Abstract:Cancer stem cells and mutant p53 expressing tumors are highly dependent on the mevalonate pathway. Statins inhibit this pathway resulting in growth inhibition of these cells independent of inhibition of cholesterol biosynthesis and of protein farnesylation. Protein prenylation substrates farnesyl‐ and geranylgeranyl diphosphates are synthesized by the mevalonate pathway without producing their corresponding isoprenols. However, cells incorporate exogenously supplied isoprenols into mevalonate pathway metabolit… Show more
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