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首页> 外文期刊>American Journal of Physiology >Altered transit and bacterial overgrowth in the cystic fibrosis mouse small intestine.
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Altered transit and bacterial overgrowth in the cystic fibrosis mouse small intestine.

机译:小鼠小肠囊性纤维化的运输和细菌过度生长改变。

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摘要

Small intestinal bacterial overgrowth (SIBO) may play an important role in the gastrointestinal complications of cystic fibrosis (CF). This work explored two potential factors in development of SIBO in the CF (cftr(tm1UNC)) mouse: impaired Paneth cell innate defenses and altered gastrointestinal motility. Postnatal differentiation of Paneth cells was followed by Defcr, Lyzs, and Ang4 gene expression, and SIBO was measured by quantitative PCR of the bacterial 16S rRNA gene. Paneth cell gene expression was low in 4-day-old CF and wild-type (WT) mice and increased similarly in both groups of mice between 12 and 16 days. Peak Paneth cell gene expression was reached by 40 days of age and was less for Defcr and Lyzs in CF mice compared with WT, whereas Ang4 levels were greater in CF mice. SIBO occurred by postnatal day 8 in CF mice, which is before Paneth cell development. With the use of gavaged rhodamine-dextran to follow motility, gastric emptying in CF mice was slightly decreased compared with WT, and small intestinal transit was dramatically less. Since antibiotics improve weight gain in CF mice, their effects on gastric emptying and small intestinal transit were determined. Antibiotics did not affect gastric emptying or transit in CF mice but did significantly slow intestinal transit in WT mice, suggesting a potential role of normal microflora in regulating transit. In conclusion, small intestinal transit was significantly slower in CF mice, and this is likely a major factor in SIBO in CF.
机译:小肠细菌过度生长(SIBO)可能在囊性纤维化(CF)的胃肠道并发症中起重要作用。这项工作探讨了CF(cftr(tm1UNC))小鼠中SIBO发育的两个潜在因素:Paneth细胞先天防御能力受损和胃肠蠕动改变。 Paneth细胞的产后分化后是Defcr,Lyzs和Ang4基因表达,SIBO是通过细菌16S rRNA基因的定量PCR测定的。 Paneth细胞基因表达在4天大的CF和野生型(WT)小鼠中较低,并且在两组小鼠中在12至16天之间相似地增加。与WT相比,CF小鼠的Pancr细胞基因峰值表达达到了40天,而Defcr和Lyzs的峰值Paneth细胞基因表达则比WT小,而CF4小鼠的Ang4水平更高。 SIBO发生在CF小鼠的出生后第8天,也就是Paneth细胞发育之前。通过使用管饲的若丹明-右旋糖酐追踪运动性,与野生型相比,CF小鼠的胃排空略有减少,小肠运输明显减少。由于抗生素可改善CF小鼠的体重增加,因此确定了它们对胃排空和小肠运输的影响。抗生素不会影响CF小鼠的胃排空或转运,但会显着减慢WT小鼠的肠道转运,提示正常菌群在调节转运中具有潜在作用。总之,CF小鼠的小肠运输明显减慢,这可能是CF中SIBO的主要因素。

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