Preferential Attachment of Peritoneal Tumor Metastases to Omental Immune Aggregates and Possible Role of a Unique Vascular Microenvironment in Metastatic Survival and Growth

Scott A. Gerber^*, Viktoriya Y. Rybalko^*, Chad E. Bigelow, Amit A. Lugade^*, Thomas H. Foster, John G. Frelinger^* and Edith M. Lord^*

From the Departments of Microbiology and Immunology^* and Imaging Sciences, University of Rochester Medical Center, Rochester, New York

Controlling metastases remains a critical problem in cancerbiology. Within the peritoneal cavity, omental tissue is a commonsite for metastatic disease arising from intraperitoneal tumors;however, it is unknown why this tissue is so favorable for metastatictumor growth. Using five different tumor cell lines in threedifferent strains of mice, we found that the omentum was a majorsite of metastases growth for intraperitoneal tumors. Furthermore,initial attachment and subsequent growth were limited to specificsites within the omentum, consisting of organized aggregatesof immune cells. These immune aggregates contained a complexnetwork of capillaries exhibiting a high vascular density, whichappear to contribute to the survival of metastatic cells. Wefound that the vasculature within these aggregates containedCD105⁺ vessels and vascular sprouts, both indicators of activeangiogenesis. A subset of mesothelial cells situated atop theimmune aggregates was found to be hypoxic, and a similar proportionwas observed to secrete vascular endothelial growth factor-A.These data provide a physiological mechanism by which metastatictumor cells preferentially grow at sites rich in proangiogenicvessels, apparently stimulated by angiogenic factors producedby mesothelial cells. These sites provide metastatic cells witha microenvironment highly conducive to survival and subsequentgrowth.

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