dominant negative mutant of the E. coli RNA helicase DbpA blocks assembly of the 50S ribosomal subunit

Escherichia coli DbpA is an ATP-dependent RNA helicase with specificity for hairpin 92 of 23S ribosomal RNA, an important part of the peptidyl transferase center. The R331A active site mutant of DbpA confers a dominant slow growth and cold sensitive phenotype when overexpressed in E. coli containing...

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Bibliographic Details
Published in:Nucleic acids research 2009-10, Vol.37 (19), p.6503-6514
Main Authors: Sharpe Elles, Lisa M, Sykes, Michael T, Williamson, James R, Uhlenbeck, Olke C
Format: Article
Language:English
Subjects:
DEAD-box RNA Helicases - genetics
DEAD-box RNA Helicases - metabolism
DEAD-box RNA Helicases - physiology
Escherichia coli
Escherichia coli - genetics
Escherichia coli Proteins - genetics
Escherichia coli Proteins - metabolism
Escherichia coli Proteins - physiology
Mutation
Nucleic Acid Enzymes
Ribosomal Proteins - chemistry
Ribosome Subunits, Large, Bacterial - metabolism
RNA, Ribosomal - metabolism
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Summary:Escherichia coli DbpA is an ATP-dependent RNA helicase with specificity for hairpin 92 of 23S ribosomal RNA, an important part of the peptidyl transferase center. The R331A active site mutant of DbpA confers a dominant slow growth and cold sensitive phenotype when overexpressed in E. coli containing endogenous DbpA. Ribosome profiles from cells overexpressing DbpA R331A display increased levels of 50S and 30S subunits and decreased levels 70S ribosomes. Profiles run at low Mg2+ exhibit fewer 50S subunits and accumulate a 45S particle that contains incompletely processed and undermodified 23S rRNA in addition to reduced levels of several ribosomal proteins that bind late in the assembly pathway. Unlike mature 50S subunits, these 45S particles can stimulate the ATPase activity of DbpA, indicating that hairpin 92 has not yet been sequestered within the 50S subunit. Overexpression of the inactive DbpA R331A mutant appears to block assembly at a late stage when the peptidyl transferase center is formed, indicating a possible role for DbpA promoting this conformational change.
ISSN:0305-1048
1362-4962
DOI:10.1093/nar/gkp711