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聚合物化人血清白蛋白的合成及生物物理性质。

Synthesis and biophysical properties of polymerized human serum albumin.

机构信息

William G. Lowrie Dept. of Chemical and Biomolecular Engineering, The Ohio State University, Columbus, OH 43210, USA.

出版信息

Biotechnol Prog. 2011 Jan-Feb;27(1):290-6. doi: 10.1002/btpr.531. Epub 2011 Jan 6.

Abstract

The use of many plasma expanders (PEs) is often limited by undesirable side effects, such as red blood cell (RBC) aggregation (hydroxyethyl starch), nephrotoxicity (dextran), and extravasation (albumin). Despite its natural prevalence in the bloodstream, human serum albumin (HSA) can increase the risk of mortality when administered to patients with increased vascular permeability (i.e., patients suffering from burns, septic shock, and endothelial dysfunction). The harmful extravasation of HSA can be limited by polymerizing HSA to increase its molecular size. In this study, HSA was nonspecifically cross-linked with glutaraldehyde at different cross-link densities by varying the molar ratio of glutaraldehyde to HSA. The results of this study show that the weight-averaged molecular weight (MW), viscosity, and extent of RBC aggregation of polymerized HSA increases with increasing cross-link density, whereas the colloid osmotic pressure (COP) decreases with increasing cross-link density. Interestingly, circular dichroism measurements indicate that the secondary structure of HSA is unaffected by polymerization. Altogether, these results show that glutaraldehyde can effectively cross-link HSA to produce high MW polymers, yielding a novel series of potential PEs that exhibit low COP and high viscosity.

摘要

许多血浆扩容剂(PEs)的使用常常受到不良副作用的限制,如红细胞(RBC)聚集(羟乙基淀粉)、肾毒性(右旋糖酐)和渗出(白蛋白)。尽管人血清白蛋白(HSA)在血液中自然存在,但当给予血管通透性增加的患者(即烧伤、感染性休克和内皮功能障碍的患者)时,它会增加死亡率的风险。通过聚合 HSA 来增加其分子量,可以限制 HSA 的有害渗出。在这项研究中,HSA 与戊二醛在不同的交联密度下通过改变戊二醛与 HSA 的摩尔比进行非特异性交联。研究结果表明,聚合 HSA 的重均分子量(MW)、粘度和 RBC 聚集程度随交联密度的增加而增加,而胶体渗透压(COP)随交联密度的增加而降低。有趣的是,圆二色性测量表明 HSA 的二级结构不受聚合的影响。总的来说,这些结果表明戊二醛可以有效地交联 HSA 以产生高分子量聚合物,从而产生一系列具有低 COP 和高粘度的新型潜在 PEs。

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