School of Biomedical Sciences, Lo Kwee-Seong Integrated Biomedical Sciences Building, The Chinese University of Hong Kong, Hong Kong, SAR, China.
Department of Obstetrics and Gynaecology, Prince of Wales Hospital, The Chinese University of Hong Kong, Hong Kong, SAR, China.
Autism Res. 2018 Aug;11(8):1098-1109. doi: 10.1002/aur.1950. Epub 2018 Apr 2.
PTEN is a tumor suppressor gene inactivated in over 30% of human cancers. It encodes a lipid phosphatase that serves as a gatekeeper of the phosphoinositide 3-kinase signaling pathway. Germline mutation frequently occurs in this gene in patients diagnosed with PTEN Hamartoma Tumor Syndrome (PHTS). PHTS individuals are characterized by macrocephaly, benign growth of multiple tissues and increased tumor risk. In addition, autistic phenotypes are found in 10-20% of individuals carrying the germline PTEN mutation with macrocephaly. In this report, 13 suspected PHTS patients were screened for mutation in the PTEN gene. A missense variant (c. 302T > C) substituting the isoleucine at codon 101 to a threonine, a single nucleotide insertion (c. 327-328insC) causing a frame shift mutation and termination at codon 109, and a nonsense variant (c. 1003C > T) truncated the protein at codon 335 were identified. The I101T mutation significantly reduced PTEN protein expression levels by 2.5- to 4.0-fold. Mechanistically, I101T reduced the protein half-life of PTEN possibly due to enhanced polyubiquitination at Lysine 13. However, the I101T mutant retained almost 30% of the lipid phosphatase activity of the wild-type protein. Finally, the I101T mutant has reduced phosphorylation at a PTEN auto-dephosphorylation site at Threonine 366 and a lowered ratio of nuclear to cytosolic protein level. These partial losses of multiple PTEN biochemical functions may contribute to the tissue overgrowth and autistic features of this PHTS patient. Autism Res 2018, 11: 1098-1109. © 2018 The Authors Autism Research published by International Society for Autism Research and Wiley Periodicals, Inc. LAY SUMMARY: The genetics of autism spectrum disorders is highly complex with individual risk influenced by both genetic and environmental factors. Mutation in the human PTEN gene confers a high risk of developing autistic behavior. This report revealed that PTEN mutations occurred in 23% of a selected group of Hong Kong patients harboring autistic features with gross overgrowth symptoms. Detailed characterization of a PTEN mutation revealed reduced protein stability as one of the underlying mechanisms responsible for reduced PTEN activity.
PTEN 是一种在超过 30%的人类癌症中失活的肿瘤抑制基因。它编码一种脂质磷酸酶,作为磷酸肌醇 3-激酶信号通路的守门员。在被诊断患有 PTEN 错构瘤肿瘤综合征(PHTS)的患者中,该基因经常发生种系突变。PHTS 个体的特征是大头畸形、多种组织的良性生长和增加的肿瘤风险。此外,携带种系 PTEN 突变和大头畸形的个体中有 10-20% 存在自闭症表型。在本报告中,筛选了 13 名疑似 PHTS 患者的 PTEN 基因突变。发现了一个错义变异(c.302T>C),导致密码子 101 的异亮氨酸替换为苏氨酸,一个单核苷酸插入(c.327-328insC)导致移码突变和密码子 109 处的终止,以及一个无义变异(c.1003C>T)在密码子 335 处截断蛋白。I101T 突变使 PTEN 蛋白表达水平降低 2.5-4.0 倍。机制上,I101T 可能通过增强赖氨酸 13 的多泛素化来降低 PTEN 的蛋白半衰期。然而,I101T 突变体保留了野生型蛋白近 30%的脂质磷酸酶活性。最后,I101T 突变体在 PTEN 自身去磷酸化的 Thr366 位点的磷酸化减少,核蛋白与胞质蛋白水平的比值降低。这些多个 PTEN 生化功能的部分丧失可能导致该 PHTS 患者的组织过度生长和自闭症特征。自闭症研究 2018, 11: 1098-1109。©2018 自闭症研究协会国际协会和 Wiley 期刊出版公司出版。概述:自闭症谱系障碍的遗传学非常复杂,个体风险受遗传和环境因素的共同影响。人类 PTEN 基因突变使自闭症行为的发生风险增加。本报告显示,在香港一组具有过度生长症状和自闭症特征的选定患者中,PTEN 突变的发生率为 23%。对 PTEN 突变的详细特征分析表明,蛋白稳定性降低是导致 PTEN 活性降低的潜在机制之一。
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