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a modern mode of activation for nucleic acid enzymes现代模式核酸酶的激活
A Modern Mode of Activation for Nucleic Acid Enzymes
´ . ` .
Dominique Levesque , Francis P. Briere , Jean-Pierre Perreault*
´ ´ ´ ´ ´ ´
RNA Group/Groupe ARN, Departement de Biochimie, Faculte de medecine et des sciences de la sante, Universite de Sherbrooke, Sherbrooke, Quebec,
Canada
Through evolution, enzymes have developed subtle modes of activation in order to ensure the sufficiently high substrate
specificity required by modern cellular metabolism. One of these modes is the use of a target-dependent module (i.e. a docking
domain) such as those found in signalling kinases. Upon the binding of the target to a docking domain, the substrate is
positioned within the catalytic site. The prodomain acts as a target-dependent module switching the kinase from an off state
to an on state. As compared to the allosteric mode of activation, there is no need for the presence of a third partner. None of
the ribozymes discovered to date have such a mode of activation, nor does any other known RNA. Starting from a specific on/
off adaptor for the hepatitis delta virus ribozyme, that differs but has a mechanism reminiscent of this signalling kinase, we
have adapted this mode of activation, using the techniques of molecular engineering, to both catalytic RNAs and DNAs
exhibiting various activities. Specifically, we adapted three cleaving ribozymes (hepatitis delta virus, hammerhead and hairpin
ribozymes), a cleaving 10-23 deoxyribozyme, a ligating hairpin ribozyme and an artificially selected capping ribozyme. In each
case, there was a significant gain in terms of substrate specificity. Even if this mode of control is unreported for natural
catalytic nucleic acids, its use needs not be limite
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