Automated Clinical Grade Expansion of Regulatory T Cells in a Fully Closed System

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2019 Feb 20

PMID 30778344

Citations 18

Authors

Jose Manuel Marin Morales

Nadine Munch

Katja Peter

Daniel Freund

Uta Oelschlagel

Kristina Holig

Thea Bohm

Anne-Christine Flach

Jorg Kessler

Ezio Bonifacio

Martin Bornhauser

Anke Fuchs

Affiliations

Soon will be listed here.

Abstract

Adoptive transfer of T regulatory cells (Treg) has been successfully exploited in the context of graft-versus-host disease, transplantation, and autoimmune disease. For the majority of applications, clinical administration of Treg requires laborious expansion and typically involves open handling for culture feeds and repetitive sampling. Here we show results from our approach to translate manual Treg manufacturing to the fully closed automated CliniMACS Prodigy® system reducing contamination risk, hands-on time, and quality variation from human intervention. Polyclonal Treg were isolated from total nucleated cells obtained through leukapheresis of healthy donors by CD8 cell depletion and subsequent CD25 enrichment. Treg were expanded with the CliniMACS Prodigy® device using clinical-grade cell culture medium, rapamycin, IL-2, and αCD3/αCD28 beads for 13-14 days. We successfully integrated expansion bead removal and final formulation into the automated procedure, finalizing the process with a ready to use product for bedside transfusion. Automated Treg expansion was conducted in parallel to an established manual manufacturing process using G-Rex cell culture flasks. We could prove similar expansion kinetics leading to a cell yield of up to 2.12 × 10 cells with the CliniMACS Prodigy® and comparable product phenotype of >90% CD4CD25CD127FOXP3 cells that had similar immunosuppressive function. Efficiency of expansion bead depletion was comparable to the CliniMACS® Plus system and the final ready-to-infuse product had phenotype stability and high vitality after overnight storage. We anticipate this newly developed closed system expansion approach to be a starting point for the development of enhanced throughput clinical scale Treg manufacture, and for safe automated generation of antigen-specific Treg grafted with a chimeric antigen receptor (CAR Treg).

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