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马来酰亚胺聚乙二醇对血红蛋白表面修饰的分子模拟研究

Molecular modeling studies of surface decoration of hemoglobin by maleimide PEG.

作者信息

Prabhakaran M, Manjula Belur N, Acharya Seetharama A

机构信息

Department of Biomedical Engineering, Florida International University, Miami, Florida 33174, USA.

出版信息

Artif Cells Blood Substit Immobil Biotechnol. 2006;34(4):381-93. doi: 10.1080/10731190600769164.

Abstract

Surface decoration of hemoglobin (Hb) with six copies of PEG-5K employing thiolation mediated PEGylation platform neutralizes the vasoaconstricive activity of acellular Hb. The molecular size homogeneity of hexaPEGylated Hb, in spite of the fact that the PEGylation is distributed at multiple sites and PEGylation at each of the sites is not quantitative, is an unusual aspect of this PEGylation reaction. We have introduced three cys residues-Cys-13 (alpha), Cys-111 (alpha), and Cys-13 (beta)-onto Hb by molecular modeling. This new mutant Hb with four reactive Cys residues has been used to build molecular models of PEGylated Hbs with two, four, six, and eight PEG-chains of different masses. The calculated loss of surface area was used to design and gain insight into the structure and the surface shielding of PEGylated Hbs. The modeling shows the adequate surface coverage of the protein hemoglobin with six copies of PEG-5K chains and also exhibits more surface coverage of the hemoglobin as compared to that afforded by two copies of PEG-20K chains.

摘要

利用硫醇化介导的聚乙二醇化平台,用六个拷贝的PEG - 5K对血红蛋白(Hb)进行表面修饰,可中和无细胞血红蛋白的血管收缩活性。尽管聚乙二醇化分布在多个位点且每个位点的聚乙二醇化并非定量,但六聚乙二醇化血红蛋白的分子大小均一性是该聚乙二醇化反应的一个不同寻常之处。我们通过分子建模在血红蛋白上引入了三个半胱氨酸残基——Cys - 13(α)、Cys - 111(α)和Cys - 13(β)。这种带有四个反应性半胱氨酸残基的新型突变血红蛋白已被用于构建具有不同质量的两条、四条、六条和八条聚乙二醇链的聚乙二醇化血红蛋白的分子模型。计算得到的表面积损失用于设计并深入了解聚乙二醇化血红蛋白的结构和表面屏蔽。建模显示,六个拷贝的PEG - 5K链能充分覆盖蛋白质血红蛋白的表面,并且与两个拷贝的PEG - 20K链相比,血红蛋白的表面覆盖率更高。

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