Stem Cells Translational Medicine (Aug 2019)

Design and Validation of an Automated Process for the Expansion of Peripheral Blood‐Derived CD34+ Cells for Clinical Use After Myocardial Infarction

  • Claire Saucourt,
  • Sandrine Vogt,
  • Amandine Merlin,
  • Christophe Valat,
  • Anthony Criquet,
  • Laurence Harmand,
  • Brigitte Birebent,
  • Hélène Rouard,
  • Christian Himmelspach,
  • Éric Jeandidier,
  • Anne‐Gaële Chartois‐Leauté,
  • Sophie Derenne,
  • Laurence Koehl,
  • Joe‐Elie Salem,
  • Jean‐Sébastien Hulot,
  • Céline Tancredi,
  • Anne Aries,
  • Sébastien Judé,
  • Eric Martel,
  • Serge Richard,
  • Luc Douay,
  • Philippe Hénon

DOI
https://doi.org/10.1002/sctm.17-0277
Journal volume & issue
Vol. 8, no. 8
pp. 822 – 832

Abstract

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Abstract We previously demonstrated that intracardiac delivery of autologous peripheral blood‐derived CD34+ stem cells (SCs), mobilized by granulocyte‐colony stimulating factor (G‐CSF) and collected by leukapheresis after myocardial infarction, structurally and functionally repaired the damaged myocardial area. When used for cardiac indication, CD34+ cells are now considered as Advanced Therapy Medicinal Products (ATMPs). We have industrialized their production by developing an automated device for ex vivo CD34+‐SC expansion, starting from a whole blood (WB) sample. Blood samples were collected from healthy donors after G‐CSF mobilization. Manufacturing procedures included: (a) isolation of total nuclear cells, (b) CD34+ immunoselection, (c) expansion and cell culture recovery in the device, and (d) expanded CD34+ cell immunoselection and formulation. The assessment of CD34+ cell counts, viability, and immunophenotype and sterility tests were performed as quality tests. We established graft acceptance criteria and performed validation processes in three cell therapy centers. 59.4 × 106 ± 36.8 × 106 viable CD34+ cells were reproducibly generated as the final product from 220 ml WB containing 17.1 × 106 ± 8.1 × 106 viable CD34+ cells. CD34+ identity, genetic stability, and telomere length were consistent with those of basal CD34+ cells. Gram staining and mycoplasma and endotoxin analyses were negative in all cases. We confirmed the therapeutic efficacy of both CD34+‐cell categories in experimental acute myocardial infarct (AMI) in immunodeficient rats during preclinical studies. This reproducible, automated, and standardized expansion process produces high numbers of CD34+ cells corresponding to the approved ATMP and paves the way for a phase I/IIb study in AMI, which is currently recruiting patients. Stem Cells Translational Medicine 2019;8:822&832

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