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The Structural Basis of Ribosome Activity in Peptide Bond Synthesis
Poul Nissen,1*Jeffrey Hansen,1*Nenad Ban,1*Peter B. Moore,12Thomas A. Steitz123
Using the atomic structures of the large ribosomal subunit from
Haloarcula marismortui and its complexes with two substrateanalogs, we establish that the ribosome is a ribozyme and addressthe
catalytic properties of its all-RNA active site. Both substrateanalogs
are contacted exclusively by conserved ribosomal RNA (rRNA)residues
from domain V of 23S rRNA; there are no protein side-chainatoms closer than about 18 angstroms to the peptide bond beingsynthesized. The mechanism of peptide bond synthesis appears toresemble the reverse of the acylation step in serine proteases,with
the base of A2486 (A2451 in Escherichia coli) playing thesame general base role as histidine-57 in chymotrypsin. The unusualpKa (where Ka is the acid
dissociation constant) required forA2486 to perform this function may
derive in part from its hydrogenbonding to G2482 (G2447 in E. coli), which also interacts witha buried phosphate that could
stabilize unusual tautomers of thesetwo bases. The polypeptide exit
tunnel is largely formed by RNAbut has significant contributions from
proteins L4, L22, and L39e,and its exit is encircled by proteins L19,
L22, L23, L24, L29,and L31e.
1 Department of Molecular Biophysics and
Biochemistry and
2 Department of Chemistry, Yale
University, and
3 Howard Hughes Medical Institute,
New Haven, CT 06520-8114, USA.
*
These authors contributed equally to this work.
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PERSPECTIVES
Thomas R. Cech (11 August 2000) Science289 (5481), 878.
[DOI: 10.1126/science.289.5481.878] |Summary »|Full Text »
RESEARCH ARTICLES
Nenad Ban, Poul Nissen, Jeffrey Hansen, Peter B. Moore, and Thomas A. Steitz (11 August 2000) Science289 (5481), 905.
[DOI: 10.1126/science.289.5481.905] |Abstract »|Full Text »|PDF »
REPORTS
Gregory W. Muth, Lori Ortoleva-Donnelly, and Scott A. Strobel (11 August 2000) Science289 (5481), 947.
[DOI: 10.1126/science.289.5481.947] |Abstract »|Full Text »|PDF »
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