TY - JOUR
T1 - The Second International Consensus Guidelines on the Management of BK Polyomavirus in Kidney Transplantation
AU - The Transplantation Society International BK Polyomavirus Consensus Group
AU - Kotton, Camille N.
AU - Kamar, Nassim
AU - Wojciechowski, David
AU - Eder, Michael
AU - Hopfer, Helmut
AU - Randhawa, Parmjeet
AU - Sester, Martina
AU - Comoli, Patrizia
AU - Silva, Helio Tedesco
AU - Knoll, Greg
AU - Brennan, Daniel C.
AU - Trofe-Clark, Jennifer
AU - Pape, Lars
AU - Axelrod, David
AU - Kiberd, Bryce
AU - Wong, Germaine
AU - Hirsch, Hans H.
AU - Caillard, Sophie
AU - Fernandez-Ruiz, Mario
AU - Oberbauer, Rainer
AU - Pierrotti, Ligia
AU - Drachenberg, Cinthia
AU - Heher, Yael
AU - Huang, Gang
AU - Mengel, Michael
AU - Buenrostro, Luis Morales
AU - Nankivell, Brian
AU - Bertels, Laurie
AU - Vathsala, Anantharaman
AU - Halary, Franck
AU - Heim, Albert
AU - Kumar, Deepali
AU - Leuzinger, Karoline
AU - Rinaldo, Christine Hanssen
AU - Schaenman, Joanna
AU - Slavin, Monica
AU - Tedesco-Silva, Helio
AU - Schaub, Stefan
AU - Benotmane, Ilies
AU - Theodoropoulos, Nicole
AU - Helantera, Ilkka
AU - Witzke, Oliver
AU - Chadban, Steven
AU - Bagchi, Soumita
AU - Elfadawy, Nissreen
AU - Dharnidharka, Vikas R.
AU - Hattori, Motoshi
AU - Venkataramanan, Raman
AU - Tönshoff, Burkhard
AU - Laskin, Benjamin
N1 - Publisher Copyright:
© 2024 Wolters Kluwe.
PY - 2024/9/1
Y1 - 2024/9/1
N2 - BK polyomavirus (BKPyV) remains a significant challenge after kidney transplantation. International experts reviewed current evidence and updated recommendations according to Grading of Recommendations, Assessment, Development, and Evaluations (GRADE). Risk factors for BKPyV-DNAemia and biopsy-proven BKPyV-nephropathy include recipient older age, male sex, donor BKPyV-viruria, BKPyV-seropositive donorAseronegative recipient, tacrolimus, acute rejection, and higher steroid exposure. To facilitate early intervention with limited allograft damage, all kidney transplant recipients should be screened monthly for plasma BKPyV-DNAemia loads until month 9, then every 3 mo until 2 y posttransplant (3 y for children). In resource-limited settings, urine cytology screening at similar time points can exclude BKPyV-nephropathy, and testing for plasma BKPyV-DNAemia when decoy cells are detectable. For patients with BKPyV-DNAemia loads persisting >1000 copies/mL, or exceeding 10000 copies/mL (or equivalent), or with biopsy-proven BKPyV-nephropathy, immunosuppression should be reduced according to predefined steps targeting antiproliferative drugs, calcineurin inhibitors, or both. In adults without graft dysfunction, kidney allograft biopsy is not required unless the immunological risk is high. For children with persisting BKPyV-DNAemia, allograft biopsy may be considered even without graft dysfunction. Allograft biopsies should be interpreted in the context of all clinical and laboratory findings, including plasma BKPyV-DNAemia. Immunohistochemistry is preferred for diagnosing biopsy-proven BKPyV-nephropathy. Routine screening using the proposed strategies is cost-effective, improves clinical outcomes and quality of life. Kidney retransplantation subsequent to BKPyV-nephropathy is feasible in otherwise eligible recipients if BKPyV-DNAemia is undetectable; routine graft nephrectomy is not recommended. Current studies do not support the usage of leflunomide, cidofovir, quinolones, or IVIGs. Patients considered for experimental treatments (antivirals, vaccines, neutralizing antibodies, and adoptive T cells) should be enrolled in clinical trials.
AB - BK polyomavirus (BKPyV) remains a significant challenge after kidney transplantation. International experts reviewed current evidence and updated recommendations according to Grading of Recommendations, Assessment, Development, and Evaluations (GRADE). Risk factors for BKPyV-DNAemia and biopsy-proven BKPyV-nephropathy include recipient older age, male sex, donor BKPyV-viruria, BKPyV-seropositive donorAseronegative recipient, tacrolimus, acute rejection, and higher steroid exposure. To facilitate early intervention with limited allograft damage, all kidney transplant recipients should be screened monthly for plasma BKPyV-DNAemia loads until month 9, then every 3 mo until 2 y posttransplant (3 y for children). In resource-limited settings, urine cytology screening at similar time points can exclude BKPyV-nephropathy, and testing for plasma BKPyV-DNAemia when decoy cells are detectable. For patients with BKPyV-DNAemia loads persisting >1000 copies/mL, or exceeding 10000 copies/mL (or equivalent), or with biopsy-proven BKPyV-nephropathy, immunosuppression should be reduced according to predefined steps targeting antiproliferative drugs, calcineurin inhibitors, or both. In adults without graft dysfunction, kidney allograft biopsy is not required unless the immunological risk is high. For children with persisting BKPyV-DNAemia, allograft biopsy may be considered even without graft dysfunction. Allograft biopsies should be interpreted in the context of all clinical and laboratory findings, including plasma BKPyV-DNAemia. Immunohistochemistry is preferred for diagnosing biopsy-proven BKPyV-nephropathy. Routine screening using the proposed strategies is cost-effective, improves clinical outcomes and quality of life. Kidney retransplantation subsequent to BKPyV-nephropathy is feasible in otherwise eligible recipients if BKPyV-DNAemia is undetectable; routine graft nephrectomy is not recommended. Current studies do not support the usage of leflunomide, cidofovir, quinolones, or IVIGs. Patients considered for experimental treatments (antivirals, vaccines, neutralizing antibodies, and adoptive T cells) should be enrolled in clinical trials.
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U2 - 10.1097/TP.0000000000004976
DO - 10.1097/TP.0000000000004976
M3 - Review article
C2 - 38605438
AN - SCOPUS:85197296665
SN - 0041-1337
VL - 108
SP - 1834
EP - 1866
JO - Transplantation
JF - Transplantation
IS - 9
ER -