Compensation mechanism in tumor cell migration

Wolf, Katarina; Mazo, Irina B.; Leung, Harry; Engelke, Katharina; Andrian, Ulrich H. von; Deryugina, Elena I.; Strongin, Alex Y.; Bröcker, Eva‐B.; Friedl, Peter

doi:10.1083/jcb.200209006

articleThe Journal of Cell BiologyJan 13, 2003BRONZE OA

Compensation mechanism in tumor cell migration

KWKatarina Wolf IBIrina B. Mazo HLHarry Leung KEKatharina Engelke UHUlrich H. von Andrian

University of Würzburg · Children's Hospital · +3 more institutions

PubMed

Indexed incrossrefpubmed

Abstract

Invasive tumor dissemination in vitro and in vivo involves the proteolytic degradation of ECM barriers. This process, however, is only incompletely attenuated by protease inhibitor-based treatment, suggesting the existence of migratory compensation strategies. In three-dimensional collagen matrices, spindle-shaped proteolytically potent HT-1080 fibrosarcoma and MDA-MB-231 carcinoma cells exhibited a constitutive mesenchymal-type movement including the coclustering of beta 1 integrins and MT1-matrix metalloproteinase (MMP) at fiber bindings sites and the generation of tube-like proteolytic degradation tracks. Near-total inhibition of MMPs, serine proteases, cathepsins, and other proteases, however, induced a…

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Topics

Keywords

Biology
Cell biology
Proteases
Cell migration
Cathepsin
Matrix metalloproteinase
Integrin
Extracellular matrix

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