ARRB1 通过促进自噬抑制细胞外基质降解和髓核细胞凋亡,并减轻椎间盘退变。

IF 4.6 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Xuejian Dan , Xiaochuan Gu , Ying Zi , Jiahui Xu , Chenggang Wang , Chen Li , Xiao Hu , Zhourui Wu , Yan Yu , Bin Ma
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引用次数: 0

摘要

目的:椎间盘退行性变(IVDD)是导致下背痛(LBP)的主要原因。β-阿司匹林1(ARRB1)是一种多功能蛋白,可调节多种病理过程。本研究旨在探讨 ARRB1 在 IVDD 中的作用:方法:检测 ARRB1 在 IVDD 大鼠髓核(NP)中的表达。然后用含有 shArrb1(LV-shArrb1)和过表达 Arrb1(LV-oeArrb1)的慢病毒感染大鼠髓核细胞(NPCs)。通过测量细胞凋亡、细胞外基质降解和自噬通量,研究了 Arrb1 在血清缺乏的鼻咽癌中的作用。在体内实验中,将 LV-oeArrb1 慢病毒注射到 IVDD 大鼠的 NP 组织中,以评估 Arrb1 过表达对 NP 的影响:结果:在IVDD大鼠的NP组织中,ARRB1和裂解的caspase-3表达增加,LC3II/LC3I蛋白表达比例上调。敲除 Arrb1 会加剧血清缺失条件下大鼠 NPC 的细胞外基质降解、细胞凋亡和自噬通量受损,而过表达 Arrb1 则会显著逆转这些影响。ARRB1 与 Beclin 1 相互作用,Arrb1 基因敲除抑制了 Beclin1-PIK3C3 核心复合物的形成。自噬抑制剂 3-甲基腺嘌呤(3-MA)抵消了 Arrb1 过表达对血清缺乏的鼻咽癌的保护作用。此外,Arrb1的过表达抑制了细胞凋亡和细胞外基质降解,促进了NP的自噬,并延缓了大鼠IVDD的发生:结论:ARRB1可通过上调自噬防止NPC的细胞外基质降解和凋亡,改善IVDD的进展,是治疗IVDD的一种创新策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

ARRB1 inhibits extracellular matrix degradation and apoptosis of nucleus pulposus cells by promoting autophagy and attenuates intervertebral disc degeneration

ARRB1 inhibits extracellular matrix degradation and apoptosis of nucleus pulposus cells by promoting autophagy and attenuates intervertebral disc degeneration

Objective

Intervertebral disc degeneration (IVDD) is the leading cause of lower back pain (LBP). β-arrestin 1 (ARRB1) is a multifunctional protein that regulates numerous pathological processes. The aim of this study was to investigate the role of ARRB1 in IVDD.

Methods

The expression of ARRB1 in nucleus pulposus (NP) of rats with IVDD was assayed. Next, rat nucleus pulposus cells (NPCs) were infected with lentiviruses containing shArrb1 (LV-shArrb1) and overexpressing Arrb1 (LV-oeArrb1). The roles of Arrb1 in serum-deprived NPCs were investigated by measuring apoptosis, extracellular matrix degradation, and autophagic flux. For experiments in vivo, LV-oeArrb1 lentivirus was injected into the NP tissues of IVDD rats to evaluate the effects of Arrb1 overexpression on NP.

Results

In the NP tissues of IVDD rats, ARRB1 and cleaved caspase-3 expression increased, and the ratio of LC3II/LC3I protein expression was upregulated. Arrb1 knockdown aggravated extracellular matrix degradation, cellular apoptosis, and impairment of autophagic flux in rat NPCs under serum-deprived conditions, whereas Arrb1 overexpression significantly reversed these effects. ARRB1 interacted with Beclin 1, and Arrb1 knockdown suppressed the formation of the Beclin1-PIK3C3 core complex. The autophagy inhibitor 3-methyladenine (3-MA) offset the protective effects of Arrb1 overexpression in serum-deprived NPCs. Furthermore, Arrb1 overexpression inhibited apoptosis and extracellular matrix degradation, promoted autophagy in NP, and delayed the development of IVDD in rats.

Conclusion

ARRB1 prevents extracellular matrix degradation and apoptosis of NPCs by upregulating autophagy and ameliorating IVDD progression, presenting an innovative strategy for the treatment of IVDD.

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来源期刊
CiteScore
10.00
自引率
2.00%
发文量
151
审稿时长
44 days
期刊介绍: BBA Molecular Cell Research focuses on understanding the mechanisms of cellular processes at the molecular level. These include aspects of cellular signaling, signal transduction, cell cycle, apoptosis, intracellular trafficking, secretory and endocytic pathways, biogenesis of cell organelles, cytoskeletal structures, cellular interactions, cell/tissue differentiation and cellular enzymology. Also included are studies at the interface between Cell Biology and Biophysics which apply for example novel imaging methods for characterizing cellular processes.
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