Department of Neuromuscular Diseases, UCL Queen Square Institute of Neurology, London, WC1N 3BG, UK.
Neurobiology and Medical Genetics Laboratory, "Nicolae Testemitanu" State University of Medicine and Pharmacy, 165, Stefan cel Mare si Sfant Boulevard, MD, 2004, Chisinau, Republic of Moldova.
Nat Commun. 2024 Mar 13;15(1):2269. doi: 10.1038/s41467-024-46354-0.
Primary familial brain calcification (PFBC) is characterized by calcium deposition in the brain, causing progressive movement disorders, psychiatric symptoms, and cognitive decline. PFBC is a heterogeneous disorder currently linked to variants in six different genes, but most patients remain genetically undiagnosed. Here, we identify biallelic NAA60 variants in ten individuals from seven families with autosomal recessive PFBC. The NAA60 variants lead to loss-of-function with lack of protein N-terminal (Nt)-acetylation activity. We show that the phosphate importer SLC20A2 is a substrate of NAA60 in vitro. In cells, loss of NAA60 caused reduced surface levels of SLC20A2 and a reduction in extracellular phosphate uptake. This study establishes NAA60 as a causal gene for PFBC, provides a possible biochemical explanation of its disease-causing mechanisms and underscores NAA60-mediated Nt-acetylation of transmembrane proteins as a fundamental process for healthy neurobiological functioning.
原发性家族性脑钙化为一种大脑钙沉积的疾病,导致进行性运动障碍、精神症状和认知能力下降。原发性家族性脑钙化是一种异质性疾病,目前与六个不同基因的变异有关,但大多数患者的遗传诊断仍然未知。在这里,我们在七个常染色体隐性遗传的原发性家族性脑钙化的家庭的十名个体中鉴定出 NAA60 的双等位基因变异。NAA60 变异导致缺乏功能,缺乏蛋白质 N 端(Nt)乙酰化活性。我们表明,磷酸载体 SLC20A2 是体外 NAA60 的底物。在细胞中,NAA60 的缺失导致 SLC20A2 的表面水平降低和细胞外磷酸盐摄取减少。这项研究将 NAA60 确立为原发性家族性脑钙化的致病基因,为其致病机制提供了可能的生化解释,并强调了 NAA60 介导的跨膜蛋白 Nt 乙酰化作为健康神经生物学功能的基本过程。
