Tang Pei-Ciao, Um Seyoung, Mayfield Anderson B, Bracho Olena R, Castillo Christian Del, Dinh Christine T, Dykxhoorn Derek M, Liu Xue Zhong
Equal contribution: Pei-Ciao Tang and Seyoung Um.
Lead contact: Pei-Ciao Tang.
bioRxiv. 2024 Sep 26:2024.09.24.614711. doi: 10.1101/2024.09.24.614711.
NF2-Related Schwannomatosis (previously referred to as Neurofibromatosis Type 2, or NF2) is a genetic-associated disease resulting from mutations in the gene, . encodes the merlin protein, which acts as a tumor suppressor. Bilateral vestibular schwannoma (VS) is a hallmark of NF2. Although the exactly molecular mechanism mediating NF2-driven schwannomatosis remain unclear, it is known that defective Merlin protein functionality leads to abnormal cell proliferation. Herein, we utilized a human induced pluripotent stem cell (hiPSC)-based Schwann cell (SC) model to investigate the role of merlin in human SCs. SCs were derived from hiPSCs carrying a mutation (c.191 T > C; p. L64P), its isogenic wild-type control cell line, and a NF2 patient-derived hiPSC line. NF2 mutant SCs showed abnormal cellular morphology and proliferation. Proteomic analyses identified novel interaction partners for Merlin - Arkadia and SKOR2. Our results established a new model in which merlin interacts with Arkadia and SKOR2 and this interaction is required for the proper activation of the SMAD-dependent pathway in TGFβ signaling.
与NF2相关的神经鞘瘤病(以前称为2型神经纤维瘤病,或NF2)是一种由基因 突变引起的遗传相关疾病。 编码默林蛋白,该蛋白起肿瘤抑制作用。双侧前庭神经鞘瘤(VS)是NF2的标志。尽管介导NF2驱动的神经鞘瘤病的确切分子机制尚不清楚,但已知有缺陷的默林蛋白功能会导致细胞异常增殖。在此,我们利用基于人诱导多能干细胞(hiPSC)的雪旺细胞(SC)模型来研究默林在人雪旺细胞中的作用。雪旺细胞来源于携带 突变(c.191 T > C;p.L64P)的hiPSC、其同基因野生型对照细胞系以及一名NF2患者来源的hiPSC系。NF2突变的雪旺细胞表现出异常的细胞形态和增殖。蛋白质组学分析确定了默林的新相互作用伙伴——Arkadia和SKOR2。我们的结果建立了一个新模型,其中默林与Arkadia和SKOR2相互作用,并且这种相互作用是TGFβ信号中SMAD依赖途径正确激活所必需的。
