Efficacy of intermittent pyrazinamide in experimental murine tuberculosis

J.M. Dickinson, D.A. Mitchison
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引用次数: 9

Abstract

CFLP mice were infected intravenously with Mycobacterium tuberculosis strain H37Rv and the progress of chemotherapy was followed by counts of viable bacilli in the lung and spleen. After spleen counts had reached log10 7.0, 12 experimental groups, each containing 10 mice, were treated for 8 weeks with pyrazinamide (PZA) given in mean daily dosages of 100, 200 or 400 mg/kg/day, with the interval between the doses within each dosage group being 1, 2,4 or 8 days. All mice were also given 25 mg isoniazid/kg daily. An increase in the mean daily dosage from 100 mg PZA/kg to 400 mg PZA/kg resulted in a decrease of spleen viable counts at the end of treatment from log10 4.2 to log10 3.8. The organ counts, averaged over the full dosage range, were little altered by spacing out the interval between doses from 1–4 days, while increasing dose size proportionately: the counts with low mean dosages tended, however, to decrease (indicating improved efficacy) while those with high mean dosages increased (P<0.001). Counts increased when the interval was 8 days. Spacing out the doses while keeping the dose size constant resulted in progressive loss of efficacy. These findings suggest that, if PZA is given intermittently, the size of the dose should be increased, though not quite proportionately, to maintain full efficacy. Even with such an increase in dose, however, once weekly treatment would be less effective.

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间歇性吡嗪酰胺治疗实验性小鼠肺结核的疗效
采用H37Rv结核分枝杆菌静脉感染CFLP小鼠,观察化疗进展,肺、脾活杆菌计数。脾脏计数达到log10 7.0后,12个实验组,每组10只小鼠,分别给予吡嗪酰胺(PZA) 100、200、400 mg/kg/day的平均日剂量,每组剂量间隔为1、2、4、8天,治疗8周。所有小鼠每天给予异烟肼25 mg /kg。将平均日剂量从100 mg PZA/kg增加到400 mg PZA/kg,导致脾脏活菌计数在治疗结束时从log10 4.2减少到log10 3.8。在1-4天的剂量间隔中,器官计数在整个剂量范围内的平均值几乎没有改变,同时按比例增加剂量大小:然而,低平均剂量的计数倾向于减少(表明疗效改善),而高平均剂量的计数则增加(P<0.001)。间隔8天,计数增加。在保持剂量大小不变的情况下,间隔剂量导致疗效逐渐丧失。这些发现表明,如果间歇性地给予PZA,剂量的大小应该增加,尽管不是完全成比例,以保持充分的疗效。然而,即使增加了这样的剂量,每周一次的治疗效果也会降低。
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