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Literature DB >> 27274902

Late-Stage Diversification of Biologically Active Molecules via Chemoenzymatic C-H Functionalization.

Landon J Durak¹, James T Payne¹, Jared C Lewis¹.

Abstract

Engineered variants of rebeccamycin halogenase were used to selectively halogenate a number of biologically active aromatic compounds. Subsequent Pd-catalyzed cross-coupling reactions on the crude extracts of these reactions were used to install aryl, amine, and ether substituents at the halogenation site. This simple, chemoenzymatic method enables non-directed functionalization of C-H bonds on a range of substrates to provide access to derivatives that would be challenging or inefficient to prepare by other means.

Entities: Chemical Disease Species

Keywords: C-H Functionalization; Chemoenzymatic; Cross-Coupling; Halogenase; Late-Stage Diversification

Year: 2016 PMID： 27274902 PMCID： PMC4890977 DOI： 10.1021/acscatal.5b02558

Source DB: PubMed Journal: ACS Catal Impact factor: 13.084

30 in total

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6. Behavioural effects of pinoline in the rat forced swimming, open field and elevated plus-maze tests.

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7. Directed evolution of RebH for site-selective halogenation of large biologically active molecules.

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10. Chemoenzymatic elaboration of monosaccharides using engineered cytochrome P450BM3 demethylases.

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Journal: Proc Natl Acad Sci U S A Date: 2009-09-15 Impact factor: 11.205

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2. Structure-Guided Reprogramming of a Hydroxylase To Halogenate Its Small Molecule Substrate.

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Review 3. Understanding and Improving the Activity of Flavin-Dependent Halogenases via Random and Targeted Mutagenesis.

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4. Understanding Flavin-Dependent Halogenase Reactivity via Substrate Activity Profiling.

Authors: Mary C Andorfer; Jonathan E Grob; Christine E Hajdin; Julia R Chael; Piro Siuti; Jeremiah Lilly; Kian L Tan; Jared C Lewis
Journal: ACS Catal Date: 2017-01-31 Impact factor: 13.084

5. A Panel of TrpB Biocatalysts Derived from Tryptophan Synthase through the Transfer of Mutations that Mimic Allosteric Activation.

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6. A Diverse Library of Chiral Cyclopropane Scaffolds via Chemoenzymatic Assembly and Diversification of Cyclopropyl Ketones.

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