Chimeric Antigen Receptor T Cell Therapies: A Review of Cellular Kinetic‐Pharmacodynamic Modeling Approaches

Anwesha Chaudhury; Xu Zhu; Lulu Chu; Ardeshir Goliaei; Carl H. June; Jeffrey D. Kearns; Andrew M. Stein

doi:10.1002/jcph.1691

Chimeric Antigen Receptor T Cell Therapies: A Review of Cellular Kinetic‐Pharmacodynamic Modeling Approaches

Anwesha Chaudhury(Novartis (China)), Xu Zhu(Novartis (Switzerland)), Lulu Chu(Novartis (China)), Ardeshir Goliaei(Novartis (China)), Carl H. June(University of Pennsylvania), Jeffrey D. Kearns(Novartis (China)), Andrew M. Stein(Novartis (China))

The Journal of Clinical Pharmacology

November 1, 2020

10.1002/jcph.1691

Cited by 68

Abstract

Chimeric antigen receptor T cell (CAR-T cell) therapies have shown significant efficacy in CD19+ leukemias and lymphomas. There remain many challenges and questions for improving next-generation CAR-T cell therapies, and mathematical modeling of CAR-T cells may play a role in supporting further development. In this review, we introduce a mathematical modeling taxonomy for a set of relatively simple cellular kinetic-pharmacodynamic models that describe the in vivo dynamics of CAR-T cell and their interactions with cancer cells. We then discuss potential extensions of this model to include target binding, tumor distribution, cytokine-release syndrome, immunophenotype differentiation, and genotypic heterogeneity.

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