Autism-related KLHL17 and SYNPO act in concert to control activity-dependent dendritic spine enlargement and the spine apparatus.

IF 7.8 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
PLoS Biology Pub Date : 2023-08-31 eCollection Date: 2023-08-01 DOI:10.1371/journal.pbio.3002274
Hsiao-Tang Hu, Yung-Jui Lin, Ueh-Ting Tim Wang, Sue-Ping Lee, Yae-Huei Liou, Bi-Chang Chen, Yi-Ping Hsueh
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引用次数: 0

Abstract

Dendritic spines, the tiny and actin-rich protrusions emerging from dendrites, are the subcellular locations of excitatory synapses in the mammalian brain that control synaptic activity and plasticity. Dendritic spines contain a specialized form of endoplasmic reticulum (ER), i.e., the spine apparatus, required for local calcium signaling and that is involved in regulating dendritic spine enlargement and synaptic plasticity. Many autism-linked genes have been shown to play critical roles in synaptic formation and plasticity. Among them, KLHL17 is known to control dendritic spine enlargement during development. As a brain-specific disease-associated gene, KLHL17 is expected to play a critical role in the brain, but it has not yet been well characterized. In this study, we report that KLHL17 expression in mice is strongly regulated by neuronal activity and KLHL17 modulates the synaptic distribution of synaptopodin (SYNPO), a marker of the spine apparatus. Both KLHL17 and SYNPO are F-actin-binding proteins linked to autism. SYNPO is known to maintain the structure of the spine apparatus in mature spines and contributes to synaptic plasticity. Our super-resolution imaging using expansion microscopy demonstrates that SYNPO is indeed embedded into the ER network of dendritic spines and that KLHL17 is closely adjacent to the ER/SYNPO complex. Using mouse genetic models, we further show that Klhl17 haploinsufficiency and knockout result in fewer dendritic spines containing ER clusters and an alteration of calcium events at dendritic spines. Accordingly, activity-dependent dendritic spine enlargement and neuronal activation (reflected by extracellular signal-regulated kinase (ERK) phosphorylation and C-FOS expression) are impaired. In addition, we show that the effect of disrupting the KLHL17 and SYNPO association is similar to the results of Klhl17 haploinsufficiency and knockout, further strengthening the evidence that KLHL17 and SYNPO act together to regulate synaptic plasticity. In conclusion, our findings unravel a role for KLHL17 in controlling synaptic plasticity via its regulation of SYNPO and synaptic ER clustering and imply that impaired synaptic plasticity contributes to the etiology of KLHL17-related disorders.

自闭症相关的KLHL17和SYNPO共同控制活动依赖性树突棘增大和棘器。
树突棘是树突中出现的富含肌动蛋白的微小突起,是哺乳动物大脑中控制突触活动和可塑性的兴奋性突触的亚细胞位置。树突棘包含一种特殊形式的内质网(ER),即棘器,是局部钙信号传导所需的,参与调节树突棘增大和突触可塑性。许多与自闭症相关的基因已被证明在突触形成和可塑性中发挥着关键作用。其中,已知KLHL17在发育过程中控制树突棘增大。作为一种脑特异性疾病相关基因,KLHL17有望在大脑中发挥关键作用,但尚未得到很好的表征。在这项研究中,我们报道了KLHL17在小鼠中的表达受到神经元活动的强烈调节,并且KLHL17调节突触足蛋白(SYNPO)的突触分布,SYNPO是脊椎装置的标志物。KLHL17和SYNPO都是与自闭症相关的F-肌动蛋白结合蛋白。已知SYNPO可维持成熟脊柱的脊柱结构,并有助于突触可塑性。我们使用膨胀显微镜进行的超分辨率成像表明,SYNPO确实嵌入了树突棘的ER网络中,并且KLHL17与ER/SYNPO复合物紧密相邻。使用小鼠遗传模型,我们进一步表明,Klhl17单倍型充足和敲除导致含有ER簇的树突棘减少,并改变树突棘处的钙事件。因此,活性依赖性树突棘增大和神经元激活(由细胞外信号调节激酶(ERK)磷酸化和C-FOS表达反映)受损。此外,我们发现破坏KLHL17和SYNPO结合的效果与KLHL17单倍充足和敲除的结果相似,进一步加强了KLHL17与SYNPO共同调节突触可塑性的证据。总之,我们的发现揭示了KLHL17通过调节SYNPO和突触ER簇在控制突触可塑性中的作用,并暗示突触可塑性受损是KLHL17相关疾病的病因之一。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PLoS Biology
PLoS Biology 生物-生化与分子生物学
CiteScore
14.40
自引率
2.00%
发文量
359
审稿时长
3 months
期刊介绍: PLOS Biology is an open-access, peer-reviewed general biology journal published by PLOS, a nonprofit organization of scientists and physicians dedicated to making the world's scientific and medical literature freely accessible. The journal publishes new articles online weekly, with issues compiled and published monthly. ISSN Numbers: eISSN: 1545-7885 ISSN: 1544-9173
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