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Membrane scaffold proteins and tethered membrane proteins

机译:膜支架蛋白和束缚膜蛋白

摘要

Membrane proteins are difficult to express in recombinant form, purify, and characterize, at least in part due to their hydrophobic or partially hydrophobic properties. Membrane scaffold proteins (MSP) assemble with target membrane or other hydrophobic or partially hydrophobic proteins or membrane fragments to form soluble nanoscale particles which preserve their native structure and function; they are improved over liposomes and detergent micelles. In the presence of phospholipid, MSPs form nanoscopic phospholipid bilayer disks, with the MSP stabilizing the particle at the perimeter of the bilayer domain. The particle bilayer structure allows manipulation of incorporated proteins in solution or on solid supports, including for use with such surface-sensitive techniques as scanning probe microscopy or surface plasmon resonance. The nanoscale particles facilitate pharmaceutical and biological research, structure/function correlation, structure determination, bioseparation, and drug discovery.
机译:膜蛋白很难以重组形式表达,纯化和表征,至少部分由于其疏水或部分疏水特性。膜支架蛋白(MSP)与目标膜或其他疏水性或部分疏水性蛋白或膜片段组装在一起,形成可保留其天然结构和功能的可溶性纳米级颗粒;它们比脂质体和去污剂胶束有所改进。在磷脂的存在下,MSP形成纳米级的磷脂双层盘,MSP在双层结构域的周围稳定颗粒。颗粒双层结构允许处理溶液中或固体支持物上掺入的蛋白质,包括与诸如扫描探针显微镜或表面等离振子共振之类的表面敏感技术一起使用。纳米级颗粒有助于药物和生物学研究,结构/功能关联,结构确定,生物分离和药物发现。

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