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Involvement of tumor cell integrin alpha v beta 3 in hematogenous metastasis of human melanoma cells
Authors:Felding-Habermann Brunhilde  Fransvea Emilia  O'Toole Timothy E  Manzuk Lisa  Faha Barbara  Hensler Mary
Affiliation:(1) Department of Molecular and Experimental Medicine, The Scripps Research Institute, La Jolla, California, USA;(2) Present address: Clinica Medica II, Bari, Italy;(3) Present address: Department of Molecular Cardiology, Cleveland Clinic Foundation, Ohio, USA;(4) IXSYS Inc., San Diego, California, USA;(5) Present address: Biosite Diagnostics, San Diego, California, USA;(6) Present address: Canji, Inc., San Diego, California, USA;(7) Present address: Nereus Pharmaceuticals, San Diego, California, USA
Abstract:
Early metastasis is the primary cause of death in melanoma patients. The adhesion receptor integrin αvβ3 contributes to tumor cell functions that are potentially involved in melanoma growth and metastasis. We tested whether integrin αvβ3 supports metastasis of human melanoma cells when injected into the bloodstream of immune deficient mice. Comparing variants of the same melanoma cell type that expressed either αvβ3, αIIbβ3 or no β3 integrin, we found that only αvβ3 strongly supported metastasis. Inhibition of tumor cell αvβ3 function reduced melanoma metastasis significantly and prolonged animal survival. To understand mechanisms that allow αvβ3, but not αIIbβ3 to support melanoma metastasis, we analyzed proteolytic and migratory activities of the melanoma cell variants. Melanoma cells expressing αvβ3, but not those expressing αIIbβ3 or no β3 integrin, produced the active form of metalloproteinase MMP-2 and expressed elevated mRNA levels of MT1-MMP and TIMP-2. This indicates an association between αvβ3 expression and protease processing. Furthermore, αvβ3 expression was required for efficient melanoma cell migration toward the matrix proteins fibronectin and vitronectin. The results suggest that expression of integrin αvβ3 promotes the metastatic phenotype in human melanoma by supporting specific adhesive, invasive and migratory properties of the tumor cells and that the related integrin αIIbβ3 cannot substitute for αvβ3 in this respect. This revised version was published online in July 2006 with corrections to the Cover Date.
Keywords:α    3  α  IIbβ  3  integrin  melanoma  metastasis  MMP-2
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