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首页> 外文期刊>FEBS Letters >Proteolytic processing of presenilin‐1 (PS‐1) is not associated with Alzheimer's disease with or without PS‐1 mutations
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Proteolytic processing of presenilin‐1 (PS‐1) is not associated with Alzheimer's disease with or without PS‐1 mutations

机译:早老蛋白-1(PS-1)的蛋白水解过程与有或没有PS-1突变的阿尔茨海默氏病无关

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>Cerebral presenilin-1 protein (PS-1) is normally composed of the amino-terminal fragment (NTF) with M r 28 kDa and the carboxy-terminal fragment (CTF) with 18 kDa. We analyzed human PS-1 in brains with early-onset familial Alzheimer's disease (FAD) with and without PS-1 mutations to study whether mutated PS-1 was abnormally metabolized. Cerebral PS-1 were found to be cleaved into two fragments of NTF and CTF independently of the occurrence of PS-1 mutation in human brains. A small portion of PS-1 was recently found to suffer another processing by caspase-3, an apoptosis-related cysteine protease. In contrast to the recent finding that the Volga-German mutation on presenilin-2 (PS-2) affects the increasing caspase-3 PS-2 fragment, the PS-1 mutation did not cause a significant change in PS-1 fragmentation. We conclude that PS-1 fragmentation and other (probably caspase-3-mediated) digestion following apoptosis occur independently of PS-1 mutations.
机译:>脑早老素1蛋白(PS-1)通常由具有 M r 28 kDa的氨基末端片段(NTF)和羧基末端片段组成(CTF)与18 kDa。我们分析了患有和不患有PS-1突变的早发性家族性阿尔茨海默病(FAD)的大脑中的人类PS-1,以研究突变的PS-1是否被异常代谢。发现大脑PS-1可以被切割为NTF和CTF的两个片段,而与人类大脑中PS-1突变的发生无关。最近发现一小部分PS-1受到caspase-3的另一加工处理,而caspase-3是凋亡相关的半胱氨酸蛋白酶。与最近发现的早老素2上的伏尔加德国突变(PS-2)影响增加的caspase-3 PS-2片段相反,PS-1突变并未引起PS-1片段的显着变化。我们得出结论,凋亡后PS-1片段化和其他(可能是caspase-3介导的)消化独立于 PS-1 突变发生。

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