Protein-complex structure completion using IPCAS (Iterative Protein Crystal structure Automatic Solution).

نویسندگان

  • Weizhe Zhang
  • Hongmin Zhang
  • Tao Zhang
  • Haifu Fan
  • Quan Hao
چکیده

Protein complexes are essential components in many cellular processes. In this study, a procedure to determine the protein-complex structure from a partial molecular-replacement (MR) solution is demonstrated using a direct-method-aided dual-space iterative phasing and model-building program suite, IPCAS (Iterative Protein Crystal structure Automatic Solution). The IPCAS iteration procedure involves (i) real-space model building and refinement, (ii) direct-method-aided reciprocal-space phase refinement and (iii) phase improvement through density modification. The procedure has been tested with four protein complexes, including two previously unknown structures. It was possible to use IPCAS to build the whole complex structure from one or less than one subunit once the molecular-replacement method was able to give a partial solution. In the most challenging case, IPCAS was able to extend to the full length starting from less than 30% of the complex structure, while conventional model-building procedures were unsuccessful.

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عنوان ژورنال:
  • Acta crystallographica. Section D, Biological crystallography

دوره 71 Pt 7  شماره 

صفحات  -

تاریخ انتشار 2015