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3. Human Immunotypes Impose Selection on Viral Genotypes Through Viral Epitope Specificity

Author

Gabrielaite, M. Bennedbæk, M. Zucco, A.G. Ekenberg, C. Murray, D.D. Kan, V.L. Touloumi, G. Vandekerckhove, L. Turner, D. Neaton, J. Clifford Lane, H. Safo, S. Arenas-Pinto, A. Polizzotto, M.N. Günthard, H.F. Lundgren, J.D. Marvig, R.L.

Abstract

Background: Understanding the genetic interplay between human hosts and infectious pathogens is crucial for how we interpret virulence factors. Here, we tested for associations between HIV and host genetics, and interactive genetic effects on viral load (VL) in HIV-positive antiretroviral treatment-naive clinical trial participants. Methods: HIV genomes were sequenced and the encoded amino acid (AA) variants were associated with VL, human single nucleotide polymorphisms (SNPs), and imputed HLA alleles using generalized linear models with Bonferroni correction. Results: Human (388 501 SNPs) and HIV (3010 variants) genetic data were available for 2122 persons. Four HIV variants were associated with VL (P < 1.66 × 10-5). Twelve HIV variants were associated with a range of 1-512 human SNPs (P < 4.28 × 10-11). We found 46 associations between HLA alleles and HIV variants (P < 1.29 × 10-7). HIV variants and immunotypes when analyzed separately were associated with lower VL, whereas the opposite was true when analyzed in concert. Epitope binding predictions supported our observations. Conclusions: Our results show the importance of immunotype specificity on viral antigenic determinants, and the identified genetic interplay emphasizes that viral and human genetics should be studied in the context of each other. Clinical Trials Registration: NCT00867048. © 2021 The Author(s) 2021. Published by Oxford University Press for the Infectious Diseases Society of America. All rights reserved. For permissions, e-mail: journals.permissions@oup.com.

Published
2021

4. Time to virological failure of 3 classes of antiretrovirals after initiation of highly active antiretroviral therapy: results from the EuroSIDA study group

Author

Mocroft, A., Ledergerber, B., Viard, J.P., Staszewski, S., Murphy, M., Chiesi, A., Horban, A., Hansen, A.-B.E., Phillips, A.N., and Lundgren, J.D.

Subjects
Communicable diseases -- Care and treatment, Virology -- Research, Highly active antiretroviral therapy -- Health aspects, Highly active antiretroviral therapy -- Research, Health
Published
2004

5. Lipid profiles in HIV-infected patients receiving combination antiretroviral therapy: are different antiretroviral drugs associated with different lipid profiles?

Author

Fontas, E., van Leth, F., Sabin, C.A., Friis-Moller, N., Rickenbach, M., Monforte, A. d'Arminio, Kirk, O., Dupon, M., Morfeldt, L., Mateu, S., Petoumenos, K., El-Sadr, W., de Wit, S., Lundgren, J.D., Pradier, C., and Reiss, P.

Subjects
Proteolipids -- Research, Lipoproteins -- Research, Coronary heart disease -- Care and treatment, Coronary heart disease -- Research, Antiviral agents -- Health aspects, Triglycerides -- Health aspects, Triglycerides -- Research, Health
Published
2004

6. Epidemiology of AIDS dementia complex in Europe

Author

Chiesi, A., Vella, S., Dally, L.G., Pedersen, C., Danner, S., Johnson, A.M., Schwander, S., Goebel, F.D., Glauser, M., Antunes, F., and Lundgren, J.D.

Subjects
AIDS (Disease) -- Demographic aspects, Dementia -- Demographic aspects, Neurologic manifestations of general diseases -- Demographic aspects, AIDS dementia -- Demographic aspects, Health
Abstract

The risk of AIDS dementia complex (ADC) may increase with increased intravenous drug use, age, and reduced CD4+ cell count, and may decrease temporarily with zidovudine treatment. ADC is characterized by the loss of intellectual or motor abilities in advanced HIV disease. Researchers reviewed medical records of 6,548 people diagnosed with AIDS between 1979 and 1989. ADC was present in 4.5% of the people at the time of AIDS diagnosis, and developed in 7.8% of the people after AIDS diagnosis. The risk of having ADC was higher in women than in men, and higher in intravenous drug users than in other populations. Statistical analysis suggested that zidovudine use decreased the risk of developing ADC after diagnosis by about 40%, but this risk reduction was only present during the first 18 months of therapy.

Published
1996

8. HIV resistance testing and detected drug resistance in Europe

Author

Schultze, A., Phillips, A.N., Paredes, R., Battegay, M., Rockstroh, J.K., Machala, L., Tomazic, J., Girard, P.M., Januskevica, I., Gronborg-Laut, K., Lundgren, J.D., Cozzi-Lepri, A., Burger, D.M., Amsterdam institute for Infection and Immunity, Amsterdam Public Health, and Global Health

Subjects
Adult, Male, medicine.medical_specialty, Genotype, Anti-HIV Agents, prevalence, Immunology, HIV Infections, Drug resistance, Logistic regression, Odds, Cohort Studies, Internal medicine, Drug Resistance, Viral, medicine, Immunology and Allergy, Humans, Treatment Failure, Generalized estimating equation, business.industry, antiviral drug resistance, HIV, Odds ratio, HIV Protease Inhibitors, Middle Aged, Viral Load, Confidence interval, CD4 Lymphocyte Count, Europe, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Infectious Diseases, Logistic Models, Cohort, Multivariate Analysis, HIV-1, Reverse Transcriptase Inhibitors, Female, business, logistic models, Testing, Regional differences, Virological failure, Cohort study
Abstract

OBJECTIVES: To describe regional differences and trends in resistance testing among individuals experiencing virological failure and the prevalence of detected resistance among those individuals who had a genotypic resistance test done following virological failure.DESIGN: Multinational cohort study.METHODS: Individuals in EuroSIDA with virological failure (>1 RNA measurement >500 on ART after >6 months on ART) after 1997 were included. Adjusted odds ratios (aORs) for resistance testing following virological failure and aORs for the detection of resistance among those who had a test were calculated using logistic regression with generalized estimating equations.RESULTS: Compared to 74.2% of ART-experienced individuals in 1997, only 5.1% showed evidence of virological failure in 2012. The odds of resistance testing declined after 2004 (global P CONCLUSIONS: Despite a concurrent decline in virological failure and testing, drug resistance was commonly detected. This suggests a selective approach to resistance testing. The regional differences identified indicate that policy aiming to minimize the emergence of resistance is of particular relevance in some European regions, notably in the countries in Eastern Europe.

Published
2015
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9. Gender differences in the use of cardiovascular interventions in HIV-positive persons; the D:A:D Study

Author

Hatleberg, C.I., Ryom, L., El-Sadr, W., Mocroft, A., Reiss, P., Wit, S. de, Dabis, F., Pradier, C., Monforte, A., Kovari, H., Law, M., Koopmans, P.P., Keuter, M., Ven, A.J.A.M. van der, Hofstede, H.J.M. ter, Dofferhoff, A.S.M., Crevel, R. van, Albers, M.A., Bosch, M.E.W., Grintjes-Huisman, K.J.T., Zomer, B.J., Stelma, F.F., Rahamat-Langendoen, J.C., Burger, D.M., Lundgren, J.D., Sabin, C.A., Hatleberg, C.I., Ryom, L., El-Sadr, W., Mocroft, A., Reiss, P., Wit, S. de, Dabis, F., Pradier, C., Monforte, A., Kovari, H., Law, M., Koopmans, P.P., Keuter, M., Ven, A.J.A.M. van der, Hofstede, H.J.M. ter, Dofferhoff, A.S.M., Crevel, R. van, Albers, M.A., Bosch, M.E.W., Grintjes-Huisman, K.J.T., Zomer, B.J., Stelma, F.F., Rahamat-Langendoen, J.C., Burger, D.M., Lundgren, J.D., and Sabin, C.A.

Abstract

Contains fulltext : 196903.pdf (publisher's version ) (Open Access)

Published
2018

10. Cost-effectiveness of public-health policy options in the presence of pretreatment NNRTI drug resistance in sub-Saharan Africa: A modelling study

Author

Phillips, A. (Andrew), Cambiano, V. (Valentina), Nakagawa, F. (Fumiyo), Revill, P. (Paul), Jordan, M.R. (Michael), Hallett, T.B. (Timothy), Doherty, M.C. (Meg), Luca, A. (Andrea) de, Lundgren, J.D. (Jens D.), Mhangara, M. (Mutsa), Apollo, T. (Tsitsi), Mellors, J.W. (John W.), Nichols, B.E. (Brooke), Parikh, U. (Urvi), Pillay, D. (Deenan), Rinke de Wit, T.F. (Tobias), Sigaloff, K.C. (Kim), Havlir, D. (Diane), Kuritzkes, D.R. (Daniel), Pozniak, A. (Anton), Vijver, D.A.M.C. (David) van de, Vitoria, M. (Marco), Wainberg, M.A. (Mark A.), Raizes, E. (Elliot), Bertagnolio, S. (Silvia), Phillips, A. (Andrew), Cambiano, V. (Valentina), Nakagawa, F. (Fumiyo), Revill, P. (Paul), Jordan, M.R. (Michael), Hallett, T.B. (Timothy), Doherty, M.C. (Meg), Luca, A. (Andrea) de, Lundgren, J.D. (Jens D.), Mhangara, M. (Mutsa), Apollo, T. (Tsitsi), Mellors, J.W. (John W.), Nichols, B.E. (Brooke), Parikh, U. (Urvi), Pillay, D. (Deenan), Rinke de Wit, T.F. (Tobias), Sigaloff, K.C. (Kim), Havlir, D. (Diane), Kuritzkes, D.R. (Daniel), Pozniak, A. (Anton), Vijver, D.A.M.C. (David) van de, Vitoria, M. (Marco), Wainberg, M.A. (Mark A.), Raizes, E. (Elliot), and Bertagnolio, S. (Silvia)

Abstract

Background: There is concern over increasing prevalence of non-nucleoside reverse-transcriptase inhibitor (NNRTI) resistance in people initiating antiretroviral therapy (ART) in low-income and middle-income countries. We assessed the effectiveness and cost-effectiveness of alternative public health responses in countries in sub-Saharan Africa where the prevalence of pretreatment drug resistance to NNRTIs is high. Methods: The HIV Synthesis Model is an individual-based simulation model of sexual HIV transmission, progression, and the effect of ART in adults, which is based on extensive published data sources and considers specific drugs and resistance mutations. We used this model to generate multiple setting scenarios mimicking those in sub-Saharan Africa and considered the prevalence of pretreatment NNRTI drug resistance in 2017. We then compared effectiveness and cost-effectiveness of alternative policy options. We took a 20 year time horizon, used a cost effectiveness threshold of US$500 per DALY averted, and discounted DALYs and costs at 3% per year.

Published
2018
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12. Associations between HIV-RNA-based indicators and virological and clinical outcomes

Author

Laut, K.G. Shepherd, L.C. Pedersen, C. Rockstroh, J.K. Sambatakou, H. Paduta, D. Matulionyte, R. Smiatacz, T. Mulcahy, F. Lundgren, J.D. Mocroft, A. Kirk, O. Gatell, J. Gazzard, B. Horban, A. Karpov, I. Ledergerber, B. Losso, M. Monforte, A.D. Rakhmanova, A. Ristola, M. Phillips, A. Reiss, P. Rockstroh, J. De Wit, S. Grarup, J. Cozzi-Lepri, A. Thiebaut, R. Burger, D. Paredes, R. Peters, L. on behalf of EuroSIDA in EuroCoord

Abstract

Objectives: To evaluate and compare the performance of six HIV-RNA-based quality of care indicators for predicting short-term and long-term outcomes. Design: Multinational cohort study. Methods: We included EuroSIDA patients on antiretroviral therapy (ART) with at least three viral load measurements after baseline (the latest of 01/01/2001 or entry into EuroSIDA). Using multivariate Poisson regression, we modelled the association between short-term (resistance, triple-class failure) and long-term (all-cause mortality, any AIDS/non-AIDS clinical event) outcomes and the indicators: viraemia copy years; consecutive months with viral load ≥50 copies/ml; percentage of time on ART spent fully suppressed (%FS); stable on ART; 48 weeks snapshot; and current viral load. Indicators were compared using area under the ROC curve (AUC) and different measures of model fit. Results: Adjusted incidence rate ratios for all outcomes tended to increase with increasing viraemia copy years, number of consecutive months with viral load ≥50 copies/ml, current viral load and with lower %FS, but the gradient of increased risk was weak across strata. None of the indicators reliably identified those at risk of long-term outcomes (AUC 0.54-0.58), but performed consistently better with short-term outcomes [triple class failure (AUC 0.67-0.76) and resistance (AUC 0.64-0.79)]. Goodness of fit varied with the outcome evaluated, but differences between indicators were small. Conclusion: Differences between quality of care indicators were small and no indicator performed consistently better than current viral load. Given the simplicity in assessing and interpreting this indicator, we propose to use current viral load when HIV-RNA-based indicators are used to evaluate the efficacy of ART programs. Copyright © 2016 Wolters Kluwer Health, Inc. All rights reserved.

Published
2016

13. Development of a definition for Rapid Progression (RP) of renal function in HIV-positive persons: the D:A:D study

Author

Kamara, D.A., Ryom, L., Ross, M., Kirk, O., Reiss, P., Morlat, P., Moranne, O., Fux, C.A., Mocroft, A., Sabin, C., Lundgren, J.D., D:A:D Study Group, the, Posthouwer, D., Smith, C.J., Medische Microbiologie, RS: CAPHRI School for Public Health and Primary Care, and Interne Geneeskunde

Subjects
CHRONIC KIDNEY-DISEASE, FUNCTION DECLINE, Rapid progression, HIV, Kidney disease, urologic and male genital diseases, GLOMERULAR-FILTRATION-RATE, CLASSIFICATION, PREVALENCE, DIET, MORTALITY RISK, INDIVIDUALS, ANTIRETROVIRAL THERAPY, Chronic kidney disease, Estimated glomerular filtration rate, BODY-SURFACE AREA
Abstract

Background: No consensus exists on how to define abnormally rapid deterioration in renal function (Rapid Progression, RP). We developed an operational definition of RP in HIV-positive persons with baseline estimated glomerular filtration rate (eGFR) >90 ml/min/1.73 m(2) (using Cockcroft Gault) in the Data Collection on Adverse Events of Anti-HIV Drugs (D: A: D) study from 2004 to 2011. Methods: Two definitions were evaluated; RP definition A: An average eGFR decline (slope) >= 5 ml/min/1.73 m(2)/year over four years of follow-up with >= 3 eGFR measurements/year, last eGFR = 5 ml/min/1.73 m(2)/year in two consecutive years. RP definition B: An absolute annual decline >= 5 ml/min/1.73 m(2)/year in each year and last eGFR Results: 22,603 individuals had baseline eGFR >= 90 ml/min/1.73 m(2). 108/3655 (3.0%) individuals with >= 4 years' follow-up and >= 3 measurements/year experienced RP under definition A; similar proportions were observed when considering follow-up periods of three (n=195/6375; 3.1%) and two years (n=355/10756; 3.3%). In contrast under RP definition B, greater proportions experienced RP when considering two years (n=476/10756; 4.4%) instead of three (n=48/6375; 0.8%) or four (n=15/3655; 0.4%) years' follow-up. For RP definition A, 13 (12%) individuals who experienced RP progressed to CKD, and only (21) 0.6% of those without RP progressed to CKD (sensitivity 38.2% and specificity 97.4%); whereas for RP definition B, fewer RP individuals progressed to CKD. Conclusions: Our results suggest using three years' follow-up and at least two eGFR measurements per year is most appropriate for a RP definition, as it allows inclusion of a reasonable number of individuals and is associated with the known risk factors. The definition does not necessarily identify all those that progress to incident CKD, however, it can be used alongside other renal measurements to early identify and assess those at risk of developing CKD. Future analyses will use this definition to identify other risk factors for RP, including the role of antiretrovirals.

Published
2014

14. Cumulative and current exposure to potentially nephrotoxic antiretrovirals and development of chronic kidney disease in HIV-positive individuals with a normal baseline estimated glomerular filtration rate: a prospective international cohort study

Author

Mocroft, A., Lundgren, J.D., Ross, M., Fux, C.A., Reiss, P., Moranne, O., Morlat, P., Monforte, A., Kirk, O., Ryom, L., Burger, D.M., et al., Mocroft, A., Lundgren, J.D., Ross, M., Fux, C.A., Reiss, P., Moranne, O., Morlat, P., Monforte, A., Kirk, O., Ryom, L., Burger, D.M., and et al.

Abstract

Item does not contain fulltext, BACKGROUND: Whether or not the association between some antiretrovirals used in HIV infection and chronic kidney disease is cumulative is a controversial topic, especially in patients with initially normal renal function. In this study, we aimed to investigate the association between duration of exposure to antiretrovirals and the development of chronic kidney disease in people with initially normal renal function, as measured by estimated glomerular filtration rate (eGFR). METHODS: In this prospective international cohort study, HIV-positive adult participants (aged >/=16 years) from the D:A:D study (based in Europe, the USA, and Australia) with first eGFR greater than 90 mL/min per 1.73 m(2) were followed from baseline (first eGFR measurement after Jan 1, 2004) until the occurrence of one of the following: chronic kidney disease; last eGFR measurement; Feb 1, 2014; or final visit plus 6 months (whichever occurred first). Chronic kidney disease was defined as confirmed (>3 months apart) eGFR lower than 60 mL/min per 1.73 m(2). The primary outcome was the occurrence of chronic kidney disease. Poisson regression was used to estimate the incidence rate of chronic kidney disease associated with cumulative exposure to tenofovir disoproxil fumarate, ritonavir-boosted atazanavir, ritonavir-boosted lopinavir, other ritonavir-boosted protease inhibitors, or abacavir. FINDINGS: Between Jan 1, 2004, and July 26, 2013, 23,905 eligible individuals from the D:A:D study were included. Participants had a median baseline eGFR of 110 mL/min per 1.73 m(2) (IQR 100-125), a median age of 39 years (33-45), and median CD4 cell count of 441 cells per mm(3) (294-628). During a median follow-up of 7.2 years (IQR 5.1-8.9), 285 (1%) of 23,905 people developed chronic kidney disease (incidence 1.76 per 1000 person-years of follow-up [95% CI 1.56-1.97]). After adjustment, we recorded a significant increase in chronic kidney disease associated with each additional year of exposure to tenofovir d

Published
2016

15. Increased risk of cardiovascular disease (CVD) with age in HIV-positive men: a comparison of the D:A:D CVD risk equation and general population CVD risk equations

Author

Petoumenos, K., Reiss, P., Ryom, L., Rickenbach, M., Sabin, C.A., El-Sadr, W., Monforte, A., Phillips, A.N., Wit, S. de, Kirk, O., Dabis, F., Pradier, C., Lundgren, J.D., Law, M.G., Warris, A., Koopmans †, P.P., Keuter, M., and Ven, A.J. van der

Subjects
lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], cardiovascular diseases
Abstract

Contains fulltext : 138900.pdf (Publisher’s version ) (Closed access) OBJECTIVES: The aim of the study was to statistically model the relative increased risk of cardiovascular disease (CVD) per year older in Data collection on Adverse events of anti-HIV Drugs (D:A:D) and to compare this with the relative increased risk of CVD per year older in general population risk equations. METHODS: We analysed three endpoints: myocardial infarction (MI), coronary heart disease (CHD: MI or invasive coronary procedure) and CVD (CHD or stroke). We fitted a number of parametric age effects, adjusting for known risk factors and antiretroviral therapy (ART) use. The best-fitting age effect was determined using the Akaike information criterion. We compared the ageing effect from D:A:D with that from the general population risk equations: the Framingham Heart Study, CUORE and ASSIGN risk scores. RESULTS: A total of 24 323 men were included in analyses. Crude MI, CHD and CVD event rates per 1000 person-years increased from 2.29, 3.11 and 3.65 in those aged 40-45 years to 6.53, 11.91 and 15.89 in those aged 60-65 years, respectively. The best-fitting models included inverse age for MI and age + age(2) for CHD and CVD. In D:A:D there was a slowly accelerating increased risk of CHD and CVD per year older, which appeared to be only modest yet was consistently raised compared with the risk in the general population. The relative risk of MI with age was not different between D:A:D and the general population. CONCLUSIONS: We found only limited evidence of accelerating increased risk of CVD with age in D:A:D compared with the general population. The absolute risk of CVD associated with HIV infection remains uncertain.

Published
2014

16. Chronic kidney disease in patients with normal eGFR at baseline: results from EuroSIDA

Author

Ryom, L., Mocroft, A., Reiss, P., Ledergerber, B., De Wit, S., Duiculescu, D., Monforte, A.D., Murphy, M., Lundgren, J.D., and Kirk, O.

Subjects
Chronic kidney failure -- Risk factors -- Demographic aspects, Glomerular filtration rate -- Health aspects, HIV infection -- Complications and side effects, Health
Abstract

7‐11 November 2010, Tenth International Congress on Drug Therapy in HIV Infection, Glasgow, UK, Background Chronic kidney disease (CKD) is an emerging co‐morbidity among HIV patients. Recent EuroSIDA analyses identified CKD risk factors including hypertension, diabetes, hepatitis C, age>50, low CD4 count, prior AIDS [...]

Published
2010
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17. Considerations in the rationale, design and methods of the Strategic Timing of AntiRetroviral Treatment (START) study

Author

Babiker, A.G. Emery, S. Fätkenheuer, G. Gordin, F.M. Grund, B. Lundgren, J.D. Neaton, J.D. Pett, S.L. Phillips, A. Touloumi, G. Vjechaj, M.J.

Abstract

Untreated human immunodeficiency virus (HIV) infection is characterized by progressive depletion of CD4+ T lymphocyte (CD4) count leading to the development of opportunistic diseases (acquired immunodeficiency syndrome (AIDS)), and more recent data suggest that HIV is also associated with an increased risk of serious non-AIDS (SNA) diseases including cardiovascular, renal, and liver diseases and non-AIDS-defining cancers. Although combination antiretroviral treatment (ART) has resulted in a substantial decrease in morbidity and mortality in persons with HIV infection, viral eradication is not feasible with currently available drugs. The optimal time to start ART for asymptomatic HIV infection is controversial and remains one of the key unanswered questions in the clinical management of HIV-infected individuals. In this article, we outline the rationale and methods of the Strategic Timing of AntiRetroviral Treatment (START) study, an ongoing multicenter international trial designed to assess the risks and benefits of initiating ART earlier than is currently practiced. We also describe some of the challenges encountered in the design and implementation of the study and how these challenges were addressed. A total of 4000 study participants who are HIV type 1 (HIV-1) infected, ART naïve with CD4 count > 500 cells/µL are to be randomly allocated in a 1:1 ratio to start ART immediately (early ART) or defer treatment until CD4 count is

Published
2013

18. Predicting the short-term risk of diabetes in HIV-positive patients: the Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) study

Author

Petoumenos, K., Worm, S.W., Fontas, E., Weber, R., De Wit, S., Bruyand, M., Reiss, P., El-Sadr, W., Monforte, A.D., Friis-Moller, N., Lundgren, J.D., Law, M.G., Groot, R. de, and Flier, M. van der

Subjects
Pathogenesis and modulation of inflammation [N4i 1], Auto-immunity, transplantation and immunotherapy [N4i 4]
Abstract

Contains fulltext : 109117.pdf (Publisher’s version ) (Open Access) INTRODUCTION: HIV-positive patients receiving combination antiretroviral therapy (cART) frequently experience metabolic complications such as dyslipidemia and insulin resistance, as well as lipodystrophy, increasing the risk of cardiovascular disease (CVD) and diabetes mellitus (DM). Rates of DM and other glucose-associated disorders among HIV-positive patients have been reported to range between 2 and 14%, and in an ageing HIV-positive population, the prevalence of DM is expected to continue to increase. This study aims to develop a model to predict the short-term (six-month) risk of DM in HIV-positive populations and to compare the existing models developed in the general population. METHODS: All patients recruited to the Data Collection on Adverse events of Anti-HIV Drugs (D:A:D) study with follow-up data, without prior DM, myocardial infarction or other CVD events and with a complete DM risk factor profile were included. Conventional risk factors identified in the general population as well as key HIV-related factors were assessed using Poisson-regression methods. Expected probabilities of DM events were also determined based on the Framingham Offspring Study DM equation. The D:A:D and Framingham equations were then assessed using an internal-external validation process; area under the receiver operating characteristic (AUROC) curve and predicted DM events were determined. RESULTS: Of 33,308 patients, 16,632 (50%) patients were included, with 376 cases of new onset DM during 89,469 person-years (PY). Factors predictive of DM included higher glucose, body mass index (BMI) and triglyceride levels, and older age. Among HIV-related factors, recent CD4 counts of

Published
2012

19. Hepatitis c virus viremia increases the Incidence of chronic kidney disease in HIV-infected Patients

Author

Peters, L. Grint, D. Lundgren, J.D. Rockstroh, J.K. Soriano, V. Reiss, P. Grzeszczuk, A. Sambatakou, H. Mocroft, A. Kirk, O. Losso, M. Elias, C. Vetter, N. Zangerle, R. Karpov, I. Vassilenko, A. Mitsura, V.M. Suetnov, O. Clumeck, N. De Wit, S. Delforge, M. Colebunders, R. Vandekerckhove, L. Hadziosmanovic, V. Kostov, K. Begovac, J. Machala, L. Jilich, D. Sedlacek, D. Nielsen, J. Kronborg, G. Benfield, T. Larsen, M. Gerstoft, J. Katzenstein, T. Hansen, A.-B.E. Skinhøj, P. Pedersen, C. Ostergaard, L. Zilmer, K. Smidt, J. Ristola, M. Katlama, C. Viard, J.-P. Girard, P.-M. Livrozet, J.M. Vanhems, P. Pradier, C. Dabis, F. Neau, D. Schmidt, R. Van Lunzen, J. Degen, O. Stellbrink, H.J. Staszewski, S. Bogner, J. Fätkenheuer, G. Kosmidis, J. Gargalianos, P. Xylomenos, G. Perdios, J. Panos, G. Filandras, A. Karabatsaki, E. Banhegyi, D. Mulcahy, F. Yust, I. Turner, D. Burke, M. Pollack, S. Hassoun, G. Maayan, S. Vella, S. Esposito, R. Mazeu, I. Mussini, C. Arici, C. Pristera, R. Mazzotta, F. Gabbuti, A. Vullo, V. Lichtner, M. Chirianni, A. Montesarchio, E. Gargiulo, M. Antonucci, G. Testa, A. Narciso, P. Vlassi, C. Zaccarelli, M. Lazzarin, A. Castagna, A. Gianotti, N. Galli, M. Ridolfo, A. D'Arminio Monforte, A. Rozentale, B. Zeltina, I. Chaplinskas, S. Hemmer, R. Staub, T. Ormaasen, V. Maeland, A. Bruun, J. Knysz, B. Gasiorowski, J. Horban, A. Bakowska, E. Flisiak, R. Boron-Kaczmarska, A. Pynka, M. Parczewski, M. Beniowski, M. Mularska, E. Trocha, H. Jablonowska, E. Malolepsza, E. Wojcik, K. Antunes, F. Doroana, M. Caldeira, L. Mansinho, K. Maltez, F. Duiculescu, D. Babes, V. Rakhmanova, A. Zakharova, N. Buzunova, S. Jevtovic, D. Mokráš, M. Staneková, D. Tomazic, J. González-Lahoz, J. Labarga, P. Medrano, J. Moreno, S. Rodriguez, J.M. Clotet, B. Jou, A. Paredes, R. Tural, C. Puig, J. Bravo, I. Gatell, J.M. Miró, J.M. Domingo, P. Gutierrez, M. Mateo, G. Sambeat, M.A. Karlsson, A. Flamholc, L. Ledergerber, B. Weber, R. Francioli, P. Cavassini, M. Hirschel, B. Boffi, E. Furrer, H. Battegay, M. Elzi, L. Kravchenko, E. Chentsova, N. Frolov, V. Kutsyna, G. Servitskiy, S. Krasnov, M. Barton, S. Johnson, A.M. Mercey, D. Phillips, A. Johnson, M.A. Murphy, M. Weber, J. Scullard, G. Fisher, M. Leen, C. EuroSIDA in EuroCoord

Subjects
virus diseases, digestive system diseases
Abstract

Background: Several studies have reported on an association between hepatitis C virus (HCV) antibody status and the development of chronic kidney disease (CKD), but the role of HCV viremia and genotype are not well defined. Methods: Patients with at least three serum creatinine measurements after 1 January 2004 and known HCV antibody status were included. Baseline was defined as the first eligible estimated glomerular filtration rate (eGFR) (Cockcroft-Gault equation), and CKD was either a confirmed (>3 months apart) eGFR of 60 ml/min per 1.73m2 or less for patients with a baseline eGFR more than 60 ml/min per 1.73m2 or a confirmed 25% decline in eGFR for patients with a baseline eGFR of 60 ml/min per 1.73m2 or less. Incidence rates of CKD were compared between HCV groups (anti-HCV-negative, anti-HCV-positive with or without viremia) using Poisson regression. Results: Of 8235 patients with known anti-HCV status, 2052 (24.9%) were anti-HCVpositive of whom 983 (47.9%) were HCV-RNA-positive, 193 (9.4%) HCV-RNAnegative and 876 (42.7%) had unknown HCV-RNA. At baseline, the median eGFR was 97.6 (interquartile range 83.8-113.0) ml/min per 1.73m2. During 36123 personyears of follow-up (PYFU), 495 patients progressed to CKD (6.0%) with an incidence rate of 14.5 per 1000 PYFU (95% confidence interval 12.5-14.9). In a multivariate Poisson model, patients who were anti-HCV-positive with HCV viremia had a higher incidence rate of CKD, whereas patients with cleared HCV infection had a similar incidence rate of CKD compared with anti-HCV-negative patients. There was no association between CKD and HCV genotype. Conclusion: Compared with HIV-monoinfected patients, HIV-positive patients with chronic rather than cleared HCV infection were at increased risk of developing CKD, suggesting a contribution from active HCV infection toward the pathogenesis of CKD. © 2012 Wolters Kluwer Health.

Published
2012

20. A standardized algorithm for determining the underlying cause of death in HIV infection as AIDS or non-AIDS related: Results from the EuroSIDA study

Author

Kowalska, J.D. Mocroft, A. Ledergerber, B. Florence, E. Ristola, M. Begovac, J. Sambatakou, H. Pedersen, C. Lundgren, J.D. Kirk, O.

Abstract

Objectives: Analyzing changes in causes of death over time is essential for understanding the emerging trends in HIV population mortality, yet data on cause of death are often missing. This poses analytic limitations, as does the changing approach in data collection by longitudinal studies, which are a natural consequence of an increased awareness and knowledge in the field. To monitor and analyze changes in mortality over time, we have explored this issue within the EuroSIDA study and propose a standardized protocol unifying data collected and allowing for classification of all deaths as AIDS or non-AIDS related, including events with missing cause of death. Methods: Several classifications of the underlying cause of death as AIDS or non-AIDS related within the EuroSIDA study were compared: central classification (CC-reference group) based on an externally standardised method (the CoDe procedures), local cohort classification (LCC) as reported by the site investigator, and 4 algorithms (ALG) created based on survival times after specific AIDS events. Results: A total of 2,783 deaths occurred, 540 CoDe forms were collected, and 488 were used to evaluate agreements. The agreement between CC and LCC was substantial (κ = 0.7) and the agreement between CC and ALG was moderate (κ < 0.6). Consequently, a stepwise algorithm was derived prioritizing CC over LCC and, in patients with no information available, best-fit ALG. Using this algorithm, 1,332 (47.9%) deaths were classified as AIDS and 1,451 (52.1%) as non-AIDS related. Conclusions: Our proposed stepwise algorithm for classifying deaths provides a valuable tool for future research, however validation in another setting is warranted. © 2011 Thomas Land Publishers, Inc.

Published
2011

21. Changing utilization of Stavudine (d4T) in HIV-positive people in 2006-2013 in the EuroSIDA study

Author

Podlekareva, D., Grint, D., Karpov, I., Rakmanova, A., Mansinho, K., Chentsova, N., Zeltina, I., Losso, M., Parczewski, M., Lundgren, J.D., Mocroft, A., Kirk, O., Burger, D.M., et al., Podlekareva, D., Grint, D., Karpov, I., Rakmanova, A., Mansinho, K., Chentsova, N., Zeltina, I., Losso, M., Parczewski, M., Lundgren, J.D., Mocroft, A., Kirk, O., Burger, D.M., and et al.

Abstract

Item does not contain fulltext, OBJECTIVES: The long-term side effects of stavudine (d4T) led to recommendations in 2009 to phase out use of this drug. We aimed to describe temporal patterns of d4T use across Europe. METHODS: Patients taking combination antiretroviral therapy (cART) in EuroSIDA with follow-up after 1 January 2006 were included in the study. cART was defined as d4T-containing [d4T plus at least two other antiretrovirals (ARVs) from any class] or non-d4T-containing (at least three ARVs from any class, excluding d4T). Poisson regression was used to describe temporal changes in the prevalence of d4T use and factors associated with initiating d4T. RESULTS: A total of 5850 patients receiving cART on 1 January 2006 were included in the current analysis, rising to 7768 patients on January 1 2013. During this time, the prevalence of d4T use fell from 11.2% to 0.7%, with an overall decline of 19% per 6 months [95% confidence interval (CI) 19-20%]. d4T use declined fastest in Northern Europe [26% (95% CI 23-29%) per 6 months], and slowest in Eastern Europe [17% (95% CI 16-19%) per 6 months]. In multivariable Poisson regression models, new d4T initiations decreased by 14% per 6 months [adjusted incidence rate ratio (aIRR) 0.86; 95% CI 0.80-0.91]. Factors associated with initiating d4T were residence in Eastern Europe (aIRR 4.31; 95% CI 2.17-9.98) versus other European regions and HIV RNA > 400 copies/mL (aIRR 3.11; 95% CI 1.60-6.02) versus HIV RNA < 400 copies/mL. CONCLUSIONS: d4T use has declined sharply since 2006 to low levels in most regions; however, a low but persistent level of d4T use remains in Eastern Europe, where new d4T initiations post 2006 are also more common. The reasons for the regional differences may be multifactorial, but it is important to ensure that all clinicians treating HIV-positive patients are aware of the potential harmful effects associated with d4T.

Published
2015

22. Development and validation of a risk score for chronic kidney disease in HIV infection using prospective cohort data from the D:A:D study

Author

Mocroft, A., Lundgren, J.D., Ross, M., Law, M., Reiss, P., Kirk, O., Smith, C., Wentworth, D., Neuhaus, J., Fux, C.A., Moranne, O., Morlat, P., Johnson, M.A., Ryom, L., Burger, D.M., et al., Mocroft, A., Lundgren, J.D., Ross, M., Law, M., Reiss, P., Kirk, O., Smith, C., Wentworth, D., Neuhaus, J., Fux, C.A., Moranne, O., Morlat, P., Johnson, M.A., Ryom, L., Burger, D.M., and et al.

Abstract

Contains fulltext : 154981.PDF (publisher's version ) (Open Access), BACKGROUND: Chronic kidney disease (CKD) is a major health issue for HIV-positive individuals, associated with increased morbidity and mortality. Development and implementation of a risk score model for CKD would allow comparison of the risks and benefits of adding potentially nephrotoxic antiretrovirals to a treatment regimen and would identify those at greatest risk of CKD. The aims of this study were to develop a simple, externally validated, and widely applicable long-term risk score model for CKD in HIV-positive individuals that can guide decision making in clinical practice. METHODS AND FINDINGS: A total of 17,954 HIV-positive individuals from the Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) study with >/=3 estimated glomerular filtration rate (eGFR) values after 1 January 2004 were included. Baseline was defined as the first eGFR > 60 ml/min/1.73 m2 after 1 January 2004; individuals with exposure to tenofovir, atazanavir, atazanavir/ritonavir, lopinavir/ritonavir, other boosted protease inhibitors before baseline were excluded. CKD was defined as confirmed (>3 mo apart) eGFR

Published
2015

23. Sustainable HIV treatment in Africa through viral-load-informed differentiated care

Author

Phillips, A. (Andrew), Shroufi, A. (Amir), Vojnov, L. (Lara), Cohn, J. (Jennifer), Roberts, T. (Teri), Ellman, T. (Tom), Bonner, K. (Kimberly), Rousseau, C. (Christine), Garnett, G. (Geoff), Cambiano, V. (Valentina), Nakagawa, F. (Fumiyo), Ford, D. (Deborah), Bansi-Matharu, L. (Loveleen), Miners, A. (Alec), Lundgren, J.D. (Jens D.), Eaton, J.W. (Jeffrey), Parkes-Ratanshi, R. (Rosalind), Katz, Z. (Zachary), Maman, D. (David), Ford, N. (Nathan), Vitoria, M. (Marco), Doherty, M.C. (Meg), Dowdy, D. (David), Nichols, B.E. (Brooke), Murtagh, M. (Maurine), Wareham, M. (Meghan), Palamountain, K.M. (Kara M.), Chakanyuka Musanhu, C. (Christine), Stevens, W. (Wendy), Katzenstein, D. (David), Ciaranello, A. (Andrea), Barnabas, R. (Ruanne), Braithwaite, R.S. (R. Scott), Bendavid, A. (Avrom), Nathoo, K.J. (Kusum J.), Vijver, D.A.M.C. (David) van de, Wilson, D.P. (David P.), Holmes, C. (Charles), Bershteyn, A. (Anna), Walker, S. (Simon), Raizes, E. (Elliot), Jani, I. (Ilesh), Nelson, L.J. (Lisa J.), Peeling, R. (Rosanna), Terris-Prestholt, F. (Fern), Murungu, J. (Joseph), Mutasa-Apollo, T. (Tsitsi), Hallett, T.B. (Timothy), Revill, P. (Paul), Phillips, A. (Andrew), Shroufi, A. (Amir), Vojnov, L. (Lara), Cohn, J. (Jennifer), Roberts, T. (Teri), Ellman, T. (Tom), Bonner, K. (Kimberly), Rousseau, C. (Christine), Garnett, G. (Geoff), Cambiano, V. (Valentina), Nakagawa, F. (Fumiyo), Ford, D. (Deborah), Bansi-Matharu, L. (Loveleen), Miners, A. (Alec), Lundgren, J.D. (Jens D.), Eaton, J.W. (Jeffrey), Parkes-Ratanshi, R. (Rosalind), Katz, Z. (Zachary), Maman, D. (David), Ford, N. (Nathan), Vitoria, M. (Marco), Doherty, M.C. (Meg), Dowdy, D. (David), Nichols, B.E. (Brooke), Murtagh, M. (Maurine), Wareham, M. (Meghan), Palamountain, K.M. (Kara M.), Chakanyuka Musanhu, C. (Christine), Stevens, W. (Wendy), Katzenstein, D. (David), Ciaranello, A. (Andrea), Barnabas, R. (Ruanne), Braithwaite, R.S. (R. Scott), Bendavid, A. (Avrom), Nathoo, K.J. (Kusum J.), Vijver, D.A.M.C. (David) van de, Wilson, D.P. (David P.), Holmes, C. (Charles), Bershteyn, A. (Anna), Walker, S. (Simon), Raizes, E. (Elliot), Jani, I. (Ilesh), Nelson, L.J. (Lisa J.), Peeling, R. (Rosanna), Terris-Prestholt, F. (Fern), Murungu, J. (Joseph), Mutasa-Apollo, T. (Tsitsi), Hallett, T.B. (Timothy), and Revill, P. (Paul)

Published
2015
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24. Development and Validation of a Risk Score for Chronic Kidney Disease in HIV Infection Using Prospective Cohort Data from the D:A:D Study

Author

Bartlett, J., Mocroft, A., Lundgren, J.D., Ross, M., Law, M., Reiss, P., Kirk, O., Smith, C., Wentworth, D., Neuhaus, J., Fux, C.A., Moranne, O., Morlat, P., Johnson, M.A., Ryom, L., Nolan, D., Bartlett, J., Mocroft, A., Lundgren, J.D., Ross, M., Law, M., Reiss, P., Kirk, O., Smith, C., Wentworth, D., Neuhaus, J., Fux, C.A., Moranne, O., Morlat, P., Johnson, M.A., Ryom, L., and Nolan, D.

Abstract

Background Chronic kidney disease (CKD) is a major health issue for HIV-positive individuals, associated with increased morbidity and mortality. Development and implementation of a risk score model for CKD would allow comparison of the risks and benefits of adding potentially nephrotoxic antiretrovirals to a treatment regimen and would identify those at greatest risk of CKD. The aims of this study were to develop a simple, externally validated, and widely applicable long-term risk score model for CKD in HIV-positive individuals that can guide decision making in clinical practice. Methods and Findings A total of 17,954 HIV-positive individuals from the Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) study with ≥3 estimated glomerular filtration rate (eGFR) values after 1 January 2004 were included. Baseline was defined as the first eGFR > 60 ml/min/1.73 m2 after 1 January 2004; individuals with exposure to tenofovir, atazanavir, atazanavir/ritonavir, lopinavir/ritonavir, other boosted protease inhibitors before baseline were excluded. CKD was defined as confirmed (>3 mo apart) eGFR ≤ 60 ml/min/1.73 m2. Poisson regression was used to develop a risk score, externally validated on two independent cohorts. In the D:A:D study, 641 individuals developed CKD during 103,185 person-years of follow-up (PYFU; incidence 6.2/1,000 PYFU, 95% CI 5.7–6.7; median follow-up 6.1 y, range 0.3–9.1 y). Older age, intravenous drug use, hepatitis C coinfection, lower baseline eGFR, female gender, lower CD4 count nadir, hypertension, diabetes, and cardiovascular disease (CVD) predicted CKD. The adjusted incidence rate ratios of these nine categorical variables were scaled and summed to create the risk score. The median risk score at baseline was −2 (interquartile range –4 to 2). There was a 1:393 chance of developing CKD in the next 5 y in the low risk group (risk score < 0, 33 events), rising to 1:47 and 1:6 in the medium (risk score 0–4, 103 events) and high risk groups (risk s

Published
2015

26. The GDP-GTP exchange factor collybistin: an essential determinant of neuronal gephyrin clustering

Author

Harvey, K., Duguid, I.C., Alldred, M.J., Beatty, S.E., Ward, H., Keep, Nicholas H., Lingenfelter, S.E., Pearce, B.R., Lundgren, J.D., Owens, Max J., Smart, T.G., Luscher, B., Rees, M.I., and Harvey, R.J.

Subjects
bcs
Abstract

Glycine receptors (GlyRs) and specific subtypes of GABA(A) receptors are clustered at synapses by the multidomain protein gephyrin, which in turn is translocated to the cell membrane by the GDP-GTP exchange factor collybistin. We report the characterization of several new variants of collybistin, which are created by alternative splicing of exons encoding an N-terminal src homology 3 (SH3) domain and three alternate C termini (CB1, CB2, and CB3). The presence of the SH3 domain negatively regulates the ability of collybistin to translocate gephyrin to submembrane microaggregates in transfected mammalian cells. Because the majority of native collybistin isoforms appear to harbor the SH3 domain, this suggests that collybistin activity may be regulated by protein-protein interactions at the SH3 domain. We localized the binding sites for collybistin and the GlyR beta subunit to the C-terminal MoeA homology domain of gephyrin and show that multimerization of this domain is required for collybistin-gephyrin and GlyR-gephyrin interactions. We also demonstrate that gephyrin clustering in recombinant systems and cultured neurons requires both collybistin-gephyrin interactions and an intact collybistin pleckstrin homology domain. The vital importance of collybistin for inhibitory synaptogenesis is underlined by the discovery of a mutation (G55A) in exon 2 of the human collybistin gene (ARHGEF9) in a patient with clinical symptoms of both hyperekplexia and epilepsy. The clinical manifestation of this collybistin missense mutation may result, at least in part, from mislocalization of gephyrin and a major GABA(A) receptor subtype.

Published
2004

27. Deteriorating renal function and clinical outcomes in HIV-positive persons

Author

Mocroft, A., Ryom, L., Begovac, J., Monforte, A.D., Vassilenko, A., Gatell, J., Florence, E., Ormaasen, V., Kirk, O., Lundgren, J.D., Burger, D.M., et al., Mocroft, A., Ryom, L., Begovac, J., Monforte, A.D., Vassilenko, A., Gatell, J., Florence, E., Ormaasen, V., Kirk, O., Lundgren, J.D., Burger, D.M., and et al.

Abstract

Item does not contain fulltext, OBJECTIVES: To determine the relationship between measures of renal function [current estimated glomerular filtration rate (eGFR) and proportion of follow-up with a low eGFR (%FU

Published
2014

28. Trends in underlying causes of death in people with HIV from 1999 to 2011 (D:A:D): a multicohort collaboration

Author

Smith, C.J., Ryom, L., Weber, R., Morlat, P., Pradier, C., Reiss, P., Kowalska, J.D., Wit, S. de, Law, M., Sadr, W. el, Kirk, O., Friis-Moller, N., Monforte, A., Phillips, A.N., Sabin, C.A., Lundgren, J.D., Groot, R. de, Koopmans †, P.P., Keuter, M., Ven, A.J. van der, et al., Smith, C.J., Ryom, L., Weber, R., Morlat, P., Pradier, C., Reiss, P., Kowalska, J.D., Wit, S. de, Law, M., Sadr, W. el, Kirk, O., Friis-Moller, N., Monforte, A., Phillips, A.N., Sabin, C.A., Lundgren, J.D., Groot, R. de, Koopmans †, P.P., Keuter, M., Ven, A.J. van der, and et al.

Abstract

Contains fulltext : 137128.pdf (publisher's version ) (Closed access), BACKGROUND: With the advent of effective antiretroviral treatment, the life expectancy for people with HIV is now approaching that seen in the general population. Consequently, the relative importance of other traditionally non-AIDS-related morbidities has increased. We investigated trends over time in all-cause mortality and for specific causes of death in people with HIV from 1999 to 2011. METHODS: Individuals from the Data collection on Adverse events of anti-HIV Drugs (D:A:D) study were followed up from March, 1999, until death, loss to follow-up, or Feb 1, 2011, whichever occurred first. The D:A:D study is a collaboration of 11 cohort studies following HIV-1-positive individuals receiving care at 212 clinics in Europe, USA, and Australia. All fatal events were centrally validated at the D:A:D coordinating centre using coding causes of death in HIV (CoDe) methodology. We calculated relative rates using Poisson regression. FINDINGS: 3909 of the 49,731 D:A:D study participants died during the 308,719 person-years of follow-up (crude incidence mortality rate, 12.7 per 1000 person-years [95% CI 12.3-13.1]). Leading underlying causes were: AIDS-related (1123 [29%] deaths), non-AIDS-defining cancers (590 [15%] deaths), liver disease (515 [13%] deaths), and cardiovascular disease (436 [11%] deaths). Rates of all-cause death per 1000 person-years decreased from 17.5 in 1999-2000 to 9.1 in 2009-11; we saw similar decreases in death rates per 1000 person-years over the same period for AIDS-related deaths (5.9 to 2.0), deaths from liver disease (2.7 to 0.9), and cardiovascular disease deaths (1.8 to 0.9). However, non-AIDS cancers increased slightly from 1.6 per 1000 person-years in 1999-2000 to 2.1 in 2009-11 (p=0.58). After adjustment for factors that changed over time, including CD4 cell count, we detected no decreases in AIDS-related death rates (relative rate for 2009-11 vs 1999-2000: 0.92 [0.70-1.22]). However, all-cause (0.72 [0.61-0.83]), liver disease (0.48 [0.32

Published
2014

29. A survey of ATRIPLA use in clinical practice as first-line therapy in HIV-positive persons in Europe

Author

Mocroft, A., Reiss, P., Rakhmanova, A., Banhegyi, D., Phillips, A.N., Wit, S. de, Ristola, M., Lundgren, J.D., Grarup, J., Kirk, O., Burger, D.M., et al., Mocroft, A., Reiss, P., Rakhmanova, A., Banhegyi, D., Phillips, A.N., Wit, S. de, Ristola, M., Lundgren, J.D., Grarup, J., Kirk, O., Burger, D.M., and et al.

Abstract

Item does not contain fulltext, ATRIPLA is licensed for use only in HIV-positive persons whose viral loads <50 for >/= 3 months. We investigated the use of ATRIPLA as first-line antiretroviral therapy (ART) in EuroSIDA using a web-based survey performed in Autumn 2012. 96/112 clinics (85.7 %) completed the survey. Recommendations when initiating first-line ART was TRUVADA plus efavirenz in 36 (37.5 %), ATRIPLA in 35 (36.5 %), a different first-line regimen in 12 clinics (12.5 %), and no recommendation in 7 clinics (7.3 %). ATRIPLA was commonest in Northern (15/21 clinics; 71.4 %), and least common in Eastern Europe (2/31 clinics; 6.5 %; p < 0.0001). Over one-third of the participating clinics in this survey were using ATRIPLA as first-line antiretroviral therapy, despite EMA recommendations.

Published
2014

30. Factors associated with D-Dimer levels in HIV-Infected individuals

Author

Apetrei, C., Borges, Á.H., O’Connor, J.L., Phillips, A.N., Baker, J.V., Vjecha, M.J., Losso, M.H., Klinker, H., Lopardo, G., Williams, I., Lundgren, J.D., John, M., Apetrei, C., Borges, Á.H., O’Connor, J.L., Phillips, A.N., Baker, J.V., Vjecha, M.J., Losso, M.H., Klinker, H., Lopardo, G., Williams, I., Lundgren, J.D., and John, M.

Abstract

Background Higher plasma D-dimer levels are strong predictors of mortality in HIV+ individuals. The factors associated with D-dimer levels during HIV infection, however, remain poorly understood. Methods In this cross-sectional study, participants in three randomized controlled trials with measured D-dimer levels were included (N = 9,848). Factors associated with D-dimer were identified by linear regression. Covariates investigated were: age, gender, race, body mass index, nadir and baseline CD4+ count, plasma HIV RNA levels, markers of inflammation (C-reactive protein [CRP], interleukin-6 [IL-6]), antiretroviral therapy (ART) use, ART regimens, co-morbidities (hepatitis B/C, diabetes mellitus, prior cardiovascular disease), smoking, renal function (estimated glomerular filtration rate [eGFR] and cystatin C) and cholesterol. Results Women from all age groups had higher D-dimer levels than men, though a steeper increase of D-dimer with age occurred in men. Hepatitis B/C co-infection was the only co-morbidity associated with higher D-dimer levels. In this subgroup, the degree of hepatic fibrosis, as demonstrated by higher hyaluronic acid levels, but not viral load of hepatitis viruses, was positively correlated with D-dimer. Other factors independently associated with higher D-dimer levels were black race, higher plasma HIV RNA levels, being off ART at baseline, and increased levels of CRP, IL-6 and cystatin C. In contrast, higher baseline CD4+ counts and higher high-density lipoprotein cholesterol were negatively correlated with D-dimer levels. Conclusions D-dimer levels increase with age in HIV+ men, but are already elevated in women at an early age due to reasons other than a higher burden of concomitant diseases. In hepatitis B/C co-infected individuals, hepatic fibrosis, but not hepatitis viral load, was associated with higher D-dimer levels.

Published
2014

31. Continued indinavir versus switching to indinavir/ritonavir in HIV-infected patients with suppressed viral load

Author

Arnaiz, J.A., Mallolas, J., Podzamczer, D., Gerstoft, J., Lundgren, J.D., Cahn, P., Fatkenheuer, G., D'Arminio-Monforte, A., Casiro, A., Reiss, P., Burger, D.M., Stek, M., Gatell, J.M., BEST Study Team, Global Health, and Infectious diseases

Subjects
Adult, Male, medicine.medical_specialty, Settore MED/17 - Malattie Infettive, Combination therapy, medicine.medical_treatment, Immunology, HIV Infections, Indinavir, Gastroenterology, Antiretroviral Therapy, Highly Active, Internal medicine, medicine, Humans, Immunology and Allergy, Sida, Aged, Chemotherapy, Ritonavir, biology, business.industry, HIV Protease Inhibitors, Antiretroviral therapy, Clinical trials, Protease inhibitors, Middle Aged, Viral Load, biology.organism_classification, CD4 Lymphocyte Count, Surgery, Regimen, Treatment Outcome, Infectious Diseases, HIV-1, RNA, Viral, Drug Therapy, Combination, Female, Microbial pathogenesis and host defense [UMCN 4.1], Indinavir+Ritonavir, business, Viral load, medicine.drug
Abstract

Objective: To compare continued indinavir (IDV) 8-hourly (q8h) with switching to indinavir/ritonavir (IDV/RTV) 12-hourly (q12h) in HIV-positive patients having suppressed viral load with IDV q8h plus two nucleoside reverse transcriptase inhibitors (NRTI). Design: Multicentre, international, randomized, open-label study enrolling HIV-1 infected patients on IDV 800 mg q8h plus two NRTI with CD4 cell counts greater than or equal to 100 X 10(6)/l and plasma HIV RNA

Published
2003

32. CD4 cell count and viral load-specific rates of AIDS, non-AIDS and deaths according to current antiretroviral use

Author

Mocroft, A., Phillips, A.N., Gatell, J., Horban, A., Ledergerber, B., Zilmer, K., Jevtovic, D., Maltez, F., Podlekareva, D., Lundgren, J.D., Burger, D.M., et al., Mocroft, A., Phillips, A.N., Gatell, J., Horban, A., Ledergerber, B., Zilmer, K., Jevtovic, D., Maltez, F., Podlekareva, D., Lundgren, J.D., Burger, D.M., and et al.

Abstract

Item does not contain fulltext, BACKGROUND: CD4 cell count and viral loads are used in clinical trials as surrogate endpoints for assessing efficacy of newly available antiretrovirals. If antiretrovirals act through other pathways or increase the risk of disease this would not be identified prior to licensing. The aim of this study was to investigate the CD4 cell count and viral load-specific rates of fatal and nonfatal AIDS and non-AIDS events according to current antiretrovirals. METHODS: Poisson regression was used to compare overall events (fatal or nonfatal AIDS, non-AIDS or death), AIDS events (fatal and nonfatal) or non-AIDS events (fatal or nonfatal) for specific nucleoside pairs and third drugs used with more than 1000 person-years of follow-up (PYFU) after 1 January 2001. RESULTS: Nine thousand, eight hundred and one patients contributed 42372.5 PYFU, during which 1203 (437 AIDS and 766 non-AIDS) events occurred. After adjustment, there was weak evidence of a difference in the overall events rates between nucleoside pairs (global P-value = 0.084), and third drugs (global P-value = 0.031). As compared to zidovudine/lamivudine, patients taking abacavir/lamivudine [adjusted incidence rate ratio (aIRR) 1.22; 95% CI 0.99-1.49] and abacavir and one other nucleoside [aIRR 1.51; 95% CI 1.14-2.02] had an increased incidence of overall events. Comparing the third drugs, those taking unboosted atazanavir had an increased incidence of overall events compared with those taking efavirenz (aIRR 1.46; 95% CI 1.09-1.95). CONCLUSION: There was little evidence of substantial differences between antiretrovirals in the incidence of clinical disease for a given CD4 cell count or viral load, suggesting there are unlikely to be major unidentified adverse effects of specific antiretrovirals.

Published
2013

33. Association between antiretroviral exposure and renal impairment among HIV-positive persons with normal baseline renal function: the D:A:D study.

Author

Ryom, L., Mocroft, A., Kirk, O., Worm, S.W., Kamara, D.A., Reiss, P., Ross, M., Fux, C.A., Morlat, P., Moranne, O., Smith, C., Lundgren, J.D., Koopmans, P.P., Groot, R. de, Keuter, M., Ven, A.J.A.M. van der, Hofstede, H.J.M. ter, Flier, M. van der, Brouwer, A.M., Dofferhoff, A.S.M., et al., Koopmans †, P.P., Ryom, L., Mocroft, A., Kirk, O., Worm, S.W., Kamara, D.A., Reiss, P., Ross, M., Fux, C.A., Morlat, P., Moranne, O., Smith, C., Lundgren, J.D., Koopmans, P.P., Groot, R. de, Keuter, M., Ven, A.J.A.M. van der, Hofstede, H.J.M. ter, Flier, M. van der, Brouwer, A.M., Dofferhoff, A.S.M., et al., and Koopmans †, P.P.

Abstract

Contains fulltext : 125257.pdf (publisher's version ) (Closed access), BACKGROUND: Several antiretroviral agents (ARVs) are associated with chronic renal impairment, but the extent of such adverse events among human immunodeficiency virus (HIV)-positive persons with initially normal renal function is unknown. METHODS: D:A:D study participants with an estimated glomerular filtration rate (eGFR) of >/= 90 mL/min after 1 January 2004 were followed until they had a confirmed eGFR of /= 3 months apart. Predictors and eGFR-related ARV discontinuations were identified using Poisson regression. RESULTS: Of 22 603 persons, 468 (2.1%) experienced a confirmed eGFR of /= 90 mL/min. Cumulative tenofovir use (aIRR, 1.18/year [95% CI, 1.12-1.25]) and ritonavir-boosted atazanavir use (aIRR, 1.19/year [95% CI, 1.09-1.32]) were independent predictors of a confirmed eGFR of

Published
2013

34. Non-AIDS defining cancers in the D:A:D Study - time trends and predictors of survival: A cohort study

Author

Worm, S.W., Bower, M., Reiss, P., Bonnet, F., Law, M., Fätkenheuer, G., d’Arminio Monforte, A., Abrams, D.I., Grulich, A., Fontas, E., Kirk, O., Furrer, H., De Wit, S., Phillips, A., Lundgren, J.D., Sabin, C.A., Nolan, D., Worm, S.W., Bower, M., Reiss, P., Bonnet, F., Law, M., Fätkenheuer, G., d’Arminio Monforte, A., Abrams, D.I., Grulich, A., Fontas, E., Kirk, O., Furrer, H., De Wit, S., Phillips, A., Lundgren, J.D., Sabin, C.A., and Nolan, D.

Abstract

Background Non-AIDS defining cancers (NADC) are an important cause of morbidity and mortality in HIV-positive individuals. Using data from a large international cohort of HIV-positive individuals, we described the incidence of NADC from 2004–2010, and described subsequent mortality and predictors of these. Methods Individuals were followed from 1st January 2004/enrolment in study, until the earliest of a new NADC, 1st February 2010, death or six months after the patient’s last visit. Incidence rates were estimated for each year of follow-up, overall and stratified by gender, age and mode of HIV acquisition. Cumulative risk of mortality following NADC diagnosis was summarised using Kaplan-Meier methods, with follow-up for these analyses from the date of NADC diagnosis until the patient’s death, 1st February 2010 or 6 months after the patient’s last visit. Factors associated with mortality following NADC diagnosis were identified using multivariable Cox proportional hazards regression. Results Over 176,775 person-years (PY), 880 (2.1%) patients developed a new NADC (incidence: 4.98/1000PY [95% confidence interval 4.65, 5.31]). Over a third of these patients (327, 37.2%) had died by 1st February 2010. Time trends for lung cancer, anal cancer and Hodgkin’s lymphoma were broadly consistent. Kaplan-Meier cumulative mortality estimates at 1, 3 and 5 years after NADC diagnosis were 28.2% [95% CI 25.1-31.2], 42.0% [38.2-45.8] and 47.3% [42.4-52.2], respectively. Significant predictors of poorer survival after diagnosis of NADC were lung cancer (compared to other cancer types), male gender, non-white ethnicity, and smoking status. Later year of diagnosis and higher CD4 count at NADC diagnosis were associated with improved survival. The incidence of NADC remained stable over the period 2004–2010 in this large observational cohort. Conclusions The prognosis after diagnosis of NADC, in particular lung cancer and disseminated cancer, is poor but has improved somewhat over time. M

Published
2013

35. The natural history of HIV infection

Author

Sabin, C.A., Lundgren, J.D., Sabin, C.A., and Lundgren, J.D.

Abstract

PURPOSE OF REVIEW: To review recent published literature around three areas: long-term nonprogression/viral control; predictors of viral load set point/disease progression; and the potential impact of antiretroviral therapy (ART) in early HIV infection. RECENT FINDINGS: The natural course of untreated HIV infection varies widely with some HIV-positive individuals able to maintain high CD4 cell counts and/or suppressed viral load in the absence of ART. Although similar, the underlying mechanistic processes leading to long-term nonprogression and viral control are likely to differ. Concerted ongoing research efforts will hopefully identify host factors that are causally related to these phenotypes, thus providing opportunities for the development of novel treatment or preventive strategies. Although there is increasing evidence that initiation of ART during primary infection may prevent the immunological deterioration which would otherwise be seen in untreated HIV infection, recent studies do not address the longer term clinical benefits of ART at this very early stage. SUMMARY: A better understanding of the relative influences of viral, host, and environmental factors on the natural course of HIV infection has the potential to identify novel targets for intervention to prevent and treat HIV-infected persons.

Published
2013

36. Feasibility and Effectiveness of Indicator Condition-Guided Testing for HIV:Results from HIDES I (HIV Indicator Diseases across Europe Study)

Author

Sullivan, A.K., Raben, D., Reekie, J., Rayment, M., Mocroft, A., Esser, S., Leon, A., Begovac, J., Brinkman, K., Zangerle, R., Grzeszczuk, A., Vassilenko, A., Hadziosmanovic, V., Krasnov, M., Sönnerborg, A., Clumeck, N., Gatell, J., Gazzard, B., d'Arminio Monforte, A., Rockstroh, J., Lundgren, J.D., Sullivan, A.K., Raben, D., Reekie, J., Rayment, M., Mocroft, A., Esser, S., Leon, A., Begovac, J., Brinkman, K., Zangerle, R., Grzeszczuk, A., Vassilenko, A., Hadziosmanovic, V., Krasnov, M., Sönnerborg, A., Clumeck, N., Gatell, J., Gazzard, B., d'Arminio Monforte, A., Rockstroh, J., and Lundgren, J.D.

Abstract

Improved methods for targeting HIV testing among patients most likely to be infected are required; HIDES I aimed to define the methodology of a European wide study of HIV prevalence in individuals presenting with one of eight indicator conditions/diseases (ID); sexually transmitted infection, lymphoma, cervical or anal cancer/dysplasia, herpes zoster, hepatitis B/C, mononucleosis-like illness, unexplained leukocytopenia/thrombocytopenia and seborrheic dermatitis/exanthema, and to identify those with an HIV prevalence of >0.1%, a level determined to be cost effective. A staff questionnaire was performed. From October 2009- February 2011, individuals, not known to be HIV positive, presenting with one of the ID were offered an HIV test; additional information was collected on previous HIV testing behaviour and recent medical history. A total of 3588 individuals from 16 centres were included. Sixty-six tested positive for HIV, giving an HIV prevalence of 1.8% [95% CI: 1.42-2.34]; all eight ID exceeded 0.1% prevalence. Of those testing HIV positive, 83% were male, 58% identified as MSM and 9% were injecting drug users. Twenty percent reported previously having potentially HIV-related symptoms and 52% had previously tested HIV negative (median time since last test: 1.58 years); which together with the median CD4 count at diagnosis (400 cell/uL) adds weight to this strategy being effective in diagnosing HIV at an earlier stage. A positive test was more likely for non-white individuals, MSM, injecting drug users and those testing in non-Northern regions. HIDES I describes an effective strategy to detect undiagnosed HIV infection. All eight ID fulfilled the >0.1% criterion for cost effectiveness. All individuals presenting to any health care setting with one of these ID should be strongly recommended an HIV test. A strategy is being developed in collaboration with ECDC and WHO Europe to guide the implementation of this novel public health initiative across Europe.

Published
2013

37. Association between antiretroviral exposure and renal impairment among HIV-positive persons with normal baseline renal function:The D:A:D Study

Author

Nielsen, Lene Ryom, Mocroft, A., Kirk, O., Worm, S.W., Kamara, D.A., Reiss, P., Ross, Michael, Fux, C.A., Morlat, P., Moranne, O., Smith, Christian Birch, Lundgren, J.D., Nielsen, Lene Ryom, Mocroft, A., Kirk, O., Worm, S.W., Kamara, D.A., Reiss, P., Ross, Michael, Fux, C.A., Morlat, P., Moranne, O., Smith, Christian Birch, and Lundgren, J.D.

Abstract

Background. Several antiretroviral agents (ARVs) are associated with chronic renal impairment, but the extent of such adverse events among human immunodeficiency virus (HIV)-positive persons with initially normal renal function is unknown.Methods. D:A:D study participants with an estimated glomerular filtration rate (eGFR) of ≥90 mL/min after 1 January 2004 were followed until they had a confirmed eGFR of ≤70 mL/min (the threshold below which we hypothesized that renal interventions may begin to occur) or ≤60 mL/min (a value indicative of moderately severe chronic kidney disease [CKD]) or until the last eGFR measurement during follow-up. An eGFR was considered confirmed if it was detected at 2 consecutive measurements ≥3 months apart. Predictors and eGFR-related ARV discontinuations were identified using Poisson regression.Results. Of 22 603 persons, 468 (2.1%) experienced a confirmed eGFR of ≤70 mL/min (incidence rate, 4.78 cases/1000 person-years of follow-up [95% confidence interval "CI", 4.35-5.22]) and 131 (0.6%) experienced CKD (incidence rate, 1.33 cases/1000 person-years of follow-up [95% CI, 1.10-1.56]) during a median follow-up duration of 4.5 years (interquartile range [IQR], 2.7-6.1 years). A current eGFR of 60-70 mL/min caused significantly higher rates of discontinuation of tenofovir (adjusted incidence rate ratio [aIRR], 1.72 [95% CI, 1.38-2.14]) but not other ARVs compared with a current eGFR of ≥90 mL/min. Cumulative tenofovir use (aIRR, 1.18/year [95% CI, 1.12-1.25]) and ritonavir-boosted atazanavir use (aIRR, 1.19/year [95% CI, 1.09-1.32]) were independent predictors of a confirmed eGFR of ≤70 but were not significant predictors of CKD whereas ritonavir-boosted lopinavir use was a significant predictor for both end points (aIRR, 1.11/year [95% CI, 1.05-1.17] and 1.22/year [95% CI, 1.16-1.28], respectively). Associations were unaffected by censoring for concomitant ARV use but diminished after discontinuation of these ARVs.Conclusions. Tenofovir, r

Published
2013

38. Regional differences in AIDS and non-AIDS related mortality in HIV-positive individuals across Europe and Argentina: the EuroSIDA study

Author

Reekie, J., Kowalska, J.D., Karpov, I., Rockstroh, J., Karlsson, A., Rakhmanova, A., Horban, A., Kirk, O., Lundgren, J.D., Mocroft, A., Burger, D.M., et al., Reekie, J., Kowalska, J.D., Karpov, I., Rockstroh, J., Karlsson, A., Rakhmanova, A., Horban, A., Kirk, O., Lundgren, J.D., Mocroft, A., Burger, D.M., and et al.

Abstract

Contains fulltext : 109329.pdf (publisher's version ) (Open Access), BACKGROUND: Differences in access to care and treatment have been reported in Eastern Europe, a region with one of the fastest growing HIV epidemics, compared to the rest of Europe. This analysis aimed to establish whether there are regional differences in the mortality rate of HIV-positive individuals across Europe, and Argentina. METHODS: 13,310 individuals under follow-up were included in the analysis. Poisson regression investigated factors associated with the risk of death. FINDINGS: During 82,212 person years of follow-up (PYFU) 1,147 individuals died (mortality rate 14.0 per 1,000 PYFU (95% confidence interval [CI] 13.1-14.8). Significant differences between regions were seen in the rate of all-cause, AIDS and non-AIDS related mortality (global p<0.0001 for all three endpoints). Compared to South Europe, after adjusting for baseline demographics, laboratory measurements and treatment, a higher rate of AIDS related mortality was observed in East Europe (IRR 2.90, 95%CI 1.97-4.28, p<.0001), and a higher rate of non-AIDS related mortality in North Europe (IRR 1.51, 95%CI 1.24-1.82, p<.0001). The differences observed in North Europe decreased over calendar-time, in 2009-2011, the higher rate of non-AIDS related mortality was no longer significantly different to South Europe (IRR 1.07, 95%CI 0.66-1.75, p = 0.77). However, in 2009-2011, there remained a higher rate of AIDS-related mortality (IRR 2.41, 95%CI 1.11-5.25, p = 0.02) in East Europe compared to South Europe in adjusted analysis. INTERPRETATIONS: There are significant differences in the rate of all-cause mortality among HIV-positive individuals across different regions of Europe and Argentina. Individuals in Eastern Europe had an increased risk of mortality from AIDS related causes and individuals in North Europe had the highest rate of non-AIDS related mortality. These findings are important for understanding and reviewing HIV treatment strategies and policies across the European region.

Published
2012

39. Predicting the risk of cardiovascular disease in HIV-infected patients: The Data collection on Adverse Effects of Anti-HIV Drugs Study

Author

Friis-Møller, N., Thiébaut, R., Reiss, P., Weber, R., Monforte, A.D., De Wit, S., El-Sadr, W., Fontas, E., Worm, S., Kirk, O., Phillips, A., Sabin, C.A., Lundgren, J.D., Law, M.G., Mallal, S., Nolan, D., Friis-Møller, N., Thiébaut, R., Reiss, P., Weber, R., Monforte, A.D., De Wit, S., El-Sadr, W., Fontas, E., Worm, S., Kirk, O., Phillips, A., Sabin, C.A., Lundgren, J.D., Law, M.G., Mallal, S., and Nolan, D.

Abstract

Aims: HIV-infected patients receiving combination antiretroviral therapy may experience metabolic complications, potentially increasing their risk of cardiovascular diseases (CVDs). Furthermore, exposures to some antiretroviral drugs seem to be independently associated with increased CVD risk. We aimed to develop cardiovascular risk-assessment models tailored to HIV-infected patients. Methods and results: Prospective multinational cohort study. The data set included 22 625 HIV-infected patients from 20 countries in Europe and Australia who were free of CVD at entry into the Data collection on Adverse Effects of Anti-HIV Drugs Study. Using cross-validation methods, separate models were developed to predict the risk of myocardial infarction, coronary heart disease, and a composite CVD endpoint. Model performance was compared with the Framingham score. The models included age, sex, systolic blood pressure, smoking status, family history of CVD, diabetes, total cholesterol, HDL cholesterol and indinavir, lopinavir/r and abacavir exposure. The models performed well with area under the receiver operator curve statistics of 0.783 (range 0.642–0.820) for myocardial infarction, 0.776 (0.670–0.818) for coronary heart disease and 0.769 (0.695–0.824) for CVD. The models estimated more accurately the outcomes in the subgroups than the Framingham score. Conclusion: Risk equations developed from a population of HIV-infected patients, incorporating routinely collected cardiovascular risk parameters and exposure to individual antiretroviral therapy drugs, might be more useful in estimating CVD risks in HIV-infected persons than conventional risk prediction models.

Published
2010

40. Risk factors for treatment-limiting toxicities in patients starting nevirapine-containing antiretroviral therapy.

Author

Kesselring, A.M., Wit, F.W., Sabin, C.A., Lundgren, J.D., Gill, M.J., Gatell, J.M., Rauch, A., Montaner, J.S., Wolf, F. de, Reiss, P., Mocroft, A., Ven, A.J.A.M. van der, Gyssens, I.C.J., et al., Kesselring, A.M., Wit, F.W., Sabin, C.A., Lundgren, J.D., Gill, M.J., Gatell, J.M., Rauch, A., Montaner, J.S., Wolf, F. de, Reiss, P., Mocroft, A., Ven, A.J.A.M. van der, Gyssens, I.C.J., and et al.

Abstract

Contains fulltext : 81637.pdf (publisher's version ) (Closed access), BACKGROUND: This collaboration of seven observational clinical cohorts investigated risk factors for treatment-limiting toxicities in both antiretroviral-naive and experienced patients starting nevirapine-based combination antiretroviral therapy (NVPc). METHODS: Patients starting NVPc after 1 January 1998 were included. CD4 cell count at starting NVPc was classified as high (>400/microl/>250/microl for men/women, respectively) or low. Cox models were used to investigate risk factors for discontinuations due to hypersensitivity reactions (HSR, n = 6547) and discontinuation of NVPc due to treatment-limiting toxicities and/or patient/physician choice (TOXPC, n = 10,186). Patients were classified according to prior antiretroviral treatment experience and CD4 cell count/viral load at start NVPc. Models were stratified by cohort and adjusted for age, sex, nadir CD4 cell count, calendar year of starting NVPc and mode of transmission. RESULTS: Median time from starting NVPc to TOXPC and HSR were 162 days [interquartile range (IQR) 31-737] and 30 days (IQR 17-60), respectively. In adjusted Cox analyses, compared to naive patients with a low CD4 cell count, treatment-experienced patients with high CD4 cell count and viral load more than 400 had a significantly increased risk for HSR [hazard ratio 1.45, confidence interval (CI) 1.03-2.03] and TOXPC within 18 weeks (hazard ratio 1.34, CI 1.08-1.67). In contrast, treatment-experienced patients with high CD4 cell count and viral load less than 400 had no increased risk for HSR 1.10 (0.82-1.46) or TOXPC within 18 weeks (hazard ratio 0.94, CI 0.78-1.13). CONCLUSION: Our results suggest it may be relatively well tolerated to initiate NVPc in antiretroviral-experienced patients with high CD4 cell counts provided there is no detectable viremia.

Published
2009

41. Absence of a relation between efavirenz plasma concentrations and toxicity-driven efavirenz discontinuations in the EuroSIDA study.

Author

Luin, M. van, Bannister, W.P., Mocroft, A., Reiss, P., Perri, G. Di, Peytavin, G., Molto, J., Karlson, A., Castagna, A., Beniowski, M., Lundgren, J.D., Burger, D.M., Luin, M. van, Bannister, W.P., Mocroft, A., Reiss, P., Perri, G. Di, Peytavin, G., Molto, J., Karlson, A., Castagna, A., Beniowski, M., Lundgren, J.D., and Burger, D.M.

Abstract

Contains fulltext : 79598.pdf (publisher's version ) (Closed access), BACKGROUND: Co1nflicting data exist regarding the effect of efavirenz (EFV) plasma concentrations on central nervous system (CNS) toxicity. We aimed to determine whether patients with high EFV plasma concentrations have an increased likelihood of toxicity-driven EFV discontinuations. METHODS: EFV plasma concentrations were measured from patients in the EuroSIDA study starting EFV after 1 January 1999. Patients with a plasma concentration available were divided into those that discontinued EFV because of any toxicity or by the choice of the patient or physician within 2 years (TOXPC group) and those that continued EFV for > or = 2 years (no toxicity group). Multivariable logistic regression modelling was used to investigate the effects of the EFV plasma concentration and those of other potentially relevant factors on the risk of toxicity-induced EFV discontinuations. RESULTS: A total of 843 patients were included. Of these patients, 138 patients (16.4%) discontinued EFV because of TOXPC and 705 (83.6%) patients continued EFV for 22 years. A total of 20 (14.5%) patients in the TOXPC group had high EFV plasma concentrations (>4.0 mg/l) compared with 99 (14.0%) patients in the no toxicity group (P = 0.890). A positive hepatitis C status (P = 0.026), but not the EFV plasma concentration, was an independent predictor of toxicity-driven EFV discontinuations. CONCLUSIONS: No association was found between EFV plasma concentrations and the risk of EFV discontinuations because of (CNS) toxicity. This result questions the designation of EFV plasma concentrations >4.0 mg/l as being 'toxic', at least when defined by treatment discontinuation.

Published
2009

42. [Risk of virus transmission from well-treated patients with HIV?]

Author

Gerstoft, J., Mathiesen, L., Lundgren, J.D., Nielsen, H.I., Pedersen, C., Obel, N., Laursen, A., Gerstoft, J., Mathiesen, L., Lundgren, J.D., Nielsen, H.I., Pedersen, C., Obel, N., and Laursen, A.

Abstract

Udgivelsesdato: 2009/3/23

Published
2009

43. [Major breakthroughs in the medical treatment]

Author

Kirk, O., Gerstoft, J., Lundgren, J.D., Obel, N., Kirk, O., Gerstoft, J., Lundgren, J.D., and Obel, N.

Abstract

The introduction of antiretroviral combination therapy for patients with HIV infection is described as an example of a breakthrough within the field of medical treatment. The background for the breakthrough and the phases thereof are described and for comparison, the circumstances of major breakthroughs within other medical specialities are mentioned Udgivelsesdato: 2009/3/2

Published
2009

44. Use of nucleoside reverse transcriptase inhibitors and risk of myocardial infarction in HIV-infected patients enrolled in the D:A:D study: a multi-cohort collaboration.

Author

Sabin, C.A., Worm, S.W., Weber, R., Reiss, P., El-Sadr, W., Dabis, F., Wit, S. de, Law, M., d'Arminio Montforte, A., Friis-Moller, N., Kirk, O., Pradier, C., Weller, I., Phillips, A.N., Lundgren, J.D., Gyssens, I.C.J., et al., Sabin, C.A., Worm, S.W., Weber, R., Reiss, P., El-Sadr, W., Dabis, F., Wit, S. de, Law, M., d'Arminio Montforte, A., Friis-Moller, N., Kirk, O., Pradier, C., Weller, I., Phillips, A.N., Lundgren, J.D., Gyssens, I.C.J., and et al.

Abstract

Item does not contain fulltext

Published
2008

45. HIV-induced immunodeficiency and mortality from AIDS-defining and non-AIDS-defining malignancies.

Author

Montforte, A., Abrams, D., Pradier, C., Weber, R., Reiss, P., Bonnet, F., Kirk, O., Law, M., Wit, S. de, Friis-Moller, N., Phillips, A.N., Sabin, C.A., Lundgren, J.D., Gyssens, I.C.J., et al., Montforte, A., Abrams, D., Pradier, C., Weber, R., Reiss, P., Bonnet, F., Kirk, O., Law, M., Wit, S. de, Friis-Moller, N., Phillips, A.N., Sabin, C.A., Lundgren, J.D., Gyssens, I.C.J., and et al.

Abstract

Item does not contain fulltext

Published
2008

46. Changes over time in risk factors for cardiovascular disease and use of lipid-lowering drugs in HIV-infected individuals and impact on myocardial infarction.

Author

Sabin, C.A., d'Arminio Montforte, A., Friis-Moller, N., Weber, R., El-Sadr, W., Reiss, P., Kirk, O., Mercie, P., Law, M.G., Wit, S. de, Pradier, C., Phillips, A.N., Lundgren, J.D., Sabin, C.A., d'Arminio Montforte, A., Friis-Moller, N., Weber, R., El-Sadr, W., Reiss, P., Kirk, O., Mercie, P., Law, M.G., Wit, S. de, Pradier, C., Phillips, A.N., and Lundgren, J.D.

Abstract

Item does not contain fulltext

Published
2008

47. Impact of bacteremia on the pathogenesis of experimental pneumococcal meningitis:Journal of Infectious Diseases

Author

Brandt, C.T., Holm, D., Liptrot, Matthew George, Østergaard, C., Lundgren, J.D., Frimodt-Møller, N., Skovsted, I.C., Rowland, I.J., Brandt, C.T., Holm, D., Liptrot, Matthew George, Østergaard, C., Lundgren, J.D., Frimodt-Møller, N., Skovsted, I.C., and Rowland, I.J.

Abstract

Background. Bacteremia plays a major role in the outcome of pneumococcal meningitis. This experimental study investigated how bacteremia influences the pathophysiologic profile of the brain. Methods. Rats with Streptococcus pneumoniae meningitis were randomized to 1 of 3 groups of infected study rats: (1) rats with attenuated bacteremia resulting from intravenous injection of serotype-specific pneumococcal antibody, (2) rats with early-onset bacteremia resulting from concomitant intravenous infection, or (3) a meningitis control group. The blood-brain barrier (BBB) breakdown, ventricle size, brain water distribution, and brain pathologic findings were analyzed using magnetic resonance morphological and functional imaging. Laboratory data and clinical disease scores were obtained. Results. Attenuation of the bacteremic component of pneumococcal meningitis improved clinical disease symptoms and significantly reduced ventricle expansion and BBB breakdown (P <.05). Early-onset bacteremia did not further increase ventricle size or BBB leakage. Significantly increased brain edema developed among rats with both attenuated and early-onset bacteremia (P <.05). Focal brain pathologic findings were unaffected by bacteremia and were found to be associated with cerebrospinal fluid inflammation. Conclusion. Although brain lesions appear to result from local meningeal infection, systemic infection significantly contributes to clinical disease presentation and the pathophysiology of BBB breakdown and ventricle expansion. The different end points affected by the systemic and local infectious processes should be addressed in future studies. © 2008 by the Infectious Diseases Society of America. All rights reserved.

Published
2008

48. Risk of discontinuation of nevirapine due to toxicities in antiretroviral-naive and -experienced HIV-infected patients with high and low CD4(+) T-cell counts (vol 12, pg 325, 2007)

Author

Mocroft, A., Staszewski, S., Weber, R., Gatell, J., Rockstroh, J., Gasiorowski, J., Panos, G., Monforte, A.D., Rakhmanova, A., Phillips, A.N., Lundgren, J.D., Mocroft, A., Staszewski, S., Weber, R., Gatell, J., Rockstroh, J., Gasiorowski, J., Panos, G., Monforte, A.D., Rakhmanova, A., Phillips, A.N., and Lundgren, J.D.

Abstract

Udgivelsesdato: 2007

Published
2007

49. Normalisation of CD4 counts in patients with HIV-1 infection and maximum virological suppression who are taking combination antiretroviral therapy: an observational cohort study

Author

Mocroft, A., Phillips, A., Gatell, J., Ledergerber, B., Fisher, M., Clumeck, N., Losso, M., Lazzarin, A., Fatkenheuer, G., Lundgren, J.D., Mocroft, A., Phillips, A., Gatell, J., Ledergerber, B., Fisher, M., Clumeck, N., Losso, M., Lazzarin, A., Fatkenheuer, G., and Lundgren, J.D.

Abstract

Udgivelsesdato: Aug 4

Published
2007

50. Predictors of CD4 count change over 8 months of follow up in HIV-1-infected patients with a CD4 count >= 300 cells/mu L who were assigned to 7.5 MIU interleukin

Author

Fox, Z., Antunes, F., Davey, R., Gazzard, B., Klimas, N., Labriola, A., Losso, M., Neaton, J.D., Phillips, A.N., Ruxrungtham, K., Staszewski, S., Weiss, L., Lundgren, J.D., Abrams, D.I., Cooper, D.A., Darbyshire, J.H., Duncan, W.R., Emery, S., Lane, H.C., Lehrman, S., Aguilar, L., Angel, E.B., Aquilia, S., Belloso, W., Benetucci, J., Bittar, V., Cahn, P., Casiro, A., Contarelli, J., Corral, J., Daciuk, L., David, D., Ferrari, I., Fridman, D., Galache, V., Guaragna, G., Ivalo, S., Laplume, H., Lanusse, I., Lasala, M.B., Lattes, R., Lasovsky, J., Lopardo, G., Lourtau, L., Lupo, S., Maranzana, A., Marson, C., Massera, L., Sanchez, M.D., Somenzini, C., Tocci, M., Algar, S., Anderson, J., Baker, D., Blavius, K., Bloch, M., Boyle, M., Bradford, D., Britton, P., Carrall, L., Carr, A., Chuah, J., Curry, M., D'Arcy-Evans, C., Dobson, P., Doong, N., Egan, C., Ferguson, W., Finlayson, R., French, M., Frater, A., Gold, J., Habel, P., Haig, K., Holland, R., Hyland, N., Hoy, J., Hudson, J., James, R., Leung, J., Lowe, K., MacRae, K., McMurchie, M., Medland, N., Miller, S., Murray, J., Newman, R., Orth, D., Patching, J., Primrose, R., Ree, H., Richardson, R., Rogers, G., Roney, J., Roth, N., Sarangapany, J., Shaw, D., Silberberg, C., Skett, J., Williams, L., Soo, T.M., Sowden, D., Street, A., Vale, R., Villella, C., Walker, A., Watson, A., Wendt, N., Wood, H., Youds, D., Aichelburg, A., Rieger, A., Vetter, N., Clumeck, N., Wit, S. De, Kabeya, K., O'Doherty, E., Amorim, C.D., Basso, C.R., Lewi, D.S., Pereira, L.C., Silva, M. da, Souza, T.N.L., Angel, J., Bouchard, P.R., Clark, F., Cohen, J., Dambreville, M., Ellis, M., Fiset, S., Foster, A., Fraser, C., Gagnon, S., Gilmour, J., Guenette, R., Haldane, H., Hawley-Foss, N., Hyndman, S., Johnston, L., Jubinville, N., Juneau, F., Kelleher, L., LaPointe, L., Latendre-Paquette, J., Lindemulder, A., Mashinter, L., Lefebvre, E., McFarland, N., Morisseau, C., O'Neill, R., Piche, A., Ralph, E., Rouleau, D., Routy, J.P., Sandre, R., Schmidt, S., Shafran, S., Smaill, F., Stromberg, D., Trepanier, J.M., Trottier, S., Veal, S., Walmsley, S., Weiss, K., Williams, K., Young, M., Zaleschuk, B., Zarowny, D., Baadegaard, B., Black, F., Boedker, K., Gerstoft, J., Jensen, L., Mathiesen, L., Nielsen, H., Pedersen, C., Petersen, D., Aboulker, J.P., Baakili, A., Bengrait, N., Bensalem, M., Berthe, H., Bloche, M., Bazin, C., Boue, F., Bouvet, E., Brancon, C., Capitant, C., Ceppi, C., Cheneau, C., Coutellier, A., Chennebault, J.M., Coquet, F., Truchis, P. De, Delavalle, A.M., Frixon-Marin, V., Gastaut, J.A., Delfraissy, F., Eliaszeicz, M., Gallais, H., Gataut, J.A., Gilquin, J., Gonzalez-Canali, G., Gaudebout, C., Goujard, C., Hoen, B., Honore, P., Jarousse, B., Lang, J.M., Lefebvre, B., Levy, Y., Loison, J., Maignan, A., Meynard, J.L., Michon, C., Mole, M., Marsal, L., Matheron, S., Mortier, E., Oksenhendler, E., Poirier, S., Picard-Dahan, C., Ravaux, I., Raffi, F., Raguin, G., Reynes, J., Rozenbaum, W., Salmon, D., Simon, A., Spiridon, G., Viard, J.P., Vidal, M., Zucman, D., Bergmann, F., Brockmeyer, N., Faetkenheuer, G., Fenske, S., Gey, D., Goebel, F.D., Goetsch, M., Hartmann, M., Klinker, H., Kremer, G., Mantzsch, K., Mauss, S., Rockstroh, J., Rotty, J., Rund, E., Schneider, K., Fox, Z., Antunes, F., Davey, R., Gazzard, B., Klimas, N., Labriola, A., Losso, M., Neaton, J.D., Phillips, A.N., Ruxrungtham, K., Staszewski, S., Weiss, L., Lundgren, J.D., Abrams, D.I., Cooper, D.A., Darbyshire, J.H., Duncan, W.R., Emery, S., Lane, H.C., Lehrman, S., Aguilar, L., Angel, E.B., Aquilia, S., Belloso, W., Benetucci, J., Bittar, V., Cahn, P., Casiro, A., Contarelli, J., Corral, J., Daciuk, L., David, D., Ferrari, I., Fridman, D., Galache, V., Guaragna, G., Ivalo, S., Laplume, H., Lanusse, I., Lasala, M.B., Lattes, R., Lasovsky, J., Lopardo, G., Lourtau, L., Lupo, S., Maranzana, A., Marson, C., Massera, L., Sanchez, M.D., Somenzini, C., Tocci, M., Algar, S., Anderson, J., Baker, D., Blavius, K., Bloch, M., Boyle, M., Bradford, D., Britton, P., Carrall, L., Carr, A., Chuah, J., Curry, M., D'Arcy-Evans, C., Dobson, P., Doong, N., Egan, C., Ferguson, W., Finlayson, R., French, M., Frater, A., Gold, J., Habel, P., Haig, K., Holland, R., Hyland, N., Hoy, J., Hudson, J., James, R., Leung, J., Lowe, K., MacRae, K., McMurchie, M., Medland, N., Miller, S., Murray, J., Newman, R., Orth, D., Patching, J., Primrose, R., Ree, H., Richardson, R., Rogers, G., Roney, J., Roth, N., Sarangapany, J., Shaw, D., Silberberg, C., Skett, J., Williams, L., Soo, T.M., Sowden, D., Street, A., Vale, R., Villella, C., Walker, A., Watson, A., Wendt, N., Wood, H., Youds, D., Aichelburg, A., Rieger, A., Vetter, N., Clumeck, N., Wit, S. De, Kabeya, K., O'Doherty, E., Amorim, C.D., Basso, C.R., Lewi, D.S., Pereira, L.C., Silva, M. da, Souza, T.N.L., Angel, J., Bouchard, P.R., Clark, F., Cohen, J., Dambreville, M., Ellis, M., Fiset, S., Foster, A., Fraser, C., Gagnon, S., Gilmour, J., Guenette, R., Haldane, H., Hawley-Foss, N., Hyndman, S., Johnston, L., Jubinville, N., Juneau, F., Kelleher, L., LaPointe, L., Latendre-Paquette, J., Lindemulder, A., Mashinter, L., Lefebvre, E., McFarland, N., Morisseau, C., O'Neill, R., Piche, A., Ralph, E., Rouleau, D., Routy, J.P., Sandre, R., Schmidt, S., Shafran, S., Smaill, F., Stromberg, D., Trepanier, J.M., Trottier, S., Veal, S., Walmsley, S., Weiss, K., Williams, K., Young, M., Zaleschuk, B., Zarowny, D., Baadegaard, B., Black, F., Boedker, K., Gerstoft, J., Jensen, L., Mathiesen, L., Nielsen, H., Pedersen, C., Petersen, D., Aboulker, J.P., Baakili, A., Bengrait, N., Bensalem, M., Berthe, H., Bloche, M., Bazin, C., Boue, F., Bouvet, E., Brancon, C., Capitant, C., Ceppi, C., Cheneau, C., Coutellier, A., Chennebault, J.M., Coquet, F., Truchis, P. De, Delavalle, A.M., Frixon-Marin, V., Gastaut, J.A., Delfraissy, F., Eliaszeicz, M., Gallais, H., Gataut, J.A., Gilquin, J., Gonzalez-Canali, G., Gaudebout, C., Goujard, C., Hoen, B., Honore, P., Jarousse, B., Lang, J.M., Lefebvre, B., Levy, Y., Loison, J., Maignan, A., Meynard, J.L., Michon, C., Mole, M., Marsal, L., Matheron, S., Mortier, E., Oksenhendler, E., Poirier, S., Picard-Dahan, C., Ravaux, I., Raffi, F., Raguin, G., Reynes, J., Rozenbaum, W., Salmon, D., Simon, A., Spiridon, G., Viard, J.P., Vidal, M., Zucman, D., Bergmann, F., Brockmeyer, N., Faetkenheuer, G., Fenske, S., Gey, D., Goebel, F.D., Goetsch, M., Hartmann, M., Klinker, H., Kremer, G., Mantzsch, K., Mauss, S., Rockstroh, J., Rotty, J., Rund, E., and Schneider, K.

Abstract

Udgivelsesdato: 2007/3

Published
2007

Catalog

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