1umo
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THE CRYSTAL STRUCTURE OF CYTOGLOBIN: THE FOURTH GLOBIN TYPE DISCOVERED IN AMN
OverviewOverview
Cytoglobin is a recently discovered hemeprotein belonging to the globin, superfamily together with hemoglobin, myoglobin and neuroglobin. Although, distributed in almost all human tissues, cytoglobin has not been ascribed, a specific function. Human cytoglobin is composed of 190 amino acid, residues. Sequence alignments show that a protein core region (about 150, residues) is structurally related to hemoglobin and myoglobin, being, complemented by about 20 extra residues both on the N and C termini. In, the absence of exogenous ligands (e.g. O2), the cytoglobin distal HisE7, residue is coordinated to the heme Fe atom, thus decreasing the ligand, affinity. The crystal structure of human cytoglobin (2.1 A resolution, 21.3% R-factor) highlights a three-over-three alpha-helical globin fold, covering residues 18-171; the 1-17 N-terminal, and the 172-190 C-terminal, residue segments are disordered in both molecules of the crystal, asymmetric unit. Heme hexa-coordination is evident in one of the two, cytoglobin chains, whereas alternate conformation for the heme distal, region, achieving partial heme penta-coordination, is observed in the, other. Human cytoglobin displays a large apolar protein matrix cavity, next to the heme, not related to the myoglobin cavities recognized as, temporary ligand docking stations. The cavity, which may provide a heme, ligand diffusion pathway, is connected to the external space through a, narrow tunnel nestled between the globin G and H helices.
About this StructureAbout this Structure
1UMO is a Single protein structure of sequence from Homo sapiens with HEM as ligand. Structure known Active Site: AC1. Full crystallographic information is available from OCA.
ReferenceReference
Crystal structure of cytoglobin: the fourth globin type discovered in man displays heme hexa-coordination., de Sanctis D, Dewilde S, Pesce A, Moens L, Ascenzi P, Hankeln T, Burmester T, Bolognesi M, J Mol Biol. 2004 Feb 27;336(4):917-27. PMID:15095869
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