糖尿病兔周围神经中钠依赖性氨基酸摄取的缺陷。醛糖还原酶抑制剂或肌醇给药的纠正作用。

A defect in sodium-dependent amino acid uptake in diabetic rabbit peripheral nerve. Correction by an aldose reductase inhibitor or myo-inositol administration.

作者信息

Greene D A, Lattimer S A, Carroll P B, Fernstrom J D, Finegold D N

机构信息

Department of Medicine, School of Medicine, University of Pittsburgh, Pennsylvania 15261.

出版信息

J Clin Invest. 1990 May;85(5):1657-65. doi: 10.1172/JCI114617.

DOI:10.1172/JCI114617

PMID:2185278

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC296618/

Abstract

A myo-inositol-related defect in nerve sodium-potassium ATPase activity in experimental diabetes has been suggested as a possible pathogenetic factor in diabetic neuropathy. Because the sodium-potassium ATPase is essential for other sodium-cotransport systems, and because myo-inositol-derived phosphoinositide metabolites regulate multiple membrane transport processes, sodium gradient-dependent amino acid uptake was examined in vitro in endoneurial preparations derived from nondiabetic and 14-d alloxan diabetic rabbits. Untreated alloxan diabetes reduced endoneurial sodium-gradient dependent uptake of the nonmetabolized amino acid 2-aminoisobutyric acid by greater than 50%. Administration of an aldose reductase inhibitor prevented reductions in both nerve myo-inositol content and endoneurial sodium-dependent 2-aminoisobutyric acid uptake. Myo-inositol supplementation that produced a transient pharmacological elevation in plasma myo-inositol concentration, but did not raise nerve myo-inositol content, reproduced the effect of the aldose reductase inhibitor on endoneurial sodium-dependent 2-aminoisobutyric acid uptake. Phorbol myristate acetate, which acutely normalizes sodium-potassium ATPase activity in diabetic nerve, did not acutely correct 2-aminoisobutyric uptake when added in vitro. These data suggest that depletion of a small myo-inositol pool may be implicated in the pathogenesis of defects in amino acid uptake in diabetic nerve and that rapid correction of sodium-potassium ATPase activity with protein kinase C agonists in vitro does not acutely normalize sodium-dependent 2-aminoisobutyric acid uptake.

摘要

实验性糖尿病中神经钠钾ATP酶活性与肌醇相关的缺陷被认为可能是糖尿病神经病变的发病因素。由于钠钾ATP酶对其他钠共转运系统至关重要，且肌醇衍生的磷酸肌醇代谢产物调节多种膜转运过程，因此在体外研究了源自非糖尿病和14天四氧嘧啶糖尿病兔的神经内膜制剂中钠梯度依赖性氨基酸摄取。未经治疗的四氧嘧啶糖尿病使神经内膜对非代谢氨基酸2-氨基异丁酸的钠梯度依赖性摄取降低了50%以上。给予醛糖还原酶抑制剂可防止神经肌醇含量和神经内膜钠依赖性2-氨基异丁酸摄取的降低。补充肌醇可使血浆肌醇浓度短暂升高，但不会提高神经肌醇含量，其对神经内膜钠依赖性2-氨基异丁酸摄取的影响与醛糖还原酶抑制剂相同。佛波醇肉豆蔻酸酯可使糖尿病神经中的钠钾ATP酶活性迅速恢复正常，但在体外添加时并不能迅速纠正2-氨基异丁酸的摄取。这些数据表明，少量肌醇池的耗竭可能与糖尿病神经中氨基酸摄取缺陷的发病机制有关，且在体外使用蛋白激酶C激动剂快速纠正钠钾ATP酶活性并不能使钠依赖性2-氨基异丁酸摄取迅速恢复正常。