DNA Hypomethylation and Cortical Neuronal Degeneration

DNA 低甲基化和皮质神经元变性

• 批准号: 7026994
• 负责人: Guoping Fan
• 金额: $ 34.89万
• 依托单位: UNIVERSITY OF CALIFORNIA LOS ANGELES
• 依托单位国家: 美国
• 财政年份: 2005
• 资助国家: 美国
• 起止时间: 2005-03-15 至 2010-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7026994
• 关键词: DNA methylation; behavior; behavior disorders; behavior test; cell differentiation; cell morphology; cell proliferation; cellular pathology; cerebral cortex; developmental genetics; developmental neurobiology; gene expression; genetic models; genetically modified animals; hippocampus; histology; laboratory mouse; molecular pathology; neural degeneration; neurogenetics; neurons; neuropathology; p53 gene /protein; phenotype; tissue /cell culture

DESCRIPTION (provided by applicant): In mammals DNA cytosine methylation is one of the major epigenetic factors that regulate many cellular events including developmental gene expression and genomic imprinting. Alternations in DNA methylation machinery have been linked to several mental retardation disorders, including Rett, ICF, Fragile-X, and ATRX syndromes, suggesting that methylation is important for neuronal development and function. To investigate the function of DNA methylation in the central nervous system (CNS), we have recently applied the cre/loxP system to delete the maintenance DNA methyltransferase Dnmtl gene exclusively in the CNS. By crossing the Emx1-cre transgene with the Dnmtl conditional allele (Dnmt2lox), we have obtained conditional knockout mice with Dnmtl deficiency restricted to the cortex and hippocampus. Emx1-cre mediated Dnmtl gene deletion is initiated in pallial cortical precursor cells at embryonic day (E) 9-10, resulting in DNA hypomethylation in embryonic and postnatal cortical projection neurons. Mutant mice are viable in adulthood but exhibit obvious behavioral defects such as hyperactivity and hind limb clasping upon tail suspension. Morphological studies indicate that Emx1-cre; Dnmtl mutant mice exhibit massive loss of cortical volume, thus become a valuable animal model for studying the effect of DNA hypomethylation on cortical degeneration. In this proposal, we plan to first examine the time course of cortical neuronal cell death and determine the gross histological and behavioral defects in the mutant mice. Further experiments are designed to determine the effect of DNA hypomethylation on the proliferation and differentiation of precursor cells, as well as dendritic arborization of Dnmtl-/- neurons. Finally, we plan to determine the mechanism by which DNA hypomethylation induces neuronal cell death in the mutant cortex. It is known that levels of DNA methylation decrease with aging and in age-related neurodegenerative disorders such as Alzheimer's disease. Understanding the mechanism of cell death in hypomethylated cortical neurons may help us develop therapeutic strategies to prevent hypomethylation-induced neuronal degeneration.

描述（由申请人提供）：在哺乳动物中，DNA 胞嘧啶甲基化是调节许多细胞事件（包括发育基因表达和基因组印记）的主要表观遗传因素之一。 DNA 甲基化机制的改变与多种精神发育迟滞疾病有关，包括 Rett、ICF、Fragile-X 和 ATRX 综合征，这表明甲基化对于神经元发育和功能很重要。为了研究中枢神经系统（CNS）中DNA甲基化的功能，我们最近应用cre/loxP系统删除了CNS中专门的维持DNA甲基转移酶Dnmtl基因。通过将 Emx1-cre 转基因与 Dnmtl 条件等位基因 (Dnmt2lox) 杂交，我们获得了仅限于皮质和海马的 Dnmtl 缺陷的条件敲除小鼠。 Emx1-cre 介导的 Dnmtl 基因缺失在胚胎第 9-10 天在大脑皮层皮质前体细胞中启动，导致胚胎和出生后皮质投射神经元中 DNA 低甲基化。突变小鼠在成年后仍能存活，但表现出明显的行为缺陷，如多动症和悬尾时后肢紧握。形态学研究表明 Emx1-cre； Dnmtl突变小鼠表现出皮质体积的大量损失，因此成为研究DNA低甲基化对皮质变性影响的有价值的动物模型。在本提案中，我们计划首先检查皮质神经元细胞死亡的时间过程，并确定突变小鼠的总体组织学和行为缺陷。进一步的实验旨在确定 DNA 低甲基化对前体细胞增殖和分化以及 Dnmtl-/- 神经元树突状树枝化的影响。最后，我们计划确定 DNA 低甲基化诱导突变皮层神经元细胞死亡的机制。众所周知，DNA 甲基化水平会随着衰老以及与年龄相关的神经退行性疾病（例如阿尔茨海默病）而降低。了解低甲基化皮质神经元细胞死亡的机制可能有助于我们制定治疗策略来预防低甲基化诱导的神经元变性。