Multinational case-control study of risk factors for the development of late invasive pulmonary aspergillosis following kidney transplantation

Lopez-Medrano, F.; Fernandez-Ruiz, M.; Silva, J. T.; Carver, P. L.; van Delden, C.; Merino, E.; Perez-Saez, M. J.; Montero, M.; Coussement, J.; de Abreu Mazzolin, M.; Cervera, C.; Santos, L.; Sabe, N.; Scemla, A.; Cordero, E.; Cruzado-Vega, L.; Martin-Moreno, P. L.; Len, O.; Rudas, E.; Ponce de Leon, A.; Arriola, M.; Lauzurica, R.; David, M. D.; Gonzalez-Rico, C.; Henriquez-Palop, F.; Fortun, J.; Nucci, M.; Manuel, O.; Pano-Pardo, J. R.; Montejo, M.; Vena, A.; Sanchez-Sobrino, B.; Mazuecos, A.; Pascual, J.; Horcajada, J. P.; Lecompte, T.; Moreno, A.; Carratala, J.; Blanes, M.; Hernandez, D.; Hernandez-Mendez, E. A.; Farinas, M. C.; Perello-Carrascosa, M.; Munoz, P.; Andres, A.; Aguado, J. M.

doi:10.1016/j.cmi.2017.06.016

Objectives: To assess the risk factors for development of late-onset invasive pulmonary aspergillosis (IPA) after kidney transplantation (KT). Methods: We performed a multinational case-control study that retrospectively recruited 112 KT recipients diagnosed with IPA between 2000 and 2013. Controls were matched (1:1 ratio) by centre and date of transplantation. Immunosuppression-related events (IREs) included the occurrence of non-ventilator-associated pneumonia, tuberculosis, cytomegalovirus disease, and/or de novo malignancy. Results: We identified 61 cases of late (>180 days after transplantation) IPA from 24 participating centres (accounting for 54.5% (61/112) of all cases included in the overall study). Most diagnoses (54.1% (33/61)) were established within the first 36 post-transplant months, although five cases occurred more than 10 years after transplantation. Overall mortality among cases was 47.5% (29/61). Compared with controls, cases were significantly older (p 0.010) and more likely to have pre-transplant chronic obstructive pulmonary disease (p 0.001) and a diagnosis of bloodstream infection (p 0.016) and IRE (p <0.001) within the 6 months prior to the onset of late IPA. After multivariate adjustment, previous occurrence of IRE (OR 19.26; 95% CI 2.07–179.46; p 0.009) was identified as an independent risk factor for late IPA. Conclusion: More than half of IPA cases after KT occur beyond the sixth month, with some of them presenting very late. Late IPA entails a poor prognosis. We identified some risk factors that could help the clinician to delimit the subgroup of KT recipients at the highest risk for late IPA.

Multinational case-control study of risk factors for the development of late invasive pulmonary aspergillosis following kidney transplantation

Lopez-Medrano F.;Fernandez-Ruiz M.;Silva J. T.;Carver P. L.;van Delden C.;Merino E.;Perez-Saez M. J.;Montero M.;Coussement J.;de Abreu Mazzolin M.;Cervera C.;Santos L.;Sabe N.;Scemla A.;Cordero E.;Cruzado-Vega L.;Martin-Moreno P. L.;Len O.;Rudas E.;Ponce de Leon A.;Arriola M.;Lauzurica R.;David M. D.;Gonzalez-Rico C.;Henriquez-Palop F.;Fortun J.;Nucci M.;Manuel O.;Pano-Pardo J. R.;Montejo M.;Vena A.;Sanchez-Sobrino B.;Mazuecos A.;Pascual J.;Horcajada J. P.;Lecompte T.;Moreno A.;Carratala J.;Blanes M.;Hernandez D.;Hernandez-Mendez E. A.;Farinas M. C.;Perello-Carrascosa M.;Munoz P.;Andres A.;Aguado J. M.

2018-01-01

Abstract

Objectives: To assess the risk factors for development of late-onset invasive pulmonary aspergillosis (IPA) after kidney transplantation (KT). Methods: We performed a multinational case-control study that retrospectively recruited 112 KT recipients diagnosed with IPA between 2000 and 2013. Controls were matched (1:1 ratio) by centre and date of transplantation. Immunosuppression-related events (IREs) included the occurrence of non-ventilator-associated pneumonia, tuberculosis, cytomegalovirus disease, and/or de novo malignancy. Results: We identified 61 cases of late (>180 days after transplantation) IPA from 24 participating centres (accounting for 54.5% (61/112) of all cases included in the overall study). Most diagnoses (54.1% (33/61)) were established within the first 36 post-transplant months, although five cases occurred more than 10 years after transplantation. Overall mortality among cases was 47.5% (29/61). Compared with controls, cases were significantly older (p 0.010) and more likely to have pre-transplant chronic obstructive pulmonary disease (p 0.001) and a diagnosis of bloodstream infection (p 0.016) and IRE (p <0.001) within the 6 months prior to the onset of late IPA. After multivariate adjustment, previous occurrence of IRE (OR 19.26; 95% CI 2.07–179.46; p 0.009) was identified as an independent risk factor for late IPA. Conclusion: More than half of IPA cases after KT occur beyond the sixth month, with some of them presenting very late. Late IPA entails a poor prognosis. We identified some risk factors that could help the clinician to delimit the subgroup of KT recipients at the highest risk for late IPA.