Comparison of the effects of standard vs low-dose prolonged-release tacrolimus with or without ACEi/ARB on the histology and function of renal allografts

Sandra M. Cockfield; Sam Wilson; Patricia M. Campbell; Marcelo Cantarovich; Azim Gangji; Isabelle Houde; Anthony M. Jevnikar; Tammy M. Keough-Ryan; Felix Mauricio Monroy-Cuadros; Peter W. Nickerson; Michel R. Pâquet; G. V. Ramesh Prasad; Lynne Senécal; Ahmed Shoker; Jean Luc Wolff; John Howell; Jason J. Schwartz; David N. Rush

doi:10.1111/ajt.15225

Comparison of the effects of standard vs low-dose prolonged-release tacrolimus with or without ACEi/ARB on the histology and function of renal allografts

Sandra M. Cockfield, Sam Wilson, Patricia M. Campbell, Marcelo Cantarovich, Azim Gangji, Isabelle Houde, Anthony M. Jevnikar, Tammy M. Keough-Ryan, Felix Mauricio Monroy-Cuadros, Peter W. Nickerson, Michel R. Pâquet, G. V. Ramesh Prasad, Lynne Senécal, Ahmed Shoker, Jean Luc Wolff, John Howell, Jason J. Schwartz, David N. Rush

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

26 Citas (Scopus)

Resumen

Targeting the renin-angiotensin system and optimizing tacrolimus exposure are both postulated to improve outcomes in renal transplant recipients (RTRs) by preventing interstitial fibrosis/tubular atrophy (IF/TA). In this multicenter, prospective, open-label controlled trial, adult de novo RTRs were randomized in a 2 × 2 design to low- vs standard-dose (LOW vs STD) prolonged-release tacrolimus and to angiotensin-converting enzyme inhibitors/angiotensin II receptor 1 blockers (ACEi/ARBs) vs other antihypertensive therapy (OAHT). There were 2 coprimary endpoints: the prevalence of IF/TA at month 6 and at month 24. IF/TA prevalence was similar for LOW vs STD tacrolimus at month 6 (36.8% vs 39.5%; P =.80) and ACEi/ARBs vs OAHT at month 24 (54.8% vs 58.2%; P =.33). IF/TA progression decreased significantly with LOW vs STD tacrolimus at month 24 (mean [SD] change, +0.42 [1.477] vs +1.10 [1.577]; P =.0039). Across the 4 treatment groups, LOW + ACEi/ARB patients exhibited the lowest mean IF/TA change and, compared with LOW + OAHT patients, experienced significantly delayed time to first T cell–mediated rejection. Renal function was stable from month 1 to month 24 in all treatment groups. No unexpected safety findings were detected. Coupled with LOW tacrolimus dosing, ACEi/ARBs appear to reduce IF/TA progression and delay rejection relative to reduced tacrolimus exposure without renin-angiotensin system blockade. ClinicalTrials.gov identifier: NCT00933231.

Idioma original	English
Páginas (desde-hasta)	1730-1744
Número de páginas	15
Publicación	American Journal of Transplantation
Volumen	19
N.º	6
DOI	https://doi.org/10.1111/ajt.15225
Estado	Published - jun. 2019
Publicado de forma externa	Sí

Nota bibliográfica

Funding Information:
The authors of this manuscript have conflicts of interest to dis‐ close as described by the American Journal of Transplantation. Drs Campbell, Cantarovich, Cockfield, Gangji, Jevnikar, Houde, Keough‐ Ryan, Monroy‐Cuadros, Nickerson, Pâquet, Prasad, Rush, Senécal, Shoker, and Wolff report nonfinancial support from Astellas Pharma, during the conduct of the study. Grants have been received by Drs Gangji, Houde, Jevnikar, Monroy‐Cuadros, Prasad, and Rush (Astellas Pharma Canada, Inc.). Consultant fees have been received by Dr Cantarovich (Astellas Pharma Canada, Inc.), Dr Gangji (Astellas Pharma Canada, Inc.), Dr Keough‐Ryan (Astellas Pharma Canada, Inc.), Dr Nickerson (Astellas Pharma Inc., Novartis Pharma Inc. and Vitaeris Inc.), and Dr Prasad (Astellas Pharma Canada, Inc.). Personal fees have been received by Dr Rush (Astellas Pharma Canada Inc., STA Communications, Astellas Pharma Spain, Novartis Argentina SA, Astellas Pharma US Inc., Pfizer, Astellas Pharma China Inc., Astellas Pharma Taiwan Inc., Antibody Healthcare Communications, Teva Pharmaceutical Ind Ltd., Gador Argentina, and Sandoz Argentina). Drs Wilson and Schwartz are employed by Astellas Pharma Global Development. Dr Howell was previously employed by Astellas Pharma Canada, Inc.

Funding Information:
This study was supported by Astellas Pharma, Inc. The authors thank John Ashkenas, PhD (SCRIPT, Toronto, Canada) for contributions to data interpretation and to the writing of this manuscript and Hong Chen (McDougall Scientific Ltd) for contributions to the management of data analytics. Organizational support by Kara Lee McWatters (formerly an employee of Astellas Pharma Canada, Inc) and the staff of the various study sites is gratefully acknowledged.

Funding Information:
This study was supported by Astellas Pharma, Inc. The authors thank John Ashkenas, PhD (SCRIPT, Toronto, Canada) for contri‐ butions to data interpretation and to the writing of this manuscript and Hong Chen (McDougall Scientific Ltd) for contributions to the management of data analytics. Organizational support by Kara Lee McWatters (formerly an employee of Astellas Pharma Canada, Inc) and the staff of the various study sites is gratefully acknowledged.

Publisher Copyright:
© 2018 Astellas Pharma, Inc. American Journal of Transplantation published by Wiley Periodicals, Inc. on behalf of The American Society of Transplantation and the American Society of Transplant Surgeons

ASJC Scopus Subject Areas

Immunology and Allergy
Transplantation
Pharmacology (medical)

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10.1111/ajt.15225

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Cockfield, S. M., Wilson, S., Campbell, P. M., Cantarovich, M., Gangji, A., Houde, I., Jevnikar, A. M., Keough-Ryan, T. M., Monroy-Cuadros, F. M., Nickerson, P. W., Pâquet, M. R., Ramesh Prasad, G. V., Senécal, L., Shoker, A., Wolff, J. L., Howell, J., Schwartz, J. J., & Rush, D. N. (2019). Comparison of the effects of standard vs low-dose prolonged-release tacrolimus with or without ACEi/ARB on the histology and function of renal allografts. American Journal of Transplantation, 19(6), 1730-1744. https://doi.org/10.1111/ajt.15225

Comparison of the effects of standard vs low-dose prolonged-release tacrolimus with or without ACEi/ARB on the histology and function of renal allografts. / Cockfield, Sandra M.; Wilson, Sam; Campbell, Patricia M. et al.
En: American Journal of Transplantation, Vol. 19, N.º 6, 06.2019, p. 1730-1744.

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

Cockfield, SM, Wilson, S, Campbell, PM, Cantarovich, M, Gangji, A, Houde, I, Jevnikar, AM, Keough-Ryan, TM, Monroy-Cuadros, FM, Nickerson, PW, Pâquet, MR, Ramesh Prasad, GV, Senécal, L, Shoker, A, Wolff, JL, Howell, J, Schwartz, JJ & Rush, DN 2019, 'Comparison of the effects of standard vs low-dose prolonged-release tacrolimus with or without ACEi/ARB on the histology and function of renal allografts', American Journal of Transplantation, vol. 19, n.º 6, pp. 1730-1744. https://doi.org/10.1111/ajt.15225

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abstract = "Targeting the renin-angiotensin system and optimizing tacrolimus exposure are both postulated to improve outcomes in renal transplant recipients (RTRs) by preventing interstitial fibrosis/tubular atrophy (IF/TA). In this multicenter, prospective, open-label controlled trial, adult de novo RTRs were randomized in a 2 × 2 design to low- vs standard-dose (LOW vs STD) prolonged-release tacrolimus and to angiotensin-converting enzyme inhibitors/angiotensin II receptor 1 blockers (ACEi/ARBs) vs other antihypertensive therapy (OAHT). There were 2 coprimary endpoints: the prevalence of IF/TA at month 6 and at month 24. IF/TA prevalence was similar for LOW vs STD tacrolimus at month 6 (36.8% vs 39.5%; P =.80) and ACEi/ARBs vs OAHT at month 24 (54.8% vs 58.2%; P =.33). IF/TA progression decreased significantly with LOW vs STD tacrolimus at month 24 (mean [SD] change, +0.42 [1.477] vs +1.10 [1.577]; P =.0039). Across the 4 treatment groups, LOW + ACEi/ARB patients exhibited the lowest mean IF/TA change and, compared with LOW + OAHT patients, experienced significantly delayed time to first T cell–mediated rejection. Renal function was stable from month 1 to month 24 in all treatment groups. No unexpected safety findings were detected. Coupled with LOW tacrolimus dosing, ACEi/ARBs appear to reduce IF/TA progression and delay rejection relative to reduced tacrolimus exposure without renin-angiotensin system blockade. ClinicalTrials.gov identifier: NCT00933231.",

author = "Cockfield, {Sandra M.} and Sam Wilson and Campbell, {Patricia M.} and Marcelo Cantarovich and Azim Gangji and Isabelle Houde and Jevnikar, {Anthony M.} and Keough-Ryan, {Tammy M.} and Monroy-Cuadros, {Felix Mauricio} and Nickerson, {Peter W.} and P{\^a}quet, {Michel R.} and {Ramesh Prasad}, {G. V.} and Lynne Sen{\'e}cal and Ahmed Shoker and Wolff, {Jean Luc} and John Howell and Schwartz, {Jason J.} and Rush, {David N.}",

note = "Funding Information: The authors of this manuscript have conflicts of interest to dis‐ close as described by the American Journal of Transplantation. Drs Campbell, Cantarovich, Cockfield, Gangji, Jevnikar, Houde, Keough‐ Ryan, Monroy‐Cuadros, Nickerson, P{\^a}quet, Prasad, Rush, Sen{\'e}cal, Shoker, and Wolff report nonfinancial support from Astellas Pharma, during the conduct of the study. Grants have been received by Drs Gangji, Houde, Jevnikar, Monroy‐Cuadros, Prasad, and Rush (Astellas Pharma Canada, Inc.). Consultant fees have been received by Dr Cantarovich (Astellas Pharma Canada, Inc.), Dr Gangji (Astellas Pharma Canada, Inc.), Dr Keough‐Ryan (Astellas Pharma Canada, Inc.), Dr Nickerson (Astellas Pharma Inc., Novartis Pharma Inc. and Vitaeris Inc.), and Dr Prasad (Astellas Pharma Canada, Inc.). Personal fees have been received by Dr Rush (Astellas Pharma Canada Inc., STA Communications, Astellas Pharma Spain, Novartis Argentina SA, Astellas Pharma US Inc., Pfizer, Astellas Pharma China Inc., Astellas Pharma Taiwan Inc., Antibody Healthcare Communications, Teva Pharmaceutical Ind Ltd., Gador Argentina, and Sandoz Argentina). Drs Wilson and Schwartz are employed by Astellas Pharma Global Development. Dr Howell was previously employed by Astellas Pharma Canada, Inc. Funding Information: This study was supported by Astellas Pharma, Inc. The authors thank John Ashkenas, PhD (SCRIPT, Toronto, Canada) for contributions to data interpretation and to the writing of this manuscript and Hong Chen (McDougall Scientific Ltd) for contributions to the management of data analytics. Organizational support by Kara Lee McWatters (formerly an employee of Astellas Pharma Canada, Inc) and the staff of the various study sites is gratefully acknowledged. Funding Information: This study was supported by Astellas Pharma, Inc. The authors thank John Ashkenas, PhD (SCRIPT, Toronto, Canada) for contri‐ butions to data interpretation and to the writing of this manuscript and Hong Chen (McDougall Scientific Ltd) for contributions to the management of data analytics. Organizational support by Kara Lee McWatters (formerly an employee of Astellas Pharma Canada, Inc) and the staff of the various study sites is gratefully acknowledged. Publisher Copyright: {\textcopyright} 2018 Astellas Pharma, Inc. American Journal of Transplantation published by Wiley Periodicals, Inc. on behalf of The American Society of Transplantation and the American Society of Transplant Surgeons",

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AU - Cockfield, Sandra M.

AU - Wilson, Sam

AU - Campbell, Patricia M.

AU - Cantarovich, Marcelo

AU - Gangji, Azim

AU - Houde, Isabelle

AU - Jevnikar, Anthony M.

AU - Keough-Ryan, Tammy M.

AU - Monroy-Cuadros, Felix Mauricio

AU - Nickerson, Peter W.

AU - Pâquet, Michel R.

AU - Ramesh Prasad, G. V.

AU - Senécal, Lynne

AU - Shoker, Ahmed

AU - Wolff, Jean Luc

AU - Howell, John

AU - Schwartz, Jason J.

AU - Rush, David N.

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N2 - Targeting the renin-angiotensin system and optimizing tacrolimus exposure are both postulated to improve outcomes in renal transplant recipients (RTRs) by preventing interstitial fibrosis/tubular atrophy (IF/TA). In this multicenter, prospective, open-label controlled trial, adult de novo RTRs were randomized in a 2 × 2 design to low- vs standard-dose (LOW vs STD) prolonged-release tacrolimus and to angiotensin-converting enzyme inhibitors/angiotensin II receptor 1 blockers (ACEi/ARBs) vs other antihypertensive therapy (OAHT). There were 2 coprimary endpoints: the prevalence of IF/TA at month 6 and at month 24. IF/TA prevalence was similar for LOW vs STD tacrolimus at month 6 (36.8% vs 39.5%; P =.80) and ACEi/ARBs vs OAHT at month 24 (54.8% vs 58.2%; P =.33). IF/TA progression decreased significantly with LOW vs STD tacrolimus at month 24 (mean [SD] change, +0.42 [1.477] vs +1.10 [1.577]; P =.0039). Across the 4 treatment groups, LOW + ACEi/ARB patients exhibited the lowest mean IF/TA change and, compared with LOW + OAHT patients, experienced significantly delayed time to first T cell–mediated rejection. Renal function was stable from month 1 to month 24 in all treatment groups. No unexpected safety findings were detected. Coupled with LOW tacrolimus dosing, ACEi/ARBs appear to reduce IF/TA progression and delay rejection relative to reduced tacrolimus exposure without renin-angiotensin system blockade. ClinicalTrials.gov identifier: NCT00933231.

AB - Targeting the renin-angiotensin system and optimizing tacrolimus exposure are both postulated to improve outcomes in renal transplant recipients (RTRs) by preventing interstitial fibrosis/tubular atrophy (IF/TA). In this multicenter, prospective, open-label controlled trial, adult de novo RTRs were randomized in a 2 × 2 design to low- vs standard-dose (LOW vs STD) prolonged-release tacrolimus and to angiotensin-converting enzyme inhibitors/angiotensin II receptor 1 blockers (ACEi/ARBs) vs other antihypertensive therapy (OAHT). There were 2 coprimary endpoints: the prevalence of IF/TA at month 6 and at month 24. IF/TA prevalence was similar for LOW vs STD tacrolimus at month 6 (36.8% vs 39.5%; P =.80) and ACEi/ARBs vs OAHT at month 24 (54.8% vs 58.2%; P =.33). IF/TA progression decreased significantly with LOW vs STD tacrolimus at month 24 (mean [SD] change, +0.42 [1.477] vs +1.10 [1.577]; P =.0039). Across the 4 treatment groups, LOW + ACEi/ARB patients exhibited the lowest mean IF/TA change and, compared with LOW + OAHT patients, experienced significantly delayed time to first T cell–mediated rejection. Renal function was stable from month 1 to month 24 in all treatment groups. No unexpected safety findings were detected. Coupled with LOW tacrolimus dosing, ACEi/ARBs appear to reduce IF/TA progression and delay rejection relative to reduced tacrolimus exposure without renin-angiotensin system blockade. ClinicalTrials.gov identifier: NCT00933231.

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Comparison of the effects of standard vs low-dose prolonged-release tacrolimus with or without ACEi/ARB on the histology and function of renal allografts

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