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The role of the intravascular microenvironment in spontaneous metastasis development

โœ Scribed by Qingbei Zhang; Meng Yang; Jikun Shen; Lynnette M. Gerhold; Robert M Hoffman; H.Rosie Xing


Book ID
102862987
Publisher
John Wiley and Sons
Year
2010
Tongue
French
Weight
926 KB
Volume
126
Category
Article
ISSN
0020-7136

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โœฆ Synopsis


Abstract

Metastasis is primarily responsible for the morbidity and mortality of cancer. Improved therapeutic outcomes and prognosis depend on improved understanding of mechanisms regulating the establishment of early metastasis. In this study, use of green fluorescent protein (GFP)โ€expressing PCโ€3 orthotopic model of human prostate cancer and two complementary fluorescence in vivo imaging systems (Olympus OV100 and VisEn FMT) allowed for the first time realโ€time characterization of cancer cellโ€“endothelium interactions during spontaneous metastatic colonization of the liver and lung in live mice. We observed that prior to the detection of extraโ€vascular metastases, GFPโ€expressing PCโ€3 cancer cells resided initially inside the blood vessels of the liver and the lung, where they proliferated and expressed Kiโ€67 and exhibited matrix metalloprotenases (MMP) activity. Thus, the intravascular cancer cells produced their own microenvironment, where they could continue to proliferate. Extravasation occurred earlier in the lung than in the liver. Our results demonstrate that the intravascular microenvironment is a critical staging area for the development of metastasis that later can invade the parenchyma. Intravascular tumor cells may represent a therapeutic target to inhibit the development of extravascular metastases. Therefore, this imageable model of intravascular metastasis may be used for evaluation of novel antiโ€metastatic agents.


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