Selection of Guide Sequences That Direct Efficient Cleavage of mRNA by Human Ribonuclease P

4 March 1994

journal article
Published by American Association for the Advancement of Science (AAAS) in Science

Vol. 263 (5151) , 1269-1273
https://doi.org/10.1126/science.8122108

Abstract

Any RNA, when in a complex with another oligoribonucleotide known as an external guide sequence (EGS), can become a substrate for ribonuclease P. Simulation of evolution in vitro was used to select EGSs that bind tightly to a target substrate messenger RNA and that increase the efficiency of cleavage of the target by human ribonuclease P to a level equal to that achieved with natural substrates. The most efficient EGSs form transfer RNA precursor-like structures with the target RNA, in which the analog of the anticodon stem has been disrupted, an indication that selection for the optimal substrate for ribonuclease P yields an RNA structure different from that of present-day transfer RNA precursors.

Keywords

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