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Intrinsic protein disorder could be overlooked in cocrystallization conditions: An SRCD case study
Author(s) -
Németh Eszter,
Balogh Ria K.,
Borsos Katalin,
Czene Anikó,
Thulstrup Peter W.,
Gyurcsik Béla
Publication year - 2016
Publication title -
protein science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.353
H-Index - 175
eISSN - 1469-896X
pISSN - 0961-8368
DOI - 10.1002/pro.3010
Subject(s) - intermolecular force , crystallography , protein structure , protein crystallization , chemistry , circular dichroism , protein–protein interaction , nuclease , crystal structure , macromolecule , biophysics , crystallization , biology , biochemistry , enzyme , molecule , organic chemistry
X‐ray diffractometry dominates protein studies, as it can provide 3D structures of these diverse macromolecules or their molecular complexes with interacting partners: substrates, inhibitors, and/or cofactors. Here, we show that under cocrystallization conditions the results could reflect induced protein folds instead of the (partially) disordered original structures. The analysis of synchrotron radiation circular dichroism spectra revealed that the Im7 immunity protein stabilizes the native‐like solution structure of unfolded NColE7 nuclease mutants via complex formation. This is consistent with the fact that among the several available crystal structures with its inhibitor or substrate, all NColE7 structures are virtually the same. Our results draw attention to the possible structural consequence of protein modifications, which is often hidden by compensational effects of intermolecular interactions. The growing evidence on the importance of protein intrinsic disorder thus, demands more extensive complementary experiments in solution phase with the unligated form of the protein of interest.