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Imaging of radiation effects on cellular 26S proteasome function in situ.

机译:辐射对细胞26S蛋白酶体功能的原位成像。

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摘要

PURPOSE: The classical radiobiological paradigm is that DNA is the target for cell damage caused by ionising radiation. However, evidence is accumulating that other constituents, such as the membrane, organelles, and proteins, are also important targets. We have shown that the isolated 26S proteasome is one such target and here we wish to substantiate it within the cell, in situ. MATERIALS AND METHODS: We used confocal microscopy to quantitatively detect and subcellularly localise radiation-induced 26S proteasome inhibition in cells expressing an ornithine decarboxylase degron that targets a fused Zoanthus species green (ZsGreen) fluorescent protein reporter specifically to the 26S proteasome. RESULTS: Exposure of cells to a range of radiation doses, even as low as 0.05 Gy inhibited 26S activity within minutes. Initially, punctate nuclear ZsGreen fluorescence was observed that became cytoplasmic after seven hours -- a pattern distinct from the diffuse homogeneous fluorescence of cells incubated in the conventional proteasome inhibitor MG-132. CONCLUSIONS: Our study clearly indicates that the 26S proteasome is a radiation target with physiological consequences and introduces a new perspective in mechanistic investigations of cellular responses to stresses.
机译:目的:经典的放射生物学范例是DNA是电离辐射引起的细胞损伤的靶标。但是,越来越多的证据表明,其他成分(例如膜,细胞器和蛋白质)也是重要的靶标。我们已经表明,分离的26S蛋白酶体就是这样一种靶标,在这里我们希望在细胞内原位证实它。材料与方法:我们使用共聚焦显微镜在表达鸟氨酸脱羧酶地龙的细胞中定量检测并亚细胞定位了辐射诱导的26S蛋白酶体抑制,该鸟氨酸靶向融合的Zoanthus种绿色(ZsGreen)荧光蛋白报道分子,专门针对26S蛋白酶体。结果:细胞暴露于一定范围的辐射剂量下,即使在低至0.05 Gy的辐射下,也能在几分钟内抑制26S活性。最初,观察到点状核ZsGreen荧光在七个小时后变成细胞质,这种模式不同于在常规蛋白酶体抑制剂MG-132中孵育的细胞的弥散均匀荧光。结论:我们的研究清楚地表明26S蛋白酶体是具有生理后果的辐射靶标,并在细胞对应激反应的机制研究中引入了新的观点。

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