Luteolin alleviates ulcerative colitis in rats via regulating immune response, oxidative stress, and metabolic profiling

Author:

Li Bolin123,Guo Yuxi4,Jia Xuemei4,Cai Yanru1,Zhang Yunfeng53,Yang Qian523

Affiliation:

1. Department of Gastroenterology, Hebei Provincial Hospital of Chinese Medicine , Shijiazhuang , Hebei , China

2. Key Laboratory of Integrated Chinese and Western Medicine for Gastroenterology Research (Hebei) , Shijiazhuang , Hebei , China

3. Hebei Key Laboratory of Turbidity Toxin Syndrome , Shijiazhuang , Hebei , China

4. Graduate School, Hebei University of Traditional Chinese Medicine , Shijiazhuang , Hebei , China

5. Department of Gastroenterology, Hebei Provincial Hospital of Chinese Medicine , 389 Zhongshan East Road, Chang’an District , Shijiazhuang , Hebei , China

Abstract

Abstract Ulcerative colitis (UC) is an inflammatory bowel disease and associated with metabolic imbalance. Luteolin (LUT) reportedly exhibits anti-inflammatory activity. However, its regulatory effects on metabolites remain indistinct. Here, the effects of LUT on immune response and oxidative stress in UC were determined. Serum metabolomics profiles of UC rats treated with LUT were obtained utilizing liquid chromatography-mass spectrometry. The results revealed that LUT treatment alleviated colon tissue injury, colon shortening, weight loss, and inflammatory response in UC rats. Additionally, the levels of superoxide dismutase and total antioxidant capacity were elevated, but malondialdehyde content was reduced in serum of UC rats, while these changes were abrogated by LUT. Metabolomics analysis unveiled that l-malic acid, creatinine, l-glutamine, and l-lactic acid levels were remarkably decreased, while dimethyl sulfone, 5-methylcytosine, cysteine-S-sulfate, and jasmonic acid levels were notably increased after LUT treatment. Furthermore, differential metabolites primarily participated in d-glutamine and d-glutamate metabolism, glutathione metabolism, and citrate cycle pathways. In summary, these results demonstrated that LUT improved immune response, alleviated oxidative stress, and altered metabolites in UC rats. This study lays the root for further exploring the mechanism of LUT in the treatment of UC.

Publisher

Walter de Gruyter GmbH

Subject

General Medicine

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