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由替西罗莫司诱导的人血清白蛋白向原纤维聚集物的全球转变:对肾癌治疗药物影响的深入了解。

Global transition of human serum albumin to prefibrillar aggregates induced by temsirolimus: Insight into implications of anti-renal cancer drug.

机构信息

Department of Biochemistry, F/O Life Sciences, Aligarh Muslim University, Aligarh, India.

出版信息

J Mol Recognit. 2018 Apr;31(4). doi: 10.1002/jmr.2688. Epub 2017 Nov 27.

Abstract

In our study, we have characterized the prefibrillar aggregates of human serum albumin (HSA) induced by temsirolimus, anti-renal cancer drug. Molecular docking was retorted to confirm binding of HSA and temsirolimus. Temsirolimus caused the structural transition of native HSA to non-native species after prolonged incubation of 20 days. These non-native species were characterized as prefibrillar aggregates as evident by decreased intrinsic fluorescence and enhanced 8-anilino-1-naphthalene-sulphonic acid (ANS) fluorescence. Further, enhanced thioflavin T fluorescence and shift in congo red (CR) spectra of temsirolimus-incubated HSA as compared to native HSA are suggestive of global transition of HSA in presence of temsirolimus towards prefibrillar aggregates. Circular dichroism spectroscopy revealed α to β transition upon prolonged incubation with temsirolimus suggesting the formation of prefibrillar aggregates as aggregates are known to possess high β content. Scanning electron microscopy confirmed these non-native species to be prefibrillar aggregates evident by observed sheath-like structures. Comet assay was retorted to confirm genotoxic nature of these prefibrillar aggregates; DNA damage was observed for temsirolimus-incubated HSA confirming the genotoxic nature of prefibrillar aggregates. These prefibrillar aggregates are observed at heart of many pathological conditions, thus making our study clinically significant.

摘要

在我们的研究中,我们对由替西罗莫司(一种抗肾癌药物)诱导的人血清白蛋白(HSA)预纤维状聚集体进行了特征描述。采用分子对接方法来证实 HSA 与替西罗莫司的结合。经过 20 天的长时间孵育,替西罗莫司导致天然 HSA 发生结构转变为非天然构象。这些非天然构象表现出预纤维状聚集体的特征,表现为内源荧光的降低和 8-苯胺基-1-萘磺酸(ANS)荧光的增强。此外,与天然 HSA 相比,替西罗莫司孵育的 HSA 中硫代黄素 T 荧光的增强和刚果红(CR)光谱的移动表明,在替西罗莫司存在下,HSA 发生了从天然状态到预纤维状聚集体的整体转变。圆二色性光谱分析表明,在与替西罗莫司长时间孵育后发生了从 α 到 β 的转变,表明形成了预纤维状聚集体,因为聚集体通常具有较高的 β 含量。扫描电子显微镜证实了这些非天然构象为预纤维状聚集体,这可以通过观察到的鞘状结构来证明。彗星试验用于证实这些预纤维状聚集体的遗传毒性性质;替西罗莫司孵育的 HSA 中观察到 DNA 损伤,证实了预纤维状聚集体的遗传毒性性质。这些预纤维状聚集体存在于许多病理条件的核心,因此我们的研究具有临床意义。

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