Degradation-resistant trehalose analogues block utilization of trehalose by hypervirulent Clostridioides difficile

Authors

Noah D. Danielson, Central Michigan University
James Collins, Baylor College of Medicine
Alicyn I. Stothard, Central Michigan University
Qing Qing Dong, Central Michigan University
Karishma Kalera, Central Michigan University
Peter J. Woodruff PhD, University of Southern MaineFollow
Brian J. DeBosch, Washington University School of Medicine
Robert A. Britton, Baylor College of Medicine
Benjamin M. Swarts, Central Michigan University

Document Type

Article

Publication Date

4-15-2019

Publication Title

Chemical Communications

Abstract

Trehalose is used as an additive in thousands of foods, cosmetics, and pharmaceutical products, and it is being investigated as a therapeutic for multiple human diseases. However, its ability to be used as a carbon source by microbes is a concern, as highlighted by the recent finding that trehalose can be metabolized by and potentially enhance the virulence of epidemic Clostridioides difficile. Here, we show that trehalose analogues designed to resist enzymatic degradation are incapable of being used as carbon sources by C. difficile. Furthermore, we demonstrate that trehalose analogues, but not the known trehalase inhibitor validamycin A, inhibit native trehalose utilization by hypervirulent C. difficile. Thus, degradation-resistant trehalose analogues are valuable as trehalase inhibitors and as surrogates for or co-additives with trehalose in applications where enzymatic breakdown is a concern.

Recommended Citation

Danielson, N.D., Collins, J., Stothard, A.I., Dong, Q.Q., Kalera, K., Woodruff, P.J., DeBosch, B.J., Britton, R.A., & Swarts, B.M. (2019). Degradation-resistant trehalose analogues block utilization of trehalose by hypervirulent Clostridioides difficile. Chemical Communications. 55(34), 5009-5012. DOI: 10.1039/c9cc01300h