Neuregulin 4 Attenuates Podocyte Injury and Proteinuria in Part by Activating AMPK/mTOR-Mediated Autophagy in Mice

IF 3 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Juntian Deng, Qiansheng Yang, Wanyu Zhu, Yanhua Zhang, Meng Lin, Juyan She, Jing Li, Yuxin Xiao, Jun Xiao, Xinyue Xu, Hebei He, Biao Zhu, Yan Ding
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引用次数: 0

Abstract

In this study, we investigate the effect of neuregulin 4 (NRG4) on podocyte damage in a mouse model of diabetic nephropathy (DN) and we elucidate the underlying molecular mechanisms. In vivo experiments were conducted using a C57BL/6 mouse model of DN to determine the effect of NRG4 on proteinuria and podocyte injury, and in vitro experiments were performed with conditionally immortalized mouse podocytes treated with high glucose and NRG4 to assess the protective effects of NRG4 on podocyte injury. Autophagy-related protein levels and related signaling pathways were evaluated both in vivo and in vitro. The involvement of the adenosine monophosphate-activated protein kinase (AMPK)/mammalian target of rapamycin (mTOR) pathway was detected using chloroquine or AMPK inhibitors. The results showed that the AMPK/mTOR pathway was involved in the protective roles of NRG4 against high glucose-mediated podocyte injury. Also, NRG4 significantly decreased albuminuria in DN mice. PAS staining indicated that NRG4 mitigated glomerular volume and mesangium expansion in DN mice. Consistently, western blot and RT-PCR analyses confirmed that NRG4 decreased the expression of pro-fibrotic molecules in the glomeruli of DN mice. The immunofluorescence results showed that NRG4 retained expression of podocin and nephrin, whereas transmission electron microscopy revealed that NRG4 alleviated podocyte injury. In DN mice, NRG4 decreased podocyte apoptosis and increased expression of nephrin and podocin, while decreasing the expression of desmin and HIF1α. Overall, NRG4 improved albuminuria, glomerulosclerosis, glomerulomegaly, and hypoxia in DN mice. The in vitro experiments showed that NRG4 inhibited HG-induced podocyte injury and apoptosis. Furthermore, autophagy of the glomeruli decreased in DN mice, but reactivated following NRG4 intervention. NRG4 intervention was found to partially activate autophagy via the AMPK/mTOR signaling pathway. Consequently, when the AMPK/mTOR pathway was suppressed or autophagy was inhibited, the beneficial effects of NRG4 intervention on podocyte injury were diminished. These results indicate that NRG4 intervention attenuates podocyte injury and apoptosis by promoting autophagy in the kidneys of DN mice, in part, by activating the AMPK/mTOR signaling pathway.

Neuregulin 4 在一定程度上通过激活 AMPK/mTOR 介导的小鼠自噬来减轻荚膜细胞损伤和蛋白尿。
在这项研究中,我们研究了神经胶质蛋白 4(NRG4)对糖尿病肾病(DN)小鼠模型中荚膜细胞损伤的影响,并阐明了其潜在的分子机制。我们使用 C57BL/6 DN 小鼠模型进行了体内实验,以确定 NRG4 对蛋白尿和荚膜细胞损伤的影响,并使用经高糖和 NRG4 处理的条件永生化小鼠荚膜细胞进行了体外实验,以评估 NRG4 对荚膜细胞损伤的保护作用。对体内和体外自噬相关蛋白水平和相关信号通路进行了评估。使用氯喹或 AMPK 抑制剂检测了单磷酸腺苷激活的蛋白激酶(AMPK)/哺乳动物雷帕霉素靶蛋白激酶(mTOR)通路的参与情况。结果表明,AMPK/mTOR通路参与了NRG4对高糖介导的荚膜细胞损伤的保护作用。此外,NRG4 还能明显降低 DN 小鼠的白蛋白尿。PAS 染色表明,NRG4 可减轻 DN 小鼠的肾小球体积和系膜扩张。同样,Western 印迹和 RT-PCR 分析证实,NRG4 可减少 DN 小鼠肾小球中促纤维化分子的表达。免疫荧光结果显示,NRG4保留了荚膜蛋白和肾素的表达,而透射电子显微镜则显示,NRG4减轻了荚膜细胞的损伤。在 DN 小鼠中,NRG4 可减少荚膜细胞凋亡,增加肾素和荚膜蛋白的表达,同时降低 desmin 和 HIF1α 的表达。总体而言,NRG4 可改善 DN 小鼠的白蛋白尿、肾小球硬化、肾小球肿大和缺氧状况。体外实验表明,NRG4 可抑制 HG 诱导的荚膜细胞损伤和凋亡。此外,DN小鼠肾小球的自噬功能下降,但在NRG4干预后又重新激活。研究发现,NRG4 可通过 AMPK/mTOR 信号通路部分激活自噬。因此,当 AMPK/mTOR 通路被抑制或自噬被抑制时,NRG4 干预对荚膜细胞损伤的有益作用就会减弱。这些结果表明,NRG4 通过促进 DN 小鼠肾脏中的自噬,部分地通过激活 AMPK/mTOR 信号通路来减轻荚膜损伤和凋亡。
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来源期刊
Journal of cellular biochemistry
Journal of cellular biochemistry 生物-生化与分子生物学
CiteScore
9.90
自引率
0.00%
发文量
164
审稿时长
1 months
期刊介绍: The Journal of Cellular Biochemistry publishes descriptions of original research in which complex cellular, pathogenic, clinical, or animal model systems are studied by biochemical, molecular, genetic, epigenetic or quantitative ultrastructural approaches. Submission of papers reporting genomic, proteomic, bioinformatics and systems biology approaches to identify and characterize parameters of biological control in a cellular context are encouraged. The areas covered include, but are not restricted to, conditions, agents, regulatory networks, or differentiation states that influence structure, cell cycle & growth control, structure-function relationships.
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