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Knockdown of AKT3 and PI3KCA by RNA interference changes the expression of the genes that are related to apoptosis and autophagy in T98G glioblastoma multiforme cells
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نویسنده
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paul-samojedny m. ,pudełko a. ,kowalczyk m. ,fila-daniłow a. ,suchanek-raif r. ,borkowska p. ,kowalski j.
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منبع
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pharmacological reports - 2015 - دوره : 67 - شماره : 6 - صفحه:1115 -1123
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چکیده
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Introduction glioblastoma multiforme (gbm) is the most malignant and invasive human brain tumor and it is characterized by a poor prognosis and short survival time. the pi3k/akt/pten signaling pathway plays a crucial role in gbm development and it is connected with the regulation of apoptosis and autophagy. akt is involved in various aspects of cancer cell biology such as cell survival,in addition to both apoptosis and autophagy. the current study was undertaken to examine the effect of the sirnas that target akt3 and pi3kca genes on the apoptosis and autophagy of t98g cells. methods t98g cells were transfected with akt3 and/or pi3kca sirnas. alterations in the mrna expression of apoptosis- and autophagy-related genes were analyzed using qrt-pcr. lc3iia protein-positive cells were identified using flow cytometry with specific antibodies. results our findings demonstrate for the first time that the sirnas that target akt3 and pi3kca change the expression of the genes that are related to apoptosis and autophagy and change the expression of the lc3iia protein in t98g cells. conclusions thus,there is a high probability that the knockdown of these genes induces apoptosis and autophagy in t98g cells,but further studies are necessary in order to clarify and check whether autophagy induction is a positive phenomenon for the treatment of gbm. © 2015 institute of pharmacology,polish academy of sciences. published by elsevier sp. z o.o. all rights reserved.
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کلیدواژه
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AKT3 and PI3KCA genes; Apoptosis; Autophagy; Glioblastoma multiforme; siRNA
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آدرس
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department of medical genetics,school of pharmacy,division of laboratory medicine in sosnowiec,medical university of silesia,katowice, Poland, department of clinical chemistry,laboratory diagnostics in medical university of silesia in katowice, Poland, department of medical genetics,school of pharmacy,division of laboratory medicine in sosnowiec,medical university of silesia,katowice, Poland, department of medical genetics,school of pharmacy,division of laboratory medicine in sosnowiec,medical university of silesia,katowice, Poland, department of medical genetics,school of pharmacy,division of laboratory medicine in sosnowiec,medical university of silesia,katowice, Poland, department of medical genetics,school of pharmacy,division of laboratory medicine in sosnowiec,medical university of silesia,katowice, Poland, department of medical genetics,school of pharmacy,division of laboratory medicine in sosnowiec,medical university of silesia,katowice, Poland
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Authors
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