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小鼠肠道正常及可的松诱导成熟过程中α-2,6-唾液酸转移酶的区域特异性个体发生

Region-specific ontogeny of alpha-2,6-sialyltransferase during normal and cortisone-induced maturation in mouse intestine.

作者信息

Dai Dingwei, Nanthakumar N Nanda, Savidge Tor C, Newburg David S, Walker W Allan

机构信息

Shanghai Institute for Pediatric Research, Xinhua Hospital and Shanghai Second Medical University, Shanghai, People's Republic of China 200092.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2002 Mar;282(3):G480-90. doi: 10.1152/ajpgi.00531.2000.

Abstract

Regional differences in the ontogeny of mouse intestinal alpha-2,6-sialyltransferase activities (alpha-2,6-ST) and the influence of cortisone acetate (CA) on this expression were determined. High ST activity and alpha-2,6-ST mRNA levels were detected in immature small and large intestine, with activity increasing distally from the duodenum. As the mice matured, ST activity (predominantly alpha-2,6-ST) in the small intestine decreased rapidly to adult levels by the fourth postnatal week. CA precociously accelerated this region-specific ontogenic decline. A similar decline of ST mRNA levels reflected ST activity in the small, but not the large, intestine. Small intestinal sialyl alpha-2,6-linked glycoconjugates displayed similar developmental and CA induced-precocious declines when probed using Sambucus nigra agglutinin (SNA) lectin. SNA labeling demonstrated age-dependent diminished sialyl alpha2,6 glycoconjugate expression in goblet cells in the small (but not large) intestine, but no such regional specificity was apparent in microvillus membrane. This suggests differential regulation of sialyl alpha-2,6 glycoconjugates in absorptive vs. globlet cells. These age-dependent and region-specific differences in sialyl alpha-2,6 glycoconjugates may be mediated in part by altered alpha-2,6-ST gene expression regulated by trophic factors such as glucocorticoids.

摘要

确定了小鼠肠道α-2,6-唾液酸转移酶活性(α-2,6-ST)个体发育的区域差异以及醋酸可的松(CA)对该表达的影响。在未成熟的小肠和大肠中检测到高ST活性和α-2,6-ST mRNA水平,活性从十二指肠向远端增加。随着小鼠成熟,小肠中的ST活性(主要是α-2,6-ST)在出生后第四周迅速下降至成年水平。CA过早地加速了这种区域特异性的个体发育下降。ST mRNA水平的类似下降反映了小肠而非大肠中的ST活性。当使用黑接骨木凝集素(SNA)凝集素进行检测时,小肠唾液酸化α-2,6-连接的糖缀合物显示出类似的发育和CA诱导的过早下降。SNA标记显示,年龄依赖性地减少了小肠(而非大肠)杯状细胞中唾液酸化α2,6糖缀合物的表达,但在微绒毛膜中没有明显的区域特异性。这表明在吸收性细胞与杯状细胞中唾液酸化α-2,6糖缀合物的调节存在差异。唾液酸化α-2,6糖缀合物中这些年龄依赖性和区域特异性差异可能部分由营养因子如糖皮质激素调节的α-2,6-ST基因表达改变介导。

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