Cell. 2000 Jun 9;101(6):589-600.

Crystal structure of T7 gene 4 ring helicase indicates a mechanism for sequential hydrolysis of nucleotides.

Singleton MR, Sawaya MR, Ellenberger T, Wigley DB.

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Sir William Dunn School of Pathology, University of Oxford, United Kingdom.

Abstract

We have determined the crystal structure of an active, hexameric fragment of the gene 4 helicase from bacteriophage T7. The structure reveals how subunit contacts stabilize the hexamer. Deviation from expected six-fold symmetry of the hexamer indicates that the structure is of an intermediate on the catalytic pathway. The structural consequences of the asymmetry suggest a "binding change" mechanism to explain how cooperative binding and hydrolysis of nucleotides are coupled to conformational changes in the ring that most likely accompany duplex unwinding. The structure of a complex with a nonhydrolyzable ATP analog provides additional evidence for this hypothesis, with only four of the six possible nucleotide binding sites being occupied in this conformation of the hexamer. This model suggests a mechanism for DNA translocation.

PMID:: 10892646; [PubMed - indexed for MEDLINE]

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Structures reported by this article

Gp4d Helicase From Phage T7

PDB: 1E0K

Source: Enterobacteria phage T7

Method: X-Ray Diffraction

Resolution: 3.3 Å

See all 2 structures...

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