Human cystatin C, an amyloidogenic protein, dimerizes through three-dimensional domain swapping

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作者
Robert Janowski
Maciej Kozak
Elzbieta Jankowska
Zbigniew Grzonka
Anders Grubb
Magnus Abrahamson
Mariusz Jaskolski
机构
[1] Faculty of Chemistry,Department of Crystallography
[2] A. Mickiewicz University,Department of Organic Chemistry
[3] University of Gdansk,Department of Clinical Chemistry
[4] University of Lund,Department of Macromolecular Physics, Faculty of Physics
[5] Center for Biocrystallographic Research,undefined
[6] Institute of Bioorganic Chemistry,undefined
[7] Polish Academy of Sciences,undefined
[8] A. Mickiewicz University,undefined
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摘要
The crystal structure of human cystatin C, a protein with amyloidogenic properties and a potent inhibitor of cysteine proteases, reveals how the protein refolds to produce very tight two-fold symmetric dimers while retaining the secondary structure of the monomeric form. The dimerization occurs through three-dimensional domain swapping, a mechanism for forming oligomeric proteins. The reconstituted monomer-like domains are similar to chicken cystatin except for one inhibitory loop that unfolds to form the 'open interface' of the dimer. The structure explains the tendency of human cystatin C to dimerize and suggests a mechanism for its aggregation in the brain arteries of elderly people with amyloid angiopathy. A more severe 'conformational disease' is associated with the L68Q mutant of human cystatin C, which causes massive amyloidosis, cerebral hemorrhage and death in young adults. The structure of the three-dimensional domain-swapped dimers shows how the L68Q mutation destabilizes the monomers and makes the partially unfolded intermediate less unstable. Higher aggregates may arise through the three-dimensional domain-swapping mechanism occurring in an open-ended fashion in which partially unfolded molecules are linked into infinite chains.
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页码:316 / 320
页数:4
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