PEAâ15 contributes to the clinicopathology and AKTâregulated cisplatin resistance in gastric cancer.
[No authors listed]
摘要
Phosphoprotein enriched in astrocytes 15 (PEAâ15) plays an important role in controlling biological behaviors of cancer cells. In the present study, we demonstrated that PEAâ15 was overexpressed in gastric cancer tissues and associated with tumor staging, differentiation, pathological types and the prognosis of patients. Gastric cancer cells expressed variable levels of PEAâ15 and its biâphosphorylation forms, pâPEAâ15 (Ser104) and pâPEAâ15 (Ser116). To gain insight into the functional role of PEAâ15, we generated cells stably depleted of PEAâ15 and resistant to cisplatin (CDDP) from human gastric cancer cells. PEAâ15 depletion inhibited cell proliferation by reducing cyclin D1 expression through the extracellular signalâregulated kinase (ERK) pathway, resulting in cell cycle arrest at the G1 phase, and induced apoptosis by activating caspaseâ8. PEAâ15 depletion also enhanced the inhibitory effect of CDDP that caused cell cycle arrest at the S phase and also enhanced the proâapoptotic activity of CDDP in vitro and in animal models of tumorigenesis and therapeutic effects. PEAâ15 and its phosphorylated forms were overexpressed in CDDPâresistant cells, which had higher levels of pâAKT. Specific inhibition of AKT by MK2206 reduced the expression of pâPEAâ15 at the Ser116 residue, resulting in sequential downregulation of pâERK1/2, cyclin D1 and caspaseâ8 activation. However, depletion of PEAâ15 had little effect on AKT expression or phosphorylation, or its downstream factors including p27, glycogen synthase kinase 3β and caspaseâ9, indicating that the regulatory effects between PEAâ15 and AKT were unidirectional. In summary, the results indicated that PEAâ15 expression was associated with clinicopathology and prognosis in gastric cancer and was regulated by AKT to participate in CDDP resistance, indicating that it may be a potential target for overcoming CDDP resistance in the treatment of gastric cancer.
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基因功能
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原始数据
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文献解读
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