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ACS medicinal chemistry letters
Mar 14, 2019;10 (3): 374-377.

Expanded Structure-Activity Studies of Lipoxazolidinone Antibiotics.

Kaylib R Robinson, Jonathan J Mills, Joshua G Pierce
Author Information
  1. Kaylib R Robinson: Department of Chemistry and Comparative Medicine Institute, NC State University, Raleigh, North Carolina 27695, United States.
  2. Jonathan J Mills: Department of Chemistry and Comparative Medicine Institute, NC State University, Raleigh, North Carolina 27695, United States.
  3. Joshua G Pierce: Department of Chemistry and Comparative Medicine Institute, NC State University, Raleigh, North Carolina 27695, United States.
PMID: 30891143 DOI: 10.1021/acsmedchemlett.9b00015

Abstract

The lipoxazolidinone family of marine natural products, which contains an unusual 4-oxazolidinone core, was found to possess potent antimicrobial activity against methicillin resistant (MRSA). Herein, we expanded our previous synthetic efforts by preparing selected aryl derivatives of the lipoxazolidinones and further evaluating the potential to expand the activity of this class of molecules to Gram-negative pathogens. With these analogs, we explored the effect of varying the substitution pattern around the aromatic ring, increasing the chain length between the oxazolidinone core and the aryl system, and how altering the position of more polar functional groups affected the antimicrobial activity. Finally, we utilized a TolC knockout strain of to demonstrate that our compounds are subject to efflux in Gram-negative pathogens, and activity is restored in these knockouts. Together these results provide additional data for the further development of 4-oxazolidinone analogs , , and for the treatment of infectious disease.

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Grants

  1. R01 GM110154/NIGMS NIH HHS
Journal Article
Article has an altmetric score of 3

Word Cloud

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