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消瘦和非消瘦型糖尿病大鼠的快速顺行轴突运输;醛糖还原酶抑制的作用

Fast anterograde axonal transport in wasted and non-wasted diabetic rats; effects of aldose reductase inhibition.

作者信息

Whiteley S J, Townsend J, Tomlinson D R, Willars G B

出版信息

Diabetes Res. 1986 Nov;3(9):447-52.

PMID:2435444
Abstract

This study measured the velocity of the fast anterograde axonal transport of [3H]-proline-labelled proteins in sciatic motoneurones of rats with streptozotocin diabetes of 12 weeks duration and in age matched controls. Four groups of diabetic animals were studied. One of these groups remained untreated whilst 2 diabetic groups received a long-acting insulin twice weekly to limit body wasting, but to permit regular hyperglycaemia. One insulin-treated group and one other diabetic group received an aldose reductase inhibitor, "Statil" (ICI 128436) by dietary admixture. Neither diabetes alone nor any of the treatment regimes produced any significant alteration of axonal transport velocity. Sciatic nerve temperature was measured concomitantly. A slight nerve hypothermia was seen in the untreated diabetic rats, but not in either insulin-treated group. It is concluded that 2 aspects of diabetes mellitus, namely persistent hyperglycaemia and polyol pathway activity in nervous tissue are without effect on the velocity of fast orthograde axonal transport of proteins.

摘要

本研究测量了病程为12周的链脲佐菌素诱导糖尿病大鼠坐骨运动神经元中[3H] - 脯氨酸标记蛋白的快速顺向轴突运输速度,并与年龄匹配的对照组进行比较。研究了四组糖尿病动物。其中一组未接受治疗,而另外两组糖尿病动物每周两次接受长效胰岛素治疗,以限制体重减轻,但允许血糖持续升高。一组胰岛素治疗组和另一组糖尿病组通过饮食添加接受醛糖还原酶抑制剂“Statil”(ICI 128436)。单独的糖尿病以及任何治疗方案均未对轴突运输速度产生任何显著改变。同时测量了坐骨神经温度。未治疗的糖尿病大鼠出现轻微的神经低温,但胰岛素治疗组均未出现。结论是,糖尿病的两个方面,即持续性高血糖和神经组织中的多元醇途径活性,对蛋白质快速顺向轴突运输速度没有影响。

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