| Literature DB >> 31445892 |
Colin D Paul1, Kevin Bishop2, Alexus Devine1, Elliott L Paine1, Jack R Staunton1, Sarah M Thomas1, Joanna R Thomas1, Andrew D Doyle3, Lisa M Miller Jenkins1, Nicole Y Morgan4, Raman Sood2, Kandice Tanner5.
Abstract
Tumor cells encounter a myriad of physical cues upon arrest and extravasation in capillary beds. Here, we examined the role of physical factors in non-random organ colonization using a zebrafish xenograft model. We observed a two-step process by which mammalian mammary tumor cells showed non-random organ colonization. Initial homing was driven by vessel architecture, where greater numbers of cells became arrested in the topographically disordered blood vessels of the caudal vascular plexus (CVP) than in the linear vessels in the brain. Following arrest, bone-marrow- and brain-tropic clones exhibited organ-specific patterns of extravasation. Extravasation was mediated by β1 integrin, where knockdown of β1 integrin reduced extravasation in the CVP but did not affect extravasation of a brain-tropic clone in the brain. In contrast, silencing myosin 1B redirected early colonization from the brain to the CVP. Our results suggest that organ selectivity is driven by both vessel topography and cell-type-dependent extravasation. Published by Elsevier Inc.Entities:
Keywords: cancer metastasis; confined cell migration; extravasation; organ intravital imaging; organotropism; tissue architecture; tissue mechanics; topographical cues
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Year: 2019 PMID: 31445892 PMCID: PMC8276582 DOI: 10.1016/j.cels.2019.07.005
Source DB: PubMed Journal: Cell Syst ISSN: 2405-4712 Impact factor: 10.304