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PDBsum entry 1lms
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Electron transport
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PDB id
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1lms
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Contents |
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* Residue conservation analysis
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References listed in PDB file
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Key reference
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Title
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Structural model for an alkaline form of ferricytochrome c.
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Authors
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M.Assfalg,
I.Bertini,
A.Dolfi,
P.Turano,
A.G.Mauk,
F.I.Rosell,
H.B.Gray.
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Ref.
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J Am Chem Soc, 2003,
125,
2913-2922.
[DOI no: ]
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PubMed id
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Abstract
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An (15)N-enriched sample of the yeast iso-1-ferricytochrome c triple variant
(Lys72Ala/Lys79Ala/Cys102Thr) in an alkaline conformation was examined by NMR
spectroscopy. The mutations were planned to produce a cytochrome c with a single
conformer. Despite suboptimal conditions for the collection of spectra (i.e., pH
approximately equal to 11), NMR remains a suitable investigation technique
capable of taking advantage of paramagnetism. 76% of amino acids and 49% of
protons were assigned successfully. The assignment was in part achieved through
standard methods, in part through the identification of groups maintaining the
same conformation as in the native protein at pH 7 and, for a few other
residues, through a tentative analysis of internuclear distance predictions.
Lys73 was assigned as the axial ligand together with His18. In this manner, 838
meaningful NOEs for 108 amino acids, 50 backbone angle constraints, and 203
pseudocontact shifts permitted the convergence of randomly generated structures
to a family of conformers with a backbone RMSD of 1.5 +/- 0.2 A. Most of the
native cytochrome c conformation is maintained at high pH. The NOE pattern that
involves His18 clearly indicates that the proximal side of the protein,
including the 20s and 40s loops, remains essentially intact. Structural
differences are concentrated in the 70-80 loop, because of the replacement of
Met80 by Lys73 as an axial ligand, and in the 50s helix facing that loop; as a
consequence, there is increased exposure of the heme group to solvent. Based on
several spectral features, we conclude that the folded polypeptide is highly
fluxional.
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