Molecular Therapy: Methods & Clinical Development (Mar 2019)

Development of a Novel Anti-CD19 Chimeric Antigen Receptor: A Paradigm for an Affordable CAR T Cell Production at Academic Institutions

  • Maria Castella,
  • Anna Boronat,
  • Raquel Martín-Ibáñez,
  • Vanina Rodríguez,
  • Guillermo Suñé,
  • Miguel Caballero,
  • Berta Marzal,
  • Lorena Pérez-Amill,
  • Beatriz Martín-Antonio,
  • Julio Castaño,
  • Clara Bueno,
  • Olga Balagué,
  • Europa Azucena González-Navarro,
  • Carles Serra-Pages,
  • Pablo Engel,
  • Ramon Vilella,
  • Daniel Benitez-Ribas,
  • Valentín Ortiz-Maldonado,
  • Joan Cid,
  • Jaime Tabera,
  • Josep M. Canals,
  • Miquel Lozano,
  • Tycho Baumann,
  • Anna Vilarrodona,
  • Esteve Trias,
  • Elías Campo,
  • Pablo Menendez,
  • Álvaro Urbano-Ispizua,
  • Jordi Yagüe,
  • Patricia Pérez-Galán,
  • Susana Rives,
  • Julio Delgado,
  • Manel Juan

Journal volume & issue
Vol. 12
pp. 134 – 144

Abstract

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Genetically modifying autologous T cells to express an anti-CD19 chimeric antigen receptor (CAR) has shown impressive response rates for the treatment of CD19+ B cell malignancies in several clinical trials (CTs). Making this treatment available to our patients prompted us to develop a novel CART19 based on our own anti-CD19 antibody (A3B1), followed by CD8 hinge and transmembrane region, 4-1BB- and CD3z-signaling domains. We show that A3B1 CAR T cells are highly cytotoxic and specific against CD19+ cells in vitro, inducing secretion of pro-inflammatory cytokines and CAR T cell proliferation. In vivo, A3B1 CAR T cells are able to fully control disease progression in an NOD.Cg-Prkdcscid Il2rdtm1Wjl/SzJ (NSG) xenograph B-ALL mouse model. Based on the pre-clinical data, we conclude that our CART19 is clearly functional against CD19+ cells, to a level similar to other CAR19s currently being used in the clinic. Concurrently, we describe the implementation of our CAR T cell production system, using lentiviral vector and CliniMACS Prodigy, within a medium-sized academic institution. The results of the validation phase show our system is robust and reproducible, while maintaining a low cost that is affordable for academic institutions. Our model can serve as a paradigm for similar institutions, and it may help to make CAR T cell treatment available to all patients. Keywords: chimeric antigen receptor, CD19, leukemia, lymphoma, immunotherapy, 4-1BB, T cell, preclinical studies