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Solution Structure and Refolding of the Mycobacterium tuberculosis Pentapeptide Repeat Protein MfpA

机译:分枝杆菌的溶液结构和重折叠 肺结核五肽重复蛋白 制造商

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摘要

The pentapeptide repeat is a recently discovered protein fold. Mycobacterium tuberculosis MfpA is a founding member of the pentapeptide repeat protein (PRP) family that confers resistance to the antibiotic fluoroquinolone by binding to DNA gyrase and inhibiting its activity. The size, shape, and surface potential of MfpA mimics duplex DNA. As an initial step in a comprehensive biophysical analysis of the role of PRPs in the regulation of cellular topoisomerase activity and conferring antibiotic resistance, we have explored the solution structure and refolding of MfpA by fluorescence spectroscopy, CD, and analytical centrifugation. A unique CD spectrum for the pentapeptide repeat fold is described. This spectrum reveals a native structure whose β-strands and turns within the right-handed quadrilateral β-helix that define the PRP fold differ from canonical secondary structure types. MfpA refolded from urea or guanidium by dialysis or dilution forms stable aggregates of monomers whose secondary and tertiary structure are not native. In contrast, MfpA refolded using a novel “time-dependent renaturation” protocol yields protein with native secondary, tertiary, and quaternary structure. The generality of “time-dependent renaturation” to other proteins and denaturation methods is discussed.
机译:五肽重复序列是最近发现的蛋白质折叠。结核分枝杆菌MfpA是五肽重复蛋白(PRP)家族的创始成员,它通过与DNA促旋酶结合并抑制其活性赋予对氟喹诺酮类抗生素的抗性。 MfpA的大小,形状和表面电位模拟双链DNA。作为对PRP在调节细胞拓扑异构酶活性和赋予抗生素抗性中作用的全面生物物理分析的第一步,我们已经通过荧光光谱,CD和分析离心法研究了MfpA的溶液结构和重折叠。描述了五肽重复折叠的独特CD光谱。该光谱揭示了一个天然结构,该结构的β-链和右旋四边形β-螺旋内定义了PRP折叠的β链和转向不同于经典的二级结构类型。通过透析或稀释从尿素或胍中重折叠的MfpA形成稳定的单体聚集体,其二级和三级结构不是天然的。相反,使用新颖的“时间依赖性复性”方案重新折叠的MfpA产生具有天然二级,三级和四级结构的蛋白质。的普遍性 对其他蛋白质的“时间依赖性复性”和变性 方法进行了讨论。

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