Apolipoprotein E4 inhibits autophagy gene products through direct, specific binding to CLEAR motifs

载脂蛋白 E4 通过直接、特异性地结合 CLEAR 基序来抑制自噬基因产物

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作者：Paul A Parcon, Meenakshisundaram Balasubramaniam, Srinivas Ayyadevara, Richard A Jones, Ling Liu, Robert J Shmookler Reis, Steven W Barger, Robert E Mrak, W Sue T Griffin

期刊：	Alzheimers & Dementia	影响因子：	13.000
时间：	2018	起止号：	2018 Feb;14(2):230-242.
doi：	10.1016/j.jalz.2017.07.754	种属：	Human
方法学：	FCM、IF、IHC-P、WB	靶点：	APOE
研究方向：	信号转导、细胞生物学	信号通路：	Autophagy

Conclusion

ApoE4-CLEAR interactions may account for suppressed autophagy in APOE ɛ4/ɛ4 carriers and, in this way, contribute to earlier AD onset.

Methods

Autophagic gene expression was assessed in brains of controls and Alzheimer's disease (AD) patients parsed by APOE genotype and in a glioblastoma cell line expressing either apoE3 or apoE4. Computational modeling assessed interactions between apoE and mutated apoE with CLEAR or modified DNA.

Results

Three TFEB-regulated mRNA transcripts-SQSTM, MAP1LC3B, and LAMP2-were lower in AD ɛ4/ɛ4 than in AD ɛ3/ɛ3 brains. Computational modeling predicted avid specific binding of apoE4 to CLEAR motifs. ApoE was found in cellular nuclei, and in vitro binding assays suggest competition between apoE4 and TFEB at CLEAR sites.

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