Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
5898237 | Cytokine | 2012 | 8 Pages |
As part of ongoing studies to obtain a global picture of invasion related events in colorectal liver metastases, here, we report our findings on gene expression of the pro-angiogenic subgroup of chemokines, the CXCL-ELR+ chemokines. Apart from their pro-angiogenic and chemoattractant function, these chemokines appear to also contribute to tumor cell transformation, growth and invasion. In our nude mouse model of colorectal liver metastases, we found CXCL1,2,3,5 and 8 (IL-8) to be up-regulated in the tumor cells of the invasion front as compared to the tumor cells in the inner parts of the tumor. ShRNA mediated down-regulation of the most prominently up-regulated group member, CXCL1/gro-alpha resulted in inhibition of cell viability, invasion and proliferation. In vivo, down-regulation of CXCL1 resulted in a nearly complete prevention of tumor growth in nude mice. Mechanistically, auto-regulatory mechanisms involving NF-kappaB and Akt appear to be involved in pro-tumorigenic functions of CXCL1.
⺠Expression of CXCL chemokines was studied in a mouse model of liver metastasis. ⺠CXCL1,2,3,5, and 8 genes were up-regulated in the invasion front of the tumor. ⺠CXCL1 down-regulation leads to reduced cell viability, invasion and proliferation. ⺠In vivo, knock down of CXCL1 resulted in prevention of tumor growth in nude mice. ⺠NF-kB and Akt may be involved in pro-tumorigenic functions of CXCL1.