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阿尔茨海默型老年痴呆症中肽代谢和神经肽酶活性的改变。

Alterations of peptide metabolism and neuropeptidase activity in senile dementia of the Alzheimer's type.

作者信息

Waters S M, Davis T P

机构信息

Department of Pharmacology, College of Medicine, University of Arizona Health Sciences Center, Tucson 85724, USA.

出版信息

Ann N Y Acad Sci. 1997 Apr 24;814:30-9. doi: 10.1111/j.1749-6632.1997.tb46142.x.

Abstract

Work in our laboratory has shown that in addition to previously characterized changes in the level of neuropeptides in SDAT brain, the activity of degradative enzymes responsible for peptide metabolism is also affected. In addition to other reported alterations in peptide metabolism, we have observed that SS-28 degradation is increased in Brodmann area 22 whereas substance P degradation is increased in temporal cortex. Changes in the degradation of these neuropeptides known to be affected in SDAT correlate well with alterations in the activity of specific neuropeptidases. Trypsin-like serine protease activity is increased in SDAT Brodmann area 22 which parallels the increased degradation of SS-28. The activity of MEP 24.15 is decreased in temporal cortex which corresponds to the decreased degradation of substance P. Changes in the activity of these degradative enzymes in SDAT brain can potentially affect the action of other neuropeptide substrates because the neuropeptidases discussed here terminate the action of several neuropeptides. As more neuropeptide and degradative peptidase alterations are discovered in SDAT, greater emphasis may be placed on the role that peptides and neuropeptidases play in the progression of SDAT.

摘要

我们实验室的研究表明,除了先前已描述的SDAT脑内神经肽水平的变化外,负责肽代谢的降解酶的活性也受到影响。除了其他已报道的肽代谢改变外,我们还观察到,在布罗德曼22区,SS - 28的降解增加,而在颞叶皮质,P物质的降解增加。这些已知在SDAT中受影响的神经肽降解变化与特定神经肽酶活性的改变密切相关。在SDAT布罗德曼22区,类胰蛋白酶丝氨酸蛋白酶活性增加,这与SS - 28降解增加平行。在颞叶皮质,MEP 24.15的活性降低,这与P物质降解减少相对应。SDAT脑中这些降解酶活性的变化可能会影响其他神经肽底物的作用,因为这里讨论的神经肽酶会终止几种神经肽的作用。随着在SDAT中发现更多神经肽和降解肽酶的改变,可能会更加强调肽和神经肽酶在SDAT进展中所起的作用。

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