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延长氟康唑治疗对植入小鼠体内扩散小室中白色念珠菌的影响。

Effect of prolonged fluconazole treatment on Candida albicans in diffusion chambers implanted into mice.

作者信息

Sohnle Peter G, Hahn Beth L

机构信息

Division of Infectious Diseases, Department of Medicine, Medical College of Wisconsin, Milwaukee 53226, USA.

出版信息

Antimicrob Agents Chemother. 2002 Oct;46(10):3175-9. doi: 10.1128/AAC.46.10.3175-3179.2002.

Abstract

Fluconazole is an azole agent with primarily fungistatic activity in standard in vitro susceptibility tests. The present study was undertaken to develop a diffusion chamber model system in mice in order to study the in vivo effects of prolonged fluconazole treatment on Candida albicans. Chambers containing 100 C. albicans yeast cells were implanted subcutaneously on the flanks of C57BL/6 mice and were then retrieved 6 or 14 weeks later (after fluconazole treatment for 4 or 12 weeks, respectively). Leukocyte counts demonstrated that implantation of the chambers did elicit an inflammatory response but that only small numbers of inflammatory cells were able to enter the chamber interior. Treatment with fluconazole at 10 mg/kg of body weight/day for 12 weeks not only reduced the numbers of viable organisms within the chambers compared to those in untreated mice (mean +/- standard deviation of log(10) CFU of 0.7 +/- 1.2 versus 2.3 +/- 2.0; P < 0.001 by the Bonferroni test) but also increased the numbers of chambers that became sterile over the treatment period (14 of 16 versus 6 of 19; P = 0.0009 by the chi-square test). However, treatment for only 4 weeks had minimal effects on the numbers of chamber CFU, and none of the chambers became sterile during this period. Distribution of retrieved organisms between interior fluid and the chamber filters was approximately equal in all the treatment groups. This model system appears to be useful for evaluating the effects of antifungal drugs over prolonged periods in vivo. Its use in the present study demonstrates that fluconazole can increase the rate of sterilization of C. albicans foci that are protected from the host's inflammatory response.

摘要

氟康唑是一种唑类药物,在标准体外药敏试验中主要具有抑菌活性。本研究旨在建立一种小鼠扩散室模型系统,以研究长期氟康唑治疗对白色念珠菌的体内作用。将含有100个白色念珠菌酵母细胞的扩散室皮下植入C57BL/6小鼠的胁腹,然后在6周或14周后取出(分别在氟康唑治疗4周或12周后)。白细胞计数表明,扩散室的植入确实引发了炎症反应,但只有少量炎症细胞能够进入扩散室内部。以10mg/kg体重/天的剂量给予氟康唑治疗12周,与未治疗的小鼠相比,不仅降低了扩散室内活菌的数量(log(10)CFU的平均值±标准差为0.7±1.2,而未治疗小鼠为2.3±2.0;经Bonferroni检验,P<0.001),而且增加了在治疗期间变为无菌的扩散室数量(16个中有14个,而19个中有6个;经卡方检验,P=0.0009)。然而,仅治疗4周对扩散室CFU数量的影响最小,在此期间没有扩散室变为无菌。在所有治疗组中,取出的生物体在内部液体和扩散室过滤器之间的分布大致相等。该模型系统似乎可用于评估抗真菌药物在体内长时间的作用。在本研究中的应用表明,氟康唑可以提高免受宿主炎症反应影响的白色念珠菌病灶的杀菌率。

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Antifungal susceptibility testing of yeasts: a brief overview.酵母的抗真菌药敏试验:简要概述
Clin Infect Dis. 1993 Nov;17 Suppl 2:S494-500. doi: 10.1093/clinids/17.supplement_2.s494.

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