In vitro activity and In vivo efficacy of Isoliquiritigenin against Staphylococcus xylosus ATCC 700404 by IGPD target.

Qianwei Qu,Xueying Chen,Chunliu Dong,Xiaoxu Xing,Zhengze Li,God’Spower Bello-Onaghise,Xiubo Li,Xin Liu,Wenqiang Cui,Yonghui Zhou,Yanhua Li,Ruixiang Che,Jinpeng Wang,Vivek Sharma

doi:10.1371/journal.pone.0226260

Abstract

Staphylococcus xylosus (S. xylosus) is a type of coagulase-negative Staphylococcus, which was previously considered as non-pathogenic. However, recent studies have linked it with cases of mastitis in cows. Isoliquiritigenin (ISL) is a bioactive compound with pharmacological functions including antibacterial activity. In this study, we evaluated the effect of ISL on S. xylosus in vitro and in vivo. The MIC of ISL against S. xylosus was 80 μg/mL. It was observed that sub-MICs of ISL (1/2MIC, 1/4MIC, 1/8MIC) significantly inhibited the formation of S. xylosus biofilm in vitro. Previous studies have observed that inhibiting imidazole glycerol phosphate dehydratase (IGPD) concomitantly inhibited biofilm formation in S. xylosus. So, we designed experiments to target the formation of IGPD or inhibits its activities in S. xylosus ATCC 700404. The results indicated that the activity of IGPD and its histidine content decreased significantly under 1/2 MIC (40 μg/mL) ISL, and the expression of IGPD gene (hisB) and IGPD protein was significantly down-regulated. Furthermore, Bio-layer interferometry experiments showed that ISL directly interacted with IGPD protein (with strong affinity; KD = 234 μM). In addition, molecular docking was used to predict the binding mode of ISL and IGPD. In vivo tests revealed that, ISL significantly reduced TNF-α and IL-6 levels, mitigated the destruction of the mammary glands and reversed the production of inflammatory cells in mice. The results of the study suggest that, ISL may inhibit S. xylosus growth by acting on IGPD, which can be used as a target protein to treat infections caused by S. xylosus.

Highlights

Bovine mastitis is globally recognized as the most common and costly disease affecting dairy herds [1]
This study shows the antibacterial potential of Isoliquiritigenin against S. xylosus by regulating the expression of imidazole glycerol phosphate dehydratase (IGPD), and revealed the mechanism by which ISL attenuates the virulence of S.xylosus
The broth dilution method was used to determine the Minimum inhibitory concentration (MIC), which quantified the antibacterial effect of ISL on S. xylosus

Summary

Introduction

Bovine mastitis is globally recognized as the most common and costly disease affecting dairy herds [1]. More than 50 Staphylococcus species and subspecies have been characterized as causal agents of staphylococcal mastitis. CNS infection is increasingly recognized as the leading cause of clinical and subclinical dairy cow mastitis worldwide. CNS species tend to be more resistant to antimicrobials than Staphylococcus aureus (S. aureus), and they develop multi-resistance [2, 3]. Recent studies have shown that it is the main bacterial isolate in cows with cases of mastitis caused by CNS [6, 7]. Clinical isolates of S. xylosus have multiple drug-resistant phenotypes, which has made the treatment of dairy cow mastitis very difficult [6]. The need to develop new drugs with novel antibacterial mechanisms is very vital in the treatment of Staphylococcal mastitis in dairy cows

Methods

Results

Conclusion