Identification of a novel oxazolidinone (U-100480) with potent antimycobacterial activity

被引:230
作者
Barbachyn, MR
Hutchinson, DK
Brickner, SJ
Cynamon, MH
Kilburn, JO
Klemens, SP
Glickman, SE
Grega, KC
Hendges, SK
Toops, DS
Ford, CW
Zurenko, GE
机构
[1] SUNY HLTH SCI CTR,SYRACUSE,NY 13210
[2] VET AFFAIRS MED CTR,SYRACUSE,NY 13210
[3] CTR DIS CONTROL,ATLANTA,GA 30333
关键词
D O I
10.1021/jm950956y
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
During the course of our investigations in the oxazolidinone antibacterial agent area, we have identified a subclass with especially potent in vitro activity against mycobacteria. The salient structural feature of these oxazolidinone analogues, 6 (U-100480), 7 (U-101603), and 8 (U-101244), is their appended thiomorpholine moiety. The rational design, synthesis, and evaluation of the in vitro antimycobacterial activity of these analogues is described. Potent activity against a screening strain of Mycobacterium tuberculosis was demonstrated by 6 and 7 (minimum inhibitory concentrations or MIC's less than or equal to 0.125 mu g/mL). Oxazolidinones 6 and 8 exhibit MIC(90) values of 0.50 mu g/mL or less against a panel of organisms consisting of five drug-sensitive and five multidrug-resistant strains of M. tuberculosis, with 6 being the most active congener. Potent in vitro activity against other mycobacterial species was also demonstrated by 6. For example, 6 exhibited excellent in vitro activity against multiple clinical isolates of Mycobacterium avium complex (MIC's = 0.5-4 mu g/mL). Orally administered 6 displays in vivo efficacy against M. tuberculosis and M. avium similar to that of clinical comparators isoniazid and azithromycin, respectively. Consideration of these factors, along with a favorable pharmacokinetic and chronic toxicity profile in rats, suggests that 6 (U-100480) is a promising antimycobacterial agent.
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收藏
页码:680 / 685
页数:6
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