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Secretion of slow-folding proteins by a Type 1 secretion system

机译:1型分泌系统分泌缓慢折叠的蛋白质

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Protein production through dedicated secretion systems might offer an potential alternative to the conventional cytoplasmical expression. The application of Type 1 secretion systems of Gram-negative bacteria, however, where often not successful in the past for a wide range of proteins. Recently, two studies using the E. coli maltose binding protein (MalE) and the rat intestinal fatty acid binding protein (IFABP) revealed a rational to circumvent these limitations. Here, wild-type passenger proteins were not secreted, while folding mutants with decreased folding kinetics were efficiently exported to the extracellular space. Subsequently, an one-step purification protocol yielded homogeneous and active protein. Taken together, theses two studies suggest that the introduction of slow-folding mutations into a protein sequence might be the key to use Type 1 secretion systems for the biotechnological production of proteins.
机译:通过专用分泌系统产生的蛋白质可能为常规细胞质表达提供潜在的替代方法。然而,革兰氏阴性细菌的1型分泌系统的应用在过去常常无法成功用于多种蛋白质。最近,有两项研究使用 E。大肠杆菌麦芽糖结合蛋白(MalE)和大鼠肠道脂肪酸结合蛋白(IFABP)揭示了规避这些限制的合理方法。在这里,野生型过客蛋白不被分泌,而折叠动力学降低的折叠突变体被有效地输出到细胞外空间。随后,一步纯化程序产生均质且活性的蛋白质。综上所述,这两项研究表明将慢折叠突变引入蛋白质序列可能是使用1型分泌系统进行蛋白质生物技术生产的关键。

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