Your search keyword '"Afonso, Pedro Miranda"' showing total 7 results

1. A joint model for (un)bounded longitudinal markers, competing risks, and recurrent events using patient registry data

Author

Afonso, Pedro Miranda, Rizopoulos, Dimitris, Palipana, Anushka K., Gecili, Emrah, Brokamp, Cole, Clancy, John P., Szczesniak, Rhonda D., and Andrinopoulou, Eleni-Rosalina

Subjects

Statistics - Methodology

Abstract

Joint models for longitudinal and survival data have become a popular framework for studying the association between repeatedly measured biomarkers and clinical events. Nevertheless, addressing complex survival data structures, especially handling both recurrent and competing event times within a single model, remains a challenge. This causes important information to be disregarded. Moreover, existing frameworks rely on a Gaussian distribution for continuous markers, which may be unsuitable for bounded biomarkers, resulting in biased estimates of associations. To address these limitations, we propose a Bayesian shared-parameter joint model that simultaneously accommodates multiple (possibly bounded) longitudinal markers, a recurrent event process, and competing risks. We use the beta distribution to model responses bounded within any interval (a,b) without sacrificing the interpretability of the association. The model offers various forms of association, discontinuous risk intervals, and both gap and calendar timescales. A simulation study shows that it outperforms simpler joint models. We utilize the US Cystic Fibrosis Foundation Patient Registry to study the associations between changes in lung function and body mass index, and the risk of recurrent pulmonary exacerbations, while accounting for the competing risks of death and lung transplantation. Our efficient implementation allows fast fitting of the model despite its complexity and the large sample size from this patient registry. Our comprehensive approach provides new insights into cystic fibrosis disease progression by quantifying the relationship between the most important clinical markers and events more precisely than has been possible before. The model implementation is available in the R package JMbayes2.

Published

2024

2. Immunogenicity of a bivalent BA.1 COVID-19 booster vaccine in people with HIV in the Netherlands

Author

Jongkees, Marlou J., primary, Tan, Ngoc H., additional, Geers, Daryl, additional, de Vries, Rory D., additional, Geurtsvankessel, Corine H., additional, Hensley, Kathryn S., additional, Sablerolles, Roos S.G., additional, Bogers, Susanne, additional, Gommers, Lennert, additional, Blakaj, Blerdi, additional, Afonso, Pedro Miranda, additional, Hansen, Bettina E., additional, Rijnders, Bart J.A., additional, Brinkman, Kees, additional, van der Kuy, P. Hugo M., additional, Roukens, Anna H.E., additional, and Rokx, Casper, additional

Published

2024

3. Clinical and Virological Outcome of Monoclonal Antibody Therapies Across Severe Acute Respiratory Syndrome Coronavirus 2 Variants in 245 Immunocompromised Patients: A Multicenter Prospective Cohort Study

Author

Huygens, Sammy, primary, GeurtsvanKessel, Corine, additional, Gharbharan, Arvind, additional, Bogers, Susanne, additional, Worp, Nathalie, additional, Boter, Marjan, additional, Bax, Hannelore I, additional, Kampschreur, Linda M, additional, Hassing, Robert-Jan, additional, Fiets, Roel B, additional, Levenga, Henriette, additional, Afonso, Pedro Miranda, additional, Koopmans, Marion, additional, Rijnders, Bart J A, additional, and Oude Munnink, Bas B, additional

Published

2024

4. Clinical and Virological Outcome of Monoclonal Antibody Therapies Across SARS-CoV-2 Variants in 245 Immunocompromised Patients:a multicenter prospective cohort study

Author

Huygens, Sammy, GeurtsvanKessel, Corine, Gharbharan, Arvind, Bogers, Susanne, Worp, Nathalie, Boter, Marjan, Bax, Hannelore I, Kampschreur, Linda M, Hassing, Robert-Jan, Fiets, Roel B, Levenga, Henriette, Afonso, Pedro Miranda, Koopmans, Marion, Rijnders, Bart J A, Oude Munnink, Bas B, Huygens, Sammy, GeurtsvanKessel, Corine, Gharbharan, Arvind, Bogers, Susanne, Worp, Nathalie, Boter, Marjan, Bax, Hannelore I, Kampschreur, Linda M, Hassing, Robert-Jan, Fiets, Roel B, Levenga, Henriette, Afonso, Pedro Miranda, Koopmans, Marion, Rijnders, Bart J A, and Oude Munnink, Bas B

Abstract

Background. Immunocompromised patients (ICPs) have an increased risk for a severe and prolonged COVID-19. SARS-CoV-2 monoclonal antibodies (mAbs) were extensively used in these patients, but data from randomized trials that focus on ICPs are lacking. We evaluated the clinical and virological outcome of COVID-19 in ICPs treated with mAbs across SARS-CoV-2 variants. Methods. In this multicenter prospective cohort study, we enrolled B-cell- and/or T-cell-deficient patients treated with casirivimab/imdevimab, sotrovimab, or tixagevimab/cilgavimab. SARS-CoV-2 RNA was quantified and sequenced weekly, and time to viral clearance, viral genome mutations, hospitalization, and death rates were registered. Results. Two hundred and forty five patients infected with the Delta (50%) or Omicron BA.1, 2, or 5 (50%) variant were enrolled. Sixty-seven percent were vaccinated; 78 treated as outpatients, of whom 2 required hospital admission, but both survived. Of the 159 patients hospitalized at time of treatment, 43 (27%) required mechanical ventilation or died. The median time to viral clearance was 14 days (interquartile range, 7-22); however, it took >30 days in 15%. Resistance-associated spike mutations emerged in 9 patients in whom the median time to viral clearance was 63 days (95% confidence interval, 57-69; P < .001). Spike mutations were observed in 1 of 42 (2.4%) patients after treatment with 2 active mAbs, in 5 of 34 (14.7%) treated with actual monotherapy (sotrovimab), and 3 of 20 (12%) treated with functional monotherapy (ie, tixagevimab/cilgavimab against tixagevimab-resistant variant). Conclusions. Despite treatment with mAbs, morbidity and mortality of COVID-19 in ICPs remained substantial. Combination antiviral therapy should be further explored and may be preferred in severely ICPs.

Published

2024

5. Clinical and Virological Outcome of Monoclonal Antibody Therapies Across SARS-CoV-2 Variants in 245 Immunocompromised Patients: A Multicenter Prospective Cohort Study.

Author

Huygens, Sammy, GeurtsvanKessel, Corine, Gharbharan, Arvind, Bogers, Susanne, Worp, Nathalie, Boter, Marjan, Bax, Hannelore I, Kampschreur, Linda M, Hassing, Robert-Jan, Fiets, Roel B, Levenga, Henriette, Afonso, Pedro Miranda, Koopmans, Marion, Rijnders, Bart J A, and Munnink, Bas B Oude

Subjects

THERAPEUTIC use of monoclonal antibodies, T-cell lymphoma, MORTALITY, IMMUNIZATION, RESEARCH funding, VIRAL load, PATIENTS, IMMUNOCOMPROMISED patients, HOSPITAL care, HOSPITAL admission & discharge, TREATMENT effectiveness, DESCRIPTIVE statistics, LONGITUDINAL method, ANTIVIRAL agents, RESEARCH, ARTIFICIAL respiration, GENETIC mutation, COVID-19, B cell lymphoma, EVALUATION

Abstract

Background Immunocompromised patients (ICPs) have an increased risk for a severe and prolonged COVID-19. SARS-CoV-2 monoclonal antibodies (mAbs) were extensively used in these patients, but data from randomized trials that focus on ICPs are lacking. We evaluated the clinical and virological outcome of COVID-19 in ICPs treated with mAbs across SARS-CoV-2 variants. Methods In this multicenter prospective cohort study, we enrolled B-cell– and/or T-cell–deficient patients treated with casirivimab/imdevimab, sotrovimab, or tixagevimab/cilgavimab. SARS-CoV-2 RNA was quantified and sequenced weekly, and time to viral clearance, viral genome mutations, hospitalization, and death rates were registered. Results Two hundred and forty five patients infected with the Delta (50%) or Omicron BA.1, 2, or 5 (50%) variant were enrolled. Sixty-seven percent were vaccinated; 78 treated as outpatients, of whom 2 required hospital admission, but both survived. Of the 159 patients hospitalized at time of treatment, 43 (27%) required mechanical ventilation or died. The median time to viral clearance was 14 days (interquartile range, 7–22); however, it took >30 days in 15%. Resistance-associated spike mutations emerged in 9 patients in whom the median time to viral clearance was 63 days (95% confidence interval, 57–69; P <.001). Spike mutations were observed in 1 of 42 (2.4%) patients after treatment with 2 active mAbs, in 5 of 34 (14.7%) treated with actual monotherapy (sotrovimab), and 3 of 20 (12%) treated with functional monotherapy (ie, tixagevimab/cilgavimab against tixagevimab-resistant variant). Conclusions Despite treatment with mAbs, morbidity and mortality of COVID-19 in ICPs remained substantial. Combination antiviral therapy should be further explored and may be preferred in severely ICPs. [ABSTRACT FROM AUTHOR]

Published

2024

6. A Decade of Experience With Alemtuzumab Therapy for Severe or Glucocorticoid-Resistant Kidney Transplant Rejection.

Author

van Vugt, Lukas K., van der Zwan, Marieke, Groningen, Marian C. Clahsen-van, van Agteren, Madelon, Hullegie-Peelen, Daphne M., De Winter, Brenda C. M., Reinders, Marlies E. J., Afonso, Pedro Miranda, and Hesselink, Dennis A.

Subjects

GRAFT rejection, KIDNEY transplantation, ALEMTUZUMAB, B cells, OVERALL survival

Abstract

Alemtuzumab is used as lymphocyte-depleting therapy for severe or glucocorticoidresistant kidney transplant rejection. However, the long-term efficacy and toxicity of alemtuzumab therapy are unclear. Therefore, all cases of alemtuzumab anti-rejection therapy between 2012 and 2022 in our institution were investigated. Graft survival, graft function, lymphocyte depletion, serious infections, malignancies, and patient survival were analyzed and compared with a reference cohort of transplanted patients who did not require alemtuzumab anti-rejection therapy. A total of 225 patients treated with alemtuzumab were identified and compared with a reference cohort of 1,668 patients. Over 60% of grafts was salvaged with alemtuzumab therapy, but graft survival was significantly poorer compared to the reference cohort. The median time of profound T- and B lymphocyte depletion was 272 and 344 days, respectively. Serious infection rate after alemtuzumab therapy was 54.1/100 person-years. The risk of death (hazard ratio 1.75, 95%-CI 1.28--2.39) and infection-related death (hazard ratio 2.36, 95%-CI 1.35--4.11) were higher in the alemtuzumab-treated cohort. In conclusion, alemtuzumab is an effective treatment for severe kidney transplant rejection, but causes long-lasting lymphocyte depletion and is associated with frequent infections and worse patient survival outcomes. [ABSTRACT FROM AUTHOR]

Published

2023

7. Corrigendum.

Author

Barvelink B, Reijman M, Smidt S, Afonso PM, Verhaar JAN, and Colaris JW

Abstract

Competing Interests: None declared

Published

2024