Quantitative Clinical Pharmacology Supports the Bridging From i.v. Dosing and Approval of s.c. Rituximab in B‐Cell Hematological Malignancies

Quantitative Clinical Pharmacology Supports the Bridging From i.v. Dosing and Approval of s.c. Rituximab in B‐Cell Hematological Malignancies

A fixed‐dose subcutaneous (s.c.) formulation of the anti‐CD20 antibody, rituximab, has been developed to address safety, infusion time, and patient comfort concerns relating to intravenous (i.v.) dosing, and has been approved based upon a pharmacokinetic (PK)–clinical bridging strategy, which demons...

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Veröffentlicht in:Clinical pharmacology and therapeutics 2021-11, Vol.110 (5), p.1261-1272
Hauptverfasser: Jamois, Candice, Gibiansky, Ekaterina, Gibiansky, Leonid, Chavanne, Clarisse, Morcos, Peter N., McIntyre, Christine, Barrett, Martin, Lundberg, Linda, Zharkov, Artem, Boehnke, Axel, Frey, Nicolas
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container_end_page 1272
container_issue 5
container_start_page 1261
container_title Clinical pharmacology and therapeutics
container_volume 110
creator Jamois, Candice
Gibiansky, Ekaterina
Gibiansky, Leonid
Chavanne, Clarisse
Morcos, Peter N.
McIntyre, Christine
Barrett, Martin
Lundberg, Linda
Zharkov, Artem
Boehnke, Axel
Frey, Nicolas
description A fixed‐dose subcutaneous (s.c.) formulation of the anti‐CD20 antibody, rituximab, has been developed to address safety, infusion time, and patient comfort concerns relating to intravenous (i.v.) dosing, and has been approved based upon a pharmacokinetic (PK)–clinical bridging strategy, which demonstrated noninferiority of s.c. vs. i.v. dosing in malignancies, including follicular lymphoma (FL) and chronic lymphocytic leukemia (CLL). A clinical development plan was undertaken to identify rituximab s.c. doses achieving noninferior exposure to rituximab i.v., and to confirm PK–clinical bridging, with the same efficacy and similar safety. This drew upon data from 1,579 patients with FL, CLL, or diffuse large B‐cell lymphoma in 5 clinical studies, and showed minimum steady‐state serum concentration (Ctrough) as the most appropriate exposure bridging measure. Population PK models were developed, simulations were run using covariates and PK parameters from clinical studies, and exposure–efficacy and –safety analyses performed. Population PKs showed a two‐compartment model with time‐dependent and ‐independent clearances. Clearance and volume were predominantly influenced by body surface area; disposition and elimination were similar for the s.c. and i.v. formulations. After s.c. administration, patients with FL and CLL achieved noninferior exposures to i.v. dosing. Overall, rituximab exposure and route of administration did not influence clinical responses in patients with FL or CLL, and there was no association between exposure and safety events. Ctrough was shown to be an effective pharmacologic–clinical bridging parameter for rituximab in patients with FL or CLL. Clinically effective exposures are achieved with either s.c. or i.v. dosing.
doi_str_mv 10.1002/cpt.2308
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A clinical development plan was undertaken to identify rituximab s.c. doses achieving noninferior exposure to rituximab i.v., and to confirm PK–clinical bridging, with the same efficacy and similar safety. This drew upon data from 1,579 patients with FL, CLL, or diffuse large B‐cell lymphoma in 5 clinical studies, and showed minimum steady‐state serum concentration (Ctrough) as the most appropriate exposure bridging measure. Population PK models were developed, simulations were run using covariates and PK parameters from clinical studies, and exposure–efficacy and –safety analyses performed. Population PKs showed a two‐compartment model with time‐dependent and ‐independent clearances. Clearance and volume were predominantly influenced by body surface area; disposition and elimination were similar for the s.c. and i.v. formulations. After s.c. administration, patients with FL and CLL achieved noninferior exposures to i.v. dosing. 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title Quantitative Clinical Pharmacology Supports the Bridging From i.v. Dosing and Approval of s.c. Rituximab in B‐Cell Hematological Malignancies
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