细胞纤维连接蛋白通过整合素alpha4beta1介导的PARP1和SCD升高加剧α-突触核蛋白聚集。

IF 6.9 2区医学 Q1 CLINICAL NEUROLOGY

Neurotherapeutics Pub Date : 2025-09-04 DOI:10.1016/j.neurot.2025.e00729

Zifeng Huang, Hui Zhong, Yingqiong Lu, Ruoyang Yu, Muwei Zhang, Jialing Zheng, Bin Xiao, Zhidong Zhou, Yinghua Yu, Chao Deng, Kunlin Jin, Shuzhen Zhu, Chong Li, Xiaoying Cui, Karolina Poplawska-Domaszewicz, K Ray Chaudhuri, Eng-King Tan, Qing Wang

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引用次数: 0

摘要

线粒体功能障碍和脂质代谢紊乱可促进病理性α-突触核蛋白（α-syn）聚集，加速帕金森病（PD）的进展。细胞外基质是否与PD的这些病理机制有关尚不清楚。在这里，我们旨在确定细胞外基质成分细胞纤维连接蛋白（cFn）是否通过诱导线粒体能量消耗或破坏脂质稳态而导致α-syn异常。本研究使用1-甲基-4-苯基- 1,2,3,6 -四氢吡啶（MPTP）处理的PD小鼠和人神经元SH-SY5Y细胞。为了验证cFn的功能作用，我们建立了星形胶质细胞衍生的cFn蛋白递送和aav介导的cFn敲低小鼠模型。透射电镜（TEM）检测线粒体功能障碍，检测多聚腺苷磷酸核糖（PAR）聚合酶-1（PARP1）、病理性α-syn和cfn诱导的脂质代谢异常水平。我们证明了mptp处理小鼠SNpc中cFn的过量积累，cFn而不是血浆Fn （pFn）加重了神经元线粒体功能障碍和α-syn的积累。机制上，cFn通过整合素α4β1诱导PARP1活化，导致神经元NAD +耗竭和病理性α-syn聚集。此外，cFn通过与整合素α4β1结合，诱导神经元中游离脂肪酸（FAs）和甘油三酯（TAG）的增加，协同作用导致α-syn异常。我们发现cFn通过整合素α4β1诱导硬脂酰辅酶a去饱和酶（SCD）活化，并与SCD相互作用。基因消耗cFn抑制PARP1激活和SCD升高，进一步挽救了mptp处理小鼠的线粒体破坏和α-syn异常。总之，我们的研究结果表明，cFn通过整合素α4β1介导的PARP1和SCD升高加剧α-syn聚集。cfn靶向治疗可能是治疗PD的一种有前景的策略。

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Cellular fibronectin exacerbates α-synuclein aggregation via integrin alpha4beta1 mediated PARP1 and SCD elevation.

Mitochondrial dysfunction and lipid metabolic disturbance may promote pathologic α-synuclein (α-syn) aggregation, accelerating the progression of Parkinson's disease (PD). Whether extracellular matrices are associated with those pathological mechanisms in PD remains elusive. Here, we aimed to identify if cellular fibronectin (cFn), a component of extracellular matrices, contributes to α-syn abnormality via inducing mitochondrial energy depletion or disrupting lipid homeostasis. In Our study, 1-methyl-4-phenyl-1, 2,3,6-tetrahydropyridine (MPTP)-treated PD mice and human neuronal SH-SY5Y cells were used. Astrocyte-derived cFn protein delivery and AAV-mediated cFn knockdown mouse models were established to validate the functional role of cFn. Mitochondrial dysfunction was detected by transmission electron microscopy (TEM), and the level of poly (ADP‒ribose) (PAR) polymerase-1(PARP1), pathologic α-syn and cFn-induced lipid dysmetabolism was determined. We demonstrated that excessive cFn accumulated in the SNpc of MPTP-treated mice, and cFn rather than plasma Fn (pFn) exacerbated neuronal mitochondrial dysfunction and α-syn accumulation. Mechanically, cFn induced PARP1 activation via integrin α4β1, which contributed to neuronal NAD + depletion and pathologic α-syn aggregation. Furthermore, cFn induced an increase in free fatty acids (FAs) and triglycerides (TAG) in neurons by binding to integrin α4β1, which synergistically contributed to α-syn abnormality. We revealed that cFn induced stearoyl-CoA desaturase (SCD) activation via integrin α4β1, which was interacted with SCD. Genetically depleting cFn suppressed PARP1 activation and SCD elevation, which further rescued the mitochondrial disruption and α-syn abnormalities in MPTP-treated mice. Overall, our findings suggest that cFn exacerbates α-syn aggregation via integrin α4β1-mediated PARP1 and SCD elevation. cFn-targeting therapy may be a promising strategy for treating PD.

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来源期刊

Neurotherapeutics 医学-神经科学

CiteScore

11.00

自引率

3.50%

发文量

154

审稿时长

6-12 weeks

期刊介绍： Neurotherapeutics® is the journal of the American Society for Experimental Neurotherapeutics (ASENT). Each issue provides critical reviews of an important topic relating to the treatment of neurological disorders written by international authorities. The Journal also publishes original research articles in translational neuroscience including descriptions of cutting edge therapies that cross disciplinary lines and represent important contributions to neurotherapeutics for medical practitioners and other researchers in the field. Neurotherapeutics ® delivers a multidisciplinary perspective on the frontiers of translational neuroscience, provides perspectives on current research and practice, and covers social and ethical as well as scientific issues.