NMR in structure-based drug design

被引：8

作者：

Carneiro, Marta G. ^{[1
]}

Eiso, A. B. ^{[1
]}

Theisgen, Stephan ^{[1
]}

Siegal, Gregg ^{[1
]}

机构：

[1] ZoBio, JH Oortweg 19, NL-2333 CH Leiden, Netherlands

来源：

STRUCTURE-BASED DRUG DESIGN: INSIGHTS FROM ACADEMIA AND INDUSTRY | 2017年 / 61卷 / 05期

关键词：

INTRINSICALLY DISORDERED PROTEINS; AUTOMATED RESONANCE ASSIGNMENT; CHEMICAL-SHIFT; CONFORMATIONAL-CHANGES; LIGAND COMPLEXES; BINDING-SITES; 3D STRUCTURE; IDENTIFICATION; SPECTROSCOPY; INHIBITORS;

D O I：

10.1042/EBC20170037

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

NMR spectroscopy is a powerful technique that can provide valuable structural information for drug discovery endeavors. Here, we discuss the strengths (and limitations) of NMR applications to structure-based drug discovery, highlighting the different levels of resolution and throughput obtainable. Additionally, the emerging field of paramagnetic NMR in drug discovery and recent developments in approaches to speed up and automate protein-observed NMR data collection and analysis are discussed.

引用

页码：485 / 493

页数：9

共 67 条

[1] Automated and assisted RNA resonance assignment using NMR chemical shift statistics
Aeschbacher, Thomas
Schmidt, Elena
Blatter, Markus
Maris, Christophe
Duss, Olivier
Allain, Frederic H. -T.
Guentert, Peter
Schubert, Mario
[J]. NUCLEIC ACIDS RESEARCH, 2013, 41 (18) : e172
[2] Protein-ligand structure guided by backbone and side-chain proton chemical shift perturbations
Aguirre, Clementine
ten Brink, Tim
Cala, Olivier
Guichou, Jean-Francois
Krimm, Isabelle
[J]. JOURNAL OF BIOMOLECULAR NMR, 2014, 60 (2-3) : 147 - 156
[3] Comparing Binding Modes of Analogous Fragments Using NMR in Fragment-Based Drug Design: Application to PRDX5
Aguirre, Clementine
ten Brink, Tim
Guichou, Jean-Francois
Cala, Olivier
Krimm, Isabelle
[J]. PLOS ONE, 2014, 9 (07):
[4] A systematic mutagenesis-driven strategy for site-resolved NMR studies of supramolecular assemblies
Amero, Carlos
Dura, M. Asuncion
Noirclerc-Savoye, Marjolaine
Perollier, Arnaud
Gallet, Benoit
Plevin, Michael J.
Vernet, Thierry
Franzetti, Bruno
Boisbouvier, Jerome
[J]. JOURNAL OF BIOMOLECULAR NMR, 2011, 50 (03) : 229 - 236
[5] Identification of productive and futile encounters in an electron transfer protein complex
Andralojc, Witold
Hiruma, Yoshitaka
Liu, Wei-Min
Ravera, Enrico
Nojiri, Masaki
Parigi, Giacomo
Luchinat, Claudio
Ubbink, Marcellus
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2017, 114 (10) : E1840 - E1847
[6] NMR Second Site Screening for Structure Determination of Ligands Bound in the Hydrophobic Pocket of HIV-1 gp41
Balogh, Edina
Wu, Dong
Zhou, Guangyan
Gochin, Miriam
[J]. JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 2009, 131 (08) : 2821 - +
[7] Applications of NMR to structure determination of RNAs large and small
Barnwal, Ravi P.
Yang, Fan
Varani, Gabriele
[J]. ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 2017, 628 : 42 - 56
[8] FLAMEnGO 2.0: An enhanced fuzzy logic algorithm for structure-based assignment of methyl group resonances
Chao, Fa-An
Kim, Jonggul
Xia, Youlin
Milligan, Michael
Rowe, Nancy
Veglia, Gianluigi
[J]. JOURNAL OF MAGNETIC RESONANCE, 2014, 245 : 17 - 23
[9] Identification of fragments targeting an alternative pocket on HIV-1 gp41 by NMR screening and similarity searching
Chu, Shidong
Gochin, Miriam
[J]. BIOORGANIC & MEDICINAL CHEMISTRY LETTERS, 2013, 23 (18) : 5114 - 5118
[10] Use of quantitative 1H NMR chemical shift changes for ligand docking into barnase
Cioffi, Marina
Hunter, Christopher A.
Packer, Martin J.
Pandya, Maya J.
Williamson, Mike P.
[J]. JOURNAL OF BIOMOLECULAR NMR, 2009, 43 (01) : 11 - 19

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