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Enhanced sensitivity of multiple myeloma cells containing PTEN mutations to CCI-779
2002
Cancer Research
Recent work identifies the AKT kinase as a potential mediator of tumor expansion in multiple myeloma. The finding of PTEN mutations in several myeloma cell lines suggests that loss of PTEN function may be one mechanism by which AKT activity is increased in this disease. Because PTEN-deficient myeloma cells may have up-regulated activity of the mammalian target of rapamycin (mTOR), downstream of AKT, they may be particularly sensitive to mTOR inhibition. To test this hypothesis, we challenged
pmid:12208757
fatcat:v6pvj4jzl5bstdvlmf2scjuz7y