4.7 Article

Robust Revascularization in Models of Limb Ischemia Using a Clinically Translatable Human Stem Cell-Derived Endothelial Cell Product

Journal

MOLECULAR THERAPY
Volume 26, Issue 7, Pages 1669-1684

Publisher

CELL PRESS
DOI: 10.1016/j.ymthe.2018.03.017

Keywords

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Funding

  1. Medical Research Council [MR/K00719X/1]
  2. British Heart Foundation UK Cardiovascular Regenerative Medicine Centre [RM/13/2/30158]
  3. British Heart Foundation Research Excellence Award [RE/13/3/30183]
  4. British Heart Foundation [CH/09/002, RG/15/5/31446, CH/15/1/31199]
  5. Wellcome Trust Senior Investigator Award [WT103782AIA]
  6. British Heart Foundation Chair of Translational Cardiovascular Sciences [CH/11/2/28733]
  7. BHF CoRE
  8. MRC [MR/K00719X/1, G0701127] Funding Source: UKRI
  9. British Heart Foundation [RG/14/3/30706] Funding Source: researchfish
  10. Medical Research Council [MR/K00719X/1] Funding Source: researchfish

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Pluripotent stem cell-derived differentiated endothelial cells offer high potential in regenerative medicine in the cardiovascular system. With the aim of translating the use of a human stem cell-derived endothelial cell product (hESC-ECP) for treatment of critical limb ischemia (CLI) in man, we report a good manufacturing practice (GMP)-compatible protocol and detailed cell tracking and efficacy data in multiple preclinical models. The clinical-grade cell line RC11 was used to generate hESC-ECP, which was identified as mostly endothelial (60% CD31(+)/CD144(+)), with the remainder of the subset expressing various pericyte/mesenchymal stem cell markers. Cell tracking using MRI, PET, and qPCR in a murine model of limb ischemia demonstrated that hESC-ECP was detectable up to day 7 following injection. Efficacy in several murine models of limb ischemia (immunocompromised/immunocompetent mice and mice with either type I/II diabetes mellitus) demonstrated significantly increased blood perfusion and capillary density. Overall, we demonstrate a GMP-compatible hESC-ECP that improved ischemic limb perfusion and increased local angiogenesis without engraftment, paving the way for translation of this therapy.

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