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首页> 外文期刊>Biomacromolecules >Formation of Complexes between the Conjugated Polyelectrolyte Poly{(9,9-bis(6'-N,N,N- trimethylammonium)hexyl)fluorene-phenylene} Bromide (HTMA-PFP) and Human Serum Albumin
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Formation of Complexes between the Conjugated Polyelectrolyte Poly{(9,9-bis(6'-N,N,N- trimethylammonium)hexyl)fluorene-phenylene} Bromide (HTMA-PFP) and Human Serum Albumin

机译:共轭聚电解质聚{(9,9-双(6'-N,N,N-三甲基铵)己基)芴-亚苯基}溴化物(HTMA-PFP)与人血清白蛋白之间的配合物形成

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摘要

The interaction between the conjugated polyelectrolyte poly) ([9,9-bis(6'-N,N,N-trimethylammonium)hexyl]fluorene-phenylene) bromide (HTMA-PFP) and human serum albumin (HSA) has been investigated from changes observed in both the spectroscopic properties of HTMA-PFP and the intrinsic fluorescence of HSA. Absorption and fluorescence spectra of HTMA-PFP suggest that HTMA-PFP and HSA form polymer-protein complexes due to electrostatic interactions between the cationic side chains of HTMA-PFP and the negatively charged surface of the protein. Interaction between both macromolecules induces an increase in the fluorescence signal of HTMA-PFP, which suggests that hydrophobic forces also contribute to the polymer-protein complex stabilization. In addition, this interaction causes a decrease in the HSA fluorescence, partially due to static quenching and energy transfer between both macromolecules. Effects of HTMA-PFP on the thermal stability and protein conformation were explored from CD experiments. Results indicate that as polymer is added it binds to HSA and initiates unfolding. This unfolding process induces HTMA-PFP chains to become more extended, disrupting backbone interactions and increasing polymer fluorescence intensity.
机译:共轭聚电解质聚)([9,9-双(6'-N,N,N-三甲基铵)己基]芴-亚苯基)溴(HTMA-PFP)与人血清白蛋白(HSA)之间的相互作用已得到研究。 HTMA-PFP的光谱性质和HSA的固有荧光均观察到变化。 HTMA-PFP的吸收和荧光光谱表明,由于HTMA-PFP的阳离子侧链与蛋白质带负电荷的表面之间存在静电相互作用,因此HTMA-PFP和HSA形成了聚合物-蛋白质复合物。两个大分子之间的相互作用导致HTMA-PFP的荧光信号增加,这表明疏水力也有助于聚合物-蛋白质复合物的稳定。另外,这种相互作用导致HSA荧光的降低,部分是由于两个大分子之间的静态猝灭和能量转移。从CD实验中探索了HTMA-PFP对热稳定性和蛋白质构象的影响。结果表明,随着聚合物的添加,它与HSA结合并开始展开。这种展开过程诱导HTMA-PFP链变得更延伸,破坏骨架相互作用并增加聚合物荧光强度。

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