Phosphatase and tensin AG-881 concentration homolog deleted on chromosome 10 (PTEN) is a tumor suppressor protein that negatively regulates the PI3K/AKT/mTOR signaling pathway and has been found to be mutated in many different cancers [94]. In human EC, disease-causing, inherited mutations of PTEN occur in up to 80% of type I EC cases [95]. When PTEN is mutated, AKT becomes constitutively active and this inhibits LY3039478 cost its downstream targets, such as TCS1/2, through excess
phosphorylation [6, 42]. Interestingly, liver kinase B1 (LKB1), another tumor suppressor, is responsible for the phosphorylation and activation of AMPK in the liver [96], and it has been reported that single nucleotide polymorphisms in LKB1 are associated with metformin resistance in women with PCOS [97]. Moreover, approximately 21% of all EC tumors lose LKB1 protein expression and this is correlated with see more increased activation of mTOR signaling [98]. Thus it is likely
that metformin can reverse or at least reduce EC cell survival and growth through activation of AMPK that interacts with the PI3K/AKT/mTOR signaling pathway and/or through direct inhibition of mTOR and its downstream targets. Another potentially important element in the mechanism through which metformin inhibits the development of EC is related to GLUT4 activity. It is known that glucose metabolism is vital for both normal and cancer cells and that insulin can stimulate glucose uptake by GLUTs. GLUT4 – an inducible, insulin-sensitive transport protein – facilitates the entry of glucose into cells [99]. It has been shown that although endometrial cells in women with and without PCOS express GLUT4, there is a progressive decrease in endometrial GLUT4 expression from healthy women
to normoinsulinemic PCOS women to hyperinsulinemic Glutamate dehydrogenase PCOS women [81, 100–103]. Glucose uptake depends on the level of GLUT4 expression [99], and treatment with metformin increases GLUT4 mRNA and protein expression in endometrial cells from women with PCOS in vivo [81, 103] and in vitro [104], possibly through the activation of AMPK and its downstream targets such as myocyte enhancer factor 2A [81]. Endometrial stromal cells are the paracrine regulators of epithelia-derived EC It is well known that endometrial malignancy results from the cancerous transformation of the epithelial cells that line the inner surface of uterus [43]. Moreover, numerous studies have shown that the stromal component is not only supportive of tumor growth but can also be a causative factor for the initiation and development of many human cancers [105].