Selective Targeting of Phosphodiesterase 11A Transcription and Catalytic Activit

磷酸二酯酶 11A 转录和催化活性的选择性靶向

• 批准号: 9061733
• 负责人: Eugenia V Broude
• 金额: $ 22.4万
• 依托单位: UNIVERSITY OF SOUTH CAROLINA AT COLUMBIA
• 依托单位国家: 美国
• 资助国家: 美国
• 起止时间: 至
• 项目状态: 未结题
• 来源: https://reporter.nih.gov/project-details/9061733
• 关键词: Adrenal Glands; Adult; Adverse effects; Affect; Affective; Aging; Alzheimer' s Disease; Behavior; Behavioral; Binding; Biochemical; Biological Assay; Bipolar Disorder; Brain; Brain region; Cell Line; Cells; Cerebellum; Chemicals; Cognitive; Corpus striatum structure; Cyclic AMP; Cyclic GMP; Cyclic Nucleotides; Development; Diagnostic; Disease; Ectopic Expression; Enzymes; Exhibits; Family; Fluorescence Polarization; Foundations; Functional disorder; Genetic Transcription; Genomics; Hippocampal Formation; Hippocampus (Brain); Human; In Situ Hybridization; Knock-out; Knockout Mice; Lead; Lentivirus Vector; Major Depressive Disorder; Maps; Measures; Mental disorders; Molecular; Mus; Pathology; Patients; Pattern; Positron-Emission Tomography; Proteins; Rattus; Reporter; Rodent; Schizophrenia; Series; Signal Transduction; Signaling Molecule; Symptoms; Testing; Therapeutic; Therapeutic Effect; Tissues; Transcription Coactivator; aging brain; base; cis acting element; design; genetic regulatory protein; improved; in vivo; insight; mRNA Expression; neuropathology; neuropsychiatric disorder; neuropsychiatry; phosphodiesterase 11a; phosphoric diester hydrolase; promoter; protein expression; restoration; small hairpin RNA; small molecule; social stress; targeted treatment; therapeutic development

Project 3. Cyclic nucleotides (cAMP and cGMP) are intracellular signaling molecules that are critical for the development and function ofthe brain. Deficits in cAMP/cGMP signaling have been repeatedly measured in patients with Alzheimer's disease and schizophrenia. Dysfunction ofthe hippocampus (HIPP) - a brain region that modulates affective, social, stress-related, and cognitive behaviors - has also been repeatedly implicated in these neuropsychiatric diseases. We believe that selectively restoring cyclic nucleotide signaling in the HIPP of patients, without affecting signaling in normal brain regions, would relieve neuropsychiatric disease-related symptoms without causing unwanted side effects. Phosphodiesterase 11A (PDE11A) is an enzyme that breaks down both cAMP and cGMP. We have recently discovered that PDE11A is almost exclusively localized to the HIPP. Thus, we hypothesize that cAMP/cGMP signaling in the HIPP can be selectively targeted by modulating PDE11A expression and/or function. Adult PDE11A knockout (KO) mice exhibit biochemical, anatomical, and behavioral deficits that are consistent with HIPP dysfunction and neuropsychiatric disease. This suggests that augmentation of PDE11A function may prove therapeutic. To increase function of a particular enzyme, we can increase either its availability (i.e., expression) or its catalytic activity. As such, we propose a series of aims designed to understand the molecular mechanisms controlling transcription and catalytic activity of PDE11 A. In Specific Aim 1, we will determine if psychiatric disease is associated with changes in PDE11A transcription in brain and if cis-acting elements within the promoter of PDE11A are sufficient to restrict PDE11A mRNA expression to the HIPP in the healthy adult brain. In Specific Aim 2, we will identify the signaling cascades and trans-acting proteins that control PDE11A promoter activity. In Specific Aim 3, we will develop small molecule PDE11A activators and test them in PDE11A wild-type and KO mice (KOs = negative controls) using a neuropsychiatric battery that assesses efficacy and side effect liability. PDE11A may be capable of selectively restoring cAMP and cGMP signaling in a specific brain region impacted by disease, without affecting signaling elsewhere.

项目3。环核苷酸（cAMP和cGMP）是细胞内的信号分子，对脑的发育和功能至关重要。在阿尔茨海默病和精神分裂症患者中反复测量cAMP/cGMP信号传导的缺陷。海马体功能障碍（HIPP）--一个调节情感、社会、压力相关和认知行为的大脑区域--也一再被认为与这些神经精神疾病有关。我们相信，选择性地恢复患者HIPP中的环核苷酸信号传导，而不影响正常大脑区域中的信号传导，将缓解神经精神疾病相关症状，而不会引起不必要的副作用。磷酸二酯酶11 A（PDE 11 A）是一种分解cAMP和cGMP的酶。我们最近发现PDE 11 A几乎完全定位于HIPP。因此，我们假设HIPP中的cAMP/cGMP信号可以通过调节PDE 11 A表达和/或功能来选择性靶向。成年PDE 11 A敲除（KO）小鼠表现出与HIPP功能障碍和神经精神疾病一致的生化、解剖和行为缺陷。这表明PDE 11 A功能的增强可以证明是治疗性的。为了增加特定酶的功能，我们可以增加其可用性（即，表达）或其催化活性。因此，我们提出了一系列旨在了解控制PDE 11 A转录和催化活性的分子机制的目标。在具体目标1中，我们将确定精神疾病是否与脑中PDE 11 A转录的变化相关，以及PDE 11 A启动子内的顺式作用元件是否足以限制健康成人脑中PDE 11 A mRNA表达至HIPP。在具体目标2中，我们将确定控制PDE 11 A启动子活性的信号级联和反式作用蛋白。在具体目标3中，我们将开发小分子PDE 11 A激活剂，并使用评估疗效和副作用倾向的神经精神成套试验在PDE 11 A野生型和KO小鼠（科斯=阴性对照）中对其进行测试。PDE 11 A可能能够选择性地恢复受疾病影响的特定脑区域中的cAMP和cGMP信号传导，而不影响其他地方的信号传导。