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丁酸钠通过调节CHOP减轻内质网应激,并在高脂饮食喂养的肥胖小鼠模型中增强有利的抗炎脂肪组织免疫代谢。

Sodium butyrate reduces endoplasmic reticulum stress by modulating CHOP and empowers favorable anti-inflammatory adipose tissue immune-metabolism in HFD fed mice model of obesity.

作者信息

Kushwaha Vinita, Rai Prashant, Varshney Salil, Gupta Sanchita, Khandelwal Nilesh, Kumar Durgesh, Nilkanth Gaikwad Anil

机构信息

Division of Pharmacology, CSIR-Central Drug Research Institute, Lucknow, U.P 226031, India.

Academy of Scientific and Innovative Research (AcSIR) Headquarters, CSIR-HRDG, campus Sector 19, Kamla Nehru Nagar, Ghaziabad, U.P 201002, India.

出版信息

Food Chem (Oxf). 2022 Jan 25;4:100079. doi: 10.1016/j.fochms.2022.100079. eCollection 2022 Jul 30.

Abstract

Over the past decade, the gut microbiome has been linked to several diseases including gastrointestinal diseases, cancer, immune disorder and metabolic syndrome. Shifts in the gut bacterial population affect the overall metabolic health status leading towards obesity and Type II diabetes mellitus. Secondary metabolites secreted by the gut microbiome interact with various host-sensing signalling pathways and are responsible for functional modulation of immune resident cells in metabolic tissues (Blüher, 2019). Of these, short- chain fatty acids (SCFAs) i.e., acetate, propionate and butyrate have been significantly correlated with the disposition of diabetes and metabolic disorder. The altered gut microbial population depletes the intestinal barrier causing entry of LPS into circulation and towards metabolic tissues triggering pro-inflammatory responses. As butyrate has been known to maintain intestinal integrity, we aimed to assess the apparent effect of externally given sodium butyrate [NaB] on immuno-metabolic profiling of adipose tissue, and its association with metabolic and inflammatory status of adipose tissue. To assess this, we put groups of C57BL/6 mice i.e., Control fed with a regular chow diet and another group that was fed on a high fat diet (HFD, 60%) for 8 weeks. Following this, the HFD group were further subdivided into two groups one fed with HFD and the other with HFD + NaB (5%w/w) for another 8 weeks. Body composition, weight gain, body adiposity and biochemical parameters were assessed. NaB fed group showed an improved metabolic profile compared to HFD fed group. Administration of NaB also improved glucose tolerance capacity and insulin sensitivity as determined by IPGTT and ITT profiles. Earlier reports have shown gut leakage and increased LPS in circulation is the primary cause of setting up inflammation at the tissue level. Our studies exhibited that, NaB increased the expression of tight junction proteins of intestinal linings and thereby enhanced intestinal barrier integrity. The FITC dextran permeability assay further confirmed this enhanced intestinal barrier integrity. We assessed the quantitative and relative population of different types of resident immune cells from a stromal vascular fraction of adipose tissue. Flow cytometry studies revealed significantly increased M2 (CD206+ ) macrophages and Tregs (CD25+ ) relative to the M1 macrophage population and CD4+ T cells respectively in NaB treated mice, suggesting its potential role in alleviating the inflammatory profile. In a nutshell, taken together better glucose tolerance, better gut health, reduced inflammatory adipose tissue immune cells, suggest potential beneficial role of sodium butyrate in alleviating overall inflammation and metabolic dysfunction associated with obesity.

摘要

在过去十年中,肠道微生物群已与多种疾病相关联,包括胃肠道疾病、癌症、免疫紊乱和代谢综合征。肠道细菌种群的变化会影响整体代谢健康状况,导致肥胖和II型糖尿病。肠道微生物群分泌的次级代谢产物与各种宿主传感信号通路相互作用,并负责代谢组织中免疫驻留细胞的功能调节(布卢尔,2019年)。其中,短链脂肪酸(SCFAs),即乙酸盐、丙酸盐和丁酸盐,与糖尿病和代谢紊乱的发生显著相关。肠道微生物种群的改变会破坏肠道屏障,导致脂多糖进入循环并进入代谢组织,引发促炎反应。由于已知丁酸盐可维持肠道完整性,我们旨在评估外部给予丁酸钠[NaB]对脂肪组织免疫代谢谱的明显影响,及其与脂肪组织代谢和炎症状态的关联。为了评估这一点,我们将C57BL/6小鼠分为几组,一组喂食常规饲料作为对照,另一组喂食高脂肪饮食(HFD,60%)8周。在此之后,HFD组进一步细分为两组,一组继续喂食HFD,另一组喂食HFD + NaB(5%w/w),持续8周。评估了身体成分、体重增加、身体脂肪含量和生化参数。与喂食HFD的组相比,喂食NaB的组显示出改善的代谢谱。通过IPGTT和ITT曲线测定,给予NaB还改善了葡萄糖耐量和胰岛素敏感性。早期报告表明,肠道渗漏和循环中脂多糖增加是在组织水平引发炎症的主要原因。我们的研究表明,NaB增加了肠内衬紧密连接蛋白的表达,从而增强了肠道屏障的完整性。FITC葡聚糖通透性试验进一步证实了这种增强的肠道屏障完整性。我们评估了来自脂肪组织基质血管部分的不同类型驻留免疫细胞的数量和相对比例。流式细胞术研究显示,在NaB处理的小鼠中,相对于M1巨噬细胞群体和CD4 + T细胞,M2(CD206 +)巨噬细胞和调节性T细胞(CD25 +)分别显著增加,表明其在减轻炎症方面的潜在作用。简而言之,综合更好的葡萄糖耐量、更好的肠道健康、减少炎症性脂肪组织免疫细胞来看,丁酸钠在减轻与肥胖相关的整体炎症和代谢功能障碍方面具有潜在的有益作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/de62/8991629/360f5c5f5c65/gr1.jpg

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