磷蛋白组学分析揭示了胆红素缺乏诱导的神经炎症和轴突引导受损的关键蛋白。

IF 3.9 3区医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

ACS Chemical Neuroscience Pub Date : 2025-07-07 DOI:10.1021/acschemneuro.5c00117

Ming Chen, Cuiping Wu, Yaqi Cui, Bingbing Ke, Linfei Mao, Hongyang Wang, Jinhong Shen, Shankai Yin*, Mu Hu* and Chunyan Li*,

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引用次数: 0

摘要

低胆红素血症，以低胆红素水平为特征，越来越被认为是一种与各种神经发育和神经退行性疾病相关的病理状况。然而，低胆红素血症的神经病理机制尚不清楚。在本研究中，我们旨在通过磷蛋白质组学和蛋白质组学的综合分析来阐明神经元结构和功能损伤的潜在分子机制。对胆绿素还原酶a敲除（Blvra-/-）小鼠和野生型（WT）小鼠脑组织进行蛋白质组学分析，鉴定出133种差异表达蛋白。丰度降低的蛋白在轴突发生中富集，而丰度增加的蛋白主要参与PI3K-Akt信号通路，包括LAMA4和ITGA1。磷酸化蛋白质组学分析显示390种蛋白在542个位点磷酸化降低，而82种蛋白在96个位点磷酸化升高。磷酸化降低的磷酸化位点相关蛋白在神经发生和轴突引导通路中富集，而磷酸化位点增加的磷酸化位点相关蛋白则与神经元凋亡相关。Western blotting验证证实了差异表达磷酸化蛋白蛋白相互作用网络中的关键蛋白，如DPYSL2、MAPK8和PRKCD的调节，这些蛋白先前被认为与神经元的发育和退化有关。高尔基染色进一步显示，与WT小鼠相比，Blvra-/-小鼠的树突交叉点、分支点数量减少，神经突长度缩短，树突复杂性降低。这些结果表明，低胆红素水平破坏脑蛋白磷酸化调节网络，这可能导致神经炎症，促进神经元凋亡，损害神经元生长，可能导致神经发育和神经退行性疾病。

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Phosphoproteomics Profiling Reveals Key Proteins Involved in Neuroinflammation and Impaired Axon Guidance Induced by Bilirubin Deficiency

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Phosphoproteomics Profiling Reveals Key Proteins Involved in Neuroinflammation and Impaired Axon Guidance Induced by Bilirubin Deficiency

Hypobilirubinemia, characterized by low bilirubin levels, is increasingly recognized as a pathological condition linked to various neurodevelopmental and neurodegenerative diseases. However, the neuropathological mechanisms of hypobilirubinemia remain unclear. In this study, we aimed to elucidate the potential molecular mechanism of neuronal structural and functional damage through integrated phosphoproteomics and proteomics analysis. Proteomic analysis of brain tissues from Biliverdin reductase-A knockout (Blvra^–/–) mice and wild-type (WT) mice identified 133 differentially expressed proteins. Proteins with decreased abundance were enriched in axonogenesis, while proteins showing increased abundance were primarily involved in the PI3K-Akt signaling pathway, including LAMA4 and ITGA1. Phosphoproteomic analysis revealed 390 proteins with decreased phosphorylation at 542 sites, while 82 proteins had increased phosphorylation at 96 sites. Proteins associated with phosphosites showing decreased phosphorylation were enriched in neurogenesis and the axon guidance pathway, while those associated with increased phosphorylation sites were linked to neuronal apoptosis. Western blotting validation confirmed the modulation of key proteins, such as DPYSL2, MAPK8, and PRKCD, within the protein–protein interaction network of differentially expressed phosphorylated proteins, which have previously been implicated in neuronal development and degeneration. Golgi staining further revealed reduced number of dendritic intersections, branch points, shortened neurite length, and decreased dendritic complexity in Blvra^–/– mice compared to WT mice. These results indicated that low bilirubin levels disrupt brain protein phosphorylation regulatory networks, which may drive neuroinflammation, promote neuronal apoptosis, and impair neuronal growth, potentially contributing to neurodevelopmental and neurodegenerative diseases.

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来源期刊

ACS Chemical Neuroscience BIOCHEMISTRY & MOLECULAR BIOLOGY-CHEMISTRY, MEDICINAL

CiteScore

9.20

自引率

4.00%

发文量

323

审稿时长

1 months

期刊介绍： ACS Chemical Neuroscience publishes high-quality research articles and reviews that showcase chemical, quantitative biological, biophysical and bioengineering approaches to the understanding of the nervous system and to the development of new treatments for neurological disorders. Research in the journal focuses on aspects of chemical neurobiology and bio-neurochemistry such as the following: Neurotransmitters and receptors Neuropharmaceuticals and therapeutics Neural development—Plasticity, and degeneration Chemical, physical, and computational methods in neuroscience Neuronal diseases—basis, detection, and treatment Mechanism of aging, learning, memory and behavior Pain and sensory processing Neurotoxins Neuroscience-inspired bioengineering Development of methods in chemical neurobiology Neuroimaging agents and technologies Animal models for central nervous system diseases Behavioral research