Pająk Beata, Kania Elżbieta, Orzechowski Arkadiusz
Electron Microscopy Platform, Mossakowski Medical Research Centre, Polish Academy of Sciences, Pawińskiego 5, 02-106 Warsaw, Poland.
Electron Microscopy Platform, Mossakowski Medical Research Centre, Polish Academy of Sciences, Pawińskiego 5, 02-106 Warsaw, Poland ; Department of Physiological Sciences, Faculty of Veterinary Medicine, Warsaw University of Life Sciences (SGGW), Nowoursynowska 159, 02-776 Warsaw, Poland.
Biomed Res Int. 2015;2015:746092. doi: 10.1155/2015/746092. Epub 2015 Mar 10.
Pheochromocytoma PC-12 cells are immune to physiological stimuli directed to evoke programmed cell death. Besides, metabolic inhibitors are incapable of sensitizing PC-12 cells to extrinsic or intrinsic apoptosis unless they are used in toxic concentrations. Surprisingly, these cells become receptive to cell deletion after human APP-sw gene expression. We observed reduced cell viability in GFP vector + APP-sw-nucleofected cells (drop by 36%) but not in GFP vector - or GFP vector + APP-wt-nucleofected cells. Lower viability was accompanied by higher expression of Aβ 1-16 and elevated secretion of Aβ 1-40 (in average 53.58 pg/mL). At the ultrastructural level autophagy-like process was demonstrated to occur in APP-sw-nucleofected cells with numerous autophagosomes and multivesicular bodies but without autolysosomes. Human APP-sw gene is harmful to PC-12 cells and cells are additionally driven to incomplete autophagy-like process. When stimulated by TRAIL or nystatin, CLU protein expression accompanies early phase of autophagy.
嗜铬细胞瘤PC - 12细胞对旨在引发程序性细胞死亡的生理刺激具有免疫性。此外,代谢抑制剂无法使PC - 12细胞对外源性或内源性凋亡敏感,除非使用毒性浓度。令人惊讶的是,在人类APP - sw基因表达后,这些细胞变得易于发生细胞清除。我们观察到,在转染了GFP载体 + APP - sw的细胞中细胞活力降低(下降了36%),而在转染了GFP载体 - 或GFP载体 + APP - wt的细胞中则没有。较低的活力伴随着Aβ 1 - 16表达增加以及Aβ 1 - 40分泌升高(平均为53.58 pg/mL)。在超微结构水平上,在转染了APP - sw的细胞中证明发生了自噬样过程,有大量自噬体和多囊泡体,但没有自溶酶体。人类APP - sw基因对PC - 12细胞有害,并且细胞还被驱动进入不完全的自噬样过程。当受到TRAIL或制霉菌素刺激时,CLU蛋白表达伴随着自噬的早期阶段。
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