猫须草叶水提取物可预防小鼠膀胱和肾脏感染。
Aqueous extract from Orthosiphon stamineus leaves prevents bladder and kidney infection in mice.
作者信息
Sarshar S, Brandt S, Asadi Karam M R, Habibi M, Bouzari S, Lechtenberg M, Dobrindt U, Qin X, Goycoolea F M, Hensel A
机构信息
University of Münster, Institute of Pharmaceutical Biology and Phytochemistry, Corrensstrasse 48, D-48149 Münster, Germany.
Department of Molecular Biology, Pasteur Institute of Iran, Pasteur Avenue, Teheran 13164, Iran.
出版信息
Phytomedicine. 2017 May 15;28:1-9. doi: 10.1016/j.phymed.2017.02.009. Epub 2017 Feb 28.
BACKGROUND
Extracts from the leaves of Orthosiphon stamineus are used in phytotherapy for treatment of uncomplicated urinary tract infections.
PURPOSES
Evaluation of an aqueous extract against infection with uropathogenic Escherichia coli in vivo; investigation of underlying microbiological mechanisms.
STUDY DESIGN
In vivo studies in mice and in vitro investigations on cytotoxicity, antiadhesive potential, influence on bacterial gene expression and quorum sensing.
METHODS
Extract OWE was prepared by hot water extraction. For in vivo studies BALB/c mice were used in an UPEC infection model. The effect of OWE on bacterial load in bladder/kidney tissue was monitored in pre- and posttreatment. Cytotoxicity of OWE against different UPEC strains, T24 bladder/A498 kidney cells, gene expression analysis, monitoring of phenotypic motility and quorum sensing was investigated by standard methods of microbiology.
RESULTS
OWE was quantified (UHPLC) according to the content of rosmarinic acid, cichoric acid, caffeic acid. Three- and 5-day treatment of animals with OWE (750mg/kg) after transurethral infection with UPEC CFT073 reduced the bacterial load in bladder and kidney, similar to norfloxacin. Four- and 7-day pretreatment of mice prior to the infection with UPEC NU14 reduced bacterial bladder colonization. In vitro investigations indicated that OWE (≤2mg/ml) has no cytotoxic or proliferation-inhibiting activity against different UPEC strains as well as against T24 bladder and A498 kidney cells. OWE exerts a dose dependent antiadhesive activity against UPEC strains NU14 and UTI89. OWE reduced gene expression of fimH, but evoked increase of the expression of motility/fitness gene fliC. Increase of bacterial motility on gene level was confirmed by a changed bacterial phenotype by an increased bacterial motility in soft agar assay. OWE inhibited in a concentration-dependent manner bacterial quorum sensing.
CONCLUSION
OWE is assessed as a strong antiadhesive plant extract for which the traditional use in phytotherapy for UTI might be justified.
背景
猫须草叶提取物用于植物疗法治疗单纯性尿路感染。
目的
评估水提取物对体内致病性大肠杆菌感染的作用;研究潜在的微生物学机制。
研究设计
小鼠体内研究以及对细胞毒性、抗黏附潜力、对细菌基因表达和群体感应影响的体外研究。
方法
通过热水提取制备提取物OWE。在体内研究中,BALB/c小鼠用于致病性大肠杆菌感染模型。在治疗前后监测OWE对膀胱/肾脏组织中细菌载量的影响。通过微生物学标准方法研究OWE对不同致病性大肠杆菌菌株、T24膀胱/A498肾细胞的细胞毒性、基因表达分析、表型运动性监测和群体感应。
结果
根据迷迭香酸、菊苣酸、咖啡酸的含量对OWE进行定量(超高效液相色谱法)。经尿道感染致病性大肠杆菌CFT073后,用OWE(750mg/kg)对动物进行3天和5天治疗,可降低膀胱和肾脏中的细菌载量,与诺氟沙星相似。在用致病性大肠杆菌NU14感染小鼠之前进行4天和7天预处理可减少细菌在膀胱的定植。体外研究表明,OWE(≤2mg/ml)对不同致病性大肠杆菌菌株以及T24膀胱和A498肾细胞没有细胞毒性或增殖抑制活性。OWE对致病性大肠杆菌菌株NU14和UTI89具有剂量依赖性抗黏附活性。OWE降低了fimH的基因表达,但引起运动性/适应性基因fliC表达增加。通过软琼脂试验中细菌运动性增加的变化细菌表型,在基因水平上证实了细菌运动性的增加。OWE以浓度依赖性方式抑制细菌群体感应。
结论
OWE被评估为一种强大的抗黏附植物提取物,其在植物疗法中用于治疗尿路感染的传统用途可能是合理的。
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