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Therapeutic angiogenesis

by evgnadmin last modified 2008-01-02 16:07

Insufficient neoangiogenesis is an integral component of loss of organ function following chronic ischaemia or acute ischaemic injury due to atherosclerotic plaque rupture and myocardial infarction. Therapeutic angiogenesis promoting the growth of new vessels from existing vessel wall cells, in conjunction with the recruitment of circulating endothelial progenitor cells (EPCs), is therefore viewed as a highly promising strategy to revascularise ischaemic tissues and thereby improve functional recovery of injured organs. Identification of genes involved in differentiation, homing and expansion of EPCs is of paramount importance in developing ways to specifically target the cells in sufficient numbers to ischaemic tissue.

A large body of evidence indicates that angiogenesis/vasculogenesis is central in the repair process following tissue ischaemia. Therapeutic neovascularisation is therefore considered as a very promising approach to prevent the serious clinical consequences (heart failure, gangrene, neuronal disability) of abnormal tissue remodelling in patients suffering from cardiovascular ischaemic disease. Angiogenesis research was recently revolutionized by the discovery that adult angiogenesis is significantly bolstered by the recruitment of circulating endothelial progenitor cells (EPCs) that functionally incorporate into forming vessels.

The aim of this EVGN priority area is to identify novel genes, gene products, or signalling pathways that are involved in, and could be targets for, selective modulation of angiogenesis/vasculogenesis, and define the most suitable therapeutic strategies for use in clinical care





 

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