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大分子拥挤对糖化条件下血红蛋白聚集倾向和结构稳定性的影响。

Consequence of macromolecular crowding on aggregation propensity and structural stability of haemoglobin under glycating conditions.

机构信息

Department of Biochemistry, Faculty of Life Sciences, Aligarh Muslim University, Aligarh 202002, U.P., India.

Department of Biochemistry, Faculty of Life Sciences, Aligarh Muslim University, Aligarh 202002, U.P., India.

出版信息

Int J Biol Macromol. 2020 Nov 1;162:1044-1053. doi: 10.1016/j.ijbiomac.2020.06.127. Epub 2020 Jun 15.

Abstract

Cell interiors are extremely congested with biological macromolecules exerting crowding effect, influencing various physiognomies of protein life. Present work deals with effect of crowding on folding behaviour of haemoglobin (Hb) under glycating conditions. Macromolecular crowding was mimicked by concentrated solutions of dextran 70. Hb with 0.2 M fructose and ribose was incubated separately for 96 h in dilute and crowded solution to analyse conformational changes. Reduced intrinsic and ANS fluorescence, decreased Soret absorbance, enhanced turbidity, browning of protein, red shift in ThT and Congo red spectra significantly unveiled protein aggregation. FTIR and CD results revealed transition from α-helix to β-sheets confirming aggregation. Transmission electron microscopy exhibited incidence of aggregates. Macromolecular crowding was witnessed to defend conformational stability of native Hb under stress condition at 100 mg/ml dextran, noticeably indicating deceleration of aggregation. Stabilising effect of crowding was marginally better in fructosylated Hb than with ribose due to difference in their glycation potential. Contrarily, in over-crowded solution where dextran concentration was 500 mg/ml, heightened aggregation was perceived implying concentration dependant, dual nature of macromolecular crowding. The novelty of this study lies in idea of considering macromolecular crowding as a key player in regulation of protein stability which was safely ignored previously.

摘要

细胞内部充满了生物大分子,产生拥挤效应,影响蛋白质的各种表现形式。目前的工作研究了拥挤效应对糖化条件下血红蛋白(Hb)折叠行为的影响。通过使用浓度为 70 的葡聚糖溶液模拟大分子拥挤。将含有 0.2 M 果糖和核糖的 Hb 分别在稀溶液和拥挤溶液中孵育 96 h,以分析构象变化。还原型内源和 ANS 荧光、Soret 吸收减少、浊度增加、蛋白褐变、ThT 和刚果红光谱红移显著揭示了蛋白聚集。FTIR 和 CD 结果表明从α-螺旋向β-折叠的转变证实了聚集的发生。透射电子显微镜显示出聚集物的出现。大分子拥挤被证明可以在 100 mg/ml 葡聚糖的应激条件下保护天然 Hb 的构象稳定性,明显表明聚集的速度减缓。由于糖化潜力的差异,拥挤对果糖基化 Hb 的稳定作用略优于核糖基化 Hb。相反,在拥挤度更高的溶液中(葡聚糖浓度为 500 mg/ml),聚集程度增加,这表明大分子拥挤具有浓度依赖性的双重性质。这项研究的新颖之处在于将大分子拥挤视为调节蛋白质稳定性的关键因素,而这一因素之前被安全地忽略了。

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