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SOLUTION NMR STRUCTURE AND BACKBONE DYNAMICS OF THE MAJOR COLD-SHOCK PROTEIN (CSPA) FROM ESCHERICHIA-COLI - EVIDENCE FOR CONFORMATIONAL DYNAMICS IN THE SINGLE-STRANDED RNA-BINDING SITE

Authors

FENG WQ TEJERO R ZIMMERMAN DE INOUYE M MONTELIONE GT

Citation

Wq. Feng et al., SOLUTION NMR STRUCTURE AND BACKBONE DYNAMICS OF THE MAJOR COLD-SHOCK PROTEIN (CSPA) FROM ESCHERICHIA-COLI - EVIDENCE FOR CONFORMATIONAL DYNAMICS IN THE SINGLE-STRANDED RNA-BINDING SITE, Biochemistry, 37(31), 1998, pp. 10881-10896

Citations number

Categorie Soggetti

Biology

Journal title

Biochemistry → ACNP

ISSN journal

00062960

Volume

Issue

Year of publication

1998

Pages

10881 - 10896

Database

ISI

SICI code

0006-2960(1998)37:31<10881:SNSABD>2.0.ZU;2-0

Abstract

The major cold-shock protein (CspA) from Escherichia coli is a single- stranded nucleic acid-binding protein that is produced in response to cold stress. We have previously reported its overall chain fold as det ermined by NMR spectroscopy [Newkirk, K., Feng, W., Jiang, W., Tejero, R., Emerson, S. D., Inouye, M., and Montelione, G. T. (1994) Proc. Na tl. Acad. Sci. U.S.A. 91, 5114-5118]. Here we describe the complete an alysis of H-1, C-13, and N-15 resonance assignments for CspA, together with a refined solution NMR structure based on 699 conformational con straints and an analysis of backbone dynamics based on N-15 relaxation rate measurements. An extensive set of triple-resonance NMR experimen ts for obtaining the backbone and side chain resonance assignments wer e carried out on uniformly C-13- and N-15-enriched CspA. Using a subse t of these triple-resonance experiments, the computer program AUTOASSI GN provided automatic analysis of sequence-specific backbone N, C-alph a, C', H-N, H-alpha, and side chain C-beta resonance assignments. The remaining H-1, C-13, and N-15 resonance assignments for CspA were then obtained by manual analysis of additional NMR spectra. Dihedral angle constraints and stereospecific methylene H-beta resonance assignments were determined using a new conformational grid search program, HYPER , and used together with longer-range constraints as input for three-d imensional structure calculations. The resulting solution NMR structur e of CspA is a well-defined five-stranded beta-barrel with surface-exp osed aromatic groups that form a single-stranded nucleic acid-binding site. Backbone dynamics of CspA have also been characterized by N-15 T -1, T-2, and heteronuclear N-15-H-1 NOE measurements and analyzed usin g the extended Lipari-Szabo formalism. These dynamic measurements indi cate a molecular rotational correlation time tau(m), of 4.88 +/- 9.04 ns and provide evidence for fast time scale (tau(e) < 500 ps) dynamics in surface loops and motions on the microsecond to millisecond time s cale within the proposed nucleic acid-binding epitope.