Your search keyword '"Mike Youle"' showing total 148 results

1. HIV care cascade in Albania: analysis of newly diagnosed cases in 2016

Author

Arjan Harxhi, Enxhi Vrapi, Arsilda Gjataj, Esmeralda Meta, Artan Simaku, Roland Bani, Deniz Gokengin, Colette Smith, and Mike Youle

Subjects

cascade of care, antiretroviral treatment, late presentation., Medicine

Published

2020

2. Associations between baseline characteristics, CD4 cell count response and virological failure on first-line efavirenz + tenofovir + emtricitabine for HIV

Author

Oliver T. Stirrup, Caroline A. Sabin, Andrew N. Phillips, Ian Williams, Duncan Churchill, Anna Tostevin, Teresa Hill, David T. Dunn, David Asboe, Anton Pozniak, Patricia Cane, David Chadwick, Duncan Clark, Simon Collins, Valerie Delpech, Samuel Douthwaite, David Dunn, Esther Fearnhill, Kholoud Porter, Oliver Stirrup, Christophe Fraser, Anna Maria Geretti, Rory Gunson, Antony Hale, Stéphane Hué, Linda Lazarus, Andrew Leigh-Brown, Tamyo Mbisa, Nicola Mackie, Chloe Orkin, Eleni Nastouli, Deenan Pillay, Andrew Phillips, Caroline Sabin, Erasmus Smit, Kate Templeton, Peter Tilston, Erik Volz, Hongyi Zhang, Keith Fairbrother, Justine Dawkins, Siobhan O’Shea, Jane Mullen, Alison Cox, Richard Tandy, Tracy Fawcett, Mark Hopkins, Clare Booth, Lynne Renwick, Matthias L. Schmid, Brendan Payne, Jonathan Hubb, Simon Dustan, Stuart Kirk, Amanda Bradley-Stewart, Sophie Jose, Alicia Thornton, Susie Huntington, Adam Glabay, Shaadi Shidfar, Janet Lynch, James Hand, Carl de Souza, Nicky Perry, Stuart Tilbury, Elaney Youssef, Brian Gazzard, Mark Nelson, Tracey Mabika, Sundhiya Mandalia, Jane Anderson, Sajid Munshi, Frank Post, Ade Adefisan, Chris Taylor, Zachary Gleisner, Fowzia Ibrahim, Lucy Campbell, Kirsty Baillie, Richard Gilson, Nataliya Brima, Jonathan Ainsworth, Achim Schwenk, Sheila Miller, Chris Wood, Margaret Johnson, Mike Youle, Fiona Lampe, Colette Smith, Rob Tsintas, Clinton Chaloner, Samantha Hutchinson, John Walsh, Nicky Mackie, Alan Winston, Jonathan Weber, Farhan Ramzan, Mark Carder, Clifford Leen, Alan Wilson, Sheila Morris, Mark Gompels, Sue Allan, Adrian Palfreeman, Adam Lewszuk, Stephen Kegg, Akin Faleye, Victoria Ogunbiyi, Sue Mitchell, Phillip Hay, Christian Kemble, Fabiola Martin, Sarah Russell-Sharpe, Janet Gravely, Sris Allan, Andrew Harte, Anjum Tariq, Hazel Spencer, Ron Jones, Jillian Pritchard, Shirley Cumming, Claire Atkinson, Dushyant Mital, Veronica Edgell, Juli Allen, Andy Ustianowski, Cynthia Murphy, Ilise Gunder, Roy Trevelion, and Abdel Babiker

Subjects

antiretroviral therapy, ART, drug resistance, HIV, NNRTI, NRTI, Microbiology, QR1-502, Public aspects of medicine, RA1-1270

Abstract

Objectives: The aim of this study was to investigate associations between baseline characteristics and CD4 cell count response on first-line antiretroviral therapy and risk of virological failure (VF) with or without drug resistance. Methods: We conducted an analysis of UK Collaborative HIV Cohort data linked to the UK HIV Drug Resistance Database. Inclusion criteria were viral sequence showing no resistance prior to initiation of first-line efavirenz + tenofovir disoproxil fumarate + emtricitabine and virological suppression within 6 months. Outcomes of VF (≥200 copies/mL) with or without drug resistance were assessed using a competing risks approach fitted jointly with a model for CD4 cell count recovery. Hazard ratios for each VF outcome were estimated for baseline CD4 cell count and viral load and characteristics of CD4 cell count response using latent variables on a standard normal scale. Results: A total of 3640 people were included with 338 VF events; corresponding viral sequences were available in 134 with ≥1 resistance mutation in 36. VF with resistance was associated with lower baseline CD4 (0.30, 0.09–0.62), lower CD4 recovery (0.04, 0.00–0.17) and higher CD4 variability (4.40, 1.22–12.68). A different pattern of associations was observed for VF without resistance, but the strength of these results was less consistent across sensitivity analyses. Cumulative incidence of VF with resistance was estimated to be >2% at 3 years for baseline CD4 ≥350 cells/μL. Conclusion: Lower baseline CD4 cell count and suboptimal CD4 recovery are associated with VF with drug resistance. People with low CD4 cell count before ART or with suboptimal CD4 recovery on treatment should be a priority for regimens with high genetic barrier to resistance.

Published

2019

3. The effect of HIV status on the frequency and severity of acute respiratory illness.

Author

James Brown, Elisha Pickett, Colette Smith, Memory Sachikonye, Lucy Brooks, Tabitha Mahungu, David M Lowe, Sara Madge, Mike Youle, Margaret Johnson, John R Hurst, Timothy D McHugh, Ibrahim Abubakar, and Marc Lipman

Subjects

Medicine, Science

Abstract

IntroductionAntiretroviral therapy has improved the health of people living with HIV (PLW-HIV), though less is known about how this impacts on acute respiratory illness. These illnesses are a common cause of ill health in the general population and any increase in their frequency or severity in PLW-HIV might have significant implications for health-related quality of life and the development of chronic respiratory disease.MethodsIn a prospective observational cohort study following PLW-HIV and HIV negative participants for 12 months with weekly documentation of any acute respiratory illness, we compared the frequency, severity and healthcare use associated with acute respiratory illnesses to determine whether PLW-HIV continue to have a greater frequency or severity of such illnesses despite antiretroviral therapy.ResultsWe followed-up 136 HIV positive and 73 HIV negative participants for 12 months with weekly documentation of any new respiratory symptoms. We found that HIV status did not affect the frequency of acute respiratory illness: unadjusted incidence rates per person year of follow-up were 2.08 illnesses (95% CI 1.81-2.38) and 2.30 illnesses (1.94-2.70) in HIV positive and negative participants respectively, IRR 0.87 (0.70-1.07) p = 0.18. However, when acute respiratory illnesses occurred, PLW-HIV reported more severe symptoms (relative fold-change in symptom score 1.61 (1.28-2.02), p ConclusionsHIV suppression with antiretroviral therapy reduces the frequency of acute respiratory illness to background levels, however when these occur, they are associated with more severe self-reported symptoms and greater healthcare utilisation. Exploration of the reasons for this greater severity of acute respiratory illness may allow targeted interventions to improve the health of people living with HIV.Trial registrationISRCTN registry (ISRCTN38386321).

Published

2020

4. Virologic and immunologic outcomes of treatment with integrase inhibitors in a real-world setting: The RESPOND cohort consortium.

Author

Bastian Neesgaard, Amanda Mocroft, Robert Zangerle, Ferdinand Wit, Fiona Lampe, Huldrych F Günthard, Coca Necsoi, Matthew Law, Cristina Mussini, Antonella Castagna, Antonella d'Arminio Monforte, Christian Pradier, Nikoloz Chkhartisvilli, Juliana Reyes-Uruena, Jörg Janne Vehreschild, Jan-Christian Wasmuth, Anders Sönnerborg, Christoph Stephan, Lauren Greenberg, Josep M Llibre, Alain Volny-Anne, Lars Peters, Annegret Pelchen-Matthews, Vani Vannappagari, Joel Gallant, Armin Rieger, Mike Youle, Dominique Braun, Stephane De Wit, Kathy Petoumenos, Vanni Borghi, Vincenzo Spagnuolo, Tengiz Tsertsvadze, Jens Lundgren, Lene Ryom, and RESPOND study group

Subjects

Medicine, Science

Abstract

ObjectivesTo compare virologic and immunologic outcomes of integrase inhibitor (INSTI)-containing, contemporary boosted protease inhibitor (PI/b)-containing and non-nucleotide reverse transcriptase inhibitor (NNRTI)-containing regimens in a real-life setting.MethodsUsing logistic regression, virologic and immunologic outcomes of INSTI use were compared to outcomes of PI/b or NNRTI treatment 12 months after treatment start or switch, for participants in the RESPOND cohort consortium. A composite treatment outcome (cTO) was used, defining success as viral load (VL) ResultsBetween January 2012 and January 2019, 13,703 (33.0% ART-naïve) individuals were included, of whom 7,147 started/switched to a regimen with an INSTI, 3,102 to a PI/b and 3,454 to an NNRTI-containing regimen. The main reason for cTO failure in all treatment groups were changes in ART regimen. Compared to INSTIs, the adjusted odds ratio (aOR) of cTO success was significantly lower for PI/b (0.74 [95% confidence interval, CI 0.67-0.82], p ConclusionIn this large analysis of a real-world population, cTO and on-treatment success were similar between INSTIs and NNRTIs, but lower for PI/b, though residual confounding cannot be fully excluded. Obtaining favorable immunologic outcomes were more likely for INSTIs than the other drug classes.

Published

2020

5. Lower healthcare costs associated with the use of a single-pill ARV regimen in the UK, 2004-2008.

Author

Eduard J Beck, Sundhiya Mandalia, Roshni Sangha, Mike Youle, Ray Brettle, Mark Gompels, Margaret Johnson, Anton Pozniak, Achim Schwenk, Stephen Taylor, John Walsh, Ed Wilkins, Ian Williams, Brian Gazzard, and NPMS-HHC Steering Group

Subjects

Medicine, Science

Abstract

AimInvestigate the cost and effects of a single-pill versus two- or three pill first-line antiretroviral combinations in reducing viral load, increasing CD4 counts, and first-line failure rate associated with respective regimens at 6 and 12 months.MethodsPatients on first-line TDF+3TC+EFV, TDF+FTC+EFV, Truvada®+EFV or Atripla® between 1996-2008 were identified and viral load and CD4 counts measured at baseline, six and twelve months respectively. Factors that independently predicted treatment failure at six and twelve months were derived using multivariate Cox's proportional hazard regression analyses. Use and cost of hospital services were calculated at six and twelve months respectively.ResultsAll regimens reduced viral load to below the limit of detection and CD4 counts increased to similar levels at six and twelve months for all treatment regimens. No statistically significant differences were observed for rate of treatment failure at six and twelve months. People on Atripla® generated lower healthcare costs for non-AIDS patients at £5,340 (£5,254 to £5,426) per patient-semester and £9,821 (£9,719 to £9,924) per patient-year that was £1,344 (95%CI £1,222 to £1,465) less per patient-semester and £1,954 (95%CI £1,801 to £2,107) less per patient-year compared with Truvada®+EFV; healthcare costs for AIDS patients were similar across all regimens.ConclusionThe single pill regimen is as effective as the two- and three-pill regimens of the same drugs, but if started as first-line induction therapy there would be a 20% savings on healthcare costs at six and 17% of costs at twelve months compared with Truvada®+EFV, that generated the next lowest costs.

Published

2012

6. Cost-effectiveness of early treatment with first-line NNRTI-based HAART regimens in the UK, 1996-2006.

Author

Eduard J Beck, Sundhiya Mandalia, Gary Lo, Peter Sharott, Mike Youle, Jane Anderson, Guy Baily, Ray Brettle, Martin Fisher, Mark Gompels, George Kinghorn, Margaret Johnson, Brendan McCarron, Anton Pozniak, Alan Tang, John Walsh, David White, Ian Williams, Brian Gazzard, and NPMS-HHC Steering Group

Subjects

Medicine, Science

Abstract

Calculate time to first-line treatment failure, annual cost and cost-effectiveness of NNRTI versus PIboosted first-line HAART regimens in the UK, 1996-2006.Population costs for HIV services are increasing in the UK and interventions need to be effective and efficient to reduce or stabilize costs. 2NRTIs + NNRTI regimens are cost-effective regimens for first-line HAART, but these regimens have not been compared with first-line PI(boosted) regimens.Times to first-line treatment failure and annual costs were calculated for first-line HAART regimens by CD4 count when starting HAART (2006 UK prices). Cost-effectiveness of 2NRTIs+NNRTI versus 2NRTIs+PI(boosted) regimens was calculated for four CD4 strata.55% of 5,541 people living with HIV (PLHIV) started HAART with CD4 count ≤ 200 cells/mm3, many of whom were Black Africans. Annual treatment cost decreased as CD4 count increased; most marked differences were observed between starting HAART with CD4 ≤ 200 cells/mm3 compared with CD4 count >200 cells/mm3. 2NRTI+PI(boosted) and 2NRTI+NNRTI regimens were the most effective regimens across the four CD4 strata; 2NRTI + NNRTI was cost-saving or cost-effective compared with 2NRTI + PI(boosted) regimens.To ensure more effective and efficient provision of HIV services, 2NRTI+NNRTI should be started as first-line HAART regimen at CD4 counts ≤ 350 cell/mm3, unless specific contra-indications exist. This will increase the number of PLHIV receiving HAART and will initially increase population costs of providing HIV services. However, starting PLHIV earlier on cost-effective regimens will maintain them in better health and use fewer health or social services, thereby generating fewer treatment and care costs, enabling them to remain socially and economically active members of society. This does raise a number of ethical issues, which will have to be acknowledged and addressed, especially in countries with limited resources.

Published

2011

7. The cost-effectiveness of early access to HIV services and starting cART in the UK 1996-2008.

Author

Eduard J Beck, Sundhiya Mandalia, Roshni Sangha, Peter Sharott, Mike Youle, Guy Baily, Ray Brettle, Mark Gompels, Margaret Johnson, Brendan McCarron, Ed Ong, Anton Pozniak, Achim Schwenk, Stephen Taylor, John Walsh, Ed Wilkins, Ian Williams, Brian Gazzard, and NPMS-HHC Steering Group

Subjects

Medicine, Science

Abstract

To calculate use, cost and cost-effectiveness of people living with HIV (PLHIV) starting routine treatment and care before starting combination antiretroviral therapy (cART) and PLHIV starting first-line 2NRTIs+NNRTI or 2NRTIs+PI(boosted), comparing PLHIV with CD4≤200 cells/mm3 and CD4>200 cells/mm3. Few studies have calculated the use, cost and cost-effectiveness of routine treatment and care before starting cART and starting cART above and below CD4 200 cells/mm3.Use, costs and cost-effectiveness were calculated for PLHIV in routine pre-cART and starting first-line cART, comparing CD4≤200 cells/mm3 with CD4>200 cells/mm3 (2008 UK prices).cART naïve patients CD4≤200 cells/mm3 had an annual cost of £6,407 (95%CI £6,382 to £6,425) PPY compared with £2,758 (95%CI £2,752 to £2,761) PPY for those with CD4>200 cells/mm3; cost per life year gained of pre-cART treatment and care for those with CD4>200 cells/mm3 was £1,776 (cost-saving to £2,752). Annual cost for starting 2NRTIs+NNRTI or 2NRTIs+PI(boosted) with CD4≤200 cells/mm3 was £12,812 (95%CI £12,685-£12,937) compared with £10,478 (95%CI £10,376-£10,581) for PLHIV with CD4>200 cells/mm3. Cost per additional life-year gained on first-line therapy for those with CD4>200 cells/mm3 was £4639 (£3,967 to £2,960).PLHIV starting to use HIV services before CD4≤200 cells/mm3 is cost-effective and enables them to be monitored so they start cART with a CD4>200 cells/mm3, which results in better outcomes and is cost-effective. However, 25% of PLHIV accessing services continue to present with CD4≤200 cells/mm3. This highlights the need to investigate the cost-effectiveness of testing and early treatment programs for key populations in the UK.

Published

2011

8. Rising population cost for treating people living with HIV in the UK, 1997-2013.

Author

Sundhiya Mandalia, Roshni Mandalia, Gary Lo, Tim Chadborn, Peter Sharott, Mike Youle, Jane Anderson, Guy Baily, Ray Brettle, Martin Fisher, Mark Gompels, George Kinghorn, Margaret Johnson, Brendan McCarron, Anton Pozniak, Alan Tang, John Walsh, David White, Ian Williams, Brian Gazzard, Eduard J Beck, and NPMS-HHC Steering Group

Subjects

Medicine, Science

Abstract

The number of people living with HIV (PLHIV) is increasing in the UK. This study estimated the annual population cost of providing HIV services in the UK, 1997-2006 and projected them 2007-2013.Annual cost of HIV treatment for PLHIV by stage of HIV infection and type of ART was calculated (UK pounds, 2006 prices). Population costs were derived by multiplying the number of PLHIV by their annual cost for 1997-2006 and projected 2007-2013.Average annual treatment costs across all stages of HIV infection ranged from £17,034 in 1997 to £18,087 in 2006 for PLHIV on mono-therapy and from £27,649 in 1997 to £32,322 in 2006 for those on quadruple-or-more ART. The number of PLHIV using NHS services rose from 16,075 to 52,083 in 2006 and was projected to increase to 78,370 by 2013. Annual population cost rose from £104 million in 1997 to £483 million in 2006, with a projected annual cost between £721 and £758 million by 2013. When including community care costs, costs increased from £164 million in 1997, to £683 million in 2006 and between £1,019 and £1,065 million in 2013.Increased number of PLHIV using NHS services resulted in rising UK population costs. Population costs are expected to continue to increase, partly due to PLHIV's longer survival on ART and the relative lack of success of HIV preventing programs. Where possible, the cost of HIV treatment and care needs to be reduced without reducing the quality of services, and prevention programs need to become more effective. While high income countries are struggling to meet these increasing costs, middle- and lower-income countries with larger epidemics are likely to find it even more difficult to meet these increasing demands, given that they have fewer resources.

Published

2010

9. Safety, immunogenicity, and efficacy of a COVID-19 vaccine (NVX-CoV2373) co-administered with seasonal influenza vaccines: an exploratory substudy of a randomised, observer-blinded, placebo-controlled, phase 3 trial

Author

Seth Toback, Eva Galiza, Catherine Cosgrove, James Galloway, Anna L Goodman, Pauline A Swift, Sankarasubramanian Rajaram, Alison Graves-Jones, Jonathan Edelman, Fiona Burns, Angela M Minassian, Iksung Cho, Lakshmi Kumar, Joyce S Plested, E Joy Rivers, Andreana Robertson, Filip Dubovsky, Greg Glenn, Paul T Heath, Roy L. Soiza, Robin Brittain-Long, Chiara Scicluna, Carole Edwards, Lynn Mackay, Mariella D'Allesandro, Amy Nicol, Karen Norris, Sandra Mann, Heather Lawrence, Ruth Valentine, Marianne Elizabeth Viljoen, Carol H. Pretswell, Helen Nicholls, Imrozia Munsoor, Agnieszka Meyrick, Christina Kyriakidou, Shalini Iyengar, Arham Jamal, Nick Richards, Helen Price, Bridie Rowbotham, Danielle Bird, Karen Smith, Olga Littler, Kirsty Fielding, Anna Townsend-Rose, Karen Miller, Jessica Davis, Alison Elliot-Garwood, Lauren Trottier, Paul Edwards, Margaret McFarland, Orod Osanlou, Laura Longshaw, Jane Stockport, Lynne Grundy, Katharine Lucy Broad, Karen Regan, Kim Storton, Declan Ryan-Wakeling, Brad Wilson, Malathy Munisamy, John Wright, Anil Shenoy, Beverley English, Lucy Brear, Paola Cicconi, Marta Boffito, Ana Milinkovic, Ruth Byrne, Roya Movahedi, Rosalie Housman, Naveed Kara, Ellen Brown, Andrea Cipriani, Mary-Jane Attenburrow, Katharine A. Smith, Jonathan Packham, Geoff Sparrow, Richard Smith, Josephine M. Rosier, Khalid Saja, Nyasha Nago, Brian Camilleri, Anita Immanuel, Mike Hamblin, Rawlings Osagie, Mahalakshmi Mohan, Hilary Floyd, Suzanne Goddard, Sanjay Mutgi, John Evans, Sean McKeon, Neringa Vilimiene, Rosavic Chicano, Rachel Hayre, Alice Pandaan, Catherine Henshall, Sonia Serrano, Andrea Mazzella, Thurkka Rajeswaran, Moncy Mathew, Karen Bisnauthsing, Laura Bremner, Henry Fok, Franca Morselli, Paola Cinardo, Blair Merrick, Lucy Sowole, Samantha Broadhead, Natalie Palmer, Jessica Cordle, Jaimie Wilson Goldsmith, Enya Cooney, Beth Jackson, Thilina Jayatilleke, Zelda Cheng, Toby Helliwell, Adrian Chudyk, Rafaela Giemza, John Lord Villajin, Noah Yogo, Esther Makanju, Pearl Dulawan, Deepak Nagra, April Buazon, Alice Russell, Georgie Bird, Amardeep Heer, Rex Sarmiento, Balraj Sanghera, Melanie Mullin, Adam Champion, Aisling Bevan, Kinzah Iqbal, Alshia Johnson, Rebecca Clark, Sarah Shaw, Steven Shaw, Amanda Chalk, Martin Lovatt, Caroline Lillicrap, Angela Parker, Jan Hansel, Zhi Wong, Galvin Gan, Eyad Tuma, Jane Minton, Jennifer Murira, Razan Saman, Alistair Hall, Kyra Holliday, Zara Khan, James Calderwood, George Twigg, Helena Baker, Julie Corrigan, Katy Houseman, Subhra Raguvanshi, Dominic Heining, Jake Weddell, Liz Glaves, Kim Thompson, Francis Davies, Ruth Lambley Burke, Emma C. Thomson, Dinesh Saralaya, Lisa Berry, Nancy Hopewell, Leigh Gerdes, Mihaela Pacurar, Saul N. Faust, Jeremy Turner, Christopher Jeanes, Adele Cooper, Jocelyn Keshet-Price, Lou Coke, Melissa Cambell-Kelly, Ketan Dhatariya, Claire Williams, Georgina Marks, James Sudbury, Lisa Rodolico, Judy Bradley, Sharon Carr, Roisin Martin, Angelina Madden, Paul Biagioni, Sonia McKenna, Alison Clinton, Maurice O'Kane, Justin Carter, Matthew Dewhurst, Bill Wetherill, Thandiwe Hoggarth, Katrina Lennon Collins, Marie Chowdhury, Adil Nathoo, Anna Heinen, Orla MacDonald, Claudia Hurducas, Liliana Cifuentes, Harjeevan Gill, Andy Gibson, Raha West, Jane Ewing, Rachel Blacow, John Haughney, Jonathan MacDonald, John Paul Seenan, Stewart Webb, Colin O'Leary, Scott Muir, Beth White, Neil Ritchie, Daniel F. McAuley, Jonathan Stewart, Mariella D'Alessandro, Nicki Lakeman, Laura Purandare, Duncan Browne, David Tucker, Peter Luck, Angharad Everden, Lisa Trembath, Michael Visick, Nick Morley, Laura Reid, Helen Chenoweth, Kirsty Maclean, Ray P. Sheridan, Tom Burden, Craig Francis Lunt, Shirley Todd, Stephanie Estcourt, Jasmine Marie Pearce, Suzanne Wilkins, Cathryn Love-Rouse, Eva Torok-Pollok, Mike Youle, Sara Madge, Danielle Solomon, Aarti Nandani, Janet M. North, Nargis Hemat, Rachel Newport, Philip A. Kalra, Chukwuma Chukwu, Olivia Wickens, Vikki O'Loughlin, Hema Mistry, Louise Harrison, Robert Oliver, Anne-Marie Peers, Jess Zadik, Katie Doyle, David R. Chadwick, Kerry Colling, Caroline Wroe, Marie Branch, Alison Chilvers, Sarah Essex, Mark Stone, Alberto San Francisco Ramos, Emily Beales, Olivia Bird, Zsofia Danos, Hazel Fofie, Cecilia Hultin, Sabina Ikram, Fran Mabesa, Aoife Mescall, Josyanne Pereira, Jennifer Pearce, Natalina Sutton, Emma Snashall, David Neil Baxter, Sara Bennett, Debbie Suggitt, Kerry Hughes, Wiesia Woodyatt, Lynsey Beacon, Alissa Kent, Chris Cooper, Milan Rudic, Simon Tunstall, Matthew Jackson, Claire Hombersley, Patrick Moore, Rebecca Cutts, Andrew Higham, Marwan Bukhari, Mohamed Elnaggar, Michelle Glover, Fiona Richardson, Alexandra Dent, Shahzeb Mirza, Rajiv Ark, Jennie Han, Suzy V. Hope, Philip J. Mitchelmore, Rostam Osanlou, Andrew Freedman, Alison Cooper, Katherine Burton, Kashyap Katechia, Michael Barrett, Jo Salkeld, Natalie Hill, Nathaniel Lee, Jon Perkins, and Polly Fox

Subjects

Adult, Pulmonary and Respiratory Medicine, Trivalent influenza vaccine, medicine.medical_specialty, COVID-19 Vaccines, Adolescent, Influenza vaccine, Population, Placebo, Young Adult, Immunogenicity, Vaccine, Double-Blind Method, Internal medicine, Humans, Medicine, education, Adverse effect, Aged, education.field_of_study, Reactogenicity, SARS-CoV-2, business.industry, COVID-19, Articles, Middle Aged, Vaccine efficacy, Vaccination, Influenza Vaccines, Seasons, business

Abstract

Background The safety and immunogenicity profile of COVID-19 vaccines when administered concomitantly with seasonal influenza vaccines have not yet been reported. We therefore aimed to report the results of a substudy within a phase 3 UK trial, by evaluating the safety, immunogenicity, and efficacy of NVX-CoV2373 when co-administered with licensed seasonal influenza vaccines. Methods We did a planned exploratory substudy as part of the randomised, observer-blinded, placebo-controlled, phase 3 trial of the safety and efficacy of the COVID-19 vaccine (NVX-CoV2373) by co-administrating the influenza vaccine at four study hospitals in the UK. Approximately, the first 400 participants meeting the main study entry criteria—with no contraindications to influenza vaccination—were invited to join the substudy. Participants of the main study were randomly assigned (1:1) to receive two intramuscular injections of either NVX-CoV2373 (5 μg) or placebo (normal saline) 21 days apart; participants enrolled into the substudy were co-vaccinated with a single (0·5 mL) intramuscular, age-appropriate (quadrivalent influenza cell-based vaccine [Flucelvax Quadrivalent; Seqirus UK, Maidenhead] for those aged 18–64 years and adjuvanted trivalent influenza vaccine [Fluad; Seqirus UK, Maidenhead] for those ≥65 years), licensed, influenza vaccine on the opposite deltoid to that of the first study vaccine dose or placebo. The influenza vaccine was administered in an open-label manner and at the same time as the first study injection. Reactogenicity was evaluated via an electronic diary for 7 days after vaccination in addition to monitoring for unsolicited adverse events, medically attended adverse events, and serious adverse events. Immunogenicity was assessed with influenza haemagglutination inhibition and SARS-CoV-2 anti-spike protein IgG assays. Vaccine efficacy against PCR-confirmed, symptomatic COVID-19 was assessed in participants who were seronegative at baseline, received both doses of study vaccine or placebo, had no major protocol deviations affecting the primary endpoint, and had no confirmed cases of symptomatic COVID-19 from the first dose until 6 days after the second dose (per-protocol efficacy population). Immunogenicity was assessed in participants who received scheduled two doses of study vaccine, had a baseline sample and at least one post-vaccination sample, and had no major protocol violations before unmasking (per-protocol immunogenicity population). Reactogenicity was analysed in all participants who received at least one dose of NVX-CoV2373 or placebo and had data collected for reactogenicity events. Safety was analysed in all participants who received at least one dose of NVX-CoV2373 or placebo. Comparisons were made between participants of the substudy and the main study (who were not co-vaccinated for influenza). This study is registered with ClinicalTrials.gov, number NCT04583995. Findings Between Sept 28, 2020, and Nov 28, 2020, a total of 15 187 participants were randomised into the main phase 3 trial, of whom 15 139 received treatment (7569 received dose one of NVX-CoV2373 and 7570 received dose one of placebo). 431 participants were co-vaccinated with a seasonal influenza vaccine in the substudy (217 received NVX-CoV2373 plus the influenza vaccine and 214 received placebo plus the influenza vaccine). In general, the substudy participants were younger, more racially diverse, and had fewer comorbid conditions than those in the main study. Reactogenicity events were more common in the co-administration group than in the NVX-CoV2373 alone group: tenderness (113 [64·9%] of 174 vs 592 [53·3%] of 1111) or pain (69 [39·7%] vs 325 [29·3%]) at injection site, fatigue (48 [27·7%] vs 215 [19·4%]), and muscle pain (49 [28·3%] vs 237 [21·4%]). Incidences of unsolicited adverse events, treatment-related medically attended adverse events, and serious adverse events were low and balanced between the co-administration group and the NVX-CoV2373 alone group. No episodes of anaphylaxis or deaths were reported within the substudy. Co-administration resulted in no change to influenza vaccine immune response although a reduction in antibody responses to the NVX-CoV2373 vaccine was noted. NVX-CoV2373 vaccine efficacy in the substudy (ie, participants aged 18 to

Published

2022

10. Treating neuroendocrine neoplasms in the setting of HIV infection

Author

Simon Jenkinson, C Thirlwell, Kate Smith, Ashley Grossman, Fiona Burns, Man Liu, Mike Youle, Aimee R. Hayes, and Martyn Caplin

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, business.industry, 030220 oncology & carcinogenesis, Immunology, Human immunodeficiency virus (HIV), medicine, General Medicine, medicine.disease_cause, business

Abstract

BACKGROUND: There is a paucity of knowledge regarding neuroendocrine neoplasms (NEN) in patients with HIV infection. OBJECTIVE: To explore the incidence, characteristics and treatment outcomes of NEN in HIV-positive individuals. METHODS: This is a single-center, descriptive cohort study. Patients with HIV and biopsy-confirmed NEN were identified from our data registry. Data were collected retrospectively from medical records. Progression-free and overall survival (OS) were estimated using the Kaplan-Meier method. RESULTS: Nineteen HIV-positive patients with neuroendocrine tumors (NET) (n = 14), neuroendocrine carcinomas (NEC) (n = 2) or Merkel cell carcinoma (MCC) (n = 3) were included (median age at NEN diagnosis, 53 years). In 15 (79%) patients, HIV diagnosis preceded NEN diagnosis by a median of 11 years and 14 were receiving antiretroviral therapy (ART). Of those with data available, 75% had a viral load

Published

2021

11. Treatment outcomes of integrase inhibitors, boosted protease inhibitors and nonnucleoside reverse transcriptase inhibitors in antiretroviral-naïve persons starting treatment

Author

J Tiraboschi, B Neesgard, Nikoloz Chkhartishvili, A. Antinori, H Garges, Vincenzo Spagnuolo, Claudine Duvivier, Felipe Rogatto, Andri Rauch, Ferdinand W. N. M. Wit, JC Wasmuth, Kathy Petoumenos, Christoph Stephan, Antonella Castagna, C Mussini, Amanda Mocroft, Armin Rieger, Robert Zangerle, Coca Valentina Necsoi, Vanni Borghi, Fiona C Lampe, Josip Begovac, Veronica Svedhem, Lars Peters, Christian Pradier, S De Wit, Jörg J. Vehreschild, Natalie Bolokadze, Günthard Hf, Mike Youle, Lene Ryom, Infectious diseases, APH - Aging & Later Life, Mocroft, A., Neesgard, B., Zangerle, R., Rieger, A., Castagna, A., Spagnuolo, V., Antinori, A., Lampe, F. C., Youle, M., Vehreschild, J. J., Mussini, C., Borghi, V., Begovac, J., Duvivier, C., Gunthard, H. F., Rauch, A., Tiraboschi, J., Chkhartishvili, N., Bolokadze, N., Wit, F., Wasmuth, J. C., De Wit, S., Necsoi, C., Pradier, C., Svedhem, V., Stephan, C., Petoumenos, K., Garges, H., Rogatto, F., Peters, L., and Ryom, L.

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, International Cooperation, protease inhibitors, Integrase inhibitor, HIV Infections, Logistic regression, law.invention, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Acquired immunodeficiency syndrome (AIDS), Randomized controlled trial, law, Internal medicine, medicine, Humans, Pharmacology (medical), Protease inhibitor (pharmacology), 030212 general & internal medicine, HIV Integrase Inhibitors, antiretroviral naïve, Reverse-transcriptase inhibitor, business.industry, Health Policy, Middle Aged, Viral Load, medicine.disease, nonnucleoside reverse transcriptase inhibitors, 030112 virology, CD4 Lymphocyte Count, Infectious Diseases, Logistic Models, Treatment Outcome, integrase inhibitors, Cohort, HIV-1, RNA, Viral, Reverse Transcriptase Inhibitors, Female, business, Viral load, medicine.drug

Abstract

Objectives: Although outcomes of antiretroviral therapy (ART) have been evaluated in randomized controlled trials, experiences from subpopulations defined by age, CD4 count or viral load (VL) in heterogeneous real-world settings are limited. Methods: The study design was an international multicohort collaboration. Logistic regression was used to compare virological and immunological outcomes at 12±3months after starting ART with an integrase strand transfer inhibitor (INSTI), contemporary nonnucleoside reverse transcriptase inhibitor (NNRTI) or boosted protease inhibitor (PI/b) with two nucleos(t)ides after 1 January 2012. The composite treatment outcome (cTO) defined success as VL'200 HIV-1 RNA copies/mL with no regimen change and no AIDS/death events. Immunological success was defined as a CD4count '750cells/μL or a 33% increase where the baseline CD4 count was ≥500 cells/μL. Poisson regression compared clinical failures (AIDS/death≥14days after starting ART). Interactions between ART class and age, CD4 count, and VL were determined for each endpoint. Results: Of 5198 ART-naïve persons in the International Cohort Consortium of Infectious Diseases (RESPOND), 45.4% started INSTIs, 26.0% PI/b and 28.7% NNRTIs; 880 (17.4%) were aged ' 50years, 2539 (49.4%) had CD4 counts '350 cells/μL and 1891 (36.8%) had VL'100000 copies/mL. Differences in virological and immunological success and clinical failure among ART classes were similar across age groups (≤ 40, 40–50 and '50 years), CD4 count categories (≤ 350 vs. '350 cells/μL) and VL categories at ART initiation (≤ 100000 vs. '100000copies/mL), with all investigated interactions being nonsignificant (P'0.05). Conclusions: Differences among ART classes in virological, immunological and clinical outcomes in ART-naïve participants were consistent irrespective of age, immune suppression or VL at ART initiation. While confounding by indication cannot be excluded, this provides reassuring evidence that such subpopulations will equally benefit from contemporary ART.

Published

2020

12. HIV care cascade in Albania: analysis of newly diagnosed cases in 2016

Author

Colette Smith, Arjan Harxhi, Arsilda Gjataj, Enxhi Vrapi, Roland Bani, Artan Simaku, Mike Youle, Esmeralda Meta, Deniz Gökengin, and Ege Üniversitesi

Subjects

antiretroviral treatment, Pediatrics, medicine.medical_specialty, Epidemiology, business.industry, Human immunodeficiency virus (HIV), Newly diagnosed, medicine.disease_cause, Late presentation, Infectious Diseases, cascade of care, medicine, Antiretroviral treatment, Medicine, late presentation, business

Abstract

Introduction: Despite the fact that there has been a steady rise in new infections rate since the first reported case in 1993, Albania remains a low prevalence country. This was the first cascade study for Albania. The aim was to construct a cascade of care for newly human immunodeficiency virus (HIV)-diagnosed individuals in 2016 in Albania. Material and methods: This retrospective descriptive study was conducted at the HIV/AIDS Ambulatory Clinic, Infectious Disease Service, University Hospital Centre of Tirana. Medical records of patients diagnosed and enrolled in care in 2016 were retrospectively screened and data on gender, age, HIV clinical stage, CD4+ T cell count, viral load measurement, and treatment history, with antiretro-viral treatment (ART) and adherence to treatment were collected. Results: Out of 127 new HIV cases reported, 100 (78.7%) entered care. The median age was 39 years (range, 20-75 years; male, 82%). Seventy one percent started ART within a median of 56 days (range, 1-317 days) from diagnosis, 34 (47.9%) patients received tenofovir disoproxil fumarate/emtricitabine + efavirenz (EFV), and 27 (38%) zidovudine + lamivudine + EFV. Among those who started ART, 19.7% were late presenters and 54.9% were very late presenters. Viral load after initiation of ART was assessed in 25 cases, with 56% of patients achieving an undetectable HIV-RNA. Conclusions: A large proportion of people living with HIV were lost at each step of the cascade. Efforts in Albania should be focused on scaling up HIV testing, promoting adherence to ART, improving access to diagnostics, and better ART regimens as well as proper monitoring of therapy.

Published

2020

13. Epidemiological characteristics and access to end-stage liver disease care for HIV-positive patients with HCV and/or HBV coinfections in Central/Eastern European and neighboring countries – data from the ECEE network

Author

Mariana Mărdărescu, Antonios Papadopoulos, Anna Vassilenko, Kristi Rüütel, Mike Youle, Natalia Bolokadze, Agata Skrzat-Klapaczyńska, Aandrzej Horban, Arjan Harxhi, Dan Otelea, Bartłomiej Matłosz, and Justyns D. Kowalska

Subjects

medicine.medical_specialty, Turkey, medicine.medical_treatment, Human immunodeficiency virus (HIV), HIV Infections, Liver transplantation, medicine.disease_cause, Georgia (Republic), Health Services Accessibility, End Stage Liver Disease, Liver disease, Environmental health, Epidemiology, medicine, Humans, Europe, Eastern, Hepatitis, Greece, business.industry, Coinfection, virus diseases, End stage liver disease, General Medicine, medicine.disease, Hepatitis B, Hepatitis C, Eastern european, business

Abstract

OBJECTIVES. There is currently an urgent need to harmonize hepatitis standards of care for HIV-positive patients across Europe. The HIV epidemic in Central and Eastern Europe has often been driven by injecting drug use, therefore a higher rate of co-infection with HCV and HBV is expected in this region. We have investigated the epidemiological prevalence and treatment availability for end-stage liver disease in HIV/HCV/HBV coinfections in countries represented in the ECEE Network Group. METHODS. The Euroguidelines in Central and Eastern Europe (ECEE) Network Group was initiated in February 2016 to compare standards of care regarding HIV infection in the region. Information about HIV/HCV/HBV co-infections and the availability for end-stage liver disease treatment for HIV-positive patients were collected through on-line surveys. The respondents were ECEE members from 16 countries of the region. The information on co-infection prevalence was sourced from WHO, national HIV programmes, articles published in international journals, single clinic reports, and personal information in ten of the participating countries (62.5%). RESULTS. The HIV/HCV co-infection rate was from 3% to 99%. The range of reported of HIV/HBV coinfection percentages was 2.3% to 40%. HIV/HCV/HBV co-infection ranged from 0% to 9%. Regarding treatment for end-stage liver disease, liver transplantation was an available option for HIV-positive patients in only three countries (19%). CONCLUSION. Our findings revealed only a limited number of treatment options for the end-stage liver disease in HIV-positive patients for the vast majority of Central and Eastern European countries. There are gaps in epidemiological surveillance in this region. It appears there are many differences in the number of co-infected patients among Central and Eastern European and neighboring countries, but there is no unification of information sources.

Published

2019

14. Engagement in care among youth living with parenterally-acquired HIV infection in Romania

Author

Colette Smith, Roxana Radoi, Mike Youle, Cosmina Gingaras, Diana Sima, and Luminita Ene

Subjects

Adult, Male, medicine.medical_specialty, Transition to Adult Care, Health (social science), Social Psychology, Adolescent, Anti-HIV Agents, Human immunodeficiency virus (HIV), HIV Infections, Adult care, medicine.disease_cause, Health Services Accessibility, Cohort Studies, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Ambulatory Care, Medicine, Humans, 030212 general & internal medicine, Child, Aged, Aged, 80 and over, 030505 public health, business.industry, Romania, Public Health, Environmental and Occupational Health, food and beverages, virus diseases, Continuity of Patient Care, Middle Aged, Patient Acceptance of Health Care, Infectious Disease Transmission, Vertical, Treatment Outcome, Family medicine, Female, Patient Participation, 0305 other medical science, business, Cohort study, Follow-Up Studies

Abstract

Transition from adolescent to adult care can be challenging for youth living with HIV. We conducted a cohort study of youth born between 1985 and 1993 and infected with HIV parenterally, followed by the same medical team from age 15 years or first clinic visit until age 25 years or 30 November 2016. A longitudinal continuum-of-care was constructed, categorizing individuals' status for each month of follow-up as: engaged in care (EIC); not in care (NIC: no clinic visits within past year); lost-to-follow-up (LTFU: NIC and did not return to clinic); or died. Five hundred and forty-five individuals (52% male) were followed for 4775 person-years. At age 15, 92% were EIC, decreasing to 84% at age 20 and 74% at age 25. Of those EIC, HIV outcomes improved with age: 79% and 52% had a CD4 ≥200 cells/µl and VL400 cps/ml at age 15; increasing to 86% and 73% at age 20 and 87% and 80% at age 25. We conclude that youth infected during early childhood tended to disengage from care, even when followed by the same medical team for a lengthy period of time. For those that did engage in care, HIV-related outcomes improved from adolescence through adulthood.

Published

2019

15. European AIDS Clinical Society Standard of Care meeting on HIV and related coinfections: The Rome Statements

Author

T. Bereczky, Nathan Clumeck, Teresa Branco, A Horban, Nina Friis-Møller, Hansjakob Furrer, Peter Reiss, M. Brostrom, M. John Gill, Anna Maria Geretti, D Podlekareva, Enrico Girardi, Amanda Mocroft, Scott Letendre, Georg M. N. Behrens, A d'Arminio Monforte, Jens D Lundgren, Cristina Mussini, Annemarie M. J. Wensing, Manuel Battegay, Anton Pozniak, Stéphane De Wit, L. Mendao, José M. Gatell, Kholoud Porter, Mike Youle, Deniz Gökengin, Karine Lacombe, A. Antinori, Jürgen K. Rockstroh, Fiona Mulcahy, Stefano Rusconi, Sanjay Bhagani, Cristiana Oprea, Jose R. Arribas, N. Dedes, Christine Katlama, Amsterdam institute for Infection and Immunity, Amsterdam Public Health, Global Health, and Ege Üniversitesi

Subjects

Societies, Scientific, Pathology, medicine.medical_specialty, Tuberculosis, HIV Infections, access to care, coinfections, HIV, treatment, AIDS-Related Opportunistic Infections, Coinfection, Communicable Disease Control, Europe, Global Health, Humans, Standard of Care, 03 medical and health sciences, 0302 clinical medicine, Acquired immunodeficiency syndrome (AIDS), Health care, Journal Article, Medicine, Infection control, Pharmacology (medical), 030212 general & internal medicine, Clinical Conference, Health policy, business.industry, Health Policy, Hepatitis C, medicine.disease, Eastern european, Regimen, Infectious Diseases, Family medicine, 030211 gastroenterology & hepatology, business

Abstract

WOS: 000379080900004, PubMed ID: 26492497, ObjectivesThe objective of the 1st European AIDS Clinical Society meeting on Standard of Care in Europe was to raise awareness of the European scenario and come to an agreement on actions that could be taken in the future. MethodsData-driven presentations were given on specific topics followed by interactive panel discussions. ResultsIn Eastern European countries, the epidemic is largely driven by injecting drug use, in contrast with Western Europe where the infection mainly occurs through heterosexual contact. A high proportion of people living with HIV remain unaware of their infection. Substantial differences exist in Eastern Europe and Central Asia with respect to treatment coverage, regimen availability and continuity of drug supply. In 2012, tuberculosis case notification rates were 5-10 times higher in Eastern Europe compared with Western Europe, with an alarming proportion of newly diagnosed multi-drug-resistant cases. Hepatitis C is widespread in selected geographical areas and risk groups. ConclusionsThe key conclusion from the meeting was that a high-priority group of actions could be identified, including: increasing HIV awareness and testing, improving training for health care providers, ensuring equitable patient access to treatments and diagnostics for HIV and comorbidities, and implementing best practices in infection control and treatment of HIV-infected patients coinfected with tuberculosis and hepatitis C virus, for whom direct acting antiviral treatment. should be considered., Medical Research CouncilMedical Research Council UK (MRC) [MC_UU_12023/15]

Published

2016

16. High frequency of unexplained breathlessness among UK HIV positive adults

Author

Elisha Pickett, Mike Youle, Santino Capocci, Lucy Brookes, Margaret A. Johnson, Sara Madge, John R. Hurst, Marc Lipman, James W. Brown, and Swapna Mandal

Subjects

medicine.medical_specialty, business.industry, Internal medicine, Human immunodeficiency virus (HIV), Medicine, business, medicine.disease_cause

Published

2017

17. Clinical relevance of the plasma load of cytomegalovirus in patients infected with HIV-A survival analysis

Author

Mihaela Rădulescu, Victoria Aramă, Adrian Streinu-Cercel, Raluca Mihăilescu, Mike Youle, and Sorin Stefan Arama

Subjects

business.industry, Congenital cytomegalovirus infection, virus diseases, medicine.disease, Asymptomatic, Virology, Infectious Diseases, Acquired immunodeficiency syndrome (AIDS), Immunology, Medicine, Clinical significance, Young adult, medicine.symptom, business, Prospective cohort study, Viral load, Survival analysis

Abstract

To investigate whether asymptomatic cytomegalovirus (CMV) viraemia impact the course of human immunodeficiency virus (HIV) infection, this study evaluated the effect of CMV replication on progression of newly-diagnosed HIV infected individuals towards AIDS events and death. In a 3-year prospective study on co-infected patients, clinical, immunological, and virological tests were performed in a national reference hospital quarterly. CMV viraemia was quantified by RoboGene® HCMV DNA Quantification Kit (Analytik Jena, Germany), on ABI Prism® 7000 Sequence Detection System (Applied Biosystems, USA). One hundred and five patients were enrolled with a balanced sex distribution and a median age of 30.7 years. Median CD4(+) cell count at enrollment was 164/mm(3) and median HIV RNA 4.6 log10 copies/ml. Detectable CMV viraemia was found in 25.7% of the patients. Kaplan-Meier analysis showed progression of HIV infection to be significantly increased in those with active CMV replication and/or low CD4(+) cell count. Cox regression indicated the risk of developing new AIDS events was 2.6 times greater in patients with detectable CMV viraemia versus those without (CI95% 1-6.6; P = 0.04). Also in multivariate analysis, the overall risk of progression to AIDS events or death was 3-fold higher in those with detectable CMV viraemia (CI95% 1.3-6.7; P = 0.008) and 2.3-fold higher if CD4(+) cell count was below 100/mm(3) (CI95% 1-5.1; P = 0.04). In these young Romanian HIV-seropositives, active CMV replication increased morbidity, even when treated with combination antiretroviral therapy. Further studies are needed to evaluate if serial quantitative CMV-DNA levels might correlate with non-infectious inflammation-related risks in patients with HIV and active CMV infection.

Published

2014

18. Factors associated with viral rebound among highly treatment-experienced HIV-positive patients who have achieved viral suppression

Author

AN Phillips, Schlomo Staszewski, Margaret Johnson, CJ Smith, Mike Youle, Fiona C Lampe, Brenda Dauer, and Mervyn Tyrer

Subjects

Adult, Male, Viral rebound, medicine.medical_specialty, Time Factors, Anti-HIV Agents, HIV Infections, Drug Administration Schedule, Treatment experienced, Pharmacotherapy, Recurrence, Antiretroviral Therapy, Highly Active, Germany, Internal medicine, London, Humans, Medicine, Pharmacology (medical), Treatment Failure, Viral suppression, business.industry, Health Policy, Viral Load, Confidence interval, CD4 Lymphocyte Count, Regimen, Infectious Diseases, Relative risk, Immunology, HIV-1, Female, business, Viral load

Abstract

More and more highly treatment-experienced patients are achieving viral suppression. However, the durability of suppression remains unclear.Patients from Royal Free Hospital (London, UK) and JW Goethe University Hospital (Frankfurt, Germany) who had failedor = 1 antiretroviral (ARV) regimen in all three main drug classes andor = 3 previous ARV regimens and subsequently achieved viral load50 HIV-1 RNA copies/mL were included. They were followed until stopping pre-combination antiretroviral therapy, end of follow-up or viral rebound (two viral loads400 copies/mL).Two hundred and forty-seven patients contributed 723 person-years and 114 viral rebounds [rate=15.8 per 100 person-years; 95% confidence interval (CI) 12.9-18.7]. More recent calendar years of viral suppression [relative risk (RR)=0.90 per year later; 95% CI 0.81-1.00; P=0.05] and greater number of ARVs in the regimen not previously failed (RR=0.78 per 1 ARV more; 95% CI 0.65-0.95; P=0.01) were associated with lower viral rebound rates. At 0-1, 1-2, 2-3 and3 years after achieving suppression, the rebound rates were 30.9, 9.2, 4.3 and 3.5 per 100 person-years, respectively. Compared to 0-1 years, the adjusted RRs (95% CIs) after 1-2, 2-3 and3 years were 0.33 (0.18-0.58), 0.21 (0.09-0.48) and 0.14 (0.06-0.33), respectively (P0.0001).Although rebound rates are high, especially in the first year after viral suppression, this risk reduces substantially if highly treatment-experienced patients can maintain viral suppression.

Published

2009

19. Health-Related Quality of Life in a Randomized Trial of Antiretroviral Therapy for Advanced HIV Disease

Author

William Cameron, Mark Holodniy, Sheldon T. Brown, Douglas K Owens, Vilija R. Joyce, Tassos C. Kyriakides, Vandana Sundaram, Mark Sculpher, Mike Youle, Wei Yu, Ahmed M. Bayoumi, Aslam H. Anis, Susan Griffin, and Paul G. Barnett

Subjects

Adult, Male, Canada, medicine.medical_specialty, Anti-HIV Agents, Visual analogue scale, Cross-sectional study, HIV Infections, law.invention, Randomized controlled trial, Quality of life, law, Surveys and Questionnaires, Humans, Medicine, Pharmacology (medical), Veterans Affairs, business.industry, Middle Aged, Mental health, United Kingdom, United States, humanities, Clinical trial, Cross-Sectional Studies, Infectious Diseases, Socioeconomic Factors, Quality of Life, Physical therapy, Female, business, Health Utilities Index

Abstract

OBJECTIVE: To assess and compare alternative approaches of measuring preference-based health-related quality of life (HRQoL) in treatment-experienced HIV patients and evaluate their association with health status and clinical variables. DESIGN: Cross-sectional study. SETTING: Twenty-eight Veterans Affairs hospitals in the United States, 13 hospitals in Canada, and 8 hospitals in the United Kingdom. PATIENTS: Three hundred sixty-eight treatment-experienced HIV-infected patients enrolled in the Options in Management with Antiretrovirals randomized trial. MEASUREMENTS: Baseline sociodemographic and clinical indicators and baseline HRQoL using the Medical Outcome Study HIV Health Survey (MOS-HIV), the EQ-5D, the EQ-5D visual analog scale (EQ-5D VAS), the Health Utilities Index Mark 3 (HUI3), and standard gamble (SG) and time trade-off (TTO) techniques. RESULTS: The mean (SD) baseline HRQoL scores were as follows: MOS-HIV physical health summary score 41.70 (11.16), MOS-HIV mental health summary score 44.76 (11.38), EQ-5D 0.77 (0.19), HUI3 0.59 (0.32), EQ-5D VAS 65.94 (21.71), SG 0.75 (0.29), and TTO 0.80 (0.31). Correlations between MOS-HIV summary scores and EQ-5D, EQ-5D VAS, and HUI3 ranged from 0.60 to 0.70; the correlation between EQ-5D and HUI3 was 0.73; and the correlation between SG and TTO was 0.43. Preference-based HRQoL scores were related to physical, mental, social, and overall health as measured by MOS-HIV. Concomitant medication use, CD4 cell count, and HIV viral load were related to some instruments' scores. CONCLUSIONS: On average, preference-based HRQoL for treatment-experienced HIV patients was decreased relative to national norms but also highly variable. Health status and clinical variables were related to HRQoL.

Published

2009

20. Long-term clinical and surrogate marker effects of subcutaneous intermittent interleukin-2 without antiretroviral therapy in HIV-infected patients

Author

Matthew Law, Margaret Johnson, Handan Wand, Lisa Fosdick, N. Perry, Christian Herzmann, Mark T. Nelson, Mike Youle, Martin Fisher, Z Cuthbertson, and George Janossy

Subjects

CD4-Positive T-Lymphocytes, Microbiology (medical), medicine.medical_specialty, Injections, Subcutaneous, medicine.medical_treatment, HIV Infections, Cohort Studies, Aldesleukin, Internal medicine, Humans, Immunologic Factors, Medicine, Pharmacology (medical), Adverse effect, Pharmacology, Chemotherapy, business.industry, Surrogate endpoint, Area under the curve, Viral Load, CD4 Lymphocyte Count, Discontinuation, Surgery, Infectious Diseases, Anti-Retroviral Agents, Area Under Curve, Cohort, Interleukin-2, RNA, Viral, business, Viral load, Biomarkers, Follow-Up Studies

Abstract

Objectives: Subcutaneous administration of interleukin-2 (IL-2) has been shown to increase CD4 counts in HIV-infected patients. It remains unclear whether this effect is associated with a clinical benefit. Patients and methods: We conducted a long-term follow-up in the cohort of the UK-Vanguard study in which three groups of 12 antiretroviral-naive subjects with CD4 cell counts >350 cells/mm 3 received no treatment or IL-2 at either 4.5 or 7.5 MIU twice daily in 5 day cycles, respectively. Results: Mean follow-up was 376 weeks. IL-2 therapy was associated with a higher area under the curve of CD4 cell count change from baseline at week 48 but not thereafter. HIV-RNA levels were unaffected. Highly active antiretroviral therapy (HAART) was initiated after a mean of 172, 175 and 152 weeks in the control group, low-dose and high-dose IL-2 treatment group, respectively, a statistically non-significant difference. There was a tendency to start HAART soon after discontinuation of IL-2 therapy which may have been triggered by the steep decay of CD4 counts. There were two serious adverse events in the control group, seven in the low-dose IL-2 group and eight in the high-dose IL-2 group. No pattern of disease was detected, making an association with IL-2 therapy unlikely. Conclusions: We could detect neither a benefit of IL-2 therapy after week 48 nor delayed initiation of HAART. This is currently the longest follow-up data comparing IL-2 therapy with no therapy in antiretroviral-naive HIV-infected patients and does not show a persistent benefit of the intervention.

Published

2008

21. Pharmacokinetics of Acetyl-L-Carnitine Given in Single or Multiple Doses to HIV-1 Infected Patients with Toxic Peripheral Polyneuropathy

Author

Margaret Johnson, S.J Whiting, P. Byrne, Mike Youle, Christian Herzmann, and M Thomas

Subjects

Drug, business.industry, media_common.quotation_subject, Metabolite, Public Health, Environmental and Occupational Health, Human immunodeficiency virus (HIV), Pharmacology, medicine.disease_cause, Multiple dosing, Crossover study, Article, Regimen, chemistry.chemical_compound, Infectious Diseases, Pharmacokinetics, chemistry, Virology, Acetyl-L-carnitine, Medicine, business, media_common

Abstract

The use of nucleoside reverse transcriptase inhibitors in the treatment of HIV infection is associated with antiretroviral toxic polyneuropathy (ATN). Previous studies suggest that long term treatment with Acetyl-L-carnitine (ALCAR) 1.5 gram twice daily improves symptoms and promotes nerve regeneration. It is unknown whether the drug’s pharmacokinetic profile would allow for a once daily administration. Twenty three HIV-1 infected subjects taking ALCAR for ATN were enrolled in a cross over trial and switched from twice to once daily dosing. Their regimen was changed from 1.5g twice daily to 1g (4 patients), 2g (7), and 3g (12) once daily, respectively. Twelve healthy volunteers served as control. Plasma levels of ALCAR and its metabolite L-carnitine were measured. Patients receiving ALCAR had higher pre-dose levels than control subjects. Post dose levels were not significantly higher than pre dose levels in any treatment group. The pre / post dose ALCAR concentrations were 7.6 / 7.7, 7.1 / 6.8, 7.7 / 6.8, and 7.1 / 7.5 µmol/l for 1.5g twice daily, 1g once daily, 2g once daily, and 3g once daily, respectively. All values were significantly higher than the mean concentration in the control group (4.3 µmol/l). For ALCAR and L-carnitine, measurements for once daily regimens did not differ from the twice daily regimen. Once daily dosing of ALCAR can achieve similar plasma levels as twice daily dosing but intra-mitochondrial levels remain unknown. The pharmacokinetic profile of orally administered ALCAR is complex and likely to be highly affected by endogenous concentrations.

Published

2008

22. TILT: a randomized controlled trial of interruption of antiretroviral therapy with or without interleukin-2 in HIV-1 infected individuals

Author

Martin Fisher, Frank A. Post, Claudine Duvivier, Christine Katlama, Brian Angus, Mike Youle, Andrew N. Phillips, Fiona C Lampe, Abdul Babiker, Ian Williams, Bonaventura Clotet, and Giuseppe Tambussi

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Immunology, HIV Infections, Drug Administration Schedule, law.invention, Acquired immunodeficiency syndrome (AIDS), Randomized controlled trial, law, Internal medicine, Humans, Immunology and Allergy, Medicine, Sida, Dose Modification, Chemotherapy, biology, business.industry, Homosexuality, Drug holiday, Middle Aged, Viral Load, biology.organism_classification, medicine.disease, Combined Modality Therapy, CD4 Lymphocyte Count, Surgery, Log-rank test, Infectious Diseases, Anti-Retroviral Agents, HIV-1, Interleukin-2, business, Viral load, Follow-Up Studies

Abstract

Objective: We aimed to see if structured treatment interruption (STI) could be supported safely with the use of two cycles of IL-2 (4.5 MIU q12h subcutaneously 5 days) before STI to prolong the time before therapy restarted.Methods: Subjects were randomly allocated to either A - continuous ART; B - continue for 9 weeks, then STI; restart with the same ART when the CD4 count falls below 200 cells; or C-two cycles of IL-2, 8 weeks apart, while still on ART; at week 9 stop ART and use a new cycle of IL-2 alone whenever the CD4 count falls

Published

2008

23. European AIDS Clinical Society (EACS) guidelines for the clinical management and treatment of HIV-infected adults

Author

N, Clumeck, A, Pozniak, F, Raffi, Mike, Youle, Amsterdam institute for Infection and Immunity, Amsterdam Public Health, and Infectious diseases

Subjects

Adult, medicine.medical_specialty, Pediatrics, Standard of care, MEDLINE, HIV Infections, Diagnosis, Differential, Acquired immunodeficiency syndrome (AIDS), Pregnancy, Antiretroviral Therapy, Highly Active, Hiv infected, Humans, Medicine, Pharmacology (medical), Treatment Failure, Pregnancy Complications, Infectious, Patient group, Medical History Taking, Referral and Consultation, Reimbursement, business.industry, Health Policy, medicine.disease, Antiretroviral therapy, Europe, Occupational Diseases, Infectious Diseases, Family medicine, Female, business

Abstract

A working group of the European AIDS Clinical Society (EACS) have developed these guidelines for European clinicians to help them in the treatment of adults with HIV infection. This third version of the guidelines includes, as new topics, the assessment of patients at initial and subsequent clinic visits as well as post-exposure prophylaxis. A revision of the 2005 guidelines based on current data includes changes in the sections on primary HIV infection, when to initiate therapy, which drug combinations are preferred as initial combination regimens for antiretroviral-naïve patients, how to manage virological failure and the treatment of HIV during pregnancy. In Europe, there is a wide range of clinical practices in antiretroviral therapy depending on various factors such as drug registration, national policies, local availability, reimbursement and access to treatment. These can vary greatly from one country to another, especially in Central and Eastern parts of Europe. These guidelines are intended to help clinicians achieve the best care for their patients. In some countries, particularly where the quality of and access to care are not optimal, these guidelines should help AIDS societies and physicians or patient group organizations to negotiate with their national health authorities with a view to implementing what should be the standard of care for HIV-infected patients all over Europe.

Published

2008

24. Prevalence and predictors of antiretroviral drug resistance in newly diagnosed HIV-1 infection

Author

Clare Booth, Margaret Johnson, Andrew N. Phillips, Mike Youle, Anna Maria Geretti, and Ana Garcia-Diaz

Subjects

Adult, Male, Microbiology (medical), medicine.medical_specialty, Adolescent, Anti-HIV Agents, Drug resistance, HIV Antibodies, Biology, Zidovudine, Acquired immunodeficiency syndrome (AIDS), Internal medicine, Drug Resistance, Viral, Epidemiology, Prevalence, medicine, Humans, Pharmacology (medical), Seroconversion, Child, Sida, Aged, Pharmacology, Acquired Immunodeficiency Syndrome, Proteolytic enzymes, Middle Aged, medicine.disease, biology.organism_classification, Virology, CD4 Lymphocyte Count, Infectious Diseases, Mutation, Cohort, HIV-1, Female, medicine.drug

Abstract

Objectives To determine prevalence and predictors of antiretroviral drug resistance in newly diagnosed individuals with HIV-1 infection, using a systematic approach to avoid selection bias. Methods Plasma samples from all persons diagnosed HIV-1 seropositive at a large London centre between April 2004 and February 2006 underwent sequencing of HIV-1 reverse transcriptase (RT) and protease genes. Subtype was assigned by phylogenetic analysis. Resistance was scored according to the IAS-USA list (2005) modified to include T215revertants and exclude isolated E44D or V118I and minor protease mutations. Recent seroconversion was identified by HIV antibody avidity testing. Results The cohort of 239 included 169 (70.7%) males, 126 (52.7%) homosexuals, 118 (49.5%) persons of white ethnicity and 144 (60.0%) persons born outside the UK. Subtypes included B 134 (56.1%), C 46 (19.2%), A 17 (7.1%), other non-B 42 (17.6%). The prevalence of resistance mutations was 17/239 (7.1%; 95% confidence interval 4.5-11.1%), comprising 10/239 (4.2%) nucleoside/nucleotide RT inhibitor (NRTI); 4/239 (1.7%) non-nucleoside RT inhibitor (NNRTI) and 4/239 (1.7%) protease inhibitor (PI) associated mutations. Dual-class (NRTI + PI) resistance mutations were detected in 1/239 (0.4%) person. The prevalence of resistance mutations was 7/85 (8.2%) and 10/154 (6.5%) in persons with recent and established infection, respectively. In multivariate analysis, having been born in the UK and high CD4 count, but not gender, age, risk group, ethnicity or subtype, were independent predictors of resistance. Conclusions In an unselected UK cohort, subtypes other than B accounted for 43.9% of new HIV-1 diagnoses. The prevalence of resistance mutations was 7.1% and highest in those born in the UK.

Published

2007

25. Acetyl-L-Carnitine in HIV-Associated Antiretroviral Toxic Neuropathy

Author

Mike Youle

Subjects

Clinical Trials as Topic, Chemotherapy, Nucleoside analogue, Reverse-transcriptase inhibitor, medicine.medical_treatment, Stavudine, Cutaneous nerve, Peripheral Nervous System Diseases, HIV Infections, Pharmacology, Biology, Psychiatry and Mental health, Pharmacotherapy, Antiretroviral Therapy, Highly Active, Immunology, medicine, Animals, Humans, Pharmacology (medical), Neurology (clinical), Acetylcarnitine, Didanosine, Nootropic Agents, medicine.drug

Abstract

Nucleoside analogue reverse transcriptase inhibitors (NRTIs), used as part of highly active antiretroviral therapy for the treatment of HIV and AIDS, disrupt neuronal mitochondrial DNA synthesis, resulting in antiretroviral toxic neuropathy (ATN). Acetyl-L-carnitine (ALC) enhances neurotrophic support of sensory neurons, potentially causing symptom relief and nerve regeneration, and in addition has numerous other effects on metabolic function that might be of benefit in such patients.ALC has been given to HIV patients with symptomatic ATN in a number of clinical studies administered either twice daily intramuscularly or as oral sachets or tablets. It has been shown to significantly reduce a variety of validated pain ratings, and is generally safe and well tolerated. Using a measure of neuronal innervation in standardised skin biopsies of the affected area, cutaneous nerve density has been improved by the administration of ALC in subjects with symptomatic ATN and reduced epidermal and dermal innervation, associated with clinical improvement, which was maintained over a 4-year period. Improvements were seen in both the structure and function of small sensory fibres, which were sustained over time whilst subjects received ALC. Other open-label, non-randomised studies have shown similar benefits in patients with ATN in terms of pain reduction over the short term. Further placebo-controlled studies of both treatment and prophylaxis have been completed and are under analysis to characterise further the usefulness of this pathogenesis-based therapy for ATN.

Published

2007

26. Emergence of CXCR4-Using Human Immunodeficiency Virus Type 1 (HIV-1) Variants in a Minority of HIV-1-Infected Patients following Treatment with the CCR5 Antagonist Maraviroc Is from a Pretreatment CXCR4-Using Virus Reservoir

Author

Ian James, Marilyn Lewis, Manos Perros, Mike Youle, Tim M Jenkins, Jeannette M. Whitcomb, Elna van der Ryst, Anton Pozniak, and Mike Westby

Subjects

Receptors, CXCR4, Receptors, CCR5, Anti-HIV Agents, viruses, Immunology, HIV Infections, CCR5 receptor antagonist, Genes, env, Microbiology, Virus, Cell Line, HIV Envelope Protein gp160, Evolution, Molecular, Maraviroc, chemistry.chemical_compound, Cyclohexanes, Virology, Vaccines and Antiviral Agents, HIV tropism, medicine, Humans, Phylogeny, Recombination, Genetic, biology, Genetic Variation, virus diseases, Triazoles, biology.organism_classification, Clone Cells, chemistry, Insect Science, CCR5 Receptor Antagonists, Lentivirus, HIV-1, Vicriviroc, Viral disease, Viral load, medicine.drug

Abstract

Antagonists of the human immunodeficiency virus type 1 (HIV-1) coreceptor, CCR5, are being developed as the first anti-HIV agents acting on a host cell target. We monitored the coreceptor tropism of circulating virus, screened at baseline for coreceptor tropism, in 64 HIV-1-infected patients who received maraviroc (MVC, UK-427,857) as monotherapy for 10 days. Sixty-two patients harbored CCR5-tropic virus at baseline and had a posttreatment phenotype result. Circulating virus remained CCR5 tropic in 60/62 patients, 51 of whom experienced an HIV RNA reduction from baseline of >1 log 10 copies/ml, indicating that CXCR4-using variants were not rapidly selected despite CCR5-specific drug pressure. In two patients, viral load declined during treatment and CXCR4-using virus was detected at day 11. No pretreatment factor predicted the emergence of CXCR4-tropic virus during maraviroc therapy in these two patients. Phylogenetic analysis of envelope ( Env ) clones from pre- and posttreatment time points indicated that the CXCR4-using variants probably emerged by outgrowth of a pretreatment CXCR4-using reservoir, rather than via coreceptor switch of a CCR5-tropic clone under selection pressure from maraviroc. Phylogenetic analysis was also performed on Env clones from a third patient harboring CXCR4-using virus prior to treatment. This patient was enrolled due to a sample labeling error. Although this patient experienced no overall reduction in viral load in response to treatment, the CCR5-tropic components of the circulating virus did appear to be suppressed while receiving maraviroc as monotherapy. Importantly, in all three patients, circulating virus reverted to predominantly CCR5 tropic following cessation of maraviroc.

Published

2006

27. Deaths in the era of HAART: contribution of late presentation, treatment exposure, resistance and abnormal laboratory markers

Author

Colette J Smith, Di Robertson Bell, Sanjay Bhagani, Fiona C Lampe, Mike Youle, Margaret Johnson, Caroline A. Sabin, Andrew N. Phillips, Dewi Ismajani Puradiredja, and Marc Lipman

Subjects

Adult, Male, Viral rebound, medicine.medical_specialty, Pediatrics, Time Factors, Adolescent, Genotype, medicine.medical_treatment, Immunology, HIV Infections, Drug resistance, Late presentation, Antiretroviral Therapy, Highly Active, Cause of Death, Drug Resistance, Viral, HIV Seropositivity, London, medicine, Humans, Immunology and Allergy, Prospective Studies, Prospective cohort study, Aged, Cause of death, Chemotherapy, business.industry, Mortality rate, Middle Aged, Resistance mutation, CD4 Lymphocyte Count, Surgery, Infectious Diseases, Anti-Retroviral Agents, Mutation, RNA, Viral, Female, business, Biomarkers

Abstract

Objectives: To describe the characteristics of deaths that occur among HIV-positive individuals in the HAART era.Design: Observational database.Methods: Deaths were reviewed that occurred among HIV-positive individuals seen at the Royal Free Hospital, London between January 1998 and December 2003.Results: Over the study period, there were 121 deaths; death rates declined from approximately 2.0/100 person-years of follow-up in 1998-2000 to approximately 1.0/ 100 person-years of follow-up in 2001-2003. Approximately one half of deaths (45.5%) were from AIDS-related causes and 74 deaths (61.2%) occurred in individuals who had received HAART: patients had been exposed to a median of seven (range 214) antiretroviral drugs and two-fifths had started treatment in the pre-HAART era. Another 15 patients had received only non-HAART treatment regimens prior to death. The median pre-death CD4 cell counts were 68 and 167 cells/mu l among those who had and had not received HAART; 23 (31.1 %) and 4 (8.5%) had HIV RNA < 400 copies/ml, respectively. Of the patients exposed to HAART for at least 6 months and who experienced viral rebound, information was available on resistance for 26 (21.5% of the total deaths) and 19 of those tested had at least one resistance mutation (median 5, range, 1-16).Conclusions: While mortality rates among HIV-infected individuals at our centre have fallen since 1988, the deaths that do now occur are more diverse and are the result of a number of factors, including late presentation, delayed uptake of HAART and the previous use of treatment combinations that are now viewed as suboptimal. (C) 2006 Lippincott Williams & Wilkins.

Published

2006

28. Long-Term Effect of Acetyl-L-Carnitine for Antiretroviral Toxic Neuropathy

Author

Margaret Johnson, Christian Herzmann, and Mike Youle

Subjects

medicine.medical_specialty, Human immunodeficiency virus (HIV), Pain, HIV Infections, Neurological examination, medicine.disease_cause, Cohort Studies, Hypesthesia, Internal medicine, medicine, Acetyl-L-carnitine, Humans, Pharmacology (medical), Acetylcarnitine, Nootropic Agents, medicine.diagnostic_test, Nucleoside analogue, business.industry, Peripheral Nervous System Diseases, Surgery, Toxic neuropathy, Infectious Diseases, Cohort, HIV-1, Reverse Transcriptase Inhibitors, business, Follow-Up Studies, medicine.drug, Cohort study

Abstract

Nucleoside analogue reverse transcriptase inhibitors (NRTIs) used for the treatment of HIV can a cause distal symmetrical peripheral polyneuropathy by disruption of mitochondrial metabolism. Treatment with acetyl-L-carnitine (ALCAR) has shown short-term symptomatic and histological improvement. Long-term effects have not been investigated.To assess the subjective and objective degree of antiretroviral toxic neuropathy (ATN) during treatment with ALCAR.A cohort of 21 patients with ATN who commenced treatment with ALCAR between March 1999 and October 2001 was reviewed after a mean of 4.3 years using standardized questionnaires and neurological examination.Of the 21 patients, 2 had died and 3 were lost to follow-up. 16 patients were assessed. 10 were still on potentially neurotoxic drugs. 13 were still taking ALCAR. 9 were pain free. The most common symptom was numbness (mild, moderate, and severe in 12, 3, and 0 patients, respectively), followed by paraesthesia (8, 2, 2), pain (4, 3, 0), and burning (5, 2, 0). There was mildly reduced sensation in the toes of 8 patients. 13 patients reported that ALCAR had improved their symptoms very much or moderately, 2 reported no change, and 1 reported a moderate worsening.ALCAR led to long-term symptomatic improvement in most patients without the need to discontinue neurotoxic drugs. Although in this study there was no control group, this agent appears to be an effective pathogenesis-based treatment for ATN.

Published

2005

29. HIV-Associated Antiretroviral Toxic Neuropathy (ATN): A Review of Recent Advances in Pathophysiology and Treatment

Author

Mike, Youle

Subjects

Pharmacology, Polyneuropathies, Infectious Diseases, Anti-HIV Agents, Humans, Reverse Transcriptase Inhibitors, Pharmacology (medical), AIDS-Associated Nephropathy, Acetylcarnitine

Published

2005

30. An open-label randomized clinical trial of novel therapeutic strategies for HIV-infected patients in whom antiretroviral therapy has failed: rationale and design of the OPTIMA Trial

Author

Mike Youle, Sheldon T. Brown, Brian Gazzard, Mark Holodniy, Abdel Babiker, William Cameron, Joel Singer, Tassos C. Kyriakides, and Martin T. Schechter

Subjects

Adult, Research design, medicine.medical_specialty, Pediatrics, Randomization, Anti-HIV Agents, Human immunodeficiency virus (HIV), MEDLINE, HIV Infections, medicine.disease_cause, Drug Administration Schedule, law.invention, Randomized controlled trial, Acquired immunodeficiency syndrome (AIDS), law, Humans, Medicine, Sida, Pharmacology, biology, business.industry, medicine.disease, biology.organism_classification, Clinical trial, Research Design, Physical therapy, business

Abstract

OPTIMA (OPTions In Management with Antiretrovirals) is a clinical trial with a factorial randomization to evaluate the hypotheses that mega-antiretroviral therapy (ART) consisting of five or more anti-HIV drugs compared to standard-ART consisting of four or fewer anti-HIV drugs and a 3-month antiretroviral drug-free period (ARDFP) compared to no ARDFP will delay the occurrence of new or recurrent acquired immunodeficiency syndrome events or death, and prove to be more cost-effective in treating human immunodeficiency virus-infected individuals previously exposed to ART drugs from the current three main classes. The aim is to randomize 1700 participants to four treatment strategy arms: (1) ARDFP + standard-ART; (2) ARDFP + mega-ART; (3) no ARDFP + standard-ART; (4) no ARDFP + mega-ART. The planned study duration is 3.5 years with 2.5 years of intake and a minimum 1 year of follow-up. The OPTIMA Trial was initiated in June 2001 at 30 U.S. Department of Veterans' Affairs hospitals, 22 hospitals in Canada, and 25 hospitals in the United Kingdom. This is the first large-scale, multicenter, randomized controlled trial to compare the relative efficacy of these different therapeutic strategies. We discuss the rationale behind the OPTIMA Trial design as well as the issues arising from the conduct of a trial that involves three national clinical trial agencies.

Published

2003

31. The potential for CD4 cell increases in HIV-positive individuals who control viraemia with highly active antiretroviral therapy

Author

A Carroll, Colette J Smith, Margaret Johnson, Sabine Kinloch-de-Loes, Beth Prinz, Fiona C Lampe, Mike Youle, Andrew N. Phillips, Caroline A. Sabin, and Helen Gumley

Subjects

Adult, CD4-Positive T-Lymphocytes, Male, medicine.medical_specialty, medicine.medical_treatment, Immunology, HIV Infections, Gastroenterology, Zidovudine, Antiretroviral Therapy, Highly Active, Immunopathology, Internal medicine, medicine, Humans, Immunology and Allergy, Viremia, Sida, Immunodeficiency, Chemotherapy, biology, business.industry, Viral Load, biology.organism_classification, medicine.disease, CD4 Lymphocyte Count, Surgery, Infectious Diseases, Cd4 cell, Female, Viral disease, business, Viral load, Follow-Up Studies, medicine.drug

Abstract

Objectives: To study the long-term CD4 cell responses to highly active antiretroviral therapy (HAART) in treatment-naive patients whose viral loads remained below 500 copies/ml for prolonged periods. Design: A total of 237 patients whose viral loads remained below 500 copies/ml for one year or more. Median follow-up was 1.9 years. Methods: CD4 cell counts were analysed to investigate long-term immunological response using mixed-effects models with the slope allowed to change after 1, 12 and 24 months of HAART. Results: The median baseline CD4 cell count was 175 cells/mm 3 . After an initial rapid increase in the first month after HAART (97.2 cells/mm 3 a month), increases in CD4 cell counts continued less rapidly (11.6 cells/mm 3 a month). This increase slowed by 2.4 cells/mm 3 a month after one year. CD4 cell counts continued increasing after 2 years, but the rate of increase again slowed (estimated slope at 2 years 5.4 cells/mm 3 a month; decrease in slope from year 2 compared with years 1-2 3.7 cell/mm 3 a month). A total of 198 out of 211 patients (94%) with measurements at baseline and one year experienced an increase in CD4 cell counts in this interval; 81 and 67% had an increasing slope between 1 and 2 and 2 and 3 years, respectively. By the end of follow-up, CD4 cell counts had increased by 319 cells/mm 3 , and were more than 500 cells/mm 3 in 40% of patients. Conclusion: Although the rate of immune recovery slowed after 2 years, CD4 cell counts rose in most and began to return to levels seen in HIV-negative individuals.

Published

2003

32. Theoretical rationale for the use of sequential single-drug antiretroviral therapy for treatment of HIV infection

Author

Fiona C Lampe, Margaret A. Johnson, Alessandro Cozzi Lepri, Andrew N. Phillips, Clive Loveday, Mike Youle, and Caroline A. Sabin

Subjects

Drug, Oncology, medicine.medical_specialty, Anti-HIV Agents, media_common.quotation_subject, Immunology, HIV Infections, Models, Biological, Efficacy, Acquired immunodeficiency syndrome (AIDS), Internal medicine, Drug Resistance, Viral, medicine, Humans, Immunology and Allergy, media_common, biology, business.industry, medicine.disease, biology.organism_classification, Drug Resistance, Multiple, Multiple drug resistance, Regimen, Infectious Diseases, Mutation, Lentivirus, Viral disease, business, Viral load

Abstract

Background: Subpopulations of HIV with mutations associated with resistance to antiretroviral drugs often have reduced replicative capacity, so virus with resistance mutations for all existing and new antiretroviral drugs is likely to be appreciably impaired. Issues of toxicity, quality of life and economics mean that the simultaneous use of all these drugs in combination is unrealistic. We aimed to explore the use of sequential monotherapy regimens using a mathematical model of quasi-species dynamics, to see if these could take advantage of the poor replicative capacity of highly resistant virus.Methods: We assume for each of seven drugs that a single mutation is associated with the ability to replicate (effective reproductive ratio, R>1) in the presence of that drug as monotherapy. Parameters included were drug efficacy, the cost of resistance mutations and the number of new target cells arising daily.Results: The use of seven drugs in a daily/weekly sequential monotherapy cycle led to substantial viral suppression (in the presence of all resistant viral subpopulations) for a wider range of parameter values than a continuous five-drug regimen. Although on any one day/week there is a viral subpopulation with R>1 (e.g. that with resistance only to the current drug), this subpopulation does not have time to grow sufficiently during the short period when that drug is being taken.Conclusion: These results provide a rationale for trials of sequential regimens, using as wide a number of drugs with different resistance-associated mutations as possible, as a potential 'resistance-proof' strategy for achieving significant viral load suppression. (C) 2003 Lippincott Williams Wilkins.

Published

2003

33. Kaposi's Sarcoma-Associated Herpesvirus Cytotoxic T Lymphocytes Recognize and Target Darwinian Positively Selected Autologous K1 Epitopes

Author

Chris Boshoff, Mervyn Tyrer, Justin Stebbing, Dimitra Bourboulia, Joachim Sieper, Margaret A. Johnson, Stephen Henderson, Toru Kobu, Ian Williams, Wolfgang Kuon, Natalie Wilder, Frances Gotch, Mike Youle, and Nesrina Imami

Subjects

Cytotoxicity, Immunologic, Cellular immunity, viruses, Molecular Sequence Data, Immunology, HIV Infections, Context (language use), In Vitro Techniques, Biology, medicine.disease_cause, Microbiology, Epitope, Conserved sequence, Epitopes, Viral Proteins, Antigen, Virology, medicine, Antigenic variation, Humans, Amino Acid Sequence, Selection, Genetic, Kaposi's sarcoma-associated herpesvirus, Antigens, Viral, Sarcoma, Kaposi, Base Sequence, Sequence Homology, Amino Acid, virus diseases, Antigenic Variation, CTL, Insect Science, DNA, Viral, Herpesvirus 8, Human, Pathogenesis and Immunity, T-Lymphocytes, Cytotoxic

Abstract

Kaposi's sarcoma-associated herpesvirus (KSHV) is the infectious cause of Kaposi's sarcoma (KS) and certain lymphoproliferations particularly in the context of human immunodeficiency virus (HIV) type 1-induced immunosuppression. The introduction of effective therapies to treat HIV has led to a decline in the incidence of KS, suggesting that immune responses may play a role in controlling KSHV infection and pathogenesis. Cytotoxic-T-lymphocyte (CTL) activity against KSHV proteins has been demonstrated; however, the identification of KSHV CTL epitopes remains elusive and problematic. Although the herpesvirus genomic layout is generally conserved, KSHV encodes a unique hypervariable protein, K1, with intense biological selection pressure at specific amino acid sites. To investigate whether this variability is partly driven by cellular immunity, we designed K1 peptides that match only the unique viral sequence for every individual studied here (autologous peptides). We identified functional CTL epitopes within K1's most variable areas, and we show that a given individual responds only to autologous peptides and not to peptides from other individuals. Furthermore, these epitopes are highly conserved sequences within KSHV isolates from a specific strain but are not conserved between different strains. We conclude that CTL recognition contributes to K1, and therefore to KSHV, evolution.

Published

2003

34. Human Immunodeficiency Virus Rebound after Suppression to <400 Copies/mL during Initial Highly Active Antiretroviral Therapy Regimens, according to Prior Nucleoside Experience and Duration of Suppression

Author

Clive Loveday, Veronica Miller, Fiona C Lampe, Margaret Johnson, Mike Youle, Caroline A. Sabin, S Klauke, Markus Bickel, Andrew N. Phillips, Hans Wilhelm Doerr, and Schlomo Staszewski

Subjects

Adult, Male, Time Factors, Anti-HIV Agents, HIV Infections, Virus, Acquired immunodeficiency syndrome (AIDS), Abacavir, Antiretroviral Therapy, Highly Active, Drug Resistance, Viral, medicine, Humans, Immunology and Allergy, Protease inhibitor (pharmacology), Treatment Failure, Sida, biology, Nucleoside analogue, business.industry, HIV, Viral Load, biology.organism_classification, medicine.disease, Virology, CD4 Lymphocyte Count, Infectious Diseases, Disease Progression, RNA, Viral, Female, Viral disease, business, Nucleoside, medicine.drug

Abstract

This study evaluated 1433 human immunodeficiency virus (HIV)–infected patients starting highly active antiretroviral therapy (HAART), 409 (28%) of whom had prior nucleoside experience and achieved an HIV load of !400 copies/mL by 24 weeks of therapy. Three hundred seven patients experienced virus rebound during a total of 2773.3 person-years of follow-up. There was a higher rate of virus rebound among the patients with pre-HAART nucleoside experience (relative hazard [RH], 2.86; 95% confidence interval, 2.22–3.84; ) and a P ! .0001 decreasing rate of virus rebound with increasing duration of virus suppression (i.e., time since achieving a virus load of !400 HIV RNA copies/mL) among both the nucleoside-experienced and naive patients ( ), but the difference between the groups persisted into the third P ! .0001 year of follow-up ( ). Even patients who had experienced !2 months of nucleoside P p .0007 therapy before beginning HAART had an increased risk of virus rebound (RH, 1.95; P p ). It appears that only a small period of pre-HAART nucleoside therapy is sufficient to .009 confer a disadvantage, in terms of risk of virus rebound, that persists for several years.

Published

2002

35. Two-Year Outcome of a Multidrug Regimen in Patients Who Did Not Respond to a Protease Inhibitor Regimen

Author

Mike Youle, Amanda Mocroft, Margaret Johnson, Clive Loveday, Darren Ransom, Mervyn Tyrer, Alister Story, Fiona C Lampe, Deborah Wilson, Martin Fisher, and Andrew N. Phillips

Subjects

medicine.medical_specialty, Efavirenz, Reverse-transcriptase inhibitor, Salvage therapy, Biology, chemistry.chemical_compound, Regimen, Infectious Diseases, chemistry, Indinavir, Internal medicine, Immunology, medicine, Pharmacology (medical), Ritonavir, Viral load, Didanosine, medicine.drug

Abstract

In most studies, people who have not responded virologically to a protease inhibitor (PI)-containing regimen have tended to experience poor virologic responses to subsequent regimens. We describe the 2-year viral load, CD4 count, and clinical outcome of a multidrug regimen used in 60 people who had not responded virologically to a PI-containing regimen. At baseline, median CD4 count was 126/mm 3 (nadir 30/mm 3 ) and median viral load was 320,000 copies/mL. A median of five antiretroviral drugs had previously been used, of which a median of two were PIs. Of these patients, 16% had previously used another nonnucleoside reverse transcriptase inhibitor besides efavirenz. The multidrug regimen (median 5 drugs) started most commonly included efavirenz (100%), at least one PI (92%, usually indinavir/ritonavir), didanosine (78%), and hydroxyurea (74%). At year 2, 5 patients had died and 5 had no measure available. Nine patients developed a new AIDS event and 10 patients were known to have stopped all antiretroviral therapy. Thirty-one patients (52% of the whole group, 72% of those remaining on therapy with viral load value available) had viral load

Published

2002

36. Strategies of HIV management — when to switch

Author

Mike Youle

Subjects

medicine.medical_specialty, Anti-HIV Agents, business.industry, Immunology, HIV Infections, Hiv management, Viral Load, Infectious Diseases, Antiretroviral Therapy, Highly Active, Drug Resistance, Viral, Humans, Immunology and Allergy, Medicine, business, Intensive care medicine

Published

2002

37. Effect of management strategies and clinical status on costs of care for advanced HIV

Author

Paul G, Barnett, Adam, Chow, Vilija R, Joyce, Ahmed M, Bayoumi, Susan C, Griffin, Huiying, Sun, Mark, Holodniy, Sheldon T, Brown, William, Cameron, Mark, Sculpher, Mike, Youle, Aslam H, Anis, and Douglas K, Owens

Subjects

Male, Anti-HIV Agents, Coinfection, Health Status, HIV Infections, Health Care Costs, Middle Aged, Viral Load, Hepatitis C, Drug Costs, CD4 Lymphocyte Count, Hospitalization, Antiretroviral Therapy, Highly Active, Humans, Female

Abstract

To determine the association between preexisting characteristics and current health and the cost of different types of advanced human immunodeficiency virus (HIV) care.Treatment-experienced patients failing highly active antiretroviral treatment (ART) in the United States, Canada, and the United Kingdom were factorial randomized to an antiretroviral-free period and ART intensification. Cost was estimated by multiplying patient-reported utilization by a unit cost.A total of 367 participants were followed for a mean of 15.3 quarters (range 1-26). Medication accounted for most (61.8%) of the $26,832 annual cost. Cost averaged $4147 per quarter for ART, $1981 for inpatient care, $580 for outpatient care, and $346 for other medications. Cost for inpatient stays, outpatient visits, and other medications was 171% higher (P.01) and cost of ART was 32% lower (P.01) when cluster of differentiation 4 (CD4) count was50 cells/μL compared with periods when CD4 count was200 cells/μL. Some baseline characteristics, including low CD4 count, high viral load, and HIV from injection drug use with hepatitis C coinfection, had a sustained effect on cost.The association between health status and cost depended on the type of care. Indicators of poor health were associated with higher inpatient and concomitant medication costs and lower cost for ART medication. Although ART has supplanted hospitalization as the most important cost in HIV care, some patients continue to incur high hospitalization costs in periods when they are using less ART. The cost of interventions to improve the use of ART might be offset by the reduction of other costs.

Published

2014

38. Clinical relevance of the plasma load of cytomegalovirus in patients infected with HIV--a survival analysis

Author

Victoria, Aramă, Raluca, Mihăilescu, Mihaela, Rădulescu, Sorin Ştefan, Aramă, Adrian, Streinu-Cercel, Mike, Youle, and Anca, Streinu-Cercel

Subjects

Adult, Male, Adolescent, Cytomegalovirus, HIV Infections, Viral Load, Prognosis, Survival Analysis, CD4 Lymphocyte Count, Plasma, Young Adult, Cytomegalovirus Infections, Disease Progression, Humans, Female, Prospective Studies

Abstract

To investigate whether asymptomatic cytomegalovirus (CMV) viraemia impact the course of human immunodeficiency virus (HIV) infection, this study evaluated the effect of CMV replication on progression of newly-diagnosed HIV infected individuals towards AIDS events and death. In a 3-year prospective study on co-infected patients, clinical, immunological, and virological tests were performed in a national reference hospital quarterly. CMV viraemia was quantified by RoboGene® HCMV DNA Quantification Kit (Analytik Jena, Germany), on ABI Prism® 7000 Sequence Detection System (Applied Biosystems, USA). One hundred and five patients were enrolled with a balanced sex distribution and a median age of 30.7 years. Median CD4(+) cell count at enrollment was 164/mm(3) and median HIV RNA 4.6 log10 copies/ml. Detectable CMV viraemia was found in 25.7% of the patients. Kaplan-Meier analysis showed progression of HIV infection to be significantly increased in those with active CMV replication and/or low CD4(+) cell count. Cox regression indicated the risk of developing new AIDS events was 2.6 times greater in patients with detectable CMV viraemia versus those without (CI95% 1-6.6; P = 0.04). Also in multivariate analysis, the overall risk of progression to AIDS events or death was 3-fold higher in those with detectable CMV viraemia (CI95% 1.3-6.7; P = 0.008) and 2.3-fold higher if CD4(+) cell count was below 100/mm(3) (CI95% 1-5.1; P = 0.04). In these young Romanian HIV-seropositives, active CMV replication increased morbidity, even when treated with combination antiretroviral therapy. Further studies are needed to evaluate if serial quantitative CMV-DNA levels might correlate with non-infectious inflammation-related risks in patients with HIV and active CMV infection.

Published

2014

39. Health-Related Quality of Life in Individuals Infected with HIV in the Era of HAART

Author

Amanda Mocroft, Margaret Johnson, Mike Youle, Martin Fisher, A Miners, and Caroline A. Sabin

Subjects

Adult, Male, Gerontology, medicine.medical_specialty, Population, Human immunodeficiency virus (HIV), HIV Infections, medicine.disease_cause, Quality of life, Antiretroviral Therapy, Highly Active, Surveys and Questionnaires, medicine, Humans, Pharmacology (medical), education, Health related quality of life, education.field_of_study, business.industry, Disease progression, Health Surveys, Antiretroviral therapy, CD4 Lymphocyte Count, Cross-Sectional Studies, Infectious Diseases, Family medicine, Disease Progression, HIV-1, Quality of Life, Population data, RNA, Viral, Female, business, Viral load

Abstract

To compare health-related quality of life (HR-QOL) in individuals infected with HIV to general population levels and to assess the relationship between HR-QOL and markers of disease progression in the era of highly active antiretroviral therapy (HAART).This was a cross-sectional questionnaire-based study. This study included 154 individuals at least 18 years old with HIV who either were attending a London hospital or were visited by a community team in Brighton. Study participants were asked to complete two HR-QOL questionnaires. This study used HR-QOL, as measured using the Medical Outcome Study HIV Health Survey (MOS-HIV) and EuroQoL self-report (EQ-5D) questionnaires, as the main outcome measure. Responses on the EQ-5D were compared with a published general population data set. The relationships between scores on the MOS-HIV and EQ-5D questionnaires and a number of independent variables including CD4 count and viral load were also assessed.Each analysis was based on the results of at least 128 questionnaires. The mean MOS-HIV mental and physical component scores were 43.2 (SD = 12.2) and 41.8 (SD = 13.2), respectively. After adjusting for differences in age and gender, it was shown that individuals with HIV reported significantly lower EQ-5D(utility) ( p =.0001) and EQ-5D(VAS) ( p =.0001) compared with the general population. However, further analysis revealed few significant associations between markers of disease progression and HR-QOL.Individuals with HIV generally recorded significantly lower HR-QOL compared with the general population. Thus, prevention of further transmissions of the virus is still likely to prevent significant morbidity losses in addition to mortality losses, despite the availability of HAART. However, disease progression as measured is not clearly related to further reductions in HR-QOL.

Published

2001

40. The steady-state pharmacokinetics of efavirenz and nevirapine when used in combination in human immunodeficiency virus type 1-infected persons

Author

Mike Youle, Hilde Carlier, Remko van Leeuwen, Brian Gazzard, Jos H. Beijnen, Joep M. A. Lange, Julio S. G. Montaner, Margaret Johnson, Marianne Harris, Graeme Moyle, Richard M. W. Hoetelmans, Marthin O. Kwakkelstein, Peter Reiss, A.I. Veldkamp, Faculteit der Geneeskunde, and Other departments

Subjects

Adult, Cyclopropanes, Male, Nevirapine, Efavirenz, Anti-HIV Agents, HIV Infections, Pharmacology, Drug Administration Schedule, chemistry.chemical_compound, Pharmacokinetics, immune system diseases, Oxazines, parasitic diseases, medicine, Humans, Immunology and Allergy, heterocyclic compounds, Sida, biology, Reverse-transcriptase inhibitor, business.industry, virus diseases, Half-life, Viral Load, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Benzoxazines, Regimen, Infectious Diseases, chemistry, Alkynes, HIV-1, Reverse Transcriptase Inhibitors, Drug Therapy, Combination, business, Viral load, Half-Life, medicine.drug

Abstract

The steady-state pharmacokinetics of efavirenz and nevirapine, when used in combination to treat human immunodeficiency virus type 1 (HIV-1)-infected subjects, were investigated. HIV-1-infected persons who had used efavirenz (600 mg once daily) for > or =2 weeks were eligible for study inclusion. The plasma pharmacokinetics of efavirenz were determined over 24 h. Subsequently, nevirapine (400 mg once daily) was added to the regimen. After 4 weeks, the pharmacokinetics of efavirenz and nevirapine were assessed over 24 h. The differences between the pharmacokinetic parameters of efavirenz with and without nevirapine were analyzed, and the pharmacokinetics of nevirapine were compared with those in historical control patients. The exposure to efavirenz when combined with nevirapine was significantly decreased by 22% (area under the plasma concentration vs. time curve), 36% (minimum plasma concentration), and 17% (maximum plasma concentration). Nevirapine pharmacokinetics appear to be unaffected by coadministration of efavirenz, compared with data from historical control patients.

Published

2001

41. Reasons for modification and discontinuation of antiretrovirals: results from a single treatment centre

Author

Margaret Johnson, Mike Youle, Mervyn Tyrer, Amanda Mocroft, Antonia L. Moore, Alessandro Cozzi Lepri, Caroline A. Sabin, Debbie Wilson, Andrew N. Phillips, Clive Loveday, Sara Madge, and Clinton Chaloner

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Immunology, HIV Infections, law.invention, Treatment Refusal, Randomized controlled trial, law, Antiretroviral Therapy, Highly Active, Internal medicine, medicine, Humans, Immunology and Allergy, Treatment Failure, Sida, Chemotherapy, biology, business.industry, Viral Load, biology.organism_classification, CD4 Lymphocyte Count, Surgery, Discontinuation, Regimen, Infectious Diseases, Nelfinavir, Female, Ritonavir, business, Viral load, Follow-Up Studies, medicine.drug

Abstract

To describe the reasons for, and factors associated with, modification and discontinuation of highly active antiretroviral therapy (HAART) regimens at a single clinic.A total of 556 patients who started HAART at the Royal Free Hospital were included in analyses. Modification was defined as stopping or switching any antiretrovirals in the regimen, whereas discontinuation was defined as the simultaneous stopping of all antiretrovirals included in the initial regimen. Reasons were classified as immunological/virological failure (IVF) and toxicities and patient choice/poor compliance (TPC).The median CD4 count at starting HAART was 171 x 10(6) cells/l and viral load 5.07 log copies/ml. During a median follow-up of 14.2 months, 247 patients (44.4%) modified their HAART regimen, 72 due to IVF (29.1%) and 159 due to TPC (64.4%) and a total of 148 patients (26.6%) discontinued HAART. Older patients were less likely to modify HAART [relative hazard (RH), 0.73 per 10 years; P = 0.0008], as were previously treatment-naive patients (RH, 0.65; P = 0.0050), those in a clinical trial (RH, 0.64; P = 0.027) and those who started nelfinavir (RH, 0.57; P = 0.035). Patients who started with four or more drugs (RH, 2.21, P0.0001), who included ritonavir in the initial regimen (RH, 1.41; P = 0.035) or who had higher viral loads during follow-up (RH per log increase, 1.51; P0.0001) were more likely to modify HAART.There was a high rate of modification and discontinuation of HAART regimens in the first 12 months, particularly due to toxicities, patient choice or poor compliance.

Published

2001

42. Changes in CD4 lymphocyte counts after interruption of therapy in patients with viral failure on protease inhibitor-containing regimens

Author

George Janossy, Mervyn Tyrer, Margaret Johnson, Amanda Mocroft, Wayne Turnbull, Andrew N. Phillips, Clive Loveday, Deborah Wilson, Sara Madge, Angela Dykhoff, Mike Youle, and Richard Tilling

Subjects

Chemotherapy, medicine.medical_specialty, Cellular immunity, business.industry, medicine.medical_treatment, Immunology, Drug holiday, Gastroenterology, Regimen, Infectious Diseases, Pharmacotherapy, Internal medicine, medicine, Immunology and Allergy, HIV Protease Inhibitor, Viral disease, business, Viral load

Abstract

Objective: To describe the short-term changes in CD4 lymphocyte counts after the interruption of antiretroviral HIV therapy in order to increase the understanding of CD4 lymphocyte dynamics, and so that appropriate monitoring strategies can be designed.Methods: We studied 35 HIV-infected patients with late-stage disease who had therapy interruptions leading to high viral load levels, median greater than 750 000 RNA log(10) copies/ml, and in whom two CD4 cell counts (median 28 days apart) were available before beginning a salvage regimen.Results: Overall, there was a substantial decline in CD4 cell counts from a median of 125 to 83 cells/mm(3) in the average 28 day period, with median proportionate and absolute losses of 26% and 24 cells/mm(3) per month, respectively (P < 0.008). This tended to be greater in individuals studied sooner after interrupting therapy (P = 0.03) and in those with CD4 cell counts above the pre-therapy baseline (P = 0.06). There was a strong negative correlation between the proportionate increase in viral load and the absolute change in CD4 cell count (-0.66, P = 0.0002).Conclusion: Patients with relatively advanced HIV infection interrupting antiretroviral therapy after failing a protease inhibitor-containing regimen require frequent monitoring because CD4 cell counts appear to fall quite rapidly, at least in the first few weeks after interruption (C) 2000 Lippincott Williams & Wilkins.

Published

2000

43. Substantial Correlation between HIV Type 1 Drug-Associated Resistance Mutations in Plasma and Peripheral Blood Mononuclear Cells in Treatment-Experienced Patients

Author

Andrew Burke, Devereux H, Margaret Johnson, Clive Loveday, Mike Youle, and Caroline A. Sabin

Subjects

Anti-HIV Agents, Lymphocyte, Molecular Sequence Data, Immunology, HIV Infections, Drug resistance, Biology, Peripheral blood mononuclear cell, Virus, HIV Protease, Virology, Blood plasma, medicine, Humans, Codon, Drug Resistance, Microbial, biology.organism_classification, HIV Reverse Transcriptase, Reverse transcriptase, Infectious Diseases, medicine.anatomical_structure, DNA, Viral, Mutation, Lentivirus, HIV-1, Leukocytes, Mononuclear, Reverse Transcriptase Inhibitors, Drug Therapy, Combination, Viral disease

Abstract

The correlation of detectable HIV-1 drug resistance mutations in plasma and PBMCs in patients extensively treated with all antiretroviral drug classes has not been fully elucidated. The detection of mutations in PBMCs may reveal resistant HIV-1 associated with past therapies. In addition, these measures in PBMCs may have a practical value when plasma virus is at low levels that are difficult to detect with current assays. The reverse transcriptase (RT) and protease (P) genes were analyzed for drug resistance, using an in-house method carried out on 36 paired samples of plasma and PBMCs from 12 treatment-experienced patients in order to investigate resistance in the two compartments. When viruses in plasma and PBMCs were analyzed by patient, the mean of the Cohen kappa values was 0.728 (substantial agreement). When viruses were analyzed by codon the mean of the Cohen kappa values was 0.715 (substantial agreement). Baseline samples were concordant at 280 of 288 (97%) codons analyzed. This study shows that a minority of mutations associated with previous therapy can be detected in PBMCs and not in plasma. Overall, mutations in plasma and PBMCs showed a substantial correlation in extensively treated patients, suggesting that either compartment is suitable for the detection of mutations as a virological guide for clinical care.

Published

2000

44. Selected Topics from the Seventh Conference on Retroviruses and Opportunistic Infections, January 30 - February 2, 2000

Author

Bartlett Jg, Mike Youle, and Caroline A. Sabin

Subjects

Infectious Diseases, business.industry, Disease progression, Medicine, HIV Protease Inhibitor, Pharmacology (medical), business, Antiretroviral therapy, Virology

Published

2000

45. Immunological, virological and clinical response to highly active antiretroviral therapy treatment regimens in a complete clinic population

Author

Mervyn Tyrer, Clive Loveday, Margaret Johnson, Debbie Wilson, Mike Youle, Amanda Mocroft, Sabine Kinloch-de-Loes, Devereux H, Andrew N. Phillips, and Sara Madge

Subjects

medicine.medical_specialty, education.field_of_study, business.industry, Incidence (epidemiology), Immunology, Population, Salvage therapy, Surgery, Regimen, Infectious Diseases, Pharmacotherapy, Interquartile range, Internal medicine, medicine, Immunology and Allergy, Viral disease, business, education, Viral load

Abstract

BACKGROUND: Highly active antiretroviral therapy (HAART) is now widely used in clinical practice and gives rise to a range of immunological, virological and clinical responses. OBJECTIVES: To describe the immunological, virological and clinical response to HAART and to examine the frequency of modification of the HAART regimen among patients from a single treatment centre. METHODS: Kaplan-Meier estimation and incidence rates were used to describe responses to HAART (a protease inhibitor or non-nucleoside drug in addition to at least two nucleoside analogues) among 421 patients from the Royal Free Hospital in London. RESULTS: The median CD4 cell count at starting HAART was 186 x 10(6) cells/l [interquartile range (IQR) 76-310] and viral load was 5.13 log10 copies/ml (IQR 4.66-5.56). At 6 months after starting HAART, 51.1% of patients were estimated to have experienced a 100 x 10(6) cells/l increase in CD4 cell count; the median time for viral load to fall below 400 copies/ml was 3.7 months (95% confidence interval 3.2-4.4). At 6 months after the first viral load was 400 copies/ml and 12.4% were estimated to have failed if the more stringent definition of two viral loads above the limit of detection was used. Compared with the pre-HAART era, the incidence of death among patients on HAART was one sixth of that level; new AIDS-defining illnesses was one seventh; and hospital admissions was one fifth. In total, 141 patients (33.5%) stopped at least one of the antiretroviral agents included as part of their HAART regimen; the occurrence of side effects was the most common reason (n = 63; 44.7%). CONCLUSION: A good response occurred to an initial HAART regimen. There was a high rate of virological relapse, which varied considerably according to the definition of failure used. Even so, the rates of clinical progression and hospital admissions observed to date were low. Further follow-up of these patients is required to determine their long-term immunological, virological and clinical outcome.

Published

2000

46. Rapid decline in detectability of HIV-1 drug resistance mutations after stopping therapy

Author

Margaret Johnson, Mike Youle, Devereux H, and Clive Loveday

Subjects

Chemotherapy, medicine.medical_specialty, biology, Combination therapy, business.industry, medicine.medical_treatment, Immunology, Salvage therapy, Drug resistance, biology.organism_classification, Group A, Gastroenterology, Group B, Infectious Diseases, Pharmacotherapy, Internal medicine, Immunology and Allergy, Medicine, Sida, business

Abstract

Objective: To investigate the rate of decline of drug resistant viruses after stopping therapy. Design: Twenty-five patients receiving multiple combination therapies (mean five; range three to nine drugs) for more than 3 months were tested for HIV-1 resistance on therapy and off therapy. The sample off therapy was tested 6-175 day c after stopping therapy. Methods: Patients were tested for genotypic changes associated with drug resistance using an in-house automated DNA sequencing assay to detect resistance in the protease and reverse transcriptase genes. Results: All samples tested when patients were on therapy showed evidence of drug resistance (range 1-9 mutations). The patients were divided into three groups: < 2 weeks after stopping therapy, median 1.1 weeks In = 8, group A); 2 weeks-2 months, median 6.4 weeks In = 7, group B) and 2 months-6 months, median 12.9 weeks In = 10, group C). Of primary mutations (protease: 30N, 461/L, 82A, 90M; reverse transcriptase: 70R, 1841/V, 215 Y/F) detected on therapy 100% remained after stopping therapy in group A; 68% remained in group B and 15% remained in group C. For secondary mutations 98% remained in group A; 99% remained in group B and 57% in group C. Conclusions: This study showed a rapid decline in detectability of the majority of primary mutations within 13 weeks of stopping combination therapy. From this data, HIV-1 resistance testing to direct patients' therapy should only be carried out when on existing therapy, or < 2 weeks off therapy, if reliable decisions are to be made relating to future combinations.

Published

1999

47. Chronic erosive herpes simplex virus infection of the penis, a possible immune reconstitution disease

Author

Nicholas Francis, Margaret Johnson, Don C. Henderson, L. Fearfield, Brian Gazzard, Mike Youle, S.E. Barton, Christopher B Bunker, Fox Pa, and Deenan Pillay

Subjects

Adult, Male, AIDS-Related Opportunistic Infections, Lymphocyte, Human leukocyte antigen, Plasma cell, medicine.disease_cause, Immunocompromised Host, Antiretroviral Therapy, Highly Active, medicine, Humans, Pharmacology (medical), Herpes Genitalis, medicine.diagnostic_test, business.industry, Health Policy, Middle Aged, Virology, Treatment Outcome, Infectious Diseases, medicine.anatomical_structure, Herpes simplex virus, Chronic Disease, Immunology, business, Tissue typing, Penis

Abstract

Objective To report a novel clinical presentation: a chronic erosive herpes simplex virus (HSV) infection of the penis which developed in AIDS patients following the commencement of highly active antiretroviral therapy (HAART). The lesions were unresponsive to antiviral treatments which had previously been effective, and this could not be accounted for in terms of increased antiviral resistance. Design Detailed case-note review and investigation of three cases which presented at two large HIV units in London. Methods Review of all histology with immunohistochemistry for HSV, HSV drug susceptibility assays, tissue typing and measurement of in vitro lymphocyte functional activity against HSV. Results The histology of the lesions was the same in each case, with the presence of HSV on immunohistochemistry and an unusual prominence of plasma cell and eosinophils in the inflammatory infiltrate. HSV-specific lymphoproliferative responses were normal in two cases, but subnormal in a third case. All individuals shared the HLA class I molecules B72 and Cw0202 and the class II allele DRB4. Conclusion We believe this to be a previously unreported adverse consequence of HAART, the result of partial immune restoration, reminiscent of the the recently described syndrome of immune recovery vitritis.

Published

1999

48. The changing pattern of admissions to a London hospital of patients with HIV: 1988-1997

Author

Anthony Drinkwater, Marc Lipman, Simon M. Barry, Alessandro Cozzi Lepri, Mike Youle, Caroline A. Sabin, Margaret Johnson, Sabine Kinloch, Amanda Mocroft, and Andrew N. Phillips

Subjects

Cellular immunity, medicine.medical_specialty, Pediatrics, business.industry, Incidence (epidemiology), Immunology, medicine.disease, law.invention, Zidovudine, Infectious Diseases, Acquired immunodeficiency syndrome (AIDS), Randomized controlled trial, law, Epidemiology, medicine, Etiology, Immunology and Allergy, Risk factor, business, medicine.drug

Abstract

OBJECTIVE To describe the changes over time in incidence of hospital admissions among patients with HIV, reasons for hospital admission, duration of stay, relationship with CD4 T-cell count and with antiretroviral treatment. METHODS The incidence of hospital admissions during each calendar year from 1988 to 1997 inclusive was calculated using a person-years analysis. In addition the proportion of patient follow-up spent in hospital and the impact of changing treatment regimens among all patients with HIV aged > or = 14 years and with at least one CD4 T-cell count seen at the Royal Free Hospital, London was also described. RESULTS A total of 1806 patients were investigated with median follow-up of 21.1 months. Among all patients, the proportion of follow-up time spent as an in-patient decreased from 3.9% in 1988 to 1.3% in 1997 (P = 0.0015; test for trend). Hospital admissions for any cause peaked during 1989 at 72.0 per 100 patient years of follow-up (PYFU) and was 28.5 per 100 PYFU during 1997 (P 30% before 1990 to < 5% during 1997 (P = 0.026; test for trend). Hospital admissions varied greatly according to treatment regimen; in 1996 and 1997 just 0.1% of follow-up time of patients on triple antiretroviral treatment regimens was spent as a hospital admission. CONCLUSIONS Admissions to hospital began falling before the introduction of combination therapy and declined strikingly during 1996 and 1997 following the introduction of highly active antiretroviral therapy. These results have important implications for future allocation of resources and for patient management.

Published

1999

49. Compromised Immunologic Recovery in Patients Receiving Tipranavir/Ritonavir Coadministered With Tenofovir and Didanosine in Randomized Evaluation of Strategic Intervention in multidrug-reSistant patients with Tipranavir (RESIST) Studies

Author

Bonaventura Clotet, Pierre Marie Girard, Eugenia Negredo, Mike Youle, and Dietmar Neubacher

Subjects

Oncology, medicine.medical_specialty, business.industry, Drug resistance, law.invention, Multiple drug resistance, Clinical trial, Infectious Diseases, Pharmacotherapy, Randomized controlled trial, law, Internal medicine, medicine, Pharmacology (medical), business, Viral load, Didanosine, Tipranavir, medicine.drug

Published

2007

50. Safety, Pharmacokinetics, and Antiretroviral Activity of the Potent, Specific Human Immunodeficiency Virus Protease Inhibitor Nelfinavir: Results of a Phase I/II Trial and Extended Follow-up in Patients Infected with Human Immunodeficiency Virus

Author

Chris Higgs, Jo Monaghan, Graeme Moyle, William T. Prince, Sharon Chapman, Mark Nelson, Mike Youle, and Neil Clendeninn

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Anti-HIV Agents, Nausea, HIV Infections, Gastroenterology, Pharmacokinetics, Oral administration, Internal medicine, medicine, Humans, Pharmacology (medical), Adverse effect, Pharmacology, Nelfinavir, business.industry, HIV Protease Inhibitors, Surgery, Tolerability, Toxicity, medicine.symptom, Flatulence, business, Follow-Up Studies, medicine.drug

Abstract

The safety, antiretroviral activity, and pharmacokinetic profile of nelfinavir, a potent and specific inhibitor of human immunodeficiency virus (HIV) protease, were assessed in a small open-label phase I/II dose-ranging study in protease inhibitor-naive HIV-positive men. A total of 22 patients with baseline plasma HIV RNA ≥ 20,000 copies/mL and CD4+ counts between 200 and 500 cells/mm 3 were enrolled in the study. Of the 22 patients, 20 were evaluated for activity; 10 patients assigned to 771 mg/day base equivalent (300 mg three times daily) and 10 patients assigned to 1,026 mg/day base equivalent (600 mg twice daily) given monotherapy. A capsule formulation of nelfinavir was used. The initial study period was 28 days; patients showing a virologic response of 1 log 10 reduction were eligible for enrollment in an extension phase and addition of nucleoside analogues. A maximally tolerated dose of nelfinavir was not established. A dose-response relationship was observed for four (40%) patients in the 771-mg group and six (60%) patients in the 1,026-mg group experiencing a reduction from baseline in plasma HIV RNA of at least 1 log during the 28-day study. of these patients, five sustained the reduction in plasma HIV RNA beyond day 28 (2 patients receiving 771 mg/day and 3 patients receiving 1,026 mg/day). Median increases from baseline in CD4+ counts at day 28 were 216 cell/mm 3 and 86 cell/mm 3 in the 771-mg and 1,026-mg groups, respectively. After oral administration, median nelfinavir plasma concentrations on day 28 reached a maximum at 1 hour (2,966 ng/mL) in the 771-mg group and at 3 hours (3,157 ng/mL) in the 1,026-mg group. Data for 22 patients were included in the safety analysis; 12 patients (55%) reported at least one grade 2 or worse (moderate, severe, or very severe) adverse event. The most common grade 2 or worse adverse event was diarrhea, reported by two patients (20%) receiving 771 mg/day and seven patients (70%) receiving 1,026 mg/day; followed by nausea, flatulence, asthenia, and headache (each reported in 1 patient [10%] in the 771-mg group) and dizziness (reported in 1 patient [10%] receiving 1,026 mg/day). In the small subgroup (n = 6) who continued taking nelfinavir for longer periods (between 8 and 15 months), virologic responses were sustained in the majority of patients with good tolerability. Nelfinavir is an active HIV-protease inhibitor with favorable pharmacokinetics, good tolerability, and sustained antiviral effects. Results of this early phase I/II dose-ranging study provided data for the safety and antiretroviral activity of nelfinavir and led to the selection of higher doses for phase II/III trials to further optimize virologic and immunologic responses.

Published

1998