首页> 外文期刊>American Journal of Physiology >Enteral but not parenteral antibiotics enhance gut function and prevent necrotizing enterocolitis in formula-fed newborn preterm pigs
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Enteral but not parenteral antibiotics enhance gut function and prevent necrotizing enterocolitis in formula-fed newborn preterm pigs

机译:肠内但不是肠外抗生素增强肠功能,并防止公式喂养的新生早产猪中坏死性肠结肠炎

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Preterm infants are susceptible to infection and necrotizing enterocolitis (NEC) and are often treated with antibiotics. Simultaneous administration of enteral and parenteral antibiotics during the first days after preterm birth prevents formula-induced NEC lesions in pigs, but it is unknown which administration route is most effective. We hypothesized that only enteral antibiotics suppress gut bacterial colonization and NEC progression in formula-fed preterm pigs. Caesarean-deliv-ered preterm pigs (90-92% of gestation) were fed increasing amounts of infant formula from birth to day 5 and given saline (CON) or antibiotics (ampicillin, gentamicin, and metronidazole) via the enteral (ENT) or parenteral (PAR) route (n = 16-17). NEC lesions, intestinal morphology, function, microbiology, and inflammatory mediators were evaluated. NEC lesions were completely prevented in ENT pigs, whereas there were high incidences of mild NEC lesions (59-63%) in CON and PAR pigs (P < 0.001). ENT pigs had elevated intestinal weight, villus height/crypt depth ratio, and goblet cell density and reduced gut permeability, mucosal adherence of bacteria, IL-8 levels, colonic lactic acid levels, and density of Gram-positive bacteria, relative to CON pigs (P < 0.05). Values in PAR pigs were intermediate with few affected parameters (reduced lactic acid levels and density and adherence of Gram-positive bacteria, relative to CON pigs, P < 0.05). There was no evidence of increased antimicrobial resistance following the treatments. We conclude that enteral, but not parenteral, administration of antibiotics reduces gut bacterial colonization, inflammation, and NEC lesions in newborn, formula-fed preterm pigs. Delayed colonization may support intestinal structure, function, and immunity in the immediate postnatal period of formula-fed preterm neonates.
机译:早产儿易感染和坏死性小肠结肠炎(NEC),通常用抗生素治疗。在早产后的第一天同时施用肠内和肠胃外抗生素可防止猪中的公式诱导的NEC病变,但是该施用途径最有效。我们假设只有肠内抗生素抑制肠道细菌殖民和NEC进展只有配方喂养的早产猪。凯撒 - 达肽的早产猪(90-92%的妊娠)通过肠内(耳鼻喉)或给予盐水(CON)或抗生素(氨苄青霉素,庆大霉素和甲硝唑给予盐水(CON)或抗生素(氨苄青霉素)或肠胃外(PAR)途径(n = 16-17)。评估了NEC病变,肠形态,功能,微生物和炎症介质。 NEC病变被完全防止在ENT猪中,而CON和PAR猪中有温和的NEC病变(59-63%)的高发酵(P <0.001)。 ENT猪的肠体重升高,绒毛高度/隐窝深度比和脚耳细胞密度降低,细菌的渗透率降低,粘膜粘附性,IL-8水平,结肠乳酸水平和革兰氏阳性细菌的密度(P <0.05)。 PAR猪中的值是中间体,具有很少的影响参数(降低乳酸水平和密度和革兰氏阳性细菌的粘附,相对于孔猪,P <0.05)。治疗后没有抗微生物抗性增加的证据。我们得出结论,肠内,但不是肠胃外,抗生素施用降低了新生儿配方喂养早产猪的肠道细菌定植,炎症和NEC病变。延迟定植可以支持式喂养的早产新生儿的直接后期后期肠道结构,功能和免疫。

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