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生长基质对猪肺炎病原体抗菌药物药效学的影响。

Impact of growth matrix on pharmacodynamics of antimicrobial drugs for pig pneumonia pathogens.

作者信息

Dorey Lucy, Lees Peter

机构信息

The Royal Veterinary College, Hawkshead Campus, Herts, AL97TA, Hatfield, UK.

出版信息

BMC Vet Res. 2017 Jun 23;13(1):192. doi: 10.1186/s12917-017-1086-4.

Abstract

BACKGROUND

The most widely used measure of potency of antimicrobial drugs is Minimum Inhibitory Concentration (MIC). MIC is usually determined under standardised conditions in broths formulated to optimise bacterial growth on a species-by-species basis. This ensures comparability of data between laboratories. However, differences in values of MIC may arise between broths of differing chemical composition and for some drug classes major differences occur between broths and biological fluids such as serum and inflammatory exudate. Such differences must be taken into account, when breakpoint PK/PD indices are derived and used to predict dosages for clinical use. There is therefore interest in comparing MIC values in several broths and, in particular, in comparing broth values with those generated in serum. For the pig pneumonia pathogens, Actinobacillus pleuropneumoniae and Pasteurella multocida, MICs were determined for three drugs, florfenicol, oxytetracycline and marbofloxacin, in five broths [Mueller Hinton Broth (MHB), cation-adjusted Mueller Hinton Broth (CAMHB), Columbia Broth supplemented with NAD (CB), Brain Heart Infusion Broth (BHI) and Tryptic Soy Broth (TSB)] and in pig serum.

RESULTS

For each drug, similar MIC values were obtained in all broths, with one exception, marbofloxacin having similar MICs for three broths and 4-5-fold higher MICs for two broths. In contrast, for both organisms, quantitative differences between broth and pig serum MICs were obtained after correction of MICs for drug binding to serum protein (fu serum MIC). Potency was greater (fu serum MIC lower) in serum than in broths for marbofloxacin and florfenicol for both organisms. For oxytetracycline fu serum:broth MIC ratios were 6.30:1 (P. multocida) and 0.35:1 (A. pleuropneumoniae), so that potency of this drug was reduced for the former species and increased for the latter species. The chemical composition of pig serum and broths was compared; major matrix differences in 14 constituents did not account for MIC differences. Bacterial growth rates were compared in broths and pig serum in the absence of drugs; it was concluded that broth/serum MIC differences might be due to differing growth rates in some but not all instances.

CONCLUSIONS

For all organisms and all drugs investigated in this study, it is suggested that broth MICs should be adjusted by an appropriate scaling factor when used to determine pharmacokinetic/pharmacodynamic breakpoints for dosage prediction.

摘要

背景

抗菌药物效力最广泛使用的衡量指标是最低抑菌浓度(MIC)。MIC通常在标准化条件下,在为优化各菌种细菌生长而配制的肉汤中测定。这确保了各实验室之间数据的可比性。然而,不同化学成分的肉汤之间MIC值可能会出现差异,对于某些药物类别,肉汤与生物流体(如血清和炎性渗出液)之间会出现重大差异。在推导和使用断点PK/PD指数来预测临床用药剂量时,必须考虑到这些差异。因此,人们有兴趣比较几种肉汤中的MIC值,特别是将肉汤中的值与血清中产生的值进行比较。对于猪肺炎病原体胸膜肺炎放线杆菌和多杀性巴氏杆菌,在五种肉汤[穆勒-欣顿肉汤(MHB)、阳离子调整穆勒-欣顿肉汤(CAMHB)、补充NAD的哥伦比亚肉汤(CB)、脑心浸液肉汤(BHI)和胰蛋白胨大豆肉汤(TSB)]和猪血清中,测定了三种药物氟苯尼考、土霉素和马波沙星的MIC。

结果

对于每种药物,除了一个例外,在所有肉汤中获得了相似的MIC值,马波沙星在三种肉汤中的MIC相似,在两种肉汤中的MIC高4至5倍。相比之下,对于这两种微生物,在对药物与血清蛋白结合的MIC进行校正(血清游离MIC)后,肉汤和猪血清MIC之间存在定量差异。对于两种微生物,马波沙星和氟苯尼考在血清中的效力更大(血清游离MIC更低)。对于土霉素,血清游离MIC与肉汤MIC的比率分别为6.30:1(多杀性巴氏杆菌)和0.35:1(胸膜肺炎放线杆菌),因此该药物对前一种菌种的效力降低,对后一种菌种的效力增加。比较了猪血清和肉汤的化学成分;14种成分的主要基质差异并不能解释MIC差异。在无药物情况下比较了肉汤和猪血清中的细菌生长速率;得出结论,肉汤/血清MIC差异在某些但并非所有情况下可能是由于生长速率不同所致。

结论

对于本研究中调查的所有微生物和所有药物,建议在用于确定药代动力学/药效学断点以预测剂量时,应通过适当的比例因子调整肉汤MIC。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb7e/5481914/5298be1880d4/12917_2017_1086_Fig1_HTML.jpg

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