Three-dimensional solution structure and 13C assignments of barstar using nuclear magnetic resonance spectroscopy

Three-dimensional solution structure and 13C assignments of barstar using nuclear magnetic resonance spectroscopy

We present the high-resolution solution structure and 13C assignments of wild-type barstar, an 89 amino acid residue polypeptide inhibitor of barnase, derived from heteronuclear NMR techniques. These were obtained from measurements on unlabeled, uniformly 15N- and 13C/15N-labeled, and 10% 13C-labele...

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Veröffentlicht in:Biochemistry (Easton) 1994-08, Vol.33 (30), p.8866-8877
Hauptverfasser: Lubienski, Michael J, Bycroft, Mark, Freund, Stefan M. V, Fersht, Alan R
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Sprache:eng
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Bacterial Proteins - chemistry
Carbon Isotopes
Magnetic Resonance Spectroscopy
Protein Structure, Secondary
Ribonucleases - antagonists & inhibitors
Solutions
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container_end_page 8877
container_issue 30
container_start_page 8866
container_title Biochemistry (Easton)
container_volume 33
creator Lubienski, Michael J
Bycroft, Mark
Freund, Stefan M. V
Fersht, Alan R
description We present the high-resolution solution structure and 13C assignments of wild-type barstar, an 89 amino acid residue polypeptide inhibitor of barnase, derived from heteronuclear NMR techniques. These were obtained from measurements on unlabeled, uniformly 15N- and 13C/15N-labeled, and 10% 13C-labeled barstar samples that have both cysteines (at positions 40 and 82) fully reduced. In total, 30 structures were calculated by hybrid distance geometry-dynamical simulated annealing calculations. The atomic rms distribution about the mean coordinate positions is 0.42 A for all backbone atoms and 0.90 A for all atoms. The structure is composed of three parallel alpha-helices packed against a three-stranded parallel beta-sheet. A more poorly defined helix links the second beta-strand and the third major alpha-helix. The loop involved in binding barnase is extremely well defined and held rigidly by interactions from the main body of the protein to both ends and the middle of the loop. This structure will be used to aid protein engineering studies currently taking place on the free and bound states of barstar and barnase.
doi_str_mv 10.1021/bi00196a003
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subjects Bacterial Proteins - chemistry
Carbon Isotopes
Magnetic Resonance Spectroscopy
Protein Structure, Secondary
Ribonucleases - antagonists & inhibitors
Solutions
title Three-dimensional solution structure and 13C assignments of barstar using nuclear magnetic resonance spectroscopy
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