina, Valerie, Avettand-Fenoel, Veronique, Bourgeois, Christine, Chaix, Marie-Laure, Cheret, Antoine, Fischer, Hugues, Goujard, Cecile, Lascoux-Combe, Caroline, Le Palec, Annie, Petrov-Sanchez, Ventzlislava, Saez-Cirion, Asier, Seng, Remonie, Stefic, Karl, Tine, Josephine, Piet, E, Gagneux-Brunon, A, Jacomet, C, Piroth, L, Benezit, F, Goussef, M, Tattevin, P, Bani Sadr, B, Lamaury, I, Bazus, H, Robineau, O, Calin, R, Katlama, J, Denis, B, Ghosn, J, Joly, V, Khuong, M A, Caby, F C, Rouveix Nordon, E, de Truchis, P, Abgrall, S, Chéret, A, Duvivier, C, Becker, A, Miailhes, P, Abel, S, Unal, G, Makinson, A, Martin-Blondel, G, Morisot, A, Bregigeon, S, Enel, P, Allavena, C, Rabier, V, Vallet, L, Marchand, L, Saïdi, T, Costagliola, D, Grabar, S, Piet, E, Andriantsoanirina, V, Rabier, V, Fischer, H, Vallet, L, Marchand T Saïdi, L, Costagliola, D, Grabar, S, Abgrall, Sophie, Tattevin, Pierre, de Truchis, Pierre, Fischer, Hughes, Grabar, Sophie, Moreno, Santiago, Jarrín, Inma, Dalmau, David, Navarro, M Luisa, González, M Isabel, Garcia, Federico, Poveda, Eva, Iribarren, Jose Antonio, Gutiérrez, Félix, Rubio, Rafael, Vidal, Francesc, Berenguer, Juan, Muñoz-Fernández, M Ángeles, Adamis, G, Chini, M, Chrysos, G, Marangos, M, Katsarou, O, Kofteridis, D, Metallidis, S, Panagopoulos, P, Papadopoulos, A, Paparizos, V, Psychogiou, M, Sambatakou, H, Sipsas, N V, Touloumi, G, Fox, Julie, Terry, Louise, Waters, Anele, Uriel, Alison, Ustianowski, Andrew, Hackney, Pamela, Fahd, Niaz, Fidler, Sarah, Ayap, Wilbert, Molina, Marcelino, Waters, Laura, Nur, Fowsiya, Fernandez, Thomas, Nugent, Diarmuid, Pinedo, Javier, Reeves, Iain, Fong, Tracy, Nicholls, Jane, Cunningham, Laura, Pangan, Jaydee, Mackintosh, Claire, and Sharp, Louise
- Abstract
Understanding the reasons for and consequences of bodyweight change in people living with HIV initiating antiretroviral therapy (ART) is crucial to optimising long-term health and wellbeing. We aimed to examine bodyweight trends and associated factors among individuals with well estimated dates of HIV-1 seroconversion.
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- 2024
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28. Associations between baseline characteristics, CD4 cell count response and virological failure on first-line efavirenz + tenofovir + emtricitabine for HIV
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Stirrup, Oliver T., Sabin, Caroline A., Phillips, Andrew N., Williams, Ian, Churchill, Duncan, Tostevin, Anna, Hill, Teresa, Dunn, David T., Asboe, David, Pozniak, Anton, Cane, Patricia, Chadwick, David, Clark, Duncan, Collins, Simon, Delpech, Valerie, Douthwaite, Samuel, Dunn, David, Fearnhill, Esther, Porter, Kholoud, Stirrup, Oliver, Fraser, Christophe, Geretti, Anna Maria, Gunson, Rory, Hale, Antony, Hué, Stéphane, Lazarus, Linda, Leigh-Brown, Andrew, Mbisa, Tamyo, Mackie, Nicola, Orkin, Chloe, Nastouli, Eleni, Pillay, Deenan, Phillips, Andrew, Sabin, Caroline, Smit, Erasmus, Templeton, Kate, Tilston, Peter, Volz, Erik, Zhang, Hongyi, Fairbrother, Keith, Dawkins, Justine, O’Shea, Siobhan, Mullen, Jane, Cox, Alison, Tandy, Richard, Fawcett, Tracy, Hopkins, Mark, Booth, Clare, Renwick, Lynne, Schmid, Matthias L., Payne, Brendan, Hubb, Jonathan, Dustan, Simon, Kirk, Stuart, Bradley-Stewart, Amanda, Jose, Sophie, Thornton, Alicia, Huntington, Susie, Glabay, Adam, Shidfar, Shaadi, Lynch, Janet, Hand, James, de Souza, Carl, Perry, Nicky, Tilbury, Stuart, Youssef, Elaney, Gazzard, Brian, Nelson, Mark, Mabika, Tracey, Mandalia, Sundhiya, Anderson, Jane, Munshi, Sajid, Post, Frank, Adefisan, Ade, Taylor, Chris, Gleisner, Zachary, Ibrahim, Fowzia, Campbell, Lucy, Baillie, Kirsty, Gilson, Richard, Brima, Nataliya, Ainsworth, Jonathan, Schwenk, Achim, Miller, Sheila, Wood, Chris, Johnson, Margaret, Youle, Mike, Lampe, Fiona, Smith, Colette, Tsintas, Rob, Chaloner, Clinton, Hutchinson, Samantha, Walsh, John, Mackie, Nicky, Winston, Alan, Weber, Jonathan, Ramzan, Farhan, Carder, Mark, Leen, Clifford, Wilson, Alan, Morris, Sheila, Gompels, Mark, Allan, Sue, Palfreeman, Adrian, Lewszuk, Adam, Kegg, Stephen, Faleye, Akin, Ogunbiyi, Victoria, Mitchell, Sue, Hay, Phillip, Kemble, Christian, Martin, Fabiola, Russell-Sharpe, Sarah, Gravely, Janet, Allan, Sris, Harte, Andrew, Tariq, Anjum, Spencer, Hazel, Jones, Ron, Pritchard, Jillian, Cumming, Shirley, Atkinson, Claire, Mital, Dushyant, Edgell, Veronica, Allen, Juli, Ustianowski, Andy, Murphy, Cynthia, Gunder, Ilise, Trevelion, Roy, and Babiker, Abdel
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- 2019
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29. Association between inflammatory biomarker profiles and cardiovascular risk in individuals with and without HIV
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Sukumaran, Luxsena, Kunisaki, Ken M., Bakewell, Nicholas, Winston, Alan, Mallon, Patrick W.G., Doyle, Nicki, Anderson, Jane, Boffito, Marta, Haddow, Lewis, Post, Frank A., Vera, Jaime H., Sachikonye, Memory, and Sabin, Caroline A.
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- 2023
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30. Defining multimorbidity in people with HIV – what matters most?
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Sukumaran, Luxsena and Sabin, Caroline A.
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- 2023
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31. The epidemiology of kidney disease in people of African ancestry with HIV in the UK
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Hung, Rachel K.Y., Santana-Suarez, Beatriz, Binns-Roemer, Elizabeth, Campbell, Lucy, Bramham, Kate, Hamzah, Lisa, Fox, Julie, Burns, James E., Clarke, Amanda, Vincent, Rachel, Jones, Rachael, Price, David A., Onyango, Denis, Harber, Mark, Hilton, Rachel, Booth, John W., Sabin, Caroline A., Winkler, Cheryl A., and Post, Frank A.
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- 2021
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32. Comparison of Kaposi Sarcoma Risk in Human Immunodeficiency Virus-Positive Adults Across 5 Continents: A Multiregional Multicohort Study
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Judd, Ali, Zangerle, Robert, Touloumi, Giota, Warszawski, Josiane, Meyer, Laurence, Dabis, François, Krause, Murielle Mary, Ghosn, Jade, Leport, Catherine, Wittkop, Linda, Reiss, Peter, Wit, Ferdinand, Prins, Maria, Bucher, Heiner, Gibb, Diana, Fätkenheuer, Gerd, Julia, Del Amo, Obel, Niels, Thorne, Claire, Mocroft, Amanda, Kirk, Ole, Stephan, Christoph, Pérez-Hoyos, Santiago, Hamouda, Osamah, Bartmeyer, Barbara, Chkhartishvili, Nikoloz, Noguera-Julian, Antoni, Antinori, Andrea, Monforte, Antonella d’Arminio, Brockmeyer, Norbert, Prieto, Luis, Conejo, Pablo Rojo, Soriano-Arandes, Antoni, Battegay, Manuel, Kouyos, Roger, Mussini, Cristina, Tookey, Pat, Casabona, Jordi, Miró, Jose M, Castagna, Antonella, Konopnick, Deborah, Goetghebuer, Tessa, Sönnerborg, Anders, Quiros-Roldan, Eugenia, Sabin, Caroline, Teira, Ramon, Garrido, Myriam, Haerry, David, de Wit, Stéphane, Costagliola, Dominique, d’Arminio-Monforte, Antonella, del Amo, Julia, Raben, Dorthe, Chêne, Geneviève, Rojo, Conejo Pablo, Barger, Diana, Schwimmer, Christine, Termote, Monique, Campbell, Maria, Frederiksen, Casper M, Friis-Møller, Nina, Kjaer, Jesper, Brandt, Rikke Salbøl, Berenguer, Juan, Bohlius, Julia, Bouteloup, Vincent, Cozzi-Lepri, Alessandro, Davies, Mary-Anne, Dorrucci, Maria, Dunn, David, Egger, Matthias, Furrer, Hansjakob, Grabar, Sophie, Guiguet, Marguerite, Lambotte, Olivier, Leroy, Valériane, Lodi, Sara, Matheron, Sophie, Miro, Jose M, Monge, Susana, Nakagawa, Fumiyo, Paredes, Roger, Phillips, Andrew, Puoti, Massimo, Rohner, Eliane, and Schomaker, Michael
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Biomedical and Clinical Sciences ,Clinical Sciences ,Infectious Diseases ,HIV/AIDS ,Sexually Transmitted Infections ,Emerging Infectious Diseases ,Rare Diseases ,2.1 Biological and endogenous factors ,Infection ,Adolescent ,Adult ,Anti-Retroviral Agents ,CD4 Lymphocyte Count ,Cohort Studies ,Female ,HIV Infections ,HIV-1 ,Humans ,Male ,Middle Aged ,Risk Factors ,Sarcoma ,Kaposi ,Viral Load ,Young Adult ,AIDS-defining Cancer Project Working Group for IeDEA and COHERE in EuroCoord ,HIV ,Kaposi sarcoma ,antiretroviral therapy ,cohort study ,Biological Sciences ,Medical and Health Sciences ,Microbiology ,Clinical sciences - Abstract
BackgroundWe compared Kaposi sarcoma (KS) risk in adults who started antiretroviral therapy (ART) across the Asia-Pacific, South Africa, Europe, Latin, and North America.MethodsWe included cohort data of human immunodeficiency virus (HIV)-positive adults who started ART after 1995 within the framework of 2 large collaborations of observational HIV cohorts. We present incidence rates and adjusted hazard ratios (aHRs).ResultsWe included 208140 patients from 57 countries. Over a period of 1066572 person-years, 2046 KS cases were diagnosed. KS incidence rates per 100000 person-years were 52 in the Asia-Pacific and ranged between 180 and 280 in the other regions. KS risk was 5 times higher in South African women (aHR, 4.56; 95% confidence intervals [CI], 2.73-7.62) than in their European counterparts, and 2 times higher in South African men (2.21; 1.34-3.63). In Europe, Latin, and North America KS risk was 6 times higher in men who have sex with men (aHR, 5.95; 95% CI, 5.09-6.96) than in women. Comparing patients with current CD4 cell counts ≥700 cells/µL with those whose counts were
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- 2017
33. Comparison of dynamic monitoring strategies based on CD4 cell counts in virally suppressed, HIV-positive individuals on combination antiretroviral therapy in high-income countries: a prospective, observational study
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Caniglia, Ellen C, Cain, Lauren E, Sabin, Caroline A, Robins, James M, Logan, Roger, Abgrall, Sophie, Mugavero, Michael J, Hernández-Díaz, Sonia, Meyer, Laurence, Seng, Remonie, Drozd, Daniel R, Seage, George R, Bonnet, Fabrice, Dabis, Francois, Moore, Richard D, Reiss, Peter, van Sighem, Ard, Mathews, William C, del Amo, Julia, Moreno, Santiago, Deeks, Steven G, Muga, Roberto, Boswell, Stephen L, Ferrer, Elena, Eron, Joseph J, Napravnik, Sonia, Jose, Sophie, Phillips, Andrew, Justice, Amy C, Tate, Janet P, Gill, John, Pacheco, Antonio, Veloso, Valdilea G, Bucher, Heiner C, Egger, Matthias, Furrer, Hansjakob, Porter, Kholoud, Touloumi, Giota, Crane, Heidi, Miro, Jose M, Sterne, Jonathan A, Costagliola, Dominique, Saag, Michael, Hernán, Miguel A, Collaboration, HIV-CAUSAL, and Systems, Centers for AIDS Research Network of Integrated Clinical
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Medical Microbiology ,Biomedical and Clinical Sciences ,Public Health ,Health Sciences ,Sexually Transmitted Infections ,Clinical Research ,HIV/AIDS ,Infectious Diseases ,6.1 Pharmaceuticals ,Infection ,Good Health and Well Being ,Adolescent ,Adult ,Anti-HIV Agents ,CD4 Lymphocyte Count ,Developed Countries ,Drug Monitoring ,Europe ,Female ,HIV Infections ,HIV-1 ,Humans ,Male ,Middle Aged ,Prospective Studies ,Viral Load ,Young Adult ,HIV-CAUSAL Collaboration ,Centers for AIDS Research Network of Integrated Clinical Systems ,Medical and Health Sciences ,Biomedical and clinical sciences ,Health sciences - Abstract
BackgroundClinical guidelines vary with respect to the optimal monitoring frequency of HIV-positive individuals. We compared dynamic monitoring strategies based on time-varying CD4 cell counts in virologically suppressed HIV-positive individuals.MethodsIn this observational study, we used data from prospective studies of HIV-positive individuals in Europe (France, Greece, the Netherlands, Spain, Switzerland, and the UK) and North and South America (Brazil, Canada, and the USA) in The HIV-CAUSAL Collaboration and The Centers for AIDS Research Network of Integrated Clinical Systems. We compared three monitoring strategies that differ in the threshold used to measure CD4 cell count and HIV RNA viral load every 3-6 months (when below the threshold) or every 9-12 months (when above the threshold). The strategies were defined by the threshold CD4 counts of 200 cells per μL, 350 cells per μL, and 500 cells per μL. Using inverse probability weighting to adjust for baseline and time-varying confounders, we estimated hazard ratios (HRs) of death and of AIDS-defining illness or death, risk ratios of virological failure, and mean differences in CD4 cell count.Findings47 635 individuals initiated an antiretroviral therapy regimen between Jan 1, 2000, and Jan 9, 2015, and met the eligibility criteria for inclusion in our study. During follow-up, CD4 cell count was measured on average every 4·0 months and viral load every 3·8 months. 464 individuals died (107 in threshold 200 strategy, 157 in threshold 350, and 200 in threshold 500) and 1091 had AIDS-defining illnesses or died (267 in threshold 200 strategy, 365 in threshold 350, and 459 in threshold 500). Compared with threshold 500, the mortality HR was 1·05 (95% CI 0·86-1·29) for threshold 200 and 1·02 (0·91·1·14) for threshold 350. Corresponding estimates for death or AIDS-defining illness were 1·08 (0·95-1·22) for threshold 200 and 1·03 (0·96-1·12) for threshold 350. Compared with threshold 500, the 24 month risk ratios of virological failure (viral load more than 200 copies per mL) were 2·01 (1·17-3·43) for threshold 200 and 1·24 (0·89-1·73) for threshold 350, and 24 month mean CD4 cell count differences were 0·4 (-25·5 to 26·3) cells per μL for threshold 200 and -3·5 (-16·0 to 8·9) cells per μL for threshold 350.InterpretationDecreasing monitoring to annually when CD4 count is higher than 200 cells per μL compared with higher than 500 cells per μL does not worsen the short-term clinical and immunological outcomes of virally suppressed HIV-positive individuals. However, more frequent virological monitoring might be necessary to reduce the risk of virological failure. Further follow-up studies are needed to establish the long-term safety of these strategies.FundingNational Institutes of Health.
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- 2017
34. HIV replication and tuberculosis risk among people living with HIV in Europe: A multicohort analysis, 1983–2015.
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Atkinson, Andrew, Kraus, David, Banholzer, Nicolas, Miro, Jose M., Reiss, Peter, Kirk, Ole, Mussini, Cristina, Morlat, Philippe, Podlekareva, Daria, Grant, Alison D., Sabin, Caroline, van der Valk, Marc, Le Moing, Vincent, Meyer, Laurence, Seng, Remonie, Castagna, Antonella, Obel, Niels, Antoniadou, Anastasia, Salmon, Dominique, and Zwahlen, Marcel
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OPPORTUNISTIC infections ,CD4 lymphocyte count ,HIV-positive persons ,POISSON regression ,PHENOTYPIC plasticity ,TUBERCULOSIS - Abstract
Introduction: HIV replication leads to a change in lymphocyte phenotypes that impairs immune protection against opportunistic infections. We examined current HIV replication as an independent risk factor for tuberculosis (TB). Methods: We included people living with HIV from 25 European cohorts 1983–2015. Individuals <16 years or with previous TB were excluded. Person-time was calculated from enrolment (baseline) to the date of TB diagnosis or last follow-up information. We used adjusted Poisson regression and general additive regression models. Results: We included 272,548 people with a median follow-up of 5.9 years (interquartile range [IQR] 2.3–10.9). At baseline, the median CD4 cell count was 355 cells/μL (IQR 193–540) and the median HIV-RNA level 22,000 copies/mL (IQR 1,300–103,000). During 1,923,441 person-years of follow-up, 5,956 (2.2%) people developed TB. Overall, TB incidence was 3.1 per 1,000 person-years (95% confidence interval [CI] 3.02–3.18) and was four times higher in patients with HIV-RNA levels of 10,000 compared with levels <400 copies/mL in any CD4 stratum. CD4 and HIV-RNA time-updated analyses showed that the association between HIV-RNA and TB incidence was independent of CD4. The TB incidence rate ratio for people born in TB-endemic countries compared with those born in Europe was 1.8 (95% CI 1.5–2.2). Conclusions: Our results indicate that ongoing HIV replication (suboptimal HIV control) is an important risk factor for TB, independent of CD4 count. Those at highest risk of TB are people from TB-endemic countries. Close monitoring and TB preventive therapy for people with suboptimal HIV control is important. [ABSTRACT FROM AUTHOR]
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- 2024
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35. Distinct Inflammatory Phenotypes Are Associated With Subclinical and Clinical Cardiovascular Disease in People With Human Immunodeficiency Virus.
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McGettrick, Padraig, Tinago, Willard, O'Brien, Julie, Miles, Sarah, Lawler, Leo, Garcia-Leon, Alejandro, Mahon, Niall, Lambert, John, Sheehan, Gerard, Landay, Alan, Sabin, Caroline A, Cotter, Aoife G, Mallon, Patrick W G, and Study, for the HIV Understanding the Pathology of Comorbid Disease in HIV-Infected Individuals With Coronary Artery Disease (UPBEAT) Study Group and the All Ireland Infectious Diseases (AIID) Cohort
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HIV ,PRINCIPAL components analysis ,HIERARCHICAL clustering (Cluster analysis) ,INDIVIDUALIZED medicine ,PHENOTYPES - Abstract
Despite inflammation being implicated in cardiovascular disease (CVD) in people with human immunodeficiency virus (PWH), considerable heterogeneity within populations of PWH exists. Stratifying CVD risk based on inflammatory phenotype could play an important role. Using principal component analyses and unsupervised hierarchical clustering, we examined 38 biomarkers to identify inflammatory phenotypes in 2 independent cohorts of PWH. We identified 3 distinct inflammatory clusters present in both cohorts that were associated with altered risk of both subclinical CVD (cohort 1) and prevalent clinical CVD (cohort 2) after adjusting for CVD risk factors. These data support precision medicine approaches to enhance CVD risk assessment in PWH. [ABSTRACT FROM AUTHOR]
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- 2024
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36. Improving 1-Year Mortality Following Intensive Care Unit Admission in Adults with HIV: A 20-Year Observational Study.
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Kanitkar, Tanmay, Bakewell, Nicholas, Dissanayake, Oshani, Symonds, Maggie, Rimmer, Stephanie, Adlakha, Amit, Lipman, Marc C. I., Bhagani, Sanjay, Agarwal, Banwari, Sabin, Caroline A., and Miller, Robert F.
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INTENSIVE care units ,HIV infections ,ANTIRETROVIRAL agents ,RESPIRATORY insufficiency ,TREATMENT effectiveness - Abstract
Background: Despite widespread use of combination antiretroviral therapy, people with HIV (PWH) continue to have an increased risk of admission to and mortality in the intensive care unit (ICU). Mortality risk after hospital discharge is not well described. Using retrospective data on adult PWH (≥18 years) admitted to ICU from 2000-2019 in an HIV-referral centre, we describe trends in 1-year mortality after ICU admission. Methods: One-year mortality was calculated from index ICU admission to date of death; with follow-up right-censored at day 365 for people remaining alive at 1 year, or day 7 after ICU discharge if lost-to-follow-up after hospital discharge. Cox regression was used to describe the association with calendar year before and after adjustment for patient characteristics (age, sex, Acute Physiology and Chronic Health Evaluation II [APACHE II] score, CD4+ T-cell count, and recent HIV diagnosis) at ICU admission. Analyses were additionally restricted to those discharged alive from ICU using a left-truncated design, with further adjustment for respiratory failure at ICU admission in these analyses. Results: Two hundred and twenty-one PWH were admitted to ICU (72% male, median [interquartile range] age 45 [38–53] years) of whom 108 died within 1-year (cumulative 1-year survival: 50%). Overall, the hazard of 1-year mortality was decreased by 10% per year (crude hazard ratio (HR): 0.90 (95% confidence interval: 0.87-0.93)); the association was reduced to 7% per year (adjusted HR: 0.93 (0.89-0.98)) after adjustment. Conclusions were similar among the subset of 136 patients discharged alive (unadjusted: 0.91 (0.84-0.98); adjusted 0.92 (0.84, 1.02)). Conclusions: Between 2000 and 2019, 1-year mortality after ICU admission declined at this ICU. Our findings highlight the need for multi-centre studies and the importance of continued engagement in care after hospital discharge among PWH. [ABSTRACT FROM AUTHOR]
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- 2024
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37. Priorities for HIV and chronic pain research: results from a survey of individuals with lived experience.
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Robinson-Papp, Jessica, Lawrence, Steven, Wadley, Antonia, Scott, Whitney, George, Mary Catherine, Josh, Jo, O'Brien, Kelly K., Price, Collen, Uebelacker, Lisa, Edelman, E. Jennifer, Evangeli, Michael, Goodin, Burel R., Harding, Richard, Nkhoma, Kennedy, Parker, Romy, Sabin, Caroline, Slawek, Deepika, Tsui, Judith I., and Merlin, Jessica S.
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HIV infection risk factors ,SUBSTANCE abuse treatment ,CHRONIC pain treatment ,HIV prevention ,COST control ,CHRONIC pain ,RESEARCH funding ,MENTAL health ,RESEARCH evaluation ,QUESTIONNAIRES ,HIV infections ,EXPERIENCE ,PRIORITY (Philosophy) ,PATIENTS' attitudes ,MEDICAL care costs ,PATIENT participation ,DISEASE risk factors - Abstract
The Global Task Force on Chronic Pain in HIV published seven research priorities in the field of HIV-associated chronic pain in 2019: (1) causes; (2) management; (3) treatment individualization and integration with addiction treatment; (4) mental and social health factors; (5) prevalence; (6) treatment cost effectiveness; and (7) prevention. The current study used a web-based survey to determine whether the research topics were aligned with the priorities of adults with lived experiences of HIV and chronic pain. We also collected information about respondents' own pain and treatment experiences. We received 311 survey responses from mostly US-based respondents. Most respondents reported longstanding, moderate to severe, multisite pain, commonly accompanied by symptoms of anxiety and/or depression. The median number of pain treatments tried was 10 (IQR = 8, 13), with medications and exercise being the most common modalities, and opioids being viewed as the most helpful. Over 80% of respondents considered all research topics either "extremely important" or "very important". Research topic #2, which focused on optimizing management of pain in people with HIV, was accorded the greatest importance by respondents. These findings suggest good alignment between the priorities of researchers and US-based people with lived experience of HIV-associated chronic pain. [ABSTRACT FROM AUTHOR]
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- 2024
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38. Seroprevalence of immunity to hepatitis A and hepatitis B among gay, bisexual and other men who have sex with men (GBMSM) attending sexual health clinics in London and Leeds, England, 2017–2018.
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Roche, Rachel, Simmons, Ruth, Allen, Hester, Glancy, Megan, Balan, Anca-Maria, Bolea, Maria, Harris, Ross, Desai, Monica, Mohammed, Hamish, Sabin, Caroline, Ijaz, Samreen, and Mandal, Sema
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- 2024
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39. HEPCARE EUROPE- A case study of a service innovation project aiming at improving the elimination of HCV in vulnerable populations in four European cities
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Avramovic, Gordana, Reilly, Maeve, Cullen, Walter, Macías, Juan, McCombe, Geoff, McHugh, Tina, Oprea, Cristiana, Story, Alistair, Surey, Julian, Sabin, Caroline, Bivegete, Sandra, Vickerman, Peter, Walker, Josephine, Ward, Zoe, and Lambert, John S
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- 2020
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40. Cost-effectiveness of statins for primary prevention of atherosclerotic cardiovascular disease among people living with HIV in the United States
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Boettiger, David C., Newall, Anthony T., Phillips, Andrew, Bendavid, Eran, Law, Matthew G., Ryom, Lene, Reiss, Peter, Mocroft, Amanda, Bonnet, Fabrice, Weber, Rainer, El-Sadr, Wafaa, Monforte, Antonella D'Arminio, Dewit, Stephane, Pradier, Christian, Hatleberg, Camilla I., Lundgren, Jens, Sabin, Caroline, Kahn, James G., and Kazi, Dhruv S.
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Medical care, Cost of -- Statistics ,HIV patients -- Drug therapy -- Statistics ,Pravastatin -- Usage -- Economic aspects -- Statistics ,Atherosclerosis -- Prevention ,Health - Abstract
Background: Expanding statin use may help to alleviate the excess burden of atherosclerotic cardiovascular disease in people iving with HIV (PLHIV). Pravastatin and pitavastatin are preferred agents due to their lack of substantial interaction with antiretroviral therapy. We aimed to evaluate the cost-effectiveness of pravastatin and pitavastatin for the primary prevention of atherosclerotic cardiovascular disease among PLHIV in the United States. Methods: We developed a microsimulation model that randomly selected (with replacement) individuals from the Data-collection on Adverse Effects of Anti-HIV Drugs study with follow-up between 2013 and 2016. Our study population was PLHIV aged 40 to 75 years, stable on antiretroviral therapy and not currently using lipid-lowering therapy. Direct medical costs and quality-adjusted life-years (QALYs) were assigned in annual cycles and discounted at 3% per year. We assumed a willingness-to-pay threshold of $100,000/QALY gained. The interventions assessed were as follows: (1) treating no one with statins; (2) treating everyone with generic pravastatin 40 mg/day (drug cost $236/year) and (3) treating everyone with branded pitavastatin 4 mg/day (drug cost $2,828/year). The model simulated each individual's probability of experiencing atherosclerotic cardiovascular disease over 20 years. Results: Persons receiving pravastatin accrued 0.024 additional QALYs compared with those not receiving a statin, at an incremental cost of $1338, giving an incremental cost-effectiveness ratio of $56,000/QALY gained. Individuals receiving pitavastatin accumulated 0.013 additional QALYs compared with those using pravastatin, at an additional cost of $18,251, giving an incremental cost-effectiveness ratio of $1,444,000/QALY gained. These findings were most sensitive to the pill burden associated with daily statin administration, statin costs, statin efficacy and baseline atherosclerotic cardiovascular disease risk. In probabilistic sensitivity analysis, no statin was optimal in 5.2% of simulations, pravastatin was optimal in 94.8% of simulations and pitavastatin was never optimal. Conclusions: Pravastatin was projected to be cost-effective compared with no statin. With substantial price reduction, pitavastatin may be cost-effective compared with pravastatin. These findings bode well for the expanded use of statins among PLHIV in the United States. To gain greater confidence in our conclusions it is important to generate strong, HIV-specific estimates on the efficacy of statins and the quality-of-life burden associated with taking an additional daily pill. Keywords: HIV; cardiovascular disease; statin; cost-effectiveness; United States; antiretroviral therapy Received 4 September 2020; Accepted 23 February 2021, 1 | INTRODUCTION People living with HIV (PLHIV) have an elevated risk of atherosclerotic cardiovascular disease (ASCVD) compared to people without HIV [1]. This is only partially explained by the [...]
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- 2021
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41. From the micro to the macro to improve health: microorganism ecology and society in teaching infectious disease epidemiology
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Shahmanesh, Maryam, Harling, Guy, Coltart, Cordelia E M, Bailey, Heather, King, Carina, Gibbs, Jo, Seeley, Janet, Phillips, Andrew, Sabin, Caroline A, Aldridge, Robert W, Sonnenberg, Pam, Hart, Graham, Rowson, Mike, Pillay, Deenan, Johnson, Anne M, Abubakar, Ibrahim, and Field, Nigel
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- 2020
- Full Text
- View/download PDF
42. Terminal differentiation of T cells is strongly associated with CMV infection and increased in HIV-positive individuals on ART and lifestyle matched controls
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Booiman, Thijs, Wit, Ferdinand W, Girigorie, Arginell F, Maurer, Irma, De Francesco, Davide, Sabin, Caroline A, Harskamp, Agnes M, Prins, Maria, Franceschi, Claudio, Deeks, Steven G, Winston, Alan, Reiss, Peter, and Kootstra, Neeltje A
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Medical Microbiology ,Biomedical and Clinical Sciences ,Immunology ,HIV/AIDS ,Infectious Diseases ,Sexually Transmitted Infections ,Clinical Research ,2.1 Biological and endogenous factors ,Infection ,Good Health and Well Being ,Adult ,Aged ,Antiretroviral Therapy ,Highly Active ,Blood Donors ,CD4-Positive T-Lymphocytes ,CD8-Positive T-Lymphocytes ,Case-Control Studies ,Cell Differentiation ,Cytomegalovirus ,Cytomegalovirus Infections ,HIV Seropositivity ,HIV-1 ,Humans ,Life Style ,Lymphocyte Activation ,Co-morBidity in Relation to Aids (COBRA) Collaboration ,General Science & Technology - Abstract
HIV-1-positive individuals on successful antiretroviral therapy (ART) are reported to have higher rates of age-associated non-communicable comorbidities (AANCCs). HIV-associated immune dysfunction has been suggested to contribute to increased AANCC risk. Here we performed a cross-sectional immune phenotype analysis of T cells in ART-treated HIV-1-positive individuals with undetectable vireamia (HIV-positives) and HIV-1-negative individuals (HIV-negatives) over 45 years of age. In addition, two control groups were studied: HIV negative adults selected based on lifestyle and demographic factors (Co-morBidity in Relation to AIDS, or COBRA) and unselected age-matched donors from a blood bank. Despite long-term ART (median of 12.2 years), HIV-infected adults had lower CD4+ T-cell counts and higher CD8+ T-cell counts compared to well-matched HIV-negative COBRA participants. The proportion of CD38+HLA-DR+ and PD-1+ CD4+ T-cells was higher in HIV-positive cohort compared to the two HIV-negative cohorts. The proportion CD57+ and CD27-CD28- cells of both CD4+ and CD8+ T-cells in HIV-positives was higher compared to unselected adults (blood bank) as reported before but this difference was not apparent in comparison with well-matched HIV-negative COBRA participants. Multiple regression analysis showed that the presence of an increased proportion of terminally differentiated T cells was strongly associated with CMV infection. Compared to appropriately selected HIV-negative controls, HIV-positive individuals on ART with long-term suppressed viraemia exhibited incomplete immune recovery and increased immune activation/exhaustion. CMV infection rather than treated HIV infection appears to have more consistent effects on measures of terminal differentiation of T cells.
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- 2017
43. Inequalities in sexual and reproductive outcomes among women aged 16–24 in England (2012–2019)
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Solomon, Danielle, primary, Gibbs, Jo, additional, Burns, Fiona, additional, Mohammed, Hamish, additional, Migchelsen, Stephanie J, additional, and Sabin, Caroline A, additional
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- 2024
- Full Text
- View/download PDF
44. Using observational data to emulate a randomized trial of dynamic treatment-switching strategies: an application to antiretroviral therapy
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Cain, Lauren E, Saag, Michael S, Petersen, Maya, May, Margaret T, Ingle, Suzanne M, Logan, Roger, Robins, James M, Abgrall, Sophie, Shepherd, Bryan E, Deeks, Steven G, Gill, M John, Touloumi, Giota, Vourli, Georgia, Dabis, François, Vandenhende, Marie-Anne, Reiss, Peter, van Sighem, Ard, Samji, Hasina, Hogg, Robert S, Rybniker, Jan, Sabin, Caroline A, Jose, Sophie, del Amo, Julia, Moreno, Santiago, Rodríguez, Benigno, Cozzi-Lepri, Alessandro, Boswell, Stephen L, Stephan, Christoph, Pérez-Hoyos, Santiago, Jarrin, Inma, Guest, Jodie L, Monforte, Antonella D’Arminio, Antinori, Andrea, Moore, Richard, Campbell, Colin NJ, Casabona, Jordi, Meyer, Laurence, Seng, Rémonie, Phillips, Andrew N, Bucher, Heiner C, Egger, Matthias, Mugavero, Michael J, Haubrich, Richard, Geng, Elvin H, Olson, Ashley, Eron, Joseph J, Napravnik, Sonia, Kitahata, Mari M, Van Rompaey, Stephen E, Teira, Ramón, Justice, Amy C, Tate, Janet P, Costagliola, Dominique, Sterne, Jonathan AC, Hernán, Miguel A, and Systems, and the HIV-CAUSAL Collaboration on behalf of the Antiretroviral Therapy Cohort Collaboration the Centers for AIDS Research Network of Integrated Clinical
- Subjects
Epidemiology ,Health Sciences ,Clinical Research ,Infectious Diseases ,HIV/AIDS ,Sexually Transmitted Infections ,Clinical Trials and Supportive Activities ,6.1 Pharmaceuticals ,Infection ,Good Health and Well Being ,Adult ,Anti-HIV Agents ,CD4 Lymphocyte Count ,Female ,HIV Infections ,HIV-1 ,Humans ,Male ,Middle Aged ,Observational Studies as Topic ,Randomized Controlled Trials as Topic ,Survival Analysis ,United Kingdom ,Viral Load ,HIV ,antiretroviral therapy ,inverse-probability weighting ,observational studies ,mortality ,dynamic strategies ,Antiretroviral Therapy Cohort Collaboration ,the Centers for AIDS Research Network of Integrated Clinical Systems ,and the HIV-CAUSAL Collaboration ,Statistics ,Public Health and Health Services ,Public health - Abstract
BackgroundWhen a clinical treatment fails or shows suboptimal results, the question of when to switch to another treatment arises. Treatment switching strategies are often dynamic because the time of switching depends on the evolution of an individual's time-varying covariates. Dynamic strategies can be directly compared in randomized trials. For example, HIV-infected individuals receiving antiretroviral therapy could be randomized to switching therapy within 90 days of HIV-1 RNA crossing above a threshold of either 400 copies/ml (tight-control strategy) or 1000 copies/ml (loose-control strategy).MethodsWe review an approach to emulate a randomized trial of dynamic switching strategies using observational data from the Antiretroviral Therapy Cohort Collaboration, the Centers for AIDS Research Network of Integrated Clinical Systems and the HIV-CAUSAL Collaboration. We estimated the comparative effect of tight-control vs. loose-control strategies on death and AIDS or death via inverse-probability weighting.ResultsOf 43 803 individuals who initiated an eligible antiretroviral therapy regimen in 2002 or later, 2001 met the baseline inclusion criteria for the mortality analysis and 1641 for the AIDS or death analysis. There were 21 deaths and 33 AIDS or death events in the tight-control group, and 28 deaths and 41 AIDS or death events in the loose-control group. Compared with tight control, the adjusted hazard ratios (95% confidence interval) for loose control were 1.10 (0.73, 1.66) for death, and 1.04 (0.86, 1.27) for AIDS or death.ConclusionsAlthough our effective sample sizes were small and our estimates imprecise, the described methodological approach can serve as an example for future analyses.
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- 2016
45. When to Monitor CD4 Cell Count and HIV RNA to Reduce Mortality and AIDS-Defining Illness in Virologically Suppressed HIV-Positive Persons on Antiretroviral Therapy in High-Income Countries
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Caniglia, Ellen C, Sabin, Caroline, Robins, James M, Logan, Roger, Cain, Lauren E, Abgrall, Sophie, Mugavero, Michael J, Hernandez-Diaz, Sonia, Meyer, Laurence, Seng, Remonie, Drozd, Daniel R, Seage, George R, Bonnet, Fabrice, Dabis, Francois, Moore, Richard R, Reiss, Peter, van Sighem, Ard, Mathews, William C, del Amo, Julia, Moreno, Santiago, Deeks, Steven G, Muga, Roberto, Boswell, Stephen L, Ferrer, Elena, Eron, Joseph J, Napravnik, Sonia, Jose, Sophie, Phillips, Andrew, Olson, Ashley, Justice, Amy C, Tate, Janet P, Bucher, Heiner C, Egger, Matthias, Touloumi, Giota, Sterne, Jonathan A, Costagliola, Dominique, Saag, Michael, and Hernán, Miguel A
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Biomedical and Clinical Sciences ,Public Health ,Health Sciences ,Infectious Diseases ,Clinical Research ,HIV/AIDS ,Prevention ,Infection ,Good Health and Well Being ,AIDS-Related Complex ,Anti-HIV Agents ,CD4 Lymphocyte Count ,Cohort Studies ,Developed Countries ,Europe ,HIV Infections ,Humans ,Prospective Studies ,RNA ,Viral ,United States ,Viral Load ,HIV ,CD4 cell count ,HIV RNA ,monitoring ,observational studies ,mortality ,Center for AIDS Research Network of Integrated Clinical Systems and the HIV-CAUSAL Collaboration ,Clinical Sciences ,Public Health and Health Services ,Virology ,Clinical sciences ,Epidemiology ,Public health - Abstract
ObjectiveTo illustrate an approach to compare CD4 cell count and HIV-RNA monitoring strategies in HIV-positive individuals on antiretroviral therapy (ART).DesignProspective studies of HIV-positive individuals in Europe and the USA in the HIV-CAUSAL Collaboration and The Center for AIDS Research Network of Integrated Clinical Systems.MethodsAntiretroviral-naive individuals who initiated ART and became virologically suppressed within 12 months were followed from the date of suppression. We compared 3 CD4 cell count and HIV-RNA monitoring strategies: once every (1) 3 ± 1 months, (2) 6 ± 1 months, and (3) 9-12 ± 1 months. We used inverse-probability weighted models to compare these strategies with respect to clinical, immunologic, and virologic outcomes.ResultsIn 39,029 eligible individuals, there were 265 deaths and 690 AIDS-defining illnesses or deaths. Compared with the 3-month strategy, the mortality hazard ratios (95% CIs) were 0.86 (0.42 to 1.78) for the 6 months and 0.82 (0.46 to 1.47) for the 9-12 month strategy. The respective 18-month risk ratios (95% CIs) of virologic failure (RNA >200) were 0.74 (0.46 to 1.19) and 2.35 (1.56 to 3.54) and 18-month mean CD4 differences (95% CIs) were -5.3 (-18.6 to 7.9) and -31.7 (-52.0 to -11.3). The estimates for the 2-year risk of AIDS-defining illness or death were similar across strategies.ConclusionsOur findings suggest that monitoring frequency of virologically suppressed individuals can be decreased from every 3 months to every 6, 9, or 12 months with respect to clinical outcomes. Because effects of different monitoring strategies could take years to materialize, longer follow-up is needed to fully evaluate this question.
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- 2016
46. When to Monitor CD4 Cell Count and HIV RNA to Reduce Mortality and AIDS-Defining Illness in Virologically Suppressed HIV-Positive Persons on Antiretroviral Therapy in High-Income Countries: A Prospective Observational Study.
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Caniglia, Ellen C, Sabin, Caroline, Robins, James M, Logan, Roger, Cain, Lauren E, Abgrall, Sophie, Mugavero, Michael J, Hernandez-Diaz, Sonia, Meyer, Laurence, Seng, Remonie, Drozd, Daniel R, Seage, George R, Bonnet, Fabrice, Dabis, Francois, Moore, Richard R, Reiss, Peter, van Sighem, Ard, Mathews, William C, Del Amo, Julia, Moreno, Santiago, Deeks, Steven G, Muga, Roberto, Boswell, Stephen L, Ferrer, Elena, Eron, Joseph J, Napravnik, Sonia, Jose, Sophie, Phillips, Andrew, Olson, Ashley, Justice, Amy C, Tate, Janet P, Bucher, Heiner C, Egger, Matthias, Touloumi, Giota, Sterne, Jonathan A, Costagliola, Dominique, Saag, Michael, Hernán, Miguel A, and Center for AIDS Research Network of Integrated Clinical Systems and the HIV-CAUSAL Collaboration
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Center for AIDS Research Network of Integrated Clinical Systems and the HIV-CAUSAL Collaboration ,Humans ,HIV Infections ,AIDS-Related Complex ,RNA ,Viral ,Anti-HIV Agents ,CD4 Lymphocyte Count ,Viral Load ,Cohort Studies ,Prospective Studies ,Developed Countries ,United States ,Europe ,HIV ,CD4 cell count ,HIV RNA ,monitoring ,observational studies ,mortality ,RNA ,Viral ,Virology ,Clinical Sciences ,Public Health and Health Services - Abstract
ObjectiveTo illustrate an approach to compare CD4 cell count and HIV-RNA monitoring strategies in HIV-positive individuals on antiretroviral therapy (ART).DesignProspective studies of HIV-positive individuals in Europe and the USA in the HIV-CAUSAL Collaboration and The Center for AIDS Research Network of Integrated Clinical Systems.MethodsAntiretroviral-naive individuals who initiated ART and became virologically suppressed within 12 months were followed from the date of suppression. We compared 3 CD4 cell count and HIV-RNA monitoring strategies: once every (1) 3 ± 1 months, (2) 6 ± 1 months, and (3) 9-12 ± 1 months. We used inverse-probability weighted models to compare these strategies with respect to clinical, immunologic, and virologic outcomes.ResultsIn 39,029 eligible individuals, there were 265 deaths and 690 AIDS-defining illnesses or deaths. Compared with the 3-month strategy, the mortality hazard ratios (95% CIs) were 0.86 (0.42 to 1.78) for the 6 months and 0.82 (0.46 to 1.47) for the 9-12 month strategy. The respective 18-month risk ratios (95% CIs) of virologic failure (RNA >200) were 0.74 (0.46 to 1.19) and 2.35 (1.56 to 3.54) and 18-month mean CD4 differences (95% CIs) were -5.3 (-18.6 to 7.9) and -31.7 (-52.0 to -11.3). The estimates for the 2-year risk of AIDS-defining illness or death were similar across strategies.ConclusionsOur findings suggest that monitoring frequency of virologically suppressed individuals can be decreased from every 3 months to every 6, 9, or 12 months with respect to clinical outcomes. Because effects of different monitoring strategies could take years to materialize, longer follow-up is needed to fully evaluate this question.
- Published
- 2016
47. Can Hepatitis C Virus (HCV) Direct-Acting Antiviral Treatment as Prevention Reverse the HCV Epidemic Among Men Who Have Sex With Men in the United Kingdom? Epidemiological and Modeling Insights.
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Martin, Natasha K, Thornton, Alicia, Hickman, Matthew, Sabin, Caroline, Nelson, Mark, Cooke, Graham S, Martin, Thomas CS, Delpech, Valerie, Ruf, Murad, Price, Huw, Azad, Yusef, Thomson, Emma C, and Vickerman, Peter
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Humans ,Hepatitis C ,HIV Infections ,Antiviral Agents ,Incidence ,Prevalence ,Homosexuality ,Male ,Models ,Theoretical ,Male ,Coinfection ,United Kingdom ,HIV ,antiviral treatment ,hepatitis C virus ,men who have sex with men ,prevention ,Homosexuality ,Models ,Theoretical ,Sexual and Gender Minorities ,Clinical Research ,Behavioral and Social Science ,Liver Disease ,Hepatitis - C ,Prevention ,Emerging Infectious Diseases ,Digestive Diseases ,Hepatitis ,Chronic Liver Disease and Cirrhosis ,HIV/AIDS ,Infectious Diseases ,2.2 Factors relating to physical environment ,2.4 Surveillance and distribution ,Infection ,Microbiology ,Biological Sciences ,Medical and Health Sciences - Abstract
BackgroundWe report on the hepatitis C virus (HCV) epidemic among human immunodeficiency virus (HIV)-positive men who have sex with men (MSM) in the United Kingdom and model its trajectory with or without scaled-up HCV direct-acting antivirals (DAAs).MethodsA dynamic HCV transmission model among HIV-diagnosed MSM in the United Kingdom was calibrated to HCV prevalence (antibody [Ab] or RNA positive), incidence, and treatment from 2004 to 2011 among HIV-diagnosed MSM in the UK Collaborative HIV Cohort (UK CHIC). The epidemic was projected with current or scaled-up HCV treatment, with or without a 20% behavioral risk reduction.ResultsHCV prevalence among HIV-positive MSM in UK CHIC increased from 7.3% in 2004 to 9.9% in 2011, whereas primary incidence was flat (1.02-1.38 per 100 person-years). Over the next decade, modeling suggests 94% of infections are attributable to high-risk individuals, comprising 7% of the population. Without treatment, HCV chronic prevalence could have been 38% higher in 2015 (11.9% vs 8.6%). With current treatment and sustained virological response rates (status quo), chronic prevalence is likely to increase to 11% by 2025, but stabilize with DAA introduction in 2015. With DAA scale-up to 80% within 1 year of diagnosis (regardless of disease stage), and 20% per year thereafter, chronic prevalence could decline by 71% (to 3.2%) compared to status quo in 2025. With additional behavioral interventions, chronic prevalence could decline further to
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- 2016
48. Use of Contemporary Protease Inhibitors and Risk of Incident Chronic Kidney Disease in Persons With Human Immunodeficiency Virus : the Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) Study
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Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) Study Group, Ryom, Lene, Lundgren, Jens Dilling, Reiss, Peter, Kirk, Ole, Law, Matthew, Ross, Mike, Morlat, Phillip, Fux, Christoph Andreas, Fontas, Eric, De Wit, Stephane, Monforte, Antonella d’Arminio, El-Sadr, Wafaa, Phillips, Andrew, Hatleberg, Camilla Ingrid, Sabin, Caroline, and Mocroft, Amanda
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- 2019
49. Determining the Origins of Human Immunodeficiency Virus Type 1 Drug-resistant Minority Variants in People Who Are Recently Infected Using Phylogenetic Reconstruction
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UK HIV Drug Resistance Database, Mbisa, Jean L., Kirwan, Peter, Tostevin, Anna, Ledesma, Juan, Bibby, David F., Brown, Alison, Myers, Richard, Hassan, Amin S., Murphy, Gary, Asboe, David, Pozniak, Anton, Kirk, Stuart, Gill, O. Noel, Sabin, Caroline, Delpech, Valerie, and Dunn, David T.
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- 2019
50. Cessation of Cigarette Smoking and the Impact on Cancer Incidence in Human Immunodeficiency Virus–infected Persons : The Data Collection on Adverse Events of Anti-HIV Drugs Study
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Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) Study Group, Shepherd, Leah, Ryom, Lene, Law, Matthew, Petoumenos, Kathy, Hatleberg, Camilla Ingrid, Monforte, Antonella d’Arminio, Sabin, Caroline, Bower, Mark, Bonnet, Fabrice, Reiss, Peter, de Wit, Stephane, Pradier, Christian, Weber, Rainer, el-Sadr, Wafaa, Lundgren, Jens, and Mocroft, Amanda
- Published
- 2019
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