NAA60的同源变异与原发性家族性脑钙化有关。

IF 7.4 1区医学 Q1 CLINICAL NEUROLOGY

Movement Disorders Pub Date : 2024-09-04 DOI:10.1002/mds.30004

Xinhui Chen, Yihua Shi, Feng Fu, Lebo Wang, Hongying Yu, Dehao Yang, Xinchen Wang, Chenxin Ying, Haoyu Wang, Zhiru Lin, Haotian Wang, Fan Zhang, Xiaosheng Zheng, Yuru Guo, Yaoting Wang, YiHeng Zeng, Miao Zhao, Yiling Chen, Jiaxiang Li, Haibin Xia, Jiawen Chen, Bo Wang, Sheng Wu, Fei Xie, Jianhua Feng, Zhidong Cen, Wei Luo

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引用次数: 0

摘要

背景：原发性家族性脑钙化（PFBC）是一种单基因疾病，其特征是大脑双侧钙化。一半以上的 PFBC 患者的遗传基础仍然未知，这表明存在其他新的致病基因。NAA60 是最近报道的 PFBC 的新致病基因：目的：在一个常染色体隐性遗传的 PFBC 家族中确定可能的新型致病基因：我们对一个有 3 个兄弟姐妹被诊断为 PFBC 的中国近亲家庭进行了全面的遗传学研究。我们使用 Western 印迹、免疫荧光和共沉淀等方法评估了可能的新型致病基因变异对蛋白质水平的影响。我们还在基因敲除（KO）细胞系和动物模型中进一步探讨了可能的下游致病机制：结果：我们在 NAA60 中发现了一个 PFBC 共分离同源变异 c.460_461del（p.D154Lfs*113）。功能测试显示，该变体破坏了NAA60蛋白在高尔基体的定位，并加速了蛋白降解。突变的 NAA60 蛋白改变了与 PFBC 相关蛋白 PiT2 和 XPR1 的相互作用，影响了细胞内磷酸盐的平衡。NAA60 KO细胞系的进一步质谱分析表明，多种脑钙化相关蛋白的表达量减少，其中包括叶酸代谢相关蛋白--还原叶酸载体（RFC）：我们的研究证实了NAA60是常染色体隐性遗传性脑钙化症的新型致病基因。NAA60功能缺失不仅破坏了PFBC相关蛋白（如PiT2和XPR1），还破坏了其他多种脑钙化相关膜蛋白底物（如RFC），为PFBC提供了一种新的可能致病机制。© 2024 国际帕金森和运动障碍学会。

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A Homozygous Variant in NAA60 Is Associated with Primary Familial Brain Calcification.

Background: Primary familial brain calcification (PFBC) is a monogenic disorder characterized by bilateral calcifications in the brain. The genetic basis remains unknown in over half of the PFBC patients, indicating the existence of additional novel causative genes. NAA60 was a recently reported novel causative gene for PFBC.

Objective: The aim was to identify the probable novel causative gene in an autosomal recessive inherited PFBC family.

Methods: We performed a comprehensive genetic study on a consanguineous Chinese family with 3 siblings diagnosed with PFBC. We evaluated the effect of the variant in a probable novel causative gene on the protein level using Western blot, immunofluorescence, and coimmunoprecipitation. Possible downstream pathogenic mechanisms were further explored in gene knockout (KO) cell lines and animal models.

Results: We identified a PFBC co-segregated homozygous variant of c.460_461del (p.D154Lfs*113) in NAA60. Functional assays showed that this variant disrupts NAA60 protein localization to Golgi and accelerated protein degradation. The mutant NAA60 protein alters its interaction with the PFBC-related proteins PiT2 and XPR1, affecting intracellular phosphate homeostasis. Further mass spectrometry analysis in NAA60 KO cell lines revealed decreased expression of multiple brain calcification-associated proteins, including reduced folate carrier (RFC), a folate metabolism-related protein.

Conclusions: Our study replicated the identification of NAA60 as a novel causative gene for autosomal recessive PFBC, demonstrating our causative variant leads to NAA60 loss of function. The NAA60 loss of function disrupts not only PFBC-related proteins (eg, PiT2 and XPR1) but also a wide range of other brain calcification-associated membrane protein substrates (eg, RFC), and provided a novel probable pathogenic mechanism for PFBC. © 2024 International Parkinson and Movement Disorder Society.

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来源期刊

Movement Disorders 医学-临床神经学

CiteScore

13.30

自引率

8.10%

发文量

371

审稿时长

12 months

期刊介绍： Movement Disorders publishes a variety of content types including Reviews, Viewpoints, Full Length Articles, Historical Reports, Brief Reports, and Letters. The journal considers original manuscripts on topics related to the diagnosis, therapeutics, pharmacology, biochemistry, physiology, etiology, genetics, and epidemiology of movement disorders. Appropriate topics include Parkinsonism, Chorea, Tremors, Dystonia, Myoclonus, Tics, Tardive Dyskinesia, Spasticity, and Ataxia.