下丘脑和垂体在控制大鼠胎儿胰腺对葡萄糖的反应性发育中的可能作用。

Endokrinologie Pub Date : 1982-06-01
M S Mitskevich, Sapronova AYa
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引用次数: 0

摘要

为了评估下丘脑和垂体在胰腺功能活动发展中的作用,我们研究了脑切除和胎儿斩首后胰腺b细胞对葡萄糖反应性的变化。通过在培养液中加入葡萄糖诱导胰岛素分泌的变化来测定胰腺的反应性。研究发现,在发育第17.5-18.5天,对正常或糖尿病妊娠大鼠的胎儿进行斩首,切除垂体和下丘脑后,其胰腺在第21.5天仍对葡萄糖不敏感。仅在胎儿发育第17.5天切除胎儿脑时切除下丘脑也会导致胎儿胰腺对葡萄糖的敏感性丧失。下丘脑匀浆注入去脑胎儿恢复葡萄糖对b细胞的刺激作用。将断头胎儿的胰腺碎片与成年大鼠的腺垂体一起预孵育,断头效应被消除,培养基中葡萄糖浓度的增加引起胰岛素的密集释放。在体内和体外实验中,生长激素(GH)和促肾上腺皮质激素(ACTH)均具有类似的恢复作用。所获得的数据表明,下丘脑和垂体可能对大鼠产前个体发育过程中胰腺功能活动的发育起控制作用。然而,这一监管机制尚不清楚。
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Possible role of hypothalamus and hypophysis in the control of development of pancreas reactivity to the effect of glucose in rat fetuses.

To estimate the role of hypothalamus and hypophysis in the development of functional activity of pancreas, the changes of reactivity of pancreatic B-cells to glucose resulting from encephalectomy and decapitation of fetuses were investigated. Reactivity of pancreas was determined by the changes of insulin secretion induced by the addition of glucose into incubation medium. It was found that, when hypophysis and hypothalamus were removed as a result of decapitation of fetuses from normal or from diabetic pregnant rats on days 17.5-18.5 of development, their pancreas remained insensitive to glucose on 21.5 day. Removal of hypothalamus only when fetuses were encephalectomized on day 17.5 of development also resulted in the loss of sensitivity of fetal pancreas to glucose. Injection of hypothalamus homogenate to encephalectomized fetuses restored the stimulating effect of glucose on B-cells. When pancreas fragments of decapitated fetuses were preincubated together with adenohypophyses of adult rats, the decapitation effect was eliminated, and an increase of glucose concentration in the medium caused an intensive release of insulin. Similar restoring effect was induced by growth hormone (GH) and adrenocorticotrophin (ACTH) when used in in vivo and in vitro experiments. The data obtained give evidence of a possible contribution of hypothalamus and hypophysis to the control of the development of functional activity of pancreas in rat prenatal ontogenesis. However, the mechanism of this regulation remains unclear yet.

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