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Literature DB >> 33319995

Palladium-Protein Oxidative Addition Complexes by Amine-Selective Acylation.

Heemal H Dhanjee¹, Ivan Buslov¹, Ian W Windsor¹, Ronald T Raines¹, Bradley L Pentelute¹, Stephen L Buchwald¹.

Abstract

Palladium oxidative addition complexes (OACs) are traditionally accessed by treating an aryl halide-containing substrate with a palladium(0) source. Here, a new strategy to selectively prepare stable OACs from amino groups on native proteins is presented. The approach relies on an amine-selective acylation reaction that occurs without modification of a preformed palladium(II)-aryl group. Once transferred onto a protein substrate, the palladium(II)-aryl group facilitates conjugation by undergoing reaction with a second, cysteine-containing protein. This operationally simple method is applicable to native, nonengineered enzymes as well as antibodies and is carried out in an aqueous setting and open to air. The resulting Pd-protein OACs are stable, storable reagents that retain biological activity and can be used to achieve protein-protein cross-coupling at nanomolar concentrations within hours.

Entities: Chemical Disease Gene Species

Mesh：

Substances：
Amines
Proteins
Palladium

Year: 2020 PMID： 33319995 PMCID： PMC8048385 DOI： 10.1021/jacs.0c09180

Source DB: PubMed Journal: J Am Chem Soc ISSN： 0002-7863 Impact factor: 15.419

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2. A Neophyl Palladacycle as an Air- and Thermally Stable Precursor to Oxidative Addition Complexes.

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Review 4. Chemical and Enzymatic Methods for Post-Translational Protein-Protein Conjugation.

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