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人血清白蛋白(HSA)在水面上单分子层的结构、形态和可逆滞后性质。

Structure, morphology and reversible hysteresis nature of human serum albumin (HSA) monolayer on water surface.

机构信息

Soft Nano Laboratory, Physical Sciences Division, Institute of Advanced Study in Science and Technology, Vigyan Path, Paschim Boragaon, Garchuk, Guwahati, Assam 781035, India.

Soft Nano Laboratory, Physical Sciences Division, Institute of Advanced Study in Science and Technology, Vigyan Path, Paschim Boragaon, Garchuk, Guwahati, Assam 781035, India.

出版信息

Int J Biol Macromol. 2021 Mar 31;174:377-384. doi: 10.1016/j.ijbiomac.2021.01.131. Epub 2021 Jan 21.

DOI:10.1016/j.ijbiomac.2021.01.131
PMID:33485891
Abstract

Compression-decompression surface pressure (π)-specific molecular area (A) isotherm cycle of human serum albumin (HSA) monolayer is performed on water surface at four different subphase pH conditions, i.e., below and above the isoelectric point (pI ≈ 4.7) of HSA molecule. For all pH conditions, the decompression curve nearly follows the compression curve, however, at pH ≈ 5.0, hysteresis is observed at higher surface pressure. Out-of-plane structures and in-plane morphologies obtained from the X-ray reflectivity and AFM studies show that only the film thickness variation takes place with the change in surface pressure, which is also evidenced from the BAM images. With increase in surface pressure, the oblate-shaped HSA molecules start tilting making an angle with the water surface and as the monolayer is decompressed the molecules regain their initial untilted monomolecular configuration. Depending upon the subphase pH and local surface charge of the specific protein molecule, electrostatic repulsive interaction dominates over the van der Waals attraction and as a result decompression curve follows the compression curve as the molecules repel each other, however, closer to the isoelectric point as strength of the interactions reverses, a hysteresis is obtained at higher surface pressure and accordingly monolayer behaviour modifies on the water surface.

摘要

人血清白蛋白(HSA)单层在水表面上进行压缩-减压表面压力(π)-比分子面积(A)等温循环,在四个不同亚相 pH 条件下进行,即低于和高于 HSA 分子的等电点(pI≈4.7)。对于所有 pH 条件,减压曲线几乎跟随压缩曲线,然而,在 pH≈5.0 时,在较高的表面压力下观察到滞后。从 X 射线反射率和 AFM 研究中获得的面外结构和面内形态表明,仅随着表面压力的变化而发生膜厚度变化,这也从 BAM 图像中得到证明。随着表面压力的增加,扁球形 HSA 分子开始倾斜,与水面形成一定角度,当单层减压时,分子恢复初始未倾斜的单分子构型。根据亚相 pH 和特定蛋白质分子的局部表面电荷,静电排斥相互作用超过范德华吸引力,因此,随着分子相互排斥,减压曲线跟随压缩曲线,然而,更接近等电点时,相互作用的强度反转,在较高的表面压力下获得滞后,并且相应地,单层在水面上的行为发生改变。

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