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Efficient templates for Q beta replicase are formed by recombination from heterologous sequences.
Authors:A V Munishkin  L A Voronin  V I Ugarov  L A Bondareva  H V Chetverina  A B Chetverin
Affiliation:Institute of Protein Research, Academy of Sciences, Moscow, U.S.S.R.
Abstract:A very efficient replicase template has been isolated from the products of spontaneous RNA synthesis in an in vitro Q beta replicase reaction that was incubated in the absence of added RNA. This template was named RQ135 RNA because it is 135 nucleotides in length. Its sequence consists entirely of segments that are homologous to ribosomal 23 S RNA and the phage lambda origin of replication. The sequence segments are unrelated to the sequence of Q beta bacteriophage genomic RNA. Nonetheless, this natural recombinant is replicated in vitro at a rate equal to the most efficient of the known Q beta RNA variants. Apparently, the structural properties that ensure recognition of an RNA template by Q beta replicase are not confined to viral RNA, but can appear as a result of recombination among other RNAs that usually occur in cells.
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