Yuan Joy F, Beniac Daniel R, Chaconas George, Ottensmeyer F Peter
Department of Biochemistry, University of Western Ontario, London, Ontario N6A 5C1, Canada.
Genes Dev. 2005 Apr 1;19(7):840-52. doi: 10.1101/gad.1291405. Epub 2005 Mar 17.
Mu DNA transposition proceeds through a series of higher-order nucleoprotein complexes called transpososomes. The structural core of the transpososome is a tetramer of the transposase, Mu A, bound to the two transposon ends. High-resolution structural analysis of the intact transposase and the transpososome has not been successful to date. Here we report the structure of Mu A at 16-angstroms and the Type 1 transpososome at 34-angstroms resolution, by 3D reconstruction of images obtained by scanning transmission electron microscopy (STEM) at cryo-temperatures. Electron spectroscopic imaging (ESI) of the DNA-phosphorus was performed in conjunction with the structural investigation to derive the path of the DNA through the transpososome and to define the DNA-binding surface in the transposase. Our model of the transpososome fits well with the accumulated biochemical literature for this intricate transposition system, and lays a structural foundation for biochemical function, including catalysis in trans and the complex circuit of macromolecular interactions underlying Mu DNA transposition.
Mu DNA转座通过一系列称为转座体的高阶核蛋白复合物进行。转座体的结构核心是转座酶Mu A的四聚体,它与两个转座子末端结合。迄今为止,完整转座酶和转座体的高分辨率结构分析尚未成功。在此,我们通过对低温下扫描透射电子显微镜(STEM)获得的图像进行三维重建,报告了分辨率为16埃的Mu A结构和分辨率为34埃的1型转座体结构。结合结构研究进行了DNA磷的电子光谱成像(ESI),以确定DNA通过转座体的路径,并确定转座酶中的DNA结合表面。我们的转座体模型与关于这个复杂转座系统的大量生化文献非常吻合,并为生化功能奠定了结构基础,包括反式催化以及Mu DNA转座背后的大分子相互作用复杂回路。