Analyses of protein kinase C isoform expression in a colorectal cancer liver metastasis model Journal Article
| Authors: | Kuranami, M.; Cohen, A. M.; Guillem, J. G. |
| Article Title: | Analyses of protein kinase C isoform expression in a colorectal cancer liver metastasis model |
| Abstract: | Background: Protein kinase C (PKC), centrally involved in signal transdnction, has been implicated in colorectal carcinogenesis. The purpose of this study was to identify specific PKC isoform alterations associated with colorectal cancer metastases to the liver in an orthotopic transplantation nude mouse model. Materials and methods: Solid subcutaneous tumors from colorectal cancer cell lines were established in dorsal sites of nude mice (3 mice per cell Une) by subcutaneous injection of 107 cells (>90% viable). Orthotopic transplantation cecal tumors, representative of each passage (Sl-5) were examined for specific PKC isoform messenger ribonucleic acid (mRNA) expression. In addition, a cell line representative of passage S5 was established, characterized by light and electron microscopy, karyotype, clonogenicity, doubling time, and assayed for total PKC activity and PKC isoform mRNA expression. Results: After the fifth (S5) sequential orthotopic transplantation passage of the human colorectal cancer cell line, SW620, a highly metastatic clone was obtained. Relative to parental cells, metastatic SW620-S5 cells were less differentiated and demonstrated many more chromosomal abnormalities and lower clonogenicity. Total PKC activity was elevated in metastatic cells. In addition, specific PKC isoform mRNA alterations were noted: PKC-n (L) was abundantly expressed in the metastatic clone but absent from the parental cell Une; PKC-α, δ and Θ expression increased with serial orthotopic transplantation passages; PKC-δ remained unchanged, while PKC-β was absent. CONCLUSIONS: Metastases-specific PKC isoform alterations may serve as novel markers of metastases and treatment targets via specific PKC isoform modulation. © 1995. |
| Keywords: | signal transduction; controlled study; human cell; nonhuman; liver neoplasms; conference paper; colorectal cancer; mouse; animal; electron microscopy; mice; animal tissue; cell structure; gene expression; animal model; tumor cells, cultured; enzyme activity; mice, inbred balb c; colorectal neoplasms; liver metastasis; mice, nude; messenger rna; enzyme analysis; rna, messenger; protein kinase c; neoplasm transplantation; chromosome aberrations; tumor growth; chromosome analysis; karyotype; rna, neoplasm; isoenzymes; cancer transplantation; isoenzyme; colony formation; chromosome disorders; human; male; priority journal; support, non-u.s. gov't |
| Journal Title: | American Journal of Surgery |
| Volume: | 169 |
| Issue: | 1 |
| ISSN: | 0002-9610 |
| Publisher: | Elsevier Inc. |
| Date Published: | 1995-01-01 |
| Start Page: | 57 |
| End Page: | 64 |
| Language: | English |
| DOI: | 10.1016/s0002-9610(99)80110-x |
| PUBMED: | 7817999 |
| PROVIDER: | scopus |
| DOI/URL: | |
| Notes: | Article -- Export Date: 28 August 2018 -- Source: Scopus |
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