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植入后早期正常和实验性糖尿病大鼠胚胎及内脏卵黄囊中GLUT-1蛋白的细胞组织定位与调控

Cellular-tissue localization and regulation of the GLUT-1 protein in both the embryo and the visceral yolk sac from normal and experimental diabetic rats during the early postimplantation period.

作者信息

Trocino R A, Akazawa S, Takino H, Takao Y, Matsumoto K, Maeda Y, Okuno S, Nagataki S

机构信息

First Department of Internal Medicine, Nagasaki University School of Medicine, Japan.

出版信息

Endocrinology. 1994 Feb;134(2):869-78. doi: 10.1210/endo.134.2.8299581.

Abstract

We investigated the tissue-specific developmental expression and localization of GLUT-1 protein in the rat embryo and visceral yolk sac (VYS) during the organogenic periods of normal rats. The expression of GLUT-1 protein was then compared to that of experimental diabetic rats to test whether the diabetic state would affect the regulation of the glucose transporter during the early postimplantation periods (9.5-14.5 days), as we have previously demonstrated that GLUT-1 protein in embryo and VYS was down-regulated in culture with hyperglycemic medium. In the embryo, GLUT-1 protein was highly expressed during the early stages of organogenesis (between 9.5-12.5 days) and declined thereafter, whereas in the VYS, its strong expression was observed at the later stages (from 12.5-14.5 days). Immunohistochemical localization of the GLUT-1 protein in the embryo during the main periods of neurulation (9.5-11.5 days) showed that GLUT-1 immunoreactivity was principally observed in the neuroepithelial cells of the neural tube and also noted in the primitive heart, primitive gut, otic, and optic vesicles. At 12.5 days, GLUT-1 protein started to be expressed in the microvessels at the cranial portions of the neural tube, although its expression in the neuroepithelial cells still remained at the caudal (tail) portions of the neural tube. In the later stages (13.5-14.5 days) after completion of neural tube formation, GLUT-1 protein immunoreactivity substantially decreased in the neuroepithelial cells and was found mainly in the microvessels of the brain vesicles and spinal cord, whereas it continued to be expressed in the heart and eyes. In the VYS, its immunoreactivity was noticeably confined to the endodermal layer, which started as a simple layer and developed wave-like folds in the later stages. The levels of GLUT-1 protein in embryo and VYS from diabetic rats, determined by Western blot analysis, were not down-regulated compared to those in control rats at the different gestational days. Likewise, comparison of GLUT-1 protein immunoreactivity of various tissues in embryo and VYS, focusing on the neural tube, also revealed no significant differences between the two groups. We demonstrated that GLUT-1 protein is abundantly expressed in embryonic tissues and VYS during the early periods of organogenesis. The lack of down-regulation and the continuous abundant expression of the GLUT-1 protein despite the diabetic state in embryo and VYS during the early postimplantation periods may increase delivery of glucose from the VYS into various differentiating embryonic cells, leading to diabetes-induced congenital malformations.

摘要

我们研究了正常大鼠器官形成期大鼠胚胎和内脏卵黄囊(VYS)中GLUT-1蛋白的组织特异性发育表达及定位。然后将GLUT-1蛋白的表达与实验性糖尿病大鼠的表达进行比较,以测试糖尿病状态是否会在植入后早期(9.5 - 14.5天)影响葡萄糖转运蛋白的调节,因为我们之前已经证明,在高血糖培养基中培养时,胚胎和VYS中的GLUT-1蛋白会下调。在胚胎中,GLUT-1蛋白在器官形成早期(9.5 - 12.5天之间)高度表达,此后下降,而在VYS中,其强表达在后期(12.5 - 14.5天)观察到。在神经胚形成的主要时期(9.5 - 11.5天)胚胎中GLUT-1蛋白的免疫组织化学定位显示,GLUT-1免疫反应主要在神经管的神经上皮细胞中观察到,也在原始心脏、原始肠道、耳泡和视泡中发现。在12.5天时,GLUT-1蛋白开始在神经管头部的微血管中表达,尽管其在神经上皮细胞中的表达仍保留在神经管的尾部。在神经管形成完成后的后期(13.5 - 14.5天),GLUT-1蛋白免疫反应在神经上皮细胞中大幅下降,主要在脑泡和脊髓的微血管中发现,而它在心脏和眼睛中继续表达。在VYS中,其免疫反应明显局限于内胚层,内胚层开始是单层,在后期形成波浪状褶皱。通过蛋白质印迹分析确定,糖尿病大鼠胚胎和VYS中GLUT-1蛋白的水平与不同妊娠天数的对照大鼠相比没有下调。同样,聚焦于神经管,比较胚胎和VYS中各种组织的GLUT-1蛋白免疫反应性,两组之间也没有显著差异。我们证明,GLUT-1蛋白在器官形成早期在胚胎组织和VYS中大量表达。在植入后早期,尽管胚胎和VYS处于糖尿病状态,但GLUT-1蛋白缺乏下调且持续大量表达,这可能会增加葡萄糖从VYS向各种分化胚胎细胞的输送,导致糖尿病诱导的先天性畸形。

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