High-density lipoproteins (HDLs) play an important role in human health through the metabolism and trafficking of cholesterol as well as providing the feedstocks for steroid hormone biosynthesis. These particles contain proteins, primarily Apo-AI and phospholipid and progress through various structural forms including 'lipid-poor', 'discoidal' and 'spherical' entities as cholesterol esters and lipid are incorporated. The discoidal form of HDL is stabilized in solution by two encircling belts of Apo-AI. Previous protein engineering of the Apo-AI sequence has led to a series of amphipathic helical proteins, termed membrane scaffold proteins (MSPs), which have shown great value in assembling nanoscale soluble membrane bilayers, termed Nanodiscs, of homogeneous size and composition and in the assembly of numerous integral membrane proteins for biophysical and biochemical investigations. In this communication we document a protein engineering approach to generate and optimize an extended polypeptide MSP, which will self-assemble phospholipids into larger Nanodiscs with diameters of 16-17 nm. We extensively characterize these structures by size exclusion chromatography and solution X-ray scattering.
Engineering extended membrane scaffold proteins for self-assembly of soluble nanoscale lipid bilayers.
工程化延伸膜支架蛋白,用于可溶性纳米级脂质双层的自组装
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作者:Grinkova Yelena V, Denisov Ilia G, Sligar Stephen G
| 期刊: | Protein Engineering Design & Selection | 影响因子: | 3.400 |
| 时间: | 2010 | 起止号: | 2010 Nov;23(11):843-8 |
| doi: | 10.1093/protein/gzq060 | 研究方向: | 免疫/内分泌 |
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