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Featured researches published by Xiao-Jun Kong.


Toxicology and Applied Pharmacology | 2017

UPLC-Q-TOF/MS-based urine and plasma metabonomics study on the ameliorative effects of aspirin eugenol ester in hyperlipidemia rats

Ning Ma; Isam Karam; Xi-Wang Liu; Xiao-Jun Kong; Zhe Qin; Shihong Li; Zenghua Jiao; Pengcheng Dong; Ya-Jun Yang; Jian-Yong Li

ABSTRACT The main objective of this study was to investigate the ameliorative effects of aspirin eugenol ester (AEE) in hyperlipidemic rat. After five‐week oral administration of AEE in high fat diet (HFD)‐induced hyperlipidemic rats, the impact of AEE on plasma and urine metabonomics was investigated to explore the underlying mechanism by UPLC‐Q‐TOF/MS analysis. Blood lipid levels and histopathological changes of liver, stomach and duodenum were also evaluated after AEE treatment. Without obvious gastrointestinal (GI) side effects, AEE significantly relieved fatty degeneration of liver and reduced triglyceride (TG), low density lipoprotein (LDL) and total cholesterol (TCH) (P < 0.01). Clear separations of metabolic profiles were observed among control, model and AEE groups by using principal component analysis (PCA) and orthogonal partial least‐squares‐discriminate analysis (OPLS‐DA). 16 endogenous metabolites in plasma and 18 endogenous metabolites in urine involved in glycerophospholipid metabolism, fatty acid metabolism, fatty acid beta‐oxidation, amino acid metabolism, TCA cycle, sphingolipid metabolism, gut microflora and pyrimidine metabolism were considered as potential biomarkers of hyperlipidemia and be regulated by AEE administration. It might be concluded that AEE was a promising drug candidate for hyperlipidemia treatment. These findings could contribute to the understanding of action mechanisms of AEE and provide evidence for further studies. Graphical abstract Figure. No Caption available. HighlightsAspirin eugenol eater (AEE) reduced blood lipid levels.AEE relieved fatty degeneration in liver in hyperlipidemic rat.36 biomarkers associated with hyperlipidemia were regulated by AEE.Potential mechanism of AEE on hyperlipidemia was revealed by pathway analysis.


Food Chemistry | 2016

Simultaneous determination of diaveridine, trimethoprim and ormetoprim in feed using high performance liquid chromatography tandem mass spectrometry.

Ya-Jun Yang; Xi-Wang Liu; Bing Li; Shihong Li; Xiao-Jun Kong; Zhe Qin; Jian-Yong Li

This study developed and validated a simple and reliable method for detecting and quantifying DVD, TMP and OMP in feed using dichloromethane extraction followed by HPLC-MS/MS. A matrix effect evaluation was performed using the post-extraction spiking method, and levels were less than ±15% in all three feeds with their corresponding concentrations. LOD and LOQ, CCα and CCβ were 20μgkg(-1) and 40μgkg(-1), 8.68-15.55μgkg(-1) and 10.61-18.92μgkg(-1) for all analytes, respectively. Calibration curves were linear for DVD, TMP and OMP with R(2)⩾0.990 and r⩾0.995, respectively. Recoveries of low, medium and high concentrations using the proposed method ranged from 74.4 to 105.2%. Repeatability and within-laboratory reproducibility were <7.4% (RSD). The chosen seven factors had no a significant influence on robustness. The method showed good performance when it was applied to analyze other laboratory-prepared or actual feed samples.


PLOS ONE | 2018

Differences in the intestinal microbiota between uninfected piglets and piglets infected with porcine epidemic diarrhea virus

Meizhou Huang; Shengyi Wang; Hui Wang; Dongan Cui; Ya-Jun Yang; Xi-Wang Liu; Xiao-Jun Kong; Jian-Yong Li

Porcine epidemic diarrhea, a disastrous gastrointestinal disease, causes great financial losses due to its high infectivity, morbidity and mortality in suckling piglets despite the development and application of various vaccines. In this study, high-throughput sequencing was used to explore differences in the intestinal microbiota between uninfected piglets and piglets infected with porcine epidemic diarrhea virus (PEDV). The results revealed that the small intestinal microbiota of suckling piglets infected with PEDV showed low diversity and was dominated by Proteobacteria (49.1%). Additionally, the composition of the small intestinal microbiota of sucking piglets infected with PEDV showed marked differences from that of the uninfected piglets. Some of the taxa showing differences in abundance between uninfected piglets and piglets infected with PEDV were associated with cellular transport and catabolism, energy metabolism, the biosynthesis of other secondary metabolites, and amino acid metabolism as determined through the prediction of microbial function based on the bacterial 16S rRNA gene. Therefore, adjusting the intestinal microbiota might be a promising method for the prevention or treatment of PEDV.


Scientific Reports | 2017

UPLC-Q-TOF/MS-based metabonomic studies on the intervention effects of aspirin eugenol ester in atherosclerosis hamsters

Ning Ma; Ya-Jun Yang; Xi-Wang Liu; Xiao-Jun Kong; Shihong Li; Zhe Qin; Zenghua Jiao; Jian-Yong Li

Based on the pro-drug principle, aspirin and eugenol were used to synthesize aspirin eugenol ester (AEE) by esterification reaction. In present study, the anti-atherosclerosis effects of AEE were investigated in hamsters with the utilization of metabonomic approach based on UPLC-Q-TOF/MS. Biochemical parameters and histopathological injures in stomach, liver and aorta were evaluated. In atherosclerotic hamster, oral administration of AEE normalized biochemical profile such as reducing TG, TCH and LDL, and significantly reduced body weight gain, alleviated hepatic steatosis and improved pathological lesions in aorta. Slight damages in stomach mucous were found in AEE group. Plasma and urine samples in control, model and AEE groups were scattered in the partial least squares-discriminate analysis (PLS-DA) score plots. Thirteen endogenous metabolites in plasma such as lysophosphatidylcholine (LysoPC), leucine and valine, and seventeen endogenous metabolites in urine such as citric acid, phenol sulphate and phenylacetylglycine were selected as potential biomarkers associated with atherosclerosis. They were considered to be in response to anti-atherosclerosis effects of AEE, mainly involved in glycerophospholipid metabolism, amino acid metabolism and energy metabolism. This study extended the understanding of endogenous alterations of atherosclerosis and offered insights into the pharmacodynamic activity of AEE.


Molecules | 2018

Preparation and Evaluation of Oseltamivir Molecularly Imprinted Polymer Silica Gel as Liquid Chromatography Stationary Phase

Ya-Jun Yang; Xi-Wang Liu; Xiao-Jun Kong; Zhe Qin; Zenghua Jiao; Shihong Li; Jian-Yong Li

To improve the chromatographic performance of an oseltamivir (OS) molecularly imprinted polymer (MIP), silica gel coated with an MIP layer for OS (OSMIP@silica gel) was prepared by the surface molecular imprinting technology on the supporter of porous silica gel microspheres. A nonimprinted polymer with the silica gel (NIP@silica gel) was also prepared for comparison. The obtained particles were characterized through FT–IR, scanning electron microscopy, specific surface area analysis, and porosity measurements. The results indicated that the polymer was successfully synthesized and revealed the structural differences between imprinted and nonimprinted polymers. The results of static adsorption experiments showed that adsorption quantity of the OSMIP@silica gel for OS was higher than that for NIP@silica gel, and the OSMIP@silica gel had two kinds of affinity sites for OS but the NIP@silica gel had one. The chromatographic performance of the OSMIP@silica gel column had significant improvement. The imprinting factor of the OSMIP@silica gel column for OS was 1.64. Furthermore, the OSMIP@silica gel column showed good affinity and selectivity for template OS and another neuraminidase inhibitor, peramivir, but not for quinocetone. These results indicated that the prepared OSMIP could be used to simulate the activity center of neuraminidase, and the OSMIP@silica gel column could be also employed in future studies to search for more active neuraminidase inhibitor analogues from traditional Chinese herbs.


Hubei Agricultural Sciences | 2013

Advances in Pharmacological Research of Eugenol

Xiao-Jun Kong; Xi-Wang Liu; Jianyong Li; Ya-Jun Yang


BMC Veterinary Research | 2015

Regulation effect of Aspirin Eugenol Ester on blood lipids in Wistar rats with hyperlipidemia

Isam Karam; Ning Ma; Xi-Wang Liu; Shihong Li; Xiao-Jun Kong; Jian-Yong Li; Ya-Jun Yang


BMC Veterinary Research | 2016

Evaluation on antithrombotic effect of aspirin eugenol ester from the view of platelet aggregation, hemorheology, TXB2/6-keto-PGF1α and blood biochemistry in rat model

Ning Ma; Xi-Wang Liu; Ya-Jun Yang; Dong-Shuai Shen; Xiao-Le Zhao; Isam Mohamed; Xiao-Jun Kong; Jian-Yong Li


Lipids in Health and Disease | 2016

Lowering effects of aspirin eugenol ester on blood lipids in rats with high fat diet

Isam Karam; Ning Ma; Xi-Wang Liu; Xiao-Jun Kong; Xiao-Le Zhao; Ya-Jun Yang; Jian-Yong Li


Toxicology Letters | 2017

A 150-day oral dose toxicity study of aspirin eugenol ester in Wistar rats

Xiao-Le Zhao; Xiao-Jun Kong; Xi-Wang Liu; Ya-Jun Yang; Ning Ma; Zhe Qin; Shihong Li; Zenghua Jiao; Jian-Yong Li

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