4.6 Article

Repositioning of simvastatin for diabetic colon cancer: role of CDK4 inhibition and apoptosis

Journal

MOLECULAR AND CELLULAR BIOCHEMISTRY
Volume 478, Issue 10, Pages 2337-2349

Publisher

SPRINGER
DOI: 10.1007/s11010-023-04663-w

Keywords

Therapeutic switching; 1; 2 Dimethylhydrazine; Streptozotocin; CDK4; Annexin V-FITC

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The study evaluated the role of simvastatin in colon cancer associated with type 2 diabetes mellitus. It was found that simvastatin controlled diabetes and colon cancer in animal models, reduced CDK4 mRNA expression in colon tissues, and induced apoptosis. These findings suggest that simvastatin could be considered for repositioning in the treatment of colon cancer in patients with diabetes mellitus.
There is increased risk of colon cancer in both men and women having diabetes. The objective of the study was to evaluate the role of simvastatin in colon cancer associated with type 2 diabetes mellitus. Diabetes was induced by administering high fat diet with low dose streptozotocin model. 1,2 dimethylhydrazine (25 mg/kg, sc) was used for colon cancer induction. MTT assay, scratch assay, clonogenic assay and annexin V-FITC assay using flow cytometry were performed on HCT-15 cell line. Simvastatin controlled diabetes and colon cancer in animal models and reduced mRNA expression of CDK4 in colon tissues. In vitro studies revealed that simvastatin showed a decrease in cell viability and produced dose dependent decrease in clone formation. There was decrease in the rate of migration with increase in concentration of simvastatin in scratch assay. Moreover, simvastatin induced apoptosis as depicted from annexin V-FITC assay using flow cytometry as well as that revealed by tunnel assay. Our data suggest that simvastatin exhibits protective role in colon cancer associated with diabetes mellitus and acts possibly via down regulation of CDK4 and induction of apoptosis and hence can be considered for repositioning in diabetic colon cancer.

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