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Development of Cyclobutene‐ and Cyclobutane‐Functionalized Fatty Acids with Inhibitory Activity against Mycobacterium tuberculosis
Authors:Wantanee Sittiwong  Denise K Zinniel  Robert J Fenton  Darrell D Marshall  Courtney B Story  Dr Bohkyung Kim  Prof Ji‐Young Lee  Prof Robert Powers  Prof Raúl G Barletta  Prof Patrick H Dussault
Affiliation:1. Department of Chemistry, University of Nebraska‐Lincoln, Lincoln, NE 68588‐0304 (USA);2. School of Veterinary Medicine and Biomedical Sciences, University of Nebraska‐Lincoln, Lincoln, NE 68583‐0905 (USA);3. Department of Nutritional Sciences, University of Connecticut, Storrs, CT 06269‐4017 (USA)
Abstract:Eleven fatty acid analogues incorporating four‐membered carbocycles (cyclobutenes, cyclobutanes, cyclobutanones, and cyclobutanols) were investigated for the ability to inhibit the growth of Mycobacterium smegmatis (Msm) and Mycobacterium tuberculosis (Mtb). A number of the analogues displayed inhibitory activity against both mycobacterial species in minimal media. Several of the molecules displayed potent levels of inhibition against Mtb, with MIC values equal to or below those observed with the anti‐tuberculosis drugs D ‐cycloserine and isoniazid. In contrast, two of the analogues that display the greatest activity against Mtb failed to inhibit E. coli growth under either set of conditions. Thus, the active molecules identified herein may provide the basis for the development of anti‐mycobacterial agents against Mtb.
Keywords:cyclobutanes  cyclobutenes  fatty acids  mycobacteria  tuberculosis
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