Ligand-induced disorder-to-order transitions characterized by structural proteomics and molecular dynamics simulations

被引：12

作者：

Makepeace, Karl A. T. ^{[1
]}

Brodie, Nicholas I. ^{[1
]}

Popov, Konstantin I. ^{[2
]}

Gudavicius, Geoff ^{[3
]}

Nelson, Christopher J. ^{[3
]}

Petrotchenko, Evgeniy V. ^{[4
]}

Dokholyan, Nikolay V. ^{[5
]}

Borchers, Christoph H. ^{[1
,3
,4
,6
]}

机构：

[1] Univ Victoria, Genome British Columbia Prote Ctr, 3101-4464 Markham St,Vancouver Isl Technol Pk, Victoria, BC V8Z 7X8, Canada

[2] Univ N Carolina, Dept Biochem & Biophys, Chapel Hill, NC 27599 USA

[3] Univ Victoria, Dept Biochem & Microbiol, Petch Bldg,Room 270d,3800 Finnerty Rd, Victoria, BC V8P 5C2, Canada

[4] McGill Univ, Jewish Gen Hosp, Lady Davis Inst, Segal Canc Prote Ctr, Montreal, PQ H3T 1E2, Canada

[5] Penn State Coll Med, Dept Biochem & Mol Biol, Dept Pharmacol, Hershey, PA 17033 USA

[6] McGill Univ, Jewish Gen Hosp, Gerald Bronfman Dept Oncol, Montreal, PQ H3T 1E2, Canada

来源：

JOURNAL OF PROTEOMICS | 2020年 / 211卷

基金：

加拿大自然科学与工程研究理事会;

关键词：

Structural proteomics; Mass spectrometry; Molecular dynamics simulations; Protein-ligand interaction; Hydrogen/deuterium exchange; Crosslinking/mass spectrometry; Surface modification; Conformational change; Intrinsically disordered protein; Protein folding; GENERAL FORCE-FIELD; PROTEINS; FLUCTUATIONS; AGGREGATION; EFFICIENT; SOFTWARE;

D O I：

10.1016/j.jprot.2019.103544

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

For disordered proteins, ligand binding can be a critical event that changes their structural dynamics. The ability to characterize such changes would facilitate the development of drugs designed to stabilize disordered proteins, whose mis-folding is important for a number of pathologies, including neurodegenerative diseases such as Parkinson's and Alzheimer's diseases. In this study, we used hydrogen/deuterium exchange, differential cross-linking, differential surface modification, and molecular dynamics (MD) simulations to characterize the structural changes in disordered proteins that result from ligand binding. We show here that both an ATP-independent protein chaperone, Spy L32P, and the FK506 binding domain of a prolyl isomerase, FKBP-25 F145A/I223P, are disordered, yet exhibit structures that are distinct from chemically denatured unfolded states in solution, and that they undergo transitions to a more structured state upon ligand binding. These systems may serve as models for the characterization of ligand-induced disorder-to-order transitions in proteins using structural proteomics approaches. Significance: In this study, we used hydrogen/deuterium exchange, differential crosslinking, differential surface modification, and molecular-dynamics simulations to characterize the structural changes in disordered proteins that result from ligand binding. The protein-ligand systems studied here (the ATP-independent protein chaperone, Spy L32P, and the FK506 binding domain of a prolyl isomerase, FKBP-25 F145A/I223P) may serve as models for understanding ligand-induced disorder-to-order transitions in proteins. Additionally, the structural proteomic techniques demonstrated here are shown to be effective tools for the characterization of disorder-to-order transitions and can be used to facilitate study of other systems in which this class of structural transition can be used for modulating major pathological features of disease, such as the abnormal protein aggregation that occurs with Parkinson's disease and Alzheimer's disease.

引用

页数：9

共 34 条

[1] A rapid, reversible, and tunable method to regulate protein function in living cells using synthetic small molecules
Banaszynski, Laura A.
Chen, Lin-chun
Maynard-Smith, Lystranne A.
Ooi, A. G. Lisa
Wandless, Thomas J.
[J]. CELL, 2006, 126 (05) : 995 - 1004
[2] Structural interpretation of hydrogen exchange protection factors in proteins: Characterization of the native state fluctuations of C12
Best, RB
Vendruscolo, M
[J]. STRUCTURE, 2006, 14 (01) : 97 - 106
[3] Optimization of the Additive CHARMM All-Atom Protein Force Field Targeting Improved Sampling of the Backbone φ, ψ and Side-Chain χ1 and χ2 Dihedral Angles
Best, Robert B.
Zhu, Xiao
Shim, Jihyun
Lopes, Pedro E. M.
Mittal, Jeetain
Feig, Michael
MacKerell, Alexander D., Jr.
[J]. JOURNAL OF CHEMICAL THEORY AND COMPUTATION, 2012, 8 (09) : 3257 - 3273
[4] Conformational ensemble of native -synuclein in solution as determined by short-distance crosslinking constraint-guided discrete molecular dynamics simulations
Brodie, Nicholas I.
Popov, Konstantin I.
Petrotchenko, Evgeniy V.
Dokholyan, Nikolay V.
Borchers, Christoph H.
[J]. PLOS COMPUTATIONAL BIOLOGY, 2019, 15 (03)
[5] Top-Down Hydrogen-Deuterium Exchange Analysis of Protein Structures Using Ultraviolet Photodissociation
Brodie, Nicholas I.
Huguet, Romain
Zhang, Terry
Viner, Rosa
Zabrouskov, Vlad
Pan, Jingxi
Petrotchenko, Evgeniy V.
Borchers, Christoph H.
[J]. ANALYTICAL CHEMISTRY, 2018, 90 (05) : 3079 - 3082
[6] Solving protein structures using short-distance cross-linking constraints as a guide for discrete molecular dynamics simulations
Brodie, Nicholas I.
Popov, Konstantin I.
Petrotchenko, Evgeniy V.
Dokholyan, Nikolay V.
Borchers, Christoph H.
[J]. SCIENCE ADVANCES, 2017, 3 (07):
[7] Protein Misfolding, Amyloid Formation, and Human Disease: A Summary of Progress Over the Last Decade
Chiti, Fabrizio
Dobson, Christopher M.
[J]. ANNUAL REVIEW OF BIOCHEMISTRY, VOL 86, 2017, 86 : 27 - 68
[8] Rational design of a ligand-controlled protein conformational switch
Dagliyan, Onur
Shirvanyants, David
Karginov, Andrei V.
Ding, Feng
Fee, Lanette
Chandrasekaran, Srinivas N.
Freisinger, Christina M.
Smolen, Gromoslaw A.
Huttenlocher, Anna
Hahn, Klaus M.
Dokholyan, Nikolay V.
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2013, 110 (17) : 6800 - 6804
[9] Daura X, 1999, ANGEW CHEM INT EDIT, V38, P236, DOI 10.1002/(SICI)1521-3773(19990115)38:1/2<236::AID-ANIE236>3.0.CO
[10] 2-M

← 1 2 3 4 →