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锂对正常和去神经支配的神经肌肉突触后稳定性有不同的影响。

Lithium causes differential effects on postsynaptic stability in normal and denervated neuromuscular synapses.

机构信息

Neuromuscular Studies Laboratory (NeSt Lab), Department of Cell Biology, CMA Bio-Bio, Facultad de Ciencias Biológicas, Universidad de Concepción, Casilla 160-C, Concepción, Chile.

Pontificia Universidad Católica Argentina (UCA)-Scientific and Technological Research Council of Argentina (CONICET), Buenos Aires, Argentina.

出版信息

Sci Rep. 2021 Aug 26;11(1):17285. doi: 10.1038/s41598-021-96708-7.

Abstract

Lithium chloride has been widely used as a therapeutic mood stabilizer. Although cumulative evidence suggests that lithium plays modulatory effects on postsynaptic receptors, the underlying mechanism by which lithium regulates synaptic transmission has not been fully elucidated. In this work, by using the advantageous neuromuscular synapse, we evaluated the effect of lithium on the stability of postsynaptic nicotinic acetylcholine receptors (nAChRs) in vivo. We found that in normally innervated neuromuscular synapses, lithium chloride significantly decreased the turnover of nAChRs by reducing their internalization. A similar response was observed in CHO-K1/A5 cells expressing the adult muscle-type nAChRs. Strikingly, in denervated neuromuscular synapses, lithium led to enhanced nAChR turnover and density by increasing the incorporation of new nAChRs. Lithium also potentiated the formation of unstable nAChR clusters in non-synaptic regions of denervated muscle fibres. We found that denervation-dependent re-expression of the foetal nAChR γ-subunit was not altered by lithium. However, while denervation inhibits the distribution of β-catenin within endplates, lithium-treated fibres retain β-catenin staining in specific foci of the synaptic region. Collectively, our data reveal that lithium treatment differentially affects the stability of postsynaptic receptors in normal and denervated neuromuscular synapses in vivo, thus providing novel insights into the regulatory effects of lithium on synaptic organization and extending its potential therapeutic use in conditions affecting the peripheral nervous system.

摘要

氯化锂被广泛用作治疗情绪稳定剂。尽管累积的证据表明锂对突触后受体具有调节作用,但锂调节突触传递的潜在机制尚未完全阐明。在这项工作中,我们利用有利的神经肌肉突触,评估了锂对体内突触后烟碱型乙酰胆碱受体(nAChRs)稳定性的影响。我们发现,在正常神经支配的神经肌肉突触中,氯化锂通过减少 nAChRs 的内化来显著降低其周转率。在表达成人肌肉型 nAChRs 的 CHO-K1/A5 细胞中观察到类似的反应。引人注目的是,在去神经支配的神经肌肉突触中,锂通过增加新 nAChRs 的掺入来增加 nAChRs 的周转率和密度。锂还增强了去神经纤维中非突触区域不稳定的 nAChR 簇的形成。我们发现,锂对依赖去神经的胎儿 nAChR γ 亚基的再表达没有影响。然而,虽然去神经抑制了β-连环蛋白在终板内的分布,但经锂处理的纤维在突触区域的特定焦点中保留了β-连环蛋白染色。总的来说,我们的数据表明,锂处理在体内正常和去神经支配的神经肌肉突触中对突触后受体的稳定性产生不同的影响,从而为锂对突触组织的调节作用提供了新的见解,并扩展了其在影响周围神经系统的疾病中的潜在治疗用途。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/450f/8390761/80dc6f5b6587/41598_2021_96708_Fig1_HTML.jpg

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