Literature DB >> 32914793

The role of chemoenzymatic synthesis in advancing trehalose analogues as tools for combatting bacterial pathogens.

Karishma Kalera1, Alicyn I Stothard1, Peter J Woodruff2, Benjamin M Swarts1.   

Abstract

Trehalose, a disaccharide of glucose, is increasingly recognized as an important contributor to virulence in major bacterial pathogens, such as Mycobacterium tuberculosis, Clostridioides difficile, and Burkholderia pseudomallei. Accordingly, bacterial trehalose metabolic pathways that are not present in humans have gained traction as targets for antibiotic and diagnostic development. Toward this goal, trehalose can be modified through a combination of rational design and synthesis to produce functionalized trehalose analogues, which can be deployed to probe or inhibit bacterial trehalose metabolism. However, the unique α,α-1,1-glycosidic bond and C2 symmetry of trehalose make analogue synthesis via traditional chemical methods very challenging. We and others have turned to the creation of chemoenzymatic synthesis methods, which in principle allow the use of nature's trehalose-synthesizing enzymes to stereo- and regioselectively couple simple, unprotected substrates to efficiently and conveniently generate trehalose analogues. Here, we provide a contextual account of our team's development of a trehalose analogue synthesis method that employs a highly substrate-tolerant, thermostable trehalose synthase enzyme, TreT from Thermoproteus tenax. Then, in three vignettes, we highlight how chemoenzymatic synthesis has accelerated the development of trehalose-based imaging probes and inhibitors that target trehalose-utilizing bacterial pathogens. We describe the role of TreT catalysis and related methods in the development of (i) tools for in vitro and in vivo imaging of mycobacteria, (ii) anti-biofilm compounds that sensitize drug-tolerant mycobacteria to clinical anti-tubercular compounds, and (iii) degradation-resistant trehalose analogues that block trehalose metabolism in C. difficile and potentially other trehalose-utilizing bacteria. We conclude by recapping progress and discussing priorities for future research in this area, including improving the scope and scale of chemoenzymatic synthesis methods to support translational research and expanding the functionality and applicability of trehalose analogues to study and target diverse bacterial pathogens.

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Year:  2020        PMID: 32914793      PMCID: PMC7919099          DOI: 10.1039/d0cc04955g

Source DB:  PubMed          Journal:  Chem Commun (Camb)        ISSN: 1359-7345            Impact factor:   6.222


  125 in total

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Authors:  Kerry J Welsh; Robert L Hunter; Jeffrey K Actor
Journal:  Tuberculosis (Edinb)       Date:  2013-12       Impact factor: 3.131

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Journal:  Chem Commun (Camb)       Date:  2016-11-22       Impact factor: 6.222

5.  A novel trehalose synthesizing pathway in the hyperthermophilic Crenarchaeon Thermoproteus tenax: the unidirectional TreT pathway.

Authors:  Theresa Kouril; Melanie Zaparty; Jeannette Marrero; Henner Brinkmann; Bettina Siebers
Journal:  Arch Microbiol       Date:  2008-05-16       Impact factor: 2.552

6.  Cleavage of trehalose-phosphate in Bacillus subtilis is catalysed by a phospho-alpha-(1-1)-glucosidase encoded by the treA gene.

Authors:  C Helfert; S Gotsche; M K Dahl
Journal:  Mol Microbiol       Date:  1995-04       Impact factor: 3.501

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8.  Hepatocyte ALOXE3 is induced during adaptive fasting and enhances insulin sensitivity by activating hepatic PPARγ.

Authors:  Cassandra B Higgins; Yiming Zhang; Allyson L Mayer; Hideji Fujiwara; Alicyn I Stothard; Mark J Graham; Benjamin M Swarts; Brian J DeBosch
Journal:  JCI Insight       Date:  2018-08-23

9.  Transient drug-tolerance and permanent drug-resistance rely on the trehalose-catalytic shift in Mycobacterium tuberculosis.

Authors:  Jae Jin Lee; Sun-Kyung Lee; Naomi Song; Temitope O Nathan; Benjamin M Swarts; Seok-Yong Eum; Sabine Ehrt; Sang-Nae Cho; Hyungjin Eoh
Journal:  Nat Commun       Date:  2019-07-02       Impact factor: 14.919

10.  Flux through trehalose synthase flows from trehalose to the alpha anomer of maltose in mycobacteria.

Authors:  Farzana Miah; Hendrik Koliwer-Brandl; Martin Rejzek; Robert A Field; Rainer Kalscheuer; Stephen Bornemann
Journal:  Chem Biol       Date:  2013-04-18
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  4 in total

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2.  AuCl3-Catalyzed Hemiacetal Activation for the Stereoselective Synthesis of 2-Deoxy Trehalose Derivatives.

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4.  In silico analysis and a comparative genomics approach to predict pathogenic trehalase genes in the complete genome of Antarctica Shigella sp. PAMC28760.

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  4 in total

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