Functional Disruption of Alpha4 Integrin Mobilizes Bone Marrow-derived Endothelial Progenitors and Augments Ischemic Neovascularization

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 2006 Jan 13

PMID 16401693

Citations 56

Authors

Gangjian Qin

Masaaki Ii

Marcy Silver

Andrea Wecker

Evelyn Bord

Hong Ma

Mary Gavin

David A Goukassian

Young-Sup Yoon

Thalia Papayannopoulou

Takayuki Asahara

Marianne Kearney

Tina Thorne

Cynthia Curry

Liz Eaton

Lindsay Heyd

Deepika Dinesh

Raj Kishore

Yan Zhu

Douglas W Losordo

Affiliations

Soon will be listed here.

Abstract

The cell surface receptor alpha4 integrin plays a critical role in the homing, engraftment, and maintenance of hematopoietic progenitor cells (HPCs) in the bone marrow (BM). Down-regulation or functional blockade of alpha4 integrin or its ligand vascular cell adhesion molecule-1 mobilizes long-term HPCs. We investigated the role of alpha4 integrin in the mobilization and homing of BM endothelial progenitor cells (EPCs). EPCs with endothelial colony-forming activity in the BM are exclusively alpha4 integrin-expressing cells. In vivo, a single dose of anti-alpha4 integrin antibody resulted in increased circulating EPC counts for 3 d. In hindlimb ischemia and myocardial infarction, systemically administered anti-alpha4 integrin antibody increased recruitment and incorporation of BM EPCs in newly formed vasculature and improved functional blood flow recovery and tissue preservation. Interestingly, BM EPCs that had been preblocked with anti-alpha4 integrin ex vivo or collected from alpha4 integrin-deficient mice incorporated as well as control cells into the neovasculature in ischemic sites, suggesting that alpha4 integrin may be dispensable or play a redundant role in EPC homing to ischemic tissue. These data indicate that functional disruption of alpha4 integrin may represent a potential angiogenic therapy for ischemic disease by increasing the available circulating supply of EPCs.

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