Suppression of human bladder cancer growth by increased expression of C-CAM1 gene in an orthotopic model

DI Kleinerman, CPN Dinney, WW Zhang, SH Lin… - Cancer research, 1996 - AACR
DI Kleinerman, CPN Dinney, WW Zhang, SH Lin, NT Van, JT Hsieh
Cancer research, 1996AACR
Recently, we demonstrated that an immunoglobulin-like cell adhesion molecule, C-CAM,
acts as a tumor suppressor in prostate cancer. It is known that C-CAM is expressed in many
epithelial cell types. In this study, we tested the possibility that C-CAM may also suppress
bladder cancer progression. We used an orthotopic tumor model, which provides a relevant
organ condition for examining the interaction between primary tumor cells and their
microenvironment; this interaction has a critical impact on the behavior of carcinoma. We …
Abstract
Recently, we demonstrated that an immunoglobulin-like cell adhesion molecule, C-CAM, acts as a tumor suppressor in prostate cancer. It is known that C-CAM is expressed in many epithelial cell types. In this study, we tested the possibility that C-CAM may also suppress bladder cancer progression. We used an orthotopic tumor model, which provides a relevant organ condition for examining the interaction between primary tumor cells and their microenvironment; this interaction has a critical impact on the behavior of carcinoma. We constructed a recombinant adenovirus expressing C-CAM1 (an isoform of C-CAM) and infected the 253J B-V cell line, a tumorigenic human bladder carcinoma subline. In vitro, C-CAM1 protein was detected in C-CAM1 adenovirus-infected cells but not in antisense control virus-infected cells, and the levels of expression showed dose dependency. When these cells were injected orthotopically in nude mice, we found that the increased expression of C-CAM1 in the 253J B-V cells repressed the growth of 253J B-V-induced tumors. Taken together, these data indicate that C-CAM1 is a potent tumor suppressor in human bladder cancer.
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