The Human Microbiome Encodes Resistance to the Antidiabetic Drug Acarbose

Overview

Journal Nature

Specialty Science

Date 2021 Nov 25

PMID 34819672

Citations 36

Authors

Jared Balaich

Michael Estrella

Guojun Wu

Philip D Jeffrey

Abhishek Biswas

Liping Zhao

Alexei Korennykh

Mohamed S Donia

Affiliations

Soon will be listed here.

Abstract

The human microbiome encodes a large repertoire of biochemical enzymes and pathways, most of which remain uncharacterized. Here, using a metagenomics-based search strategy, we discovered that bacterial members of the human gut and oral microbiome encode enzymes that selectively phosphorylate a clinically used antidiabetic drug, acarbose, resulting in its inactivation. Acarbose is an inhibitor of both human and bacterial α-glucosidases, limiting the ability of the target organism to metabolize complex carbohydrates. Using biochemical assays, X-ray crystallography and metagenomic analyses, we show that microbiome-derived acarbose kinases are specific for acarbose, provide their harbouring organism with a protective advantage against the activity of acarbose, and are widespread in the microbiomes of western and non-western human populations. These results provide an example of widespread microbiome resistance to a non-antibiotic drug, and suggest that acarbose resistance has disseminated in the human microbiome as a defensive strategy against a potential endogenous producer of a closely related molecule.

Citing Articles

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