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A DNA-conjugated small molecule catalyst enzyme mimic for site-selective ester hydrolysis.


ABSTRACT: The challenge of site-selectivity must be overcome in many chemical research contexts, including selective functionalization in complex natural products and labeling of one biomolecule in a living system. Synthetic catalysts incorporating molecular recognition domains can mimic naturally-occurring enzymes to direct a chemical reaction to a particular instance of a functional group. We propose that DNA-conjugated small molecule catalysts (DCats), prepared by tethering a small molecule catalyst to a DNA aptamer, are a promising class of reagents for site-selective transformations. Specifically, a DNA-imidazole conjugate able to increase the rate of ester hydrolysis in a target ester by >100-fold compared with equimolar untethered imidazole was developed. Other esters are unaffected. Furthermore, DCat-catalyzed hydrolysis follows enzyme-like kinetics and a stimuli-responsive variant of the DCat enables programmable "turn on" of the desired reaction.

SUBMITTER: Flanagan ML 

PROVIDER: S-EPMC5911826 | biostudies-literature | 2018 Feb

REPOSITORIES: biostudies-literature

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A DNA-conjugated small molecule catalyst enzyme mimic for site-selective ester hydrolysis.

Flanagan Moira L ML   Arguello A Emilia AE   Colman Drew E DE   Kim Jiyeon J   Krejci Jesse N JN   Liu Shimu S   Yao Yueyu Y   Zhang Yu Y   Gorin David J DJ  

Chemical science 20180115 8


The challenge of site-selectivity must be overcome in many chemical research contexts, including selective functionalization in complex natural products and labeling of one biomolecule in a living system. Synthetic catalysts incorporating molecular recognition domains can mimic naturally-occurring enzymes to direct a chemical reaction to a particular instance of a functional group. We propose that DNA-conjugated small molecule catalysts (DCats), prepared by tethering a small molecule catalyst to  ...[more]

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