Mechanisms of PKG-induced PASMC Differentiation

PKG诱导PASMC分化的机制

• 批准号: 6908451
• 负责人: JESSE D ROBERTS
• 金额: $ 34.96万
• 依托单位: MASSACHUSETTS GENERAL HOSPITAL
• 依托单位国家: 美国
• 财政年份: 2005
• 资助国家: 美国
• 起止时间: 2005-05-01 至 2009-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6908451
• 关键词: apoptosis; cGMP dependent protein kinase; cell differentiation; cell growth regulation; cell proliferation; enzyme activity; genetic regulation; genetically modified animals; immunoprecipitation; laboratory mouse; mitogen activated protein kinase; nitric oxide; phosphorylation; protein protein interaction; protein structure function; pulmonary artery; small interfering RNA; transcription factor; vascular smooth muscle; yeast two hybrid system

DESCRIPTION (provided by applicant): Lung injury causes excessive pulmonary artery smooth muscle cell (PASMC) proliferation in the peripheral arteries of the lung and pulmonary hypertension and significant morbidity in infants and children. Laboratory studies indicate that inhaled nitric oxide (NO) attenuates pulmonary vascular disease in the developing lung. Although the protective mechanisms of NO are incompletely understood, NO regulates PASMC in part by stimulating soluble guanylate cyclase to synthesize cGMP, which stimulates cGMP-dependent protein kinase (PKG). PKG has been observed to induce PASMC differentiation by decreasing cell proliferation, increasing the expression of contractile proteins, and stimulating apoptosis. The BROAD, LONG-TERM OBJECTIVES of this grant proposal are to identify and characterize molecular mechanisms whereby PKG regulates PASMC differentiation. Recently, we identified two novel RING finger proteins, TRIM39R and axotrophin (AXOT), that interact with PKG in a yeast two-hybrid assay. Since PKG and RING finger proteins both regulate cell differentiation, they may share similar signaling pathways and RING finger proteins may mediate many of the cell regulatory activities of PKG. The central hypothesis of the proposal is that PKG regulates PASMC differentiation by interacting with RING finger proteins and regulatory proteins. Specific aim 1 examines how TRIM39R modulates PKG's regulation of PASMC proliferation, differentiation, and apoptosis. Specific aim 2 defines the molecular interaction between PKG and AXOT and defines the role of AXOT in modulating PKG's important non-vasodilatory actions in PASMC. Specific aim 3 utilizes a novel experimental approach to identify new RING finger and transcription regulating proteins phosphorylated by PKG in PASMC, based on their differential phosphorylation in cells. The studies proposed in this grant application will provide important new mechanistic information about how PKG modulates PASMC proliferation, differentiation, and apoptosis. They are likely to provide information that will lead to the development of novel therapeutic targets that can be used to prevent pulmonary vascular disease in the injured lung.

描述（由申请方提供）：肺损伤导致肺外周动脉中的肺动脉平滑肌细胞（PASMC）过度增殖和肺动脉高压，以及婴儿和儿童的显著发病率。实验室研究表明，吸入一氧化氮（NO）减轻肺血管疾病的发展肺。 虽然NO的保护机制还不完全清楚，但NO调节PASMC部分是通过刺激可溶性鸟苷酸环化酶合成cGMP，cGMP刺激cGMP依赖性蛋白激酶（PKG）。已观察到PKG通过降低细胞增殖、增加收缩蛋白的表达和刺激凋亡来诱导PASMC分化。这项拨款提案的广泛、长期的目的是鉴定和表征PKG调节PASMC分化的分子机制。最近，我们确定了两个新的环指蛋白，TRIM39 R和axotrophin（AXOT），与PKG在酵母双杂交试验相互作用。由于PKG和RING指蛋白都调节细胞分化，它们可能共享相似的信号传导途径，并且RING指蛋白可能介导PKG的许多细胞调节活性。该提案的中心假设是PKG通过与RING指蛋白和调节蛋白相互作用来调节PASMC分化。具体目标1检查TRIM39 R如何调节PKG对PASMC增殖、分化和凋亡的调节。具体目标2定义了PKG和AXOT之间的分子相互作用，并定义了AXOT在调节PKG在PASMC中的重要非血管舒张作用中的作用。 具体目标3利用一种新的实验方法，根据其在细胞中的差异磷酸化，鉴定PASMC中PKG磷酸化的新RING指和转录调节蛋白。这项研究将为PKG如何调节PASMC增殖、分化和凋亡提供重要的新机制信息。它们可能提供的信息将导致新的治疗靶点的开发，可用于预防肺血管疾病在受伤的肺。