Exosomes From Human CD34 + Stem Cells Mediate Their Proangiogenic Paracrine Activity

Author:

Sahoo Susmita1,Klychko Ekaterina1,Thorne Tina1,Misener Sol1,Schultz Kathryn M.1,Millay Meredith1,Ito Aiko1,Liu Ting1,Kamide Christine1,Agrawal Hemant1,Perlman Harris1,Qin Gangjian1,Kishore Raj1,Losordo Douglas W.1

Affiliation:

1. From the Feinberg Cardiovascular Research Institute, Northwestern University, Chicago, IL (S.S., E.K., T.T., S.M., K.M.S., M.M., A.I., T.L., C.K., G.Q., R.K., D.W.L.); Feinberg School of Medicine, Northwestern University, Chicago, IL (H.A., H.P.); and the Program in Cardiovascular Regenerative Medicine, Northwestern Memorial Hospital, Chicago, IL (D.W.L.).

Abstract

Rationale: Transplantation of human CD34 + stem cells to ischemic tissues has been associated with reduced angina, improved exercise time, and reduced amputation rates in phase 2 clinical trials and has been shown to induce neovascularization in preclinical models. Previous studies have suggested that paracrine factors secreted by these proangiogenic cells are responsible, at least in part, for the angiogenic effects induced by CD34 + cell transplantation. Objective: Our objective was to investigate the mechanism of CD34 + stem cell–induced proangiogenic paracrine effects and to examine if exosomes, a component of paracrine secretion, are involved. Methods and Results: Exosomes collected from the conditioned media of mobilized human CD34 + cells had the characteristic size (40 to 90 nm; determined by dynamic light scattering), cup-shaped morphology (electron microscopy), expressed exosome-marker proteins CD63, phosphatidylserine (flow cytometry) and TSG101 (immunoblotting), besides expressing CD34 + cell lineage marker protein, CD34. In vitro, CD34 + exosomes replicated the angiogenic activity of CD34 + cells by increasing endothelial cell viability, proliferation, and tube formation on Matrigel. In vivo, the CD34 + exosomes stimulated angiogenesis in Matrigel plug and corneal assays. Interestingly, exosomes from CD34 + cells but not from CD34 + cell–depleted mononuclear cells had angiogenic activity. Conclusions: Our data demonstrate that human CD34 + cells secrete exosomes that have independent angiogenic activity both in vitro and in vivo. CD34 + exosomes may represent a significant component of the paracrine effect of progenitor cell transplantation for therapeutic angiogenesis.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine,Physiology

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