Glycated α-Synuclein Renders Glial Cell Activation and Induces Degeneration of Dopaminergic Neurons: A Potential Implication for the Development of Parkinson's Disease.

IF 3.8 2区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY ACS Chemical Biology Pub Date : 2025-03-21 Epub Date: 2025-02-21 DOI:10.1021/acschembio.4c00777

Sayan Chatterjee, Arvind Verma, Harsh Thakkar, Ravi P Shah, Amit Khairnar

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Abstract

Accumulation of misfolded α-synuclein (α-Syn) leads to the formation of Lewy bodies and is a major hallmark of Parkinson's disease (PD). The accumulation of α-Syn involves several post-translational modifications. Recently, though, glycation of α-Syn (advanced glycation end products) and activation of the receptor for advanced glycation end products (RAGE) have been linked to neuroinflammation, which leads to oxidative stress and accumulation of α-Syn. The present study aims to detect the effect of glycated α-Syn (gly-α-Syn)-induced synucleinopathy and loss of dopaminergic (DAergic) neurons in the development of PD. We isolated, purified, and prepared glycated recombinant human α-Syn using d-ribose. Gly-α-Syn was characterized by SDS-PAGE, intact mass analysis, and bottom-up peptide sequence through LC-HRMS/MS. The aggregation propensity of gly-α-Syn has been verified by morphological and shape analysis through Bio-AFM. The gly-α-Syn (2 μg/μL) was injected stereotaxically in the substantia nigra (SN) of ICR mice (3-4 months) and compared with the normal α-Syn, d ribose, and Tris-HCl/artificial CSF groups. 56 days postsurgery (DPS), an immunohistochemical examination was conducted to investigate gly-α-Syn-induced α-Syn accumulation, neuroinflammation, and neurodegeneration. The glycation of α-Syn led to the expression of transglutaminase 2 (TGM2), an enzyme that cross-linked with AGEs and may have caused the accumulation of α-Syn. Significant RAGE activation was also observed in gly-α-Syn, which might have induced glial cell activation, resulting in oxidative stress and, ultimately, apoptosis of dopaminergic neurons. It is important to note that TGM2, phosphorylated α-Syn, RAGE expression, and glial cell activation were only found in the gly-α-Syn group and not in the other groups. This suggests that gly-α-Syn plays a major role in synucleinopathy, neuroinflammation, and neurodegeneration. Overall, the present study demonstrated glycation of α-Syn as one of the important age-associated post-translational modifications that are involved in the degeneration of dopaminergic neurons, at least in a subset of the diabetic patients susceptible to developing PD.

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糖基化α-突触核蛋白使神经胶质细胞活化并诱导多巴胺能神经元变性：帕金森病发展的潜在意义

错误折叠的α-突触核蛋白（α-Syn）的积累导致路易小体的形成，是帕金森病（PD）的主要标志。α-Syn的积累涉及多种翻译后修饰。然而，最近，α-Syn的糖基化（晚期糖基化终产物）和晚期糖基化终产物受体（RAGE）的激活与神经炎症有关，这导致氧化应激和α-Syn的积累。本研究旨在检测糖基化α-Syn （gly-α-Syn）诱导的突触核蛋白病和多巴胺能（DAergic）神经元丧失在PD发生中的作用。我们用d-核糖分离、纯化并制备了重组人α-Syn糖基化。通过SDS-PAGE、完整质谱分析和LC-HRMS/MS自下而上肽段序列对Gly-α-Syn进行了表征。生物原子力显微镜（Bio-AFM）形态分析证实了gly-α-Syn的聚集倾向。将gly-α-Syn （2 μg/μL）立体定向注射于ICR小鼠（3 ~ 4月龄）黑质（SN），并与正常α-Syn、d核糖组和Tris-HCl/人工脑脊液组进行比较。术后56 d （DPS）行免疫组化检查，观察gly-α-Syn诱导的α-Syn积累、神经炎症和神经退行性变。α-Syn的糖基化导致转谷氨酰胺酶2 （TGM2）的表达，TGM2是一种与AGEs交联的酶，可能导致α-Syn的积累。在gly-α-Syn中也观察到显著的RAGE激活，这可能诱导了胶质细胞活化，导致氧化应激，最终导致多巴胺能神经元凋亡。值得注意的是，TGM2、磷酸化α-Syn、RAGE表达和胶质细胞活化仅在gly-α-Syn组中发现，而在其他组中没有发现。这表明gly-α-Syn在突触核蛋白病、神经炎症和神经变性中起重要作用。总的来说，本研究表明α-Syn的糖基化是与年龄相关的重要翻译后修饰之一，参与多巴胺能神经元的变性，至少在一部分易患PD的糖尿病患者中是如此。

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来源期刊

ACS Chemical Biology 生物-生化与分子生物学

CiteScore

7.50

自引率

5.00%

发文量

353

审稿时长

3.3 months

期刊介绍： ACS Chemical Biology provides an international forum for the rapid communication of research that broadly embraces the interface between chemistry and biology. The journal also serves as a forum to facilitate the communication between biologists and chemists that will translate into new research opportunities and discoveries. Results will be published in which molecular reasoning has been used to probe questions through in vitro investigations, cell biological methods, or organismic studies. We welcome mechanistic studies on proteins, nucleic acids, sugars, lipids, and nonbiological polymers. The journal serves a large scientific community, exploring cellular function from both chemical and biological perspectives. It is understood that submitted work is based upon original results and has not been published previously.