1996
DOI: 10.1074/jbc.271.10.5892
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Role of β3 Integrins in Melanoma Cell Adhesion to Activated Platelets under Flow

Abstract: Mechanisms mediating tumor cell attachment to the vessel wall under flow conditions are largely unknown. Therefore we analyzed the ability of human melanoma cells to adhere to an immobilized matrix during blood flow and determined the role of platelets in this process. In a parallel plate flow chamber, M21 melanoma cells were suspended in human blood and perfused over a collagen I matrix at a wall shear rate of 50 s ؊1 (2 dynes/ cm 2 ) to simulate venous flow over a thrombogenic surface. Melanoma cell interact… Show more

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Cited by 151 publications
(157 citation statements)
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“…Expression of activated ␣v␤3 promotes tumor cell arrest during blood flow and causes a drastic increase in metastatic activity (9,15,23). Integrin activation modulates ligand recognition, cell migration, and invasion (6,7,(24)(25)(26) and endows tumor cells with crucial functions that permit or facilitate a disseminating phenotype.…”
Section: Discussionmentioning
confidence: 99%
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“…Expression of activated ␣v␤3 promotes tumor cell arrest during blood flow and causes a drastic increase in metastatic activity (9,15,23). Integrin activation modulates ligand recognition, cell migration, and invasion (6,7,(24)(25)(26) and endows tumor cells with crucial functions that permit or facilitate a disseminating phenotype.…”
Section: Discussionmentioning
confidence: 99%
“…To analyze a clinical significance of ␣v␤3 activation, we established primary metastatic cells from blood samples of stage IV breast cancer patients. These cells express integrin ␣v␤3 in an activated functional form as the receptor supports tumor cell arrest during blood flow (9,23). In these cell models, ␣v␤3 activation caused enhanced breast cancer cell migration toward fibronectin (9), vitronectin, and fibrinogen.…”
Section: Discussionmentioning
confidence: 99%
“…For example, earlier studies examining the role of nonexogenously stimulated platelets in tumor cell adhesion to ECM components under flow conditions did not indicate secondary tethering as a possible adhesion pathway. Rather, tumor cells were often found in large platelet or platelet-leukocyte thrombi (13,14), in which platelets deposited on ECM proteins supported firm adhesion of the cancerous cells (13,14). Without platelets, the tumor cells were unable to attach to the ECM proteins under consideration.…”
Section: Discussionmentioning
confidence: 99%
“…Neither of these investigations identified a role for platelets in mediating secondary tethering whereby a platelet transiently bridges an endothelium-adherent with a free-flowing leukocyte before the latter attaches to the endothelial surface. Similarly, platelet-tumor cell perfusions over components of the extracellular matrix (ECM) indicate an important role for platelets in promotion of tumor cell adhesion by bridging tumor cells to the ECM, yet secondary tethering was not evaluated (9,13,14).…”
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confidence: 99%
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