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Stabilization of the dystroglycan complex in Cajal bands of myelinating Schwann cells through plectin-mediated anchorage to vimentin filaments

机译:通过凝集素对波形蛋白丝的锚定,稳定髓鞘雪旺细胞Cajal带中的dystroglycan复合物的稳定性。

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摘要

Previous studies have unmasked plectin, a uniquely versatile intermediate filament-associated cytolinker protein, to be essential for skin and skeletal muscle integrity. Different sets of isoforms of the protein were found to stabilize cells mechanically, regulate cytoskeletal dynamics, and serve as a scaffolding platform for signaling molecules. Here, we investigated whether a similar scenario prevails in myelinating Schwann cells. Using isoform-specific antibodies, the two plectin variants predominantly expressed in the cytoplasmic compartment (Cajal bands) of Schwann cells were identified as plectin (P)1 and P1c. Coimmunoprecipitation and immunolocalization experiments revealed complex formation of Cajal band plectin with β-dystroglycan, the core component of the dystrophin glycoprotein complex that in Schwann cells is crucial for the compartmentalization and stabilization of the myelin sheath. To study the functional implications of Schwann cell-specific plectin-β-dystroglycan interaction, we generated conditional (Schwann cell-restricted) plectin knockout mice. Ablation of plectin in myelinating Schwann cells (SCs) was found not to affect myelin sheath formation but to abrogate the tight association of the dystroglycan complex with the intermediate filament cytoskeleton. We show that the disruption of this association leads to the destabilization of the dystroglycan complex combined with increased myelin sheath deformations observed in the peripheral nerve during ageing of the animal.
机译:先前的研究已经揭露了Plectin,这是一种独特的多功能中间丝相关的细胞连接蛋白,对于皮肤和骨骼肌的完整性至关重要。发现该蛋白质的不同同工型可机械稳定细胞,调节细胞骨架动力学并充当信号分子的支架平台。在这里,我们调查了髓鞘雪旺细胞中是否普遍存在类似情况。使用同工型特异性抗体,主要在雪旺氏细胞的细胞质区室(Cajal带)表达的两种Plectin变体被鉴定为Plectin(P)1和P1c。免疫共沉淀和免疫定位实验表明,Cajal带状凝集素与β-dystroglycan形成复合物,dystrophin糖蛋白复合物的核心成分在雪旺细胞中对于髓鞘的区室化和稳定至关重要。为了研究雪旺氏细胞特异性凝集素-β-dystroglycan相互作用的功能含义,我们生成了条件性(施万恩细胞限制性)凝集素敲除小鼠。发现在髓鞘雪旺细胞(SCs)中凝集素的消融不影响髓鞘的形成,但可以消除dystroglycan复合物与中间丝细胞骨架的紧密联系。我们表明,这种关联的破坏会导致dystroglycan复合物的不稳定,并伴随着动物衰老过程中在周围神经中观察到的髓鞘鞘变形的增加。

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