SPARK Program Scholar, Institute for Regenerative Cures, University of California, Sacramento, CA 95817, USA.
Stem Cell Program, UC Davis School of Medicine. The University of California, Sacramento, CA 95817, USA.
Int J Mol Sci. 2020 Feb 14;21(4):1286. doi: 10.3390/ijms21041286.
Protein Phosphatase 2 Regulatory Subunit B' Delta ()-related intellectual disability (ID) and neurodevelopmental delay results from germline de novo mutations in the gene. This gene encodes the protein PPP2R5D (also known as the B56 delta subunit), which is an isoform of the subunit family B56 of the enzyme serine/threonine-protein phosphatase 2A (PP2A). Clinical signs include intellectual disability (ID); autism spectrum disorder (ASD); epilepsy; speech problems; behavioral challenges; and ophthalmologic, skeletal, endocrine, cardiac, and genital malformations. The association of defective PP2A activity in the brain with a wide range of severity of ID, along with its role in ASD, Alzheimer's disease, and Parkinson's-like symptoms, have recently generated the impetus for further research into mutations within this gene. PP2A, together with protein phosphatase 1 (PP1), accounts for more than 90% of all phospho-serine/threonine dephosphorylations in different tissues. The specificity for a wide variety of substrates is determined through nearly 100 different PP2A holoenzymes that are formed by at least 23 types of regulatory B subunits, and two isoforms each of the catalytic subunit C and the structural subunit A. In the mammalian brain, PP2A-mediated protein dephosphorylation plays an important role in learning and memory. The PPP2R5D subunit is highly expressed in the brain and the PPP2A-PPP2R5D holoenzyme plays an important role in maintaining neurons and regulating neuronal signaling. From 2015 to 2017, 25 individuals with -related developmental disorder were diagnosed. Since then, Whole-Exome Sequencing (WES) has helped to identify more unrelated individuals clinically diagnosed with a neurodevelopmental disorder with pathological variants of . In this review, we discuss the current understanding of the clinical and genetic aspects of the disorder in the context of the known functions of the PP2A-PPP2R5D holoenzyme in the brain, as well as the pathogenic mutations in that lead to deficient PP2A-PPP2R5D dephosphorylation and their implications during development and in the etiology of autism, Parkinson's disease, Alzheimer's disease, and so forth. In the future, tools such as transgenic animals carrying pathogenic PPP2R5D mutations, and patient-derived induced pluripotent stem cell lines need to be developed in order to fully understand the effects of these mutations on different neural cell types.
蛋白磷酸酶 2 调节亚基 B'Delta()相关的智力障碍 (ID) 和神经发育迟缓是由该基因的种系从头突变引起的。该基因编码蛋白 PPP2R5D(也称为 B56 delta 亚基),它是丝氨酸/苏氨酸蛋白磷酸酶 2A (PP2A) 酶的亚基家族 B56 的同工型。临床特征包括智力障碍 (ID)、自闭症谱系障碍 (ASD)、癫痫、言语问题、行为挑战以及眼科、骨骼、内分泌、心脏和生殖畸形。大脑中 PP2A 活性缺陷与 ID 严重程度的广泛范围相关,以及其在 ASD、阿尔茨海默病和帕金森样症状中的作用,最近促使人们进一步研究该基因内的突变。PP2A 与蛋白磷酸酶 1 (PP1) 一起,占不同组织中所有磷酸丝氨酸/苏氨酸去磷酸化的 90%以上。通过至少 23 种不同的调节亚基 B 和每个催化亚基 C 和结构亚基 A 的两种同工型形成的近 100 种不同的 PP2A 全酶决定了对各种底物的特异性。在哺乳动物大脑中,PP2A 介导的蛋白去磷酸化在学习和记忆中起重要作用。PPP2R5D 亚基在大脑中高度表达,PP2A-PPP2R5D 全酶在维持神经元和调节神经元信号转导方面发挥重要作用。自 2015 年至 2017 年,共诊断出 25 名与相关发育障碍的个体。此后,全外显子组测序 (WES) 帮助鉴定了更多与神经发育障碍无关的个体,这些个体的临床诊断具有病理性变体。在本综述中,我们讨论了在已知的大脑中 PP2A-PPP2R5D 全酶的功能背景下,以及导致 PP2A-PPP2R5D 去磷酸化缺陷的致病性突变的情况下,该疾病的临床和遗传方面的最新认识及其在自闭症、帕金森病、阿尔茨海默病等疾病的发病机制中的意义。将来,需要开发携带致病性 PPP2R5D 突变的转基因动物和患者来源的诱导多能干细胞系等工具,以便充分了解这些突变对不同神经细胞类型的影响。
