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关于新型利福霉素用于结核病间歇化疗适用性的体外观察

In vitro observations on the suitability of new rifamycins for the intermittent chemotherapy of tuberculosis.

作者信息

Dickinson J M, Mitchison D A

机构信息

Department of Bacteriology, Royal Postgraduate Medical School, London.

出版信息

Tubercle. 1987 Sep;68(3):183-93. doi: 10.1016/0041-3879(87)90054-7.

Abstract

The bactericidal activity of six new rifamycin derivatives--rifabutin (RBU), FCE 22250 (F22), rifapentine (RPE), CGP 29861 (C29), CGP 7040 (C70) and CGP 27557 (C27) and rifampicin (RMP)--have been measured against log phase and, as a better test of sterilising activity, against stationary phase cultures of Mycobacterium tuberculosis, H37Rv. The order of activity of 1.0 and 0.2 mg/l rifamycin against log phase cultures was RMP greater than RPE & C27 greater than RBU & C29 greater than C70. The order of activity of 1.0 and 0.4 mg/l, adjusted for stability of the rifamycin, against stationary phase cultures was F22 & RMP greater than RBU greater than RPE greater than C27 & C29 greater than C70. Viable counts were done during and after pulsed exposures of 6, 24 or 96 h to C29 and RMP. The curves were similar though C29 was less bactericidal and the lag period before recovery was 1-2 days longer. F22, having high bactericidal activity against stationary organisms and a long half-life, was considered likely to be the most effective sterilising drug.

摘要

已测定六种新型利福霉素衍生物——利福布汀(RBU)、FCE 22250(F22)、利福喷汀(RPE)、CGP 29861(C29)、CGP 7040(C70)和CGP 27557(C27)以及利福平(RMP)对结核分枝杆菌H37Rv对数生长期培养物的杀菌活性,并且作为对杀菌活性的更好测试,还测定了它们对稳定期培养物的杀菌活性。1.0毫克/升和0.2毫克/升利福霉素对对数生长期培养物的活性顺序为:RMP>RPE和C27>RBU和C29>C70。针对稳定期培养物,根据利福霉素的稳定性调整后的1.0毫克/升和0.4毫克/升利福霉素的活性顺序为:F22和RMP>RBU>RPE>C27和C29>C70。在对C29和RMP进行6小时、24小时或96小时的脉冲暴露期间及之后进行了活菌计数。曲线相似,尽管C29的杀菌作用较弱,恢复前的延迟期长1 - 2天。F22对稳定期菌具有高杀菌活性且半衰期长,被认为可能是最有效的杀菌药物。

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