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Vascular permeability changes involved in tumor metastasis

CANCER LETTERS (2013)

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Journal

CANCER LETTERS
Volume 335, Issue 2, Pages 259-269

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.canlet.2013.03.005

Keywords

Vascular permeability; Metastasis; Vasoactive compounds; Endothelial cells; VEGF; Angptl4

Categories

Oncology

Funding

  1. National Council of Science and Technology of Mexico (CONACyT-Mexico) [45519]
  2. Miguel Aleman Foundation
  3. Mexico City Science and Technology Institute (ICyTDF) [BI11-077]

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Cancer cell extravasation resembles the leukocyte recruitment during inflammation. Evidence suggests that cancer cells need to weaken the interendothelial junctions in order to cross the endothelial barrier. Several tumor-derived vasoactive compounds have been pointed out to drive this increase in vascular permeability: VEGF, Angptl4, CCL2, SDF-1, etc. Therefore, tumor cells have a wide repertoire of soluble factors to increase vascular permeability in order to colonize new tissues. Tumor soluble factors activate different signaling pathways to induce interendothelial junction disassembly, one common element is Src kinase. Here we summarize the relevant current knowledge about vascular permeability changes involved in tumor metastasis. (c) 2013 Elsevier Ireland Ltd. All rights reserved.

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