Crystal structure of the human prion protein reveals a mechanism for oligomerization

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作者
Karen J. Knaus
Manuel Morillas
Wieslaw Swietnicki
Michael Malone
Witold K. Surewicz
Vivien C. Yee
机构
[1] Lerner Research Institute,Department of Molecular Cardiology and Center for Structural Biology
[2] Cleveland Clinic Foundation,Department of Chemistry
[3] Cleveland State University,Department of Pathology
[4] Case Western Reserve University,Department of Pharmacology
[5] Case Western Reserve University,Department of Chemistry
[6] Case Western Reserve University,Department of Physiology and Biophysics
[7] Case Western Reserve University,undefined
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The pathogenesis of transmissible encephalopathies is associated with the conversion of the cellular prion protein, PrPC, into a conformationally altered oligomeric form, PrPSc. Here we report the crystal structure of the human prion protein in dimer form at 2 Å resolution. The dimer results from the three-dimensional swapping of the C-terminal helix 3 and rearrangement of the disulfide bond. An interchain two-stranded antiparallel β-sheet is formed at the dimer interface by residues that are located in helix 2 in the monomeric NMR structures. Familial prion disease mutations map to the regions directly involved in helix swapping. This crystal structure suggests that oligomerization through 3D domain-swapping may constitute an important step on the pathway of the PrPC → PrPSc conversion.
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页码:770 / 774
页数:4
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