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Molecular insights into replication initiation by Q? replicase using ribosomal protein S1.


ABSTRACT: Ribosomal protein S1, consisting of six contiguous OB-folds, is the largest ribosomal protein and is essential for translation initiation in Escherichia coli. S1 is also one of the three essential host-derived subunits of Q? replicase, together with EF-Tu and EF-Ts, for Q? RNA replication in E. coli. We analyzed the crystal structure of Q? replicase, consisting of the virus-encoded RNA-dependent RNA polymerase (?-subunit), EF-Tu, EF-Ts and the N-terminal half of S1, which is capable of initiating Q? RNA replication. Structural and biochemical studies revealed that the two N-terminal OB-folds of S1 anchor S1 onto the ?-subunit, and the third OB-fold is mobile and protrudes beyond the surface of the ?-subunit. The third OB-fold mainly interacts with a specific RNA fragment derived from the internal region of Q? RNA, and its RNA-binding ability is required for replication initiation of Q? RNA. Thus, the third mobile OB-fold of S1, which is spatially anchored near the surface of the ?-subunit, primarily recruits the Q? RNA toward the ?-subunit, leading to the specific and efficient replication initiation of Q? RNA, and S1 functions as a replication initiation factor, beyond its established function in protein synthesis.

SUBMITTER: Takeshita D 

PROVIDER: S-EPMC4176380 | biostudies-literature | 2014

REPOSITORIES: biostudies-literature

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Molecular insights into replication initiation by Qβ replicase using ribosomal protein S1.

Takeshita Daijiro D   Yamashita Seisuke S   Tomita Kozo K  

Nucleic acids research 20140813 16


Ribosomal protein S1, consisting of six contiguous OB-folds, is the largest ribosomal protein and is essential for translation initiation in Escherichia coli. S1 is also one of the three essential host-derived subunits of Qβ replicase, together with EF-Tu and EF-Ts, for Qβ RNA replication in E. coli. We analyzed the crystal structure of Qβ replicase, consisting of the virus-encoded RNA-dependent RNA polymerase (β-subunit), EF-Tu, EF-Ts and the N-terminal half of S1, which is capable of initiatin  ...[more]

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