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在猪胸膜肺炎放线杆菌感染模型中,两种苄青霉素缓释制剂经修订给药方案后改善了药物治疗效果。

Improved pharmacotherapy after revised dosing regimens of two slow-release formulations of benzylpenicillin in an Actinobacillus pleuropneumoniae infection model in pigs.

作者信息

Sjölund Marie, Rosendal Thomas, Wallgren Per, Pringle Märit, Bondesson Ulf, Bengtsson Björn, Ekstrand Carl

机构信息

Department of Animal Health and Antimicrobial Strategies, Swedish Veterinary Agency, Ulls Väg 2B, 751 89, Uppsala, Sweden.

Department of Clinical Sciences, Faculty of Veterinary Medicine and Animal Science, Swedish University of Agricultural Sciences, Box 7054, 75007, Uppsala, Sweden.

出版信息

Acta Vet Scand. 2025 Apr 30;67(1):22. doi: 10.1186/s13028-025-00806-9.

Abstract

BACKGROUND

Actinobacillus pleuropneumoniae (APP) is a Gram-negative bacterium that causes respiratory disease in pigs, resulting in significant economic losses and reduced animal welfare. In Sweden, the drug of choice for treatment of APP infections is benzylpenicillin. However, limited pharmacokinetic and pharmacodynamic data for benzylpenicillin in pigs have led to variations in recommended dosing regimens. In this study, the impact of different dosing regimens and benzylpenicillin preparations on the progression of APP infection in pigs was investigated. Two experimental trials involving a total of 66 pigs were conducted. Pigs were intranasally inoculated with a pathogenic strain of APP serotype 2, and treatment was initiated upon the appearance of clinical signs. Two intramuscularly administered benzylpenicillin formulations, an aqueous and an oil-based suspension, were used with varying dosing regimens. The clinical outcome was assessed based on respiratory signs and rectal temperature measurements. Blood samples were collected for measuring white blood cell counts, serum antibody levels, and acute-phase protein concentrations. Necropsies were performed to evaluate lung lesions and to reisolate APP.

RESULTS

The results indicated that benzylpenicillin dosing regimens of 20-30 mg/kg administered every 12 h achieved larger benzylpenicillin plasma-exposure compared to the labelled dose of 10-30 mg/kg every 24 h. The oil-based suspension demonstrated superior efficacy compared to the aqueous suspension. Dosing regimens that maintain effective plasma concentrations of benzylpenicillin were shown to have better clinical outcomes as measured by reduced lung lesions at necropsy. Increased benzylpenicillin exposure was associated with a better ranking of overall treatment response.

CONCLUSIONS

Several dosing regimens that increased the plasma benzylpenicillin exposure were associated with better clinical success than the labelled doses. The findings support the treatment of APP-infected pigs with optimised benzylpenicillin dosing regimens. Optimising the use of existing antibiotics is crucial given the limited development of new antimicrobial agents and the need to combat antimicrobial resistance with regards to both human and animal health.

摘要

背景

胸膜肺炎放线杆菌(APP)是一种革兰氏阴性菌,可导致猪的呼吸道疾病,造成重大经济损失并降低动物福利。在瑞典,治疗APP感染的首选药物是苄青霉素。然而,关于苄青霉素在猪体内的药代动力学和药效学数据有限,导致推荐给药方案存在差异。在本研究中,研究了不同给药方案和苄青霉素制剂对猪APP感染进程的影响。进行了两项涉及总共66头猪的实验性试验。猪经鼻接种APP血清型2的致病菌株,并在出现临床症状时开始治疗。使用了两种肌肉注射的苄青霉素制剂,即水性和油基混悬液,并采用了不同的给药方案。根据呼吸体征和直肠温度测量评估临床结果。采集血样以测量白细胞计数、血清抗体水平和急性期蛋白浓度。进行尸检以评估肺部病变并重新分离APP。

结果

结果表明,与每24小时10 - 30 mg/kg的标记剂量相比,每12小时给予20 - 30 mg/kg的苄青霉素给药方案可实现更大的苄青霉素血浆暴露。油基混悬液显示出比水性混悬液更好的疗效。通过尸检时肺部病变减少来衡量,维持苄青霉素有效血浆浓度的给药方案显示出更好的临床结果。苄青霉素暴露增加与总体治疗反应的更好排名相关。

结论

几种增加血浆苄青霉素暴露的给药方案比标记剂量具有更好的临床成功率。这些发现支持用优化的苄青霉素给药方案治疗APP感染的猪。鉴于新抗菌药物的开发有限以及应对人类和动物健康方面的抗菌耐药性的必要性,优化现有抗生素的使用至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d717/12044999/6d338fd4aef7/13028_2025_806_Fig1_HTML.jpg

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