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Pdx1 inactivation restricted to the intestinal epithelium in mice alters duodenal gene expression in enterocytes and enteroendocrine cells

机译：Pdx1失活仅限于小鼠的肠上皮细胞改变了十二指肠基因在肠上皮细胞和肠内分泌细胞中的表达

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Null mutant mice lacking the transcription factor pancreatic and duodenal homeobox 1 (Pdx1) are apancreatic and survive only a few days after birth. The role of Pdx1 in regulating intestinal gene expression has therefore yet to be determined in viable mice with normal pancreatic development. We hypothesized that conditional inactivation of Pdx1 restricted to the intestinal epithelium would alter intestinal gene expression and cell differentiation. Pdx1flox/flox;VilCre mice with intestine-specific Pdx1 inactivation were generated by crossing a transgenic mouse strain expressing Cre recombinase, driven by a mouse villin 1 gene promoter fragment, with a mutant mouse strain homozygous for loxP site-flanked Pdx1. Pdx1 protein is undetectable in all epithelial cells in the intestinal epithelium of Pdx1flox/flox;VilCre mice. Goblet cell number and mRNA abundance for mucin 3 and mucin 13 genes in the proximal small intestine are comparable between Pdx1flox/flox;VilCre and control mice. Similarly, Paneth cell number and expression of Paneth cell-related genes Defa1, Defcr-rs1, and Mmp7 in the proximal small intestine remain statistically unchanged by Pdx1 inactivation. Although the number of enteroendocrine cells expressing chromogranin A/B, gastric inhibitory polypeptide (Gip), or somatostatin (Sst) is unaffected in the Pdx1flox/flox;VilCre mice, mRNA abundance for Gip and Sst is significantly reduced in the proximal small intestine. Conditional Pdx1 inactivation attenuates intestinal alkaline phosphatase (IAP) activity in the duodenal epithelium, consistent with an average 91% decrease in expression of the mouse enterocyte IAP gene, alkaline phosphatase 3 (a novel Pdx1 target candidate), in the proximal small intestine following Pdx1 inactivation. We conclude that Pdx1 is necessary for patterning appropriate gene expression in enterocytes and enteroendocrine cells of the proximal small intestine.

机译：缺少转录因子胰腺和十二指肠同源盒1（Pdx1）的无效突变小鼠是胰腺的，仅在出生后几天存活。因此，在具有正常胰腺发育的存活小鼠中，尚未确定Pdx1在调节肠道基因表达中的作用。我们假设Pdx1的条件失活仅限于肠上皮细胞，将改变肠基因表达和细胞分化。通过将表达Cre重组酶的转基因小鼠品系（由小鼠villin 1基因启动子片段驱动）与对loxP位点侧翼的Pdx1纯合的突变小鼠品系杂交，产生具有肠道特异性Pdx1失活的Pdx1flox / flox; VilCre小鼠。在Pdx1flox / flox; VilCre小鼠的肠上皮细胞的所有上皮细胞中均未检测到Pdx1蛋白。在近端小肠中，黏蛋白3和黏蛋白13基因的杯状细胞数量和mRNA丰度在Pdx1flox / flox; VilCre和对照小鼠之间可比。同样，近端小肠的Paneth细胞数和Paneth细胞相关基因Defa1，Defcr-rs1和Mmp7的表达在Pdx1失活下仍保持统计上的不变。尽管表达嗜铬粒蛋白A / B，胃抑制性多肽（Gip）或生长抑素（Sst）的肠内分泌细胞的数量在Pdx1flox / flox; VilCre小鼠中不受影响，但近端小肠中Gip和Sst的mRNA丰度却显着降低。有条件的Pdx1失活减弱了十二指肠上皮中的肠道碱性磷酸酶（IAP）活性，这与Pdx1之后的小肠近端小肠IAP基因碱性磷酸酶3（一种新型的Pdx1候选靶标）的表达平均降低了91％相一致。灭活。我们得出结论，Pdx1对于模式化近端小肠肠细胞和肠内分泌细胞中的适当基因表达是必需的。

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Chen, Chin; Fang, Rixun; Davis, Corrine; Maravelias, Charalambos; Sibley, Eric;
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年度 2009
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1. Use of transgenic mice to map cis-acting elements in the intestinal fatty acid binding protein gene (Fabpi) that control its cell lineage-specific and regional patterns of expression along the duodenal-colonic and crypt-villus axes of the gut epithelium. [J] . S M Cohn, T C Simon, K A Roth, Journal of cell biology . 1992,第1期

机译：利用转基因小鼠在肠道脂肪酸结合蛋白基因（Fabpi）中定位顺式作用元件，该顺式元件控制其细胞谱系特异性和区域表达模式，沿着肠上皮的十二指肠结肠和隐窝绒毛轴。
2. Oral consumption of cinnamon enhances the expression of immunity and lipid absorption genes in the small intestinal epithelium and alters the gut microbiota in normal mice [J] . Kim Jong-In, Lee Ju-Hoon, Song Youngju, Journal of Functional Foods . 2018,第期

机译：肉桂的口服消耗增强了小肠上皮中免疫和脂质吸收基因的表达，并在正常小鼠中改变了肠道微生物
3. Dietary carbohydrate source alters gene expression profile of intestinal epithelium in mice. [J] . Wang B, Bobe G, LaPres JJ, Nutrition and Cancer: An International Journal . 2009,第1期

机译：饮食中的碳水化合物来源会改变小鼠肠上皮的基因表达谱。
4. Effect of cysteamine on mucosa regeneration of intestinal trauma goats and on duodenal cell proliferation of cows in primary culture [C] . Z. Shen, J. He, L. Cao International Symposium on the Nutrition of Herbivores(ISNH-7); 20070917-22; Beijing(CN) . 2007

机译：半胱胺对原代培养的山羊肠粘膜再生和十二指肠细胞增殖的影响
5. Reprogramming of Different Cell Types into Pancreatic Beta Cells by Using Transcription Factor Genes Pdx1, Ngn3 and MafA. [D] . Akinci, Ersin. 2012

机译：通过使用转录因子基因Pdx1，Ngn3和MafA，将不同类型的细胞重编程为胰腺β细胞。
6. Pdx1 inactivation restricted to the intestinal epithelium in mice alters duodenal gene expression in enterocytes and enteroendocrine cells [O] . Chin Chen, Rixun Fang, Corrine Davis, -1

机译：Pdx1失活仅限于小鼠的肠上皮细胞改变了十二指肠基因在肠上皮细胞和肠内分泌细胞中的表达
7. Expression of SV-40 T antigen in the small intestinal epithelium of transgenic mice results in proliferative changes in the crypt and reentry of villus-associated enterocytes into the cell cycle but has no apparent effect on cellular differentiation programs and does not cause neoplastic transformation [O] . 1992

机译：SV-40 T抗原在转基因小鼠小肠上皮中的表达导致绒毛相关肠细胞的隐窝和折返增生增殖变化，但对细胞分化程序没有明显影响，也不会引起肿瘤转化

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