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首页> 外文期刊>Pfluegers Archiv: European Journal of Physiology >The effects of streptozotocin diabetes on sodium-glucose transporter (SGLT1) expression and function in rat jejunal and ileal villus-attached enterocytes.
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The effects of streptozotocin diabetes on sodium-glucose transporter (SGLT1) expression and function in rat jejunal and ileal villus-attached enterocytes.

机译:糖尿病链脲佐菌素对大鼠空肠和回肠绒毛附着肠上皮细胞钠葡萄糖转运蛋白(SGLT1)表达和功能的影响。

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Rats treated with streptozotocin for 17 days were used to determine the cellular origin of enhanced brush border glucose transport in the diabetic small intestine. In the jejunum of both normal and diabetic rats, phlorizin-sensitive (SGLT1-mediated) glucose transport was shown, by section autoradiography, to take place in upper villus enterocytes. The distribution of brush border SGLT1 transporters along villi, determined using immunogold cytochemistry, was similar to that found for glucose uptake. Longer villi, supporting a larger number of absorbing enterocytes in the diabetic jejunum, appeared to be responsible for increased glucose uptake in this condition. SGLT1 protein and SGLT1-mediated glucose transport were undetectable in normal distal ileal villi. However, following treatment with streptozotocin, both SGLT1 protein and SGLT1-mediated glucose transport were found to be present in basal ileal villus enterocytes. SGLT1 protein and SGLT1-mediated glucose transport both increased during enterocyte migration to the villus tip. Cellular induction of the SGLT1 transporter, as well as longer villi contribute to enhanced glucose transport in diabetic rat distal ileum. Close correlation between the positional expression of SGLT1 protein and absorptive function suggests that transporter density is an important determinant for up-regulation of sodium-dependent glucose transport in diabetes.
机译:用链脲佐菌素治疗17天的大鼠用于确定糖尿病小肠中刷状边界葡萄糖转运增强的细胞起源。在正常空腹和糖尿病大鼠的空肠中,通过断面放射自显影显示出对芦丁嗪敏感的(SGLT1介导的)葡萄糖转运发生在上绒毛肠上皮细胞中。使用免疫金细胞化学法测定的刷缘SGLT1转运蛋白沿绒毛的分布与发现的葡萄糖摄取相似。更长的绒毛支持糖尿病空肠中大量的吸收性肠上皮细胞,似乎是这种情况下葡萄糖摄取增加的原因。在正常的回肠远端绒毛中未检测到SGLT1蛋白和SGLT1介导的葡萄糖转运。但是,在用链脲佐菌素治疗后,发现在基础回肠绒毛肠上皮细胞中同时存在SGLT1蛋白和SGLT1介导的葡萄糖转运。 SGLT1蛋白和SGLT1介导的葡萄糖转运在肠细胞迁移到绒毛尖端期间均增加。 SGLT1转运蛋白的细胞诱导以及更长的绒毛有助于增强糖尿病大鼠回肠远端的葡萄糖转运。 SGLT1蛋白的位置表达与吸收功能之间密切相关,表明转运蛋白密度是糖尿病中钠依赖性葡萄糖转运的上调的重要决定因素。

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