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Alternative splicing: a promising target for pharmaceutical inhibition of pathological angiogenesis? | LitMetric

Alternative splicing: a promising target for pharmaceutical inhibition of pathological angiogenesis?

Curr Pharm Des

Laboratory of Tumour and Development Biology, GIGA-Cancer Unit, Tour de Pathologie B23, University of Liège, 4000 - Liège, Belgium.

Published: May 2011

In eukaryotes, genes consist in coding sequences (exons) interspersed with non-coding ones (introns). The regulation of alternative inclusion/exclusion of exons, or part of exons, during the maturation of the pre-mRNA into mRNA (alternative splicing) allows a dramatic increase of the protein versus the gene repertoire. In a number of cases, alternative splicing decision generates proteins with distinct, sometimes opposite, functions from a given gene. Angiogenesis is the process of vascularisation in physiological conditions and a series of pathologies, including cancer where it favours tumour progression and dissemination of metastasis. In this issue, we discuss some key examples showing how alternative splicing may induce a switch from anti-angiogenic to pro-angiogenic functions and reciprocally. For some of these splicing events, the molecular mechanisms that trigger alternative splicing toward one or the other direction start to be elucidated. The emergence of strategies enabling to regulate alternative splicing opens new routes for anti-angiogenic therapies.

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Source
http://dx.doi.org/10.2174/138161210794455012DOI Listing

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