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首页> 外文期刊>The Journal of Nutrition: Official Organ of the American Institute of Nutrition >Dietary Protein Excess during Neonatal Life Alters Colonic Microbiota and Mucosal Response to Inflammatory Mediators Later in Life in Female Pigs
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Dietary Protein Excess during Neonatal Life Alters Colonic Microbiota and Mucosal Response to Inflammatory Mediators Later in Life in Female Pigs

机译:新生儿寿命期间的膳食蛋白质过量改变了大肠癌微生物群和炎症介质的粘膜反应,后来在女性猪中的生活中的生活中

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The interplay between the colonic microbiota and gut epithelial and immune cells during the neonatal period, which establishes the structure of the microbiota and programs mucosal immunity, is affected by the diet. We hypothesized that protein-enriched milk formula would disturb this interplay through greater flux of protein entering the colon, with consequences later in life. Piglets were fed from postnatal day (PND) 2 to 28 either a normal-protein formula (NP; 51 g protein/L) or high-protein formula (HP; 77 g protein/L) and weaned at PND28, when they received standard diets until PND160. HP feeding transiently increased the quantity of protein entering the colon (PND7) but did not change the microbiota composition at PND28, except for a higher production of branched-chain fatty acids (BCFAs) in an in vitro fermentation test (P 0.05). HP piglets had greater colonic mucosa densities of cluster of differentiation (CD) 3+ and CD172+ cells and lower Il-1β and Tnfα mRNA levels at PND28 (P 0.05). Later in life (PND160), HP females, but not males, had a higher increase in colonic permeability after ex vivo oxidative stress and higher cytokine secretion in response to lipopolysaccharide in colonic explant cultures than NP females (P 0.05). HP females also had lower colonic amounts of F. prausnitzii and BCFAs (P 0.05). BCFAs displayed a dose-dependent protection against inflammation-induced alteration of barrier function in Caco-2 cells (P 0.05). In conclusion, protein-enriched formula had little impact on colonic microbiota, but it modified colonic immune cell development and had a long-term effect on adult colonic mucosa sensitivity to inflammatory insults, probably through microbiotal and hormonal factors.
机译:在新生儿期间结肠微生物群和肠道上皮细胞和免疫细胞之间的相互作用,其建立了微生物群的结构和粘膜免疫力,受到饮食的影响。我们假设富含蛋白质的牛奶配方将通过进入结肠的更大蛋白质的蛋白质扰乱这种相互作用,并且在生命后后果。仔猪从后期(PND)2至28中喂养正常蛋白质(NP; 51g蛋白/ L)或高蛋白质式(HP; 77g蛋白/ L)并在PND28中断奶,当时他们收到标准饮食直到pnd160。 HP喂养瞬时增加进入结肠的蛋白质的量(PND7),但除了在体外发酵试验中较高生产支链脂肪酸(BCFA)之外的PND28的Microbiota组合物(P <0.05)。 HP仔猪在PND28下具有更大的分化(CD)3+和CD172 +细胞和降低IL-1β和TNFαmRNA水平的含量较大的分化粘膜密度(P <0.05)。在生活中的后期(PND160),HP雌性但不是男性,在离子氧化胁迫后的结肠渗透性和较高的细胞因子分泌后,响应于脂多糖在结肠癌培养物中的脂多糖而不是NP女性(P <0.05)。惠普女性还具有较低的F.Prausnitzii和BCFA的结肠量(P <0.05)。 BCFA展示了对Caco-2细胞中的炎症诱导的抗扰动功能的改变的剂量依赖性保护(P <0.05)。总之,富含蛋白质的公式对结肠微生物产生影响,但它改性结肠免疫细胞发育,并且对成年结肠粘膜敏感性对炎症性损伤的敏感性有长期影响,可能是通过微生物和激素因素。

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