首页> 外文期刊>International Journal of Obesity >Commensal Hafnia alvei strain reduces food intake and fat mass in obese mice-a new potential probiotic for appetite and body weight management
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Commensal Hafnia alvei strain reduces food intake and fat mass in obese mice-a new potential probiotic for appetite and body weight management

机译:非团结的Hafnia Alvei菌株降低了肥胖小鼠的食物摄入和脂肪肿块 - 一种新的潜在益生菌,可用于食欲和体重管理

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Based on the recent identification of E.coli heat shock protein ClpB as a mimetic of the anorexigenic -melanocyte stimulating hormone (-MSH), the objective of this study was to preclinically validate Hafnia alvei, a ClpB-producing commensal bacterium as a potential probiotic for appetite and body weight management in overweight and obesity. The involvement of enterobacterial ClpB in the putative anti-obesity effects was studied using ClpB-deficient E.coli. A food-grade H. alvei HA4597 strain synthetizing the ClpB protein with an -MSH-like motif was selected as a candidate probiotic to be tested in ob/ob and high-fat diet (HFD)-fed obese and overweight mice. The relevance of the enterobacterial ClpB gene to human obesity was studied by in silico analysis of fecal metagenomes of 569 healthy individuals from the "MetaHIT" database. Chronic per os administration of native but not ClpB-deficient E.coli strain reduced body weight gain (p < 0.05) and daily meal frequency (p < 0.001) in ob/ob mice. Oral gavage of H.alvei for 18 and 46 days in ob/ob and HFD-fed obese mice, respectively, was well tolerated, reduced body weight gain and fat mass in both obesity models (p < 0.05) and decreased food intake in hyperphagic ob/ob mice (p < 0.001). Elevated fat tissue levels of phosphorylated hormone-sensitive lipase were detected in H.alvei -treated ob/ob mice (p < 0.01). Enterobacterial ClpB gene richness was lower in obese vs. non-obese humans (p < 0.0001) and correlated negatively with BMI in genera of Enterobacter, Klebsiella and Hafnia. H.alvei HA4597 strain reduces food intake, body weight and fat mass gain in hyperphagic and obese mice. These data combined with low enterobacterial ClpB gene abundance in the microbiota of obese humans provide the rationale for using H.alvei as a probiotic for appetite and body weight management in overweight and obesity.
机译:基于E.COLI热休克蛋白CLPB的最近鉴定为厌氧 - Melanocyte刺激激素(-MSH)的模拟物,本研究的目的是呈呈呈呈呈尿乳头氏症的目的,将产生的共生细菌为潜在的益生菌对于超重和肥胖的食欲和体重管理。使用CLPB缺陷的大肠杆菌研究了肠杆菌CLPB在推定的抗肥胖效应中的参与。选择具有-MSH样上的CLPB蛋白的食品级H.Alvei Ha4597菌株作为候选益生菌,以在OB / OB和高脂饮食(HFD)的肥胖和超重小鼠中进行测试。通过从“Metahit”数据库的569个健康个体的粪便分析中,研究了肠杆菌CLPB基因对人肥胖的相关性。慢性每对OS本地但不是CLPB缺陷的大肠杆菌菌株减少体重增加(P <0.05)和OB / OB小鼠的每日膳食频率(P <0.001)。在OB / OB和HFD喂养的肥胖小鼠中,H.alvei的口服饲养18和46天,肥胖模型(P <0.05)中的体重增加和脂肪块减少,减少了倍频OB / OB小鼠(P <0.001)。在H.Alvei -Treated OB / OB小鼠中检测到磷酸化激素敏感脂肪酶的升高组织水平(P <0.01)。肥胖的CLPB基因富含肥胖与非肥胖人类(P <0.0001)较低,并与肠道杆菌,Klebsiella和Hafnia的BMI负相关。 H.Alvei Ha4597菌株可降低食物摄入量,体重和肥胖小鼠的脂肪群。这些数据与肥胖人类微生物群中的低肠杆菌CLPB基因丰富提供了使用H.Alvei作为益生菌的基本原理,用于超重和肥胖的食欲和体重管理。
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