阿尔茨海默病淀粉样β肽通过p75神经营养因子受体/PLAIDD诱导神经杂交细胞死亡的分子特征
Molecular characterization of neurohybrid cell death induced by Alzheimer's amyloid-beta peptides via p75NTR/PLAIDD.
作者信息
Hashimoto Yuichi, Kaneko Yuka, Tsukamoto Emi, Frankowski Harald, Kouyama Keisuke, Kita Yoshiko, Niikura Takako, Aiso Sadakazu, Bredesen Dale E, Matsuoka Masaaki, Nishimoto Ikuo
机构信息
Department of Pharmacology, KEIO University School of Medicine, Shinanomachi, Tokyo, Japan.
出版信息
J Neurochem. 2004 Aug;90(3):549-58. doi: 10.1111/j.1471-4159.2004.02513.x.
One of the most important pathological features of Alzheimer's disease (AD) is extracellular senile plaques, whose major component is amyloid-beta peptides (Abeta). Abeta binds to the extracellular domain of p75NTR (p75 neurotrophin receptor) and induces neuronal cell death. We investigated the molecular mechanism of Abeta-induced neurotoxicity in detail from the standpoint of interaction between p75NTR and its recently identified relative, PLAIDD (p75-like apoptosis-inducing death domain). Using F11 neuronal hybrid cells, we demonstrate that there are two distinct pathways for Abeta-induced toxicity mediated by p75NTR. One pathway that has been previously elucidated, is mediated by p75NTR, Go, JNK, NADPH oxidase and caspase3-related caspases. We found that PLAIDD and Gi proteins, heterotrimeric G proteins, are involved in the alternative Abeta-induced neurotoxicity mediated by p75NTR. The alternative pathway triggered by Abeta is thus mediated by p75NTR, PLAIDD, Gi, JNK, NADPH oxidase and caspase3-related caspases. In addition, we found that HN, ADNF, IGF-I, or bFGF inhibits both pathways of Abeta-induced neurotoxicity mediated by p75NTR.
阿尔茨海默病(AD)最重要的病理特征之一是细胞外老年斑,其主要成分是β淀粉样肽(Aβ)。Aβ与p75神经营养因子受体(p75NTR)的细胞外结构域结合并诱导神经元细胞死亡。我们从p75NTR与其最近发现的相关蛋白PLAIDD(p75样凋亡诱导死亡结构域)之间相互作用的角度详细研究了Aβ诱导神经毒性的分子机制。利用F11神经元杂交细胞,我们证明p75NTR介导的Aβ诱导毒性存在两条不同的途径。一条先前已阐明的途径由p75NTR、Go、JNK、NADPH氧化酶和caspase3相关半胱天冬酶介导。我们发现PLAIDD和Gi蛋白(异源三聚体G蛋白)参与了由p75NTR介导的另一条Aβ诱导神经毒性途径。因此,由Aβ触发的另一条途径由p75NTR、PLAIDD、Gi、JNK、NADPH氧化酶和caspase3相关半胱天冬酶介导。此外,我们发现HN、ADNF、IGF-I或bFGF可抑制p75NTR介导的Aβ诱导神经毒性的两条途径。
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