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首页> 外文期刊>Molecular BioSystems >Fecal metabonomic study of a polysaccharide, MDG-1 from Ophiopogon japonicus on diabetic mice based on gas chromatography/time-of-flight mass spectrometry (GC TOF/MS)
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Fecal metabonomic study of a polysaccharide, MDG-1 from Ophiopogon japonicus on diabetic mice based on gas chromatography/time-of-flight mass spectrometry (GC TOF/MS)

机译:基于气相色谱/飞行时间质谱(GC TOF / MS)的麦冬多糖MDG-1对糖尿病小鼠的粪便代谢组学研究

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摘要

Type 2 Diabetes Metlitus (T2DM) is a chronic metabolic disorder with systemic complications and has been a worldwide epidemic. Ophiopogon japonicus is a traditional Chinese medicine used to treat diabetes for thousands of years. From our previous work, we know that MDG-1, a water-soluble p-D-fructan polysaccharide from O. japonicas could treat T2DM experimentally. However, MDG-1 is poorly absorbed and its mechanism of action is still unknown. Therefore, a GC TOF/MS-based metabonomic approach in combination with multivariate statistical analysis was performed to investigate the mechanism of MDG-1 in a spontaneous diabetic model. Female diabetic KKay mice (21 weeks old) were randomly divided into a diabetic group (n = 6, gavaged with distilled water) and a MDG-1-Diabetic group (n = 7, gavaged with MDG-1, 300 mg kg~(-1)) and female C57BL/6 mice (21 weeks old) were set as controls (n = 6, gavaged with distilled water). After 8-weeks of treatment feces samples were collected for GC-TOF/MS analysis. Consequently, 12 potential biomarkers were identified, including monosugars (D-tagatose, D-lyxose, D-erythrose, xylo-hexos-5-ulose, 2-deoxy-galactose), butanedioic acid, amino acids (phenylalanine, L-lysine, L-methionine, L-aspartic acid) and purine derivatives (7H-purine, 2'-deoxyinosine). We assume the monosugars and butanedioic acid were the fermentation products of MDG-1 by intestinal microbes and MDG-1 actions against diabetes might be accomplished through the absorbable monosugars and butanedioic acid via suppressing intestinal glucose absorption, enhancing liver glycogenesis, inhibiting glycogenolysis and promoting GLP-1 secretion. Besides, MDG-1 might alleviate diabetes and diabetic nephropathy by reducing 7H-purine and 2'-deoxyinosine. Further omics-driven studies including genomics, proteomics and metabonomics were considered to be carried out to provide direct evidence of gut microbiome contribution to MDG-1 actions.
机译:Metlitus 2型糖尿病(T2DM)是一种具有系统性并发症的慢性代谢性疾病,已经成为一种全球流行病。麦冬是一种治疗糖尿病已有数千年的传统中药。从我们以前的工作中,我们知道MDG-1是一种来自O.japonicas的水溶性p-D-果聚糖多糖,可以通过实验治疗T2DM。但是,MDG-1吸收不良,其作用机理仍然未知。因此,基于GC TOF / MS的代谢组学方法与多变量统计分析相结合,以研究自发性糖尿病模型中MDG-1的机制。将雌性糖尿病KKay小鼠(21周龄)随机分为糖尿病组(n = 6,用蒸馏水灌胃)和MDG-1糖尿病组(n = 7,用MDG-1,灌胃300 mg / kg)。 -1))和雌性C57BL / 6小鼠(21周大)设为对照组(n = 6,用蒸馏水灌胃)。处理8周后,收集粪便样品用于GC-TOF / MS分析。因此,鉴定出了12种潜在的生物标记,包括单糖(D-塔格糖,D-lyxose,D-erythrose,xylo-hexos-5-ulose,2-deoxy-半乳糖),丁二酸,氨基酸(苯丙氨酸,L-赖氨酸, L-蛋氨酸,L-天冬氨酸)和嘌呤衍生物(7H-嘌呤,2'-脱氧肌苷)。我们假设单糖和丁二酸是肠道微生物对MDG-1的发酵产物,而MDG-1对糖尿病的作用可能是通过可吸收的单糖和丁二酸通过抑制肠道葡萄糖吸收,增强肝脏糖原生成,抑制糖原分解和促进GLP来实现的。 -1分泌。此外,MDG-1可能通过减少7H-嘌呤和2'-脱氧肌苷减轻糖尿病和糖尿病肾病。包括基因组学,蛋白质组学和代谢组学在内的更多由组学驱动的研究被认为可以提供肠道微生物组对MDG-1作用的直接证据。

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  • 来源
    《Molecular BioSystems》 |2014年第2期|304-312|共9页
  • 作者单位

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China;

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China;

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China,College of Chinese Material Medico, Shanghai University of Traditional Chinese Medicine, Shanghai, 201203, PR China;

    Center for Chinese Medical Therapy and Systems Biology, E-Institute, Shanghai University of Traditional Chinese Medicine, Shanghai, 201203, PR China;

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China;

    College of Chinese Material Medico, Shanghai University of Traditional Chinese Medicine, Shanghai, 201203, PR China;

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China;

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China;

    Engineering Research Center of Modern Preparation Technology of TCM, Ministry of Education, Shanghai University of Traditional Chinese Medicine, 1200 Cailun Road, Shanghai, 201203, PR China;

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