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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >FAD mutants unable to increase neurotoxic Abeta 42 suggest that mutation effects on neurodegeneration may be independent of effects on Abeta.
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FAD mutants unable to increase neurotoxic Abeta 42 suggest that mutation effects on neurodegeneration may be independent of effects on Abeta.

机译:无法增加神经毒性Abeta 42的FAD突变体表明,突变对神经变性的影响可能独立于对Abeta的影响。

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摘要

Strong support for a primary causative role of the Abeta peptides in the development of Alzheimer's disease (AD) neurodegeneration derives from reports that presenilin familial AD (FAD) mutants alter amyloid precursor protein processing, thus increasing production of neurotoxic Abeta 1-42 (Abeta 42). This effect of FAD mutants is also reflected in an increased ratio of peptides Abeta 42 over Abeta 1-40 (Abeta 40). In the present study, we show that several presenilin 1 FAD mutants failed to increase production of Abeta 42 or the Abeta 42/40 ratio. Our data suggest that the mechanism by which FAD mutations promote neurodegeneration and AD may be independent of their effects on Abeta production.
机译:对Abeta肽在阿尔茨海默氏病(AD)神经退行性疾病发展中起主要作用的有力支持来自以下报道:早老素家族AD(FAD)突变体改变淀粉样前体蛋白的加工过程,从而增加了神经毒性Abeta 1-42(Abeta 42 )。 FAD突变体的这种作用还反映在肽Abeta 42相对于Abeta 1-40(Abeta 40)的比率增加中。在本研究中,我们显示了几个早老素1 FAD突变体未能增加Abeta 42或Abeta 42/40的产生。我们的数据表明,FAD突变促进神经变性和AD的机制可能与它们对Abe​​ta产生的影响无关。

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