Dual effect of Krasd12 knockdown on tumorigenesis : increased immune-mediated tumor clearance and abrogation of tumor malignancy

Activating mutations in the human KRAS proto-oncogene are acquired during the earliest stages of colorectal cancer development. If mutant KRAS is to be used as a target for therapy in colorectal cancer, tumor growth should depend on its continued presence. Here, we report that stable knockdown of Kr...

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Published inOncogene Vol. 24; no. 56; pp. 8338 - 8342
Main Authors SMAKMAN, Niels, VEENENDAAL, Liesbeth M, VAN DIEST, Paul, BOS, Rinke, OFFRINGA, Rienk, BOREL RINKES, Inne H. M, KRANENBURG, Onno
Format Journal Article
LanguageEnglish
Published Basingstoke Nature Publishing 15.12.2005
Nature Publishing Group
Subjects
Biological and medical sciences
Cancer
Cell cycle
Cell physiology
Cell transformation and carcinogenesis. Action of oncogenes and antioncogenes
Colorectal cancer
Colorectal carcinoma
Cytokines
Fundamental and applied biological sciences. Psychology
Immune clearance
Immune system
Interleukin 18
Malignancy
Molecular and cellular biology
Morbidity
Mutants
Mutation
RNA-mediated interference
Tumor cells
Tumorigenesis
Tumors
Netherlands
malignancy
Ras
colorectal
interleukin-18
Clearance
Malignant tumor
Carcinogenesis
immune- evasion
Interleukin 18
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Summary:Activating mutations in the human KRAS proto-oncogene are acquired during the earliest stages of colorectal cancer development. If mutant KRAS is to be used as a target for therapy in colorectal cancer, tumor growth should depend on its continued presence. Here, we report that stable knockdown of Kras(D12) in murine C26 colorectal cancer cells by RNA interference resulted in loss of transformed properties in vitro. The incidence of subcutaneous tumor formation was reduced by 60% and the lag time was increased sevenfold. Kras(D12)-knockdown tumors grew noninvasively and did not cause morbidity. Remarkably, some of the Kras(D12)-knockdown tumors regressed spontaneously, which rendered these mice resistant to parental C26 tumor growth. In immune-deficient hosts, the incidence of tumor formation by Kras(D12)-knockdown cells was 100%. None of these tumors regressed spontaneously. We conclude that the reduced incidence of tumor formation by Kras(D12)-knockdown cells is due to tumor cell clearance by the host immune system, but not to an intrinsic inability of these cells to grow out as tumors. Interestingly, Kras(D12) knockdown resulted in increased production of interleukin 18 (Il-18), an immune-stimulatory cytokine that has been implicated in limiting colorectal tumor formation. Thus, mutant Kras(D12) suppresses Il-18 production in colorectal tumor cells, which may contribute to evasion of the local immune system during tumor development.
ISSN:0950-9232
1476-5594
DOI:10.1038/sj.onc.1208995