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

Jamois, Candice; Gibiansky, Ekaterina; Gibiansky, Leonid; Chavanne, Clarisse; Morcos, Peter N.; McIntyre, Christine; Barrett, Martin; Lundberg, Linda; Zharkov, Artem; Boehnke, Axel; Frey, Nicolas

doi:10.1002/cpt.2308

Cited by 4 publications

(3 citation statements)

References 45 publications

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“…Jamois et al present application of PK-clinical bridging to the model-informed development and approval of a fixed-dose subcutaneously administered formulation of the anti-CD20 antibody rituximab, for the treatment of hematologic malignancies. 16 Based on prior knowledge from clinical experience on intravenously administered rituximab that trough concentrations correlated with efficacy, and biological support based on an expectation that sustained saturation of Bcell CD20 receptors should be relevant for efficacy, the clinical development program was designed to underwrite the dosage for subcutaneous administration based on demonstration of noninferior trough concentrations. Phase III trials included PK noninferiority as their primary objective-a testament to the pivotal role played by quantitative clinical pharmacology in the development plan.…”

Section: Midd In Oncology Drug Development: Challenges and Opportunit...mentioning

confidence: 99%

Model‐Informed Drug Development: Connecting the Dots With a Totality of Evidence Mindset to Advance Therapeutics

Venkatakrishnan

Graaf

2021

Clin Pharma and Therapeutics

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The Merriam-Webster dictionary offers the essential meaning of a model as "a usually small copy of something," or "a set of ideas and numbers that describe the past, present, or future state of something." Model-informed drug development (MIDD) involves the strategic creation and integration of mathematical models for knowledge management, predictions, and decision making in pharmaceutical research and development. These models can "connect the dots" across various inputs related to drug properties, disease biology, patient characteristics and trial designs, transforming data to knowledge, enhancing efficiency in drug discovery and development, and maximizing therapeutic potential. This issue of Clinical Pharmacology and Therapeutics (CPT) includes Original Research Articles, Reviews, and Perspectives illustrating recent advances in established and emerging areas of MIDD, highlighting opportunities for interdisciplinary and cross-sector collaboration for enhancing impact.

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Section: Midd In Oncology Drug Development: Challenges and Opportunit...mentioning

confidence: 99%

Model‐Informed Drug Development: Connecting the Dots With a Totality of Evidence Mindset to Advance Therapeutics

Venkatakrishnan

Graaf

2021

Clin Pharma and Therapeutics

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“…Due to target-mediated drug disposition, elimination phase of the majority of these mAbs was described with dual clearance, linear at higher concentrations when saturation of the target is achieved, and non-linear at lower concentrations. The exceptions were rituximab, which has a time-dependent component due to B-cell depletion, 52,53 and pertuzumab, whose model did not enclose the non-linear component. 54 In the denosumab model, a quasi-steady-state approximation was used to characterize non-linear clearance.…”

Section: Sc Administration Of Mabs In Oncologymentioning

confidence: 99%

“…Population pharmacokinetic (PK) parameters of monoclonal antibodies (mAbs) available as subcutaneous (SC) formulations[52][53][54][55][56][57][58] …”

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confidence: 99%

Pharmacokinetic characterization, benefits and barriers of subcutaneous administration of monoclonal antibodies in oncology

Homšek

Spasić

Nikolić

et al. 2022

J Oncol Pharm Pract

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Objective Therapeutic monoclonal antibodies in oncology are slowly becoming the dominant treatment option for many different cancer types. The main route of administration, infusion, requires extensive product preparations, patient hospitalization and close monitoring. Patient comfort improvement, staff workload reduction and cost savings dictated the development of subcutaneous formulations. The aim of this review is to present pharmacokinetic characteristics of subcutaneous products, discuss the differences between intravenous and subcutaneous routes and to point out the advantages as well as challenges of administration route shift from the formulation development and pharmacometric angle. Data sources Food and Drug administration's Purple book database and electronic medicines compendium were used to identify monoclonal antibodies in oncology approved as subcutaneous forms. Using keywords subcutaneous, monoclonal antibodies, pharmacokinetics, model, as well as specific drugs previously identified, both PubMed and ScienceDirect databases were researched. Data summary There are currently six approved subcutaneous onco-monoclonal antibodies on the market. For each of them, exposure to the drug was similar in relation to infusion, treatment effectiveness was the same, administration was well tolerated by the patients and costs of the medical service were reduced. Conclusion Development of subcutaneous forms for existing and emerging new monoclonal antibodies for cancer treatment as well as shifting from administration via infusion should be encouraged due to patient preference, lower costs and overall lack of substantial differences in efficacy and safety between the two routes.

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Model‐informed Evidence for Clinical Non‐inferiority of Every‐2‐Weeks Versus Standard Weekly Dosing Schedule of Cetuximab in Metastatic Colorectal Cancer

Milenković‐Grišić,

Hayes,

Farrell

et al. 2024

Clin Pharma and Therapeutics

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Cetuximab was initially developed and approved as a first‐line treatment in patients with unresectable metastatic colorectal cancer (mCRC) for weekly administration (250 mg/m2 Q1W with 400 mg/m2 loading dose). An every‐2‐weeks schedule (500 mg/m2 Q2W) was approved recently by several health authorities. Being synchronized with chemotherapy, Q2W administration should improve patients' convenience and healthcare resource utilization. Herein, we present evidence of non‐inferiority of Q2W cetuximab, compared with Q1W dosing using pharmacometrics modeling and clinical trial simulation (CTS). Pooled data from five phase I–III clinical trials in 852 patients with KRAS wild‐type mCRC treated with Q1W or Q2W cetuximab were modeled using a population exposure–tumor size (TS) model linked to overall survival (OS); exposure was derived from a previously established population pharmacokinetic model. A semi‐mechanistic TS model adapted from the Claret model incorporated killing rate proportional to cetuximab area under the concentration‐time curve over 2 weeks (AUC) with Eastern Cooperative Oncology Group (ECOG) status as covariate on baseline TS. The OS was modeled with Weibull hazard using ECOG, baseline TS, primary tumor location, and predicted percent change in TS at 8 weeks as covariates. Model‐based simulations revealed indistinguishable early tumor shrinkage and survival between Q2W vs. Q1W cetuximab. CTS evaluated OS non‐inferiority (predefined margin of 1.25) in 1,000 trials, each with 2,000 virtual patients receiving Q2W or Q1W cetuximab (1:1), and demonstrated non‐inferiority in 94% of cases. Taken together, these analyses provide model‐based evidence for clinical non‐inferiority of Q2W vs. Q1W cetuximab in mCRC with potential benefits to patients and healthcare providers.

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

Cited by 4 publications

References 45 publications

Model‐Informed Drug Development: Connecting the Dots With a Totality of Evidence Mindset to Advance Therapeutics

Model‐Informed Drug Development: Connecting the Dots With a Totality of Evidence Mindset to Advance Therapeutics

Pharmacokinetic characterization, benefits and barriers of subcutaneous administration of monoclonal antibodies in oncology

Model‐informed Evidence for Clinical Non‐inferiority of Every‐2‐Weeks Versus Standard Weekly Dosing Schedule of Cetuximab in Metastatic Colorectal Cancer

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