4.7 Article

MT1-MMP collagenolytic activity is regulated through association with tetraspanin CD151 in primary endothelial cells

Journal

BLOOD
Volume 112, Issue 8, Pages 3217-3226

Publisher

AMER SOC HEMATOLOGY
DOI: 10.1182/blood-2008-02-139394

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Funding

  1. Ministerio de Educacion y Ciencia [BFU2005-08435/BMC, SAF2005-02228]
  2. Ayuda a la Investigacion Basica 2002 from Juan March Foundation
  3. European Network [MAIN LSHG-CT-2003-502935]
  4. Contrato-Investigador FIS 0019 from Instituto de Salud Carlos III

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MT1-MMP plays a key role in endothelial function, as underscored by the angiogenic defects found in MT1-MMP deficient mice. We have studied the molecular interactions that underlie the functional regulation of MT1-MMP. At lateral endothelial cell junctions, MT1-MMP colocalizes with tetraspanin CD151 (Tspan 24) and its associated partner alpha 3 beta 1 integrin. Biochemical and FRET analyses show that MT1-MMP, through its hemopexin domain, associates tightly with CD151, thus forming alpha 3 beta 1 integrin/CD151/MT1-MMP ternary complexes. siRNA knockdown of HUVEC CD151 expression enhanced MT1-MMP-mediated activation of MMP2, and the same activation was seen in ex vivo lung endothelial cells isolated from CD151-deficient mice. However, analysis of collagen degradation in these experimental models revealed a diminished MT1-MMP enzymatic activity in confined areas around the cell periphery. CD151 knockdown affected both MT1-MMP subcellular localization and its inclusion into detergent-resistant membrane domains, and prevented biochemical association of the metalloproteinase with the integrin alpha 3 beta 1. These data provide evidence for a novel regulatory role of tetraspanin microdomains on the collagenolytic activity of MT1-MMP and indicate that CD151 is a key regulator of MT1-MMP in endothelial homeostasis.

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