TY - JOUR
T1 - Safety of everolimus with reduced calcineurin inhibitor exposure in de novo kidney transplants
T2 - An analysis from the randomized transform study
AU - on behalf of the TRANSFORM Investigators
AU - Tedesco-Silva, Helio
AU - Pascual, Julio
AU - Viklicky, Ondrej
AU - Basic-Jukic, Nikolina
AU - Cassuto, Elisabeth
AU - Kim, Dean Y.
AU - Cruzado, Josep M.
AU - Sommerer, Claudia
AU - Adel Bakr, Mohamed
AU - Garcia, Valter D.
AU - Uyen, Huynh Do
AU - Russ, Graeme
AU - Soo Kim, Myoung
AU - Kuypers, Dirk
AU - Buchler, Matthias
AU - Citterio, Franco
AU - Gutierrez, Maria Pilar Hernandez
AU - Bernhardt, Peter
AU - Chadban, Steve
AU - Jardine, Alan
AU - Friede, Tim
AU - Maldonado, Rafael
AU - Massari, Pablo
AU - Aleman, Silvina
AU - Maurich, Silvia
AU - Gaite, Luis E.
AU - Raffaele, Pablo
AU - Imperiali, Nora
AU - Campbell, Scott
AU - Chadban, Steve
AU - Hughes, Peter
AU - Irish, Ashley
AU - Kanellis, John
AU - Lim, Wai
AU - O'Connell, Philip J.
AU - Russ, Graeme
AU - Endre, Zoltan
AU - Mount, Peter
AU - Hengster, Paul
AU - Neudorfer, Peter
AU - Oberbauer, Rainer
AU - Pratschke, Johann
AU - Kuypers, Dirk
AU - Bosmans, Jean Louis
AU - Broeders, Emine N.
AU - Weekers, Laurent
AU - Silva, Helio Tedesco
AU - Neto, Elias D.
AU - Mor, Eytan
AU - Nakache, Richard
N1 - Publisher Copyright:
Copyright © 2019 Wolters Kluwer Health, Inc. All rights reserved.
PY - 2019/9/1
Y1 - 2019/9/1
N2 - Background. The safety profiles of standard therapy versus everolimus with reduced-exposure calcineurin inhibitor (CNI) therapy using contemporary protocols in de novo kidney transplant recipients have not been compared in detail. Methods. TRANSFORM was a randomized, international trial in which de novo kidney transplant patients were randomized to everolimus with reduced-exposure CNI (N = 1014) or mycophenolic acid (MPA) with standard-exposure CNI (N = 1012), both with induction and corticosteroids. Results. Within the safety population (everolimus 1014, MPA 1012), adverse events with a suspected relation to study drug occurred in 62.9% versus 59.2% of patients given everolimus or MPA, respectively (P = 0.085). Hyperlipidemia, interstitial lung disease, peripheral edema, proteinuria, stomatitis/mouth ulceration, thrombocytopenia, and wound healing complications were more frequent with everolimus, whereas diarrhea, nausea, vomiting, leukopenia, tremor, and insomnia were more frequent in the MPA group. The incidence of viral infections (17.2% versus 29.2%; P < 0.001), cytomegalovirus (CMV) infections (8.1% versus 20.1%; P < 0.001), CMV syndrome (13.6% versus 23.0%, P = 0.044), and BK virus (BKV) infections (4.3% versus 8.0%, P < 0.001) were less frequent with everolimus. CMV infection was less common with everolimus versus MPA after adjusting for prophylaxis therapy in the D+/R- subgroup (P < 0.001). Study drug was discontinued more frequently due to rejection or impaired healing with everolimus, and more often due to BKV infection or BKV nephropathy with MPA. Conclusions. De novo everolimus with reduced-exposure CNI yielded a comparable incidence, though a distinctly different pattern, of adverse events versus current standard of care. Both regimens are safe and effective, yet their distinct profiles may enable tailoring for individual kidney transplant recipients.
AB - Background. The safety profiles of standard therapy versus everolimus with reduced-exposure calcineurin inhibitor (CNI) therapy using contemporary protocols in de novo kidney transplant recipients have not been compared in detail. Methods. TRANSFORM was a randomized, international trial in which de novo kidney transplant patients were randomized to everolimus with reduced-exposure CNI (N = 1014) or mycophenolic acid (MPA) with standard-exposure CNI (N = 1012), both with induction and corticosteroids. Results. Within the safety population (everolimus 1014, MPA 1012), adverse events with a suspected relation to study drug occurred in 62.9% versus 59.2% of patients given everolimus or MPA, respectively (P = 0.085). Hyperlipidemia, interstitial lung disease, peripheral edema, proteinuria, stomatitis/mouth ulceration, thrombocytopenia, and wound healing complications were more frequent with everolimus, whereas diarrhea, nausea, vomiting, leukopenia, tremor, and insomnia were more frequent in the MPA group. The incidence of viral infections (17.2% versus 29.2%; P < 0.001), cytomegalovirus (CMV) infections (8.1% versus 20.1%; P < 0.001), CMV syndrome (13.6% versus 23.0%, P = 0.044), and BK virus (BKV) infections (4.3% versus 8.0%, P < 0.001) were less frequent with everolimus. CMV infection was less common with everolimus versus MPA after adjusting for prophylaxis therapy in the D+/R- subgroup (P < 0.001). Study drug was discontinued more frequently due to rejection or impaired healing with everolimus, and more often due to BKV infection or BKV nephropathy with MPA. Conclusions. De novo everolimus with reduced-exposure CNI yielded a comparable incidence, though a distinctly different pattern, of adverse events versus current standard of care. Both regimens are safe and effective, yet their distinct profiles may enable tailoring for individual kidney transplant recipients.
UR - http://www.scopus.com/inward/record.url?scp=85068416125&partnerID=8YFLogxK
U2 - 10.1097/TP.0000000000002626
DO - 10.1097/TP.0000000000002626
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C2 - 30801548
AN - SCOPUS:85068416125
SN - 0041-1337
VL - 103
SP - 1953
EP - 1963
JO - Transplantation
JF - Transplantation
IS - 9
ER -