Inhibition of NLRP1 inflammasome improves autophagy dysfunction and Aβ disposition in APP/PS1 mice.

IF 4.7 2区 心理学 Q1 BEHAVIORAL SCIENCES
Xuewang Li, Han Zhang, Liu Yang, Xianan Dong, Yuli Han, Yong Su, Weiping Li, Weizu Li
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引用次数: 2

Abstract

Increasing evidence has shown that the NOD-like receptor protein 1 (NLRP1) inflammasome is associated with Aβ generation and deposition, which contributes to neuronal damage and neuronal-inflammation in Alzheimer's disease (AD). However, the specific mechanism of NLRP1 inflammasome in the pathogenesis of AD is still unclear. It has been reported that autophagy dysfunction can aggravate the pathological symptoms of AD and plays an important role in regulating Aβ generation and clearance. We hypothesized that NLRP1 inflammasome activation may induce autophagy dysfunction contributing to the progression of AD. In the present study, we observed the relationship between Aβ generation and NLRP1 inflammasome activation, as well as AMPK/mTOR mediated-autophagy dysfunction in WT 9-month-old (M) mice, APP/PS1 6 M and APP/PS1 9 M mice. Additionally, we further studied the effect of NLRP1 knockdown on cognitive function, Aβ generation, neuroinflammation and AMPK/mTOR mediated autophagy in APP/PS1 9 M mice. Our results indicated that NLRP1 inflammasome activation and AMPK/mTOR mediated-autophagy dysfunction are closely implicated in Aβ generation and deposition in APP/PS1 9 M mice, but not in APP/PS1 6 M mice. Meanwhile, we found that knockdown of NLRP1 significantly improved learning and memory impairments, decreased the expressions of NLRP1, ASC, caspase-1, p-NF-κB, IL-1β, APP, CTF-β, BACE1 and Aβ1-42, and decreased the level of p-AMPK, Beclin 1 and LC3 II, and increased the level of p-mTOR and P62 in APP/PS1 9 M mice. Our study suggested that inhibition of NLRP1 inflammasome activation improves AMPK/mTOR mediated-autophagy dysfunction, resulting in the decrease of Aβ generation, and NLRP1 and autophagy might be important targets to delay the progression of AD.

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抑制NLRP1炎性体可改善APP/PS1小鼠的自噬功能障碍和Aβ配置。
越来越多的证据表明,nod样受体蛋白1 (NLRP1)炎症小体与Aβ的产生和沉积有关,这有助于阿尔茨海默病(AD)的神经元损伤和神经元炎症。然而,NLRP1炎性体在AD发病中的具体机制尚不清楚。有报道称,自噬功能障碍可加重AD的病理症状,并在调节Aβ的产生和清除中起重要作用。我们假设NLRP1炎性小体激活可能诱导自噬功能障碍,促进AD的进展。在本研究中,我们在WT 9月龄(M)小鼠、APP/PS1 6 M和APP/PS1 9 M小鼠中观察了Aβ生成与NLRP1炎性小体激活以及AMPK/mTOR介导的自噬功能障碍之间的关系。此外,我们进一步研究了NLRP1敲低对APP/PS1 9m小鼠认知功能、Aβ生成、神经炎症和AMPK/mTOR介导的自噬的影响。我们的研究结果表明,NLRP1炎性体激活和AMPK/mTOR介导的自噬功能障碍与APP/PS1 9 M小鼠的Aβ生成和沉积密切相关,而与APP/PS1 6 M小鼠无关。同时,我们发现NLRP1的下调显著改善了APP/PS1 9m小鼠的学习和记忆障碍,降低了NLRP1、ASC、caspase-1、p-NF-κB、IL-1β、APP、CTF-β、BACE1和a -β 1-42的表达,降低了p-AMPK、Beclin 1和LC3 II的水平,升高了p-mTOR和P62的水平。我们的研究提示,抑制NLRP1炎性小体激活可改善AMPK/mTOR介导的自噬功能障碍,导致Aβ生成减少,NLRP1和自噬可能是延缓AD进展的重要靶点。
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来源期刊
Behavioral and Brain Functions
Behavioral and Brain Functions 医学-行为科学
CiteScore
5.90
自引率
0.00%
发文量
11
审稿时长
6-12 weeks
期刊介绍: A well-established journal in the field of behavioral and cognitive neuroscience, Behavioral and Brain Functions welcomes manuscripts which provide insight into the neurobiological mechanisms underlying behavior and brain function, or dysfunction. The journal gives priority to manuscripts that combine both neurobiology and behavior in a non-clinical manner.
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