Muffels Irena J J, Carter Theodore, Rehmann Holger, Vastert Sebastiaan J, Verrijn Stuart Annemarie A, Blank Andreas C, Garde Aurore, van der Zwaag Bert, De Lange Iris M, Giltay Jacques C, van Gassen Koen L I, Koop Klaas, Asensio Cedric S, van Hasselt Peter M
Department of Metabolic Diseases, Wilhelmina Children's Hospital, University Medical Center Utrecht, Utrecht, the Netherlands.
Department of Biological Sciences, College of Natural Sciences and Mathematics, Denver, CO, USA.
iScience. 2025 May 5;28(6):112585. doi: 10.1016/j.isci.2025.112585. eCollection 2025 Jun 20.
LIM kinase 1 (LIMK1) plays a pivotal role in dynamic actin remodeling through phosphorylation of cofilin, thereby regulating exocytosis. We report two individuals harboring variants with dissimilar phenotypes: one exhibited epileptic encephalopathy and developmental delay, while the other showed common variable immune deficiency and glucose dysregulation. We suspected that the divergent phenotypic features arose from opposing effects on LIMK1 activity. Indeed, actin polymerization was significantly decreased in individual 1, whereas it was increased in individual 2. Insulin-secreting cell lines expressing the variant of individual 1 exhibited significantly slower exocytosis, contrasting the rapid and uncontrolled exocytosis in individual 2. Intriguingly, both variants led to increased overall insulin secretion. This first report of two individuals with variants with divergent effects on cofilin phosphorylation and actin polymerization, reveals that LIMK1 has an important role in tuned insulin exocytosis. These distinct exocytosis defects may underlie the glucose dysregulation observed.
LIM激酶1(LIMK1)通过对丝切蛋白进行磷酸化,在动态肌动蛋白重塑中起关键作用,从而调节胞吐作用。我们报告了两名携带不同表型变异体的个体:其中一名表现为癫痫性脑病和发育迟缓,而另一名则表现为常见可变免疫缺陷和葡萄糖调节异常。我们怀疑不同的表型特征源于对LIMK1活性的相反影响。事实上,个体1中的肌动蛋白聚合显著减少,而个体2中的肌动蛋白聚合增加。表达个体1变异体的胰岛素分泌细胞系表现出明显较慢的胞吐作用,这与个体2中快速且不受控制的胞吐作用形成对比。有趣的是,两种变异体均导致总体胰岛素分泌增加。这是首次报道两名携带对丝切蛋白磷酸化和肌动蛋白聚合有不同影响的变异体的个体,揭示了LIMK1在调节胰岛素胞吐作用中具有重要作用。这些明显的胞吐缺陷可能是所观察到的葡萄糖调节异常的基础。
Zotero 插件
