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The presence of cross-beta-structure as a key determinant of carbonic anhydrase amyloid fibrils cytotoxicity

机译:交叉β结构的存在作为碳酸酐酶淀粉样蛋白原纤蛋白淀粉样细胞毒性的关键决定因素

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In most cases high cytotoxicity is characteristic of aggregates formed during lag phase of amyloid formation, whereas mature fibrils represent the depot of protein molecules incapable of damaging cell membranes. However, new experimental data show that in cases of some proteins the fibrils are the most toxic type of aggregates. Meanwhile, structural characteristics of cytotoxic fibrils and mechanisms of their cell damaging action are insufficiently explored. This work is dedicated to studying amyloid aggregation of bovine carbonic anhydrase (BCA) and effect of aggregates formed at different stages of amyloid formation on viability of the cells. Here we demonstrate that oligomers formed during lag phase do not decrease cell viability, whereas protofibrils and amyloids of BCA are cytotoxic. Obtained results allow concluding that toxicity of BCA aggregates is associated with the presence of amyloid cross-beta-structure, which signature is absorbance peak at low wavenumbers at FTIR spectra (1615-1630 cm(-1)). Our data suppose that cross-beta-core of BCA amyloid fibrils is responsible for their cytotoxicity. (C) 2020 Elsevier Inc. All rights reserved.
机译:在大多数情况下,高细胞毒性是在淀粉样蛋白形成的滞后阶段期间形成的聚集体的特征,而成熟的原纤维代表蛋白质分子的贮库不能破坏细胞膜。然而,新的实验数据显示,在一些蛋白质的情况下,原纤维是最有毒类型的聚集体。同时,细胞毒性原纤维的结构特征及其细胞破坏作用的机制是不够的。该作品专用于研究牛碳酸酐酶(BCA)的淀粉样蛋白聚集和在细胞的可生存能力的不同阶段形成的聚集体的作用。在这里,我们证明在滞后期期间形成的低聚物不会降低细胞活力,而BCA的原生纤维和BCA的淀粉样蛋白是细胞毒性。获得的结果允许结束性,BCA聚集体的毒性与淀粉样蛋白交叉β结构的存在有关,该致脂蛋白杂交结构在FTIR光谱(1615-1630cm(-1))处的低波纹中的吸光度峰值。我们的数据假设BCA淀粉样纤维的交叉β核是它们的细胞毒性。 (c)2020 Elsevier Inc.保留所有权利。

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