Endothelial progenitor
cells are rapidly recruited to myocardium and mediate protective effect
of ischemic preconditioning via "imported" nitric oxide synthase
activity
Ii M, Nishimura H, Iwakura A, Wecker A, Eaton E, Asahara T and Losordo
D W
Circulation 111(9):1114-20 (2005)
SUMMARY
BACKGROUND: The function of bone marrow-derived endothelial progenitor
cells (EPCs) in repair of ischemic tissue has been the subject of intense
scrutiny, and the capacity of these cells to contribute significantly
to new blood vessels remains controversial. The possibility that EPCs
could act as reservoirs of cytokines has been implied by several observations;
however, a specific role for cytokine delivery has not been identified.
METHODS AND RESULTS: We performed a series of experiments that revealed
the rapid recruitment of EPCs to the myocardium by very short periods
of ischemia, so-called ischemic preconditioning. The recruited EPCs express
an array of potentially cardioprotective cytokines including nitric oxide
synthase isoforms. Bone marrow transplantation studies, using donor marrow
null for nitric oxide synthase isoforms, revealed that both endothelial
and inducible nitric oxide synthase derived from bone marrow cells play
essential roles in the cardioprotective effect that normally occurs after
ischemic preconditioning. CONCLUSIONS: These findings provide novel insights
about the role of bone marrow-derived cells in ischemic preconditioning
and also reveal that distinct mechanisms regulate recovery after ischemia-reperfusion
and chronic ischemic injury.
LINK
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&dopt=Citation&list_uids=15723985
