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N-酰基乙醇胺磷脂在缺血大鼠脑中的年龄依赖性积累。一项(31)P核磁共振和酶活性研究。

Age dependent accumulation of N-acyl-ethanolamine phospholipids in ischemic rat brain. A (31)P NMR and enzyme activity study.

作者信息

Moesgaard B, Petersen G, Jaroszewski J W, Hansen H S

机构信息

Department of Pharmacology, The Royal Danish School of Pharmacy, DK-2100 Copenhagen, Denmark.

出版信息

J Lipid Res. 2000 Jun;41(6):985-90.

Abstract

N-acyl-ethanolamine phospholipids (NAPE) can be formed as a stress response during neuronal injury, and they are precursors for N-acyl-ethanolamines (NAE), some of which are endocannabinoids. The levels of NAPE accumulated during post-decapitative ischemia (6 h at 37 degrees C) were studied in rat brains of various age (1, 6, 12, 19, 30, and approximately 70 days) by the use of (31)P NMR spectroscopy of lipid extracts. This ability to accumulate NAPE was compared with the activity of N-acyltransferase and of NAPE-hydrolyzing phospholipase D (NAPE-PLD) in brain microsomes. These two enzymes are involved in the formation and degradation of NAPE, respectively. The results showed that 1) the ability to accumulate NAPE during post-decapitative ischemia is especially high in the youngest rats and is markedly reduced in older brains [in 1-day-old rat brains NAPE accumulated to 1.5% of total phospholipids, while in 30-day-old rat brains NAPE accumulation could not be detected (detection limit 0.09%)] and 2) this age pattern of accumulation can be explained by a combination of the decreased activity of N-acyltransferase and the increased activity of NAPE-PLD during development. These results point out that it would be advantageous to investigate a potential cytoprotective role of NAPE in the brains of very young rats.

摘要

N-酰基乙醇胺磷脂(NAPE)可在神经元损伤时作为应激反应形成,它们是N-酰基乙醇胺(NAE)的前体,其中一些是内源性大麻素。通过对脂质提取物进行(31)P核磁共振波谱分析,研究了不同年龄(1、6、12、19、30和约70天)大鼠脑在断头后缺血(37℃下6小时)期间积累的NAPE水平。将这种积累NAPE的能力与脑微粒体中N-酰基转移酶和NAPE水解磷脂酶D(NAPE-PLD)的活性进行了比较。这两种酶分别参与NAPE的形成和降解。结果表明:1)在断头后缺血期间积累NAPE的能力在最年幼的大鼠中特别高,而在老年大鼠脑中则明显降低[在1日龄大鼠脑中,NAPE积累至总磷脂的1.5%,而在30日龄大鼠脑中未检测到NAPE积累(检测限为0.09%)];2)这种积累的年龄模式可以通过发育过程中N-酰基转移酶活性降低和NAPE-PLD活性增加的共同作用来解释。这些结果指出,研究NAPE在非常年幼大鼠脑中的潜在细胞保护作用将是有益的。

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