LIM Homeodomain Factors and Pituitary Gene Expression

LIM 同源域因子和垂体基因表达

• 批准号: 7191650
• 负责人: RICHARD A MAURER
• 金额: $ 33.65万
• 依托单位: OREGON HEALTH & SCIENCE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-03-01 至 2009-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7191650
• 关键词: Address; Adult; Affinity; Alleles; Anabolism; Binding; Cells; Complex; DNA; Defect; Development; Drosophila genus; Elements; Gene Expression; Gene Targeting; Genes; Genetic Screening; Genetic Transcription; Glycoproteins; Goals; Gonadotropins; Hormones; Individual; LIM Domain; Laboratories; Maps; Mediating; Modeling; Mus; Mutation; Neuraxis; Other Finding; Phosphorylation; Pituitary Gland; Play; Population; Preparation; Role; Site; Specificity; Testing; Thyrotropin; Transcriptional Activation; adapter protein; alpha Subunit Glycoprotein Hormones; cofactor; dimer; genetic manipulation; homeodomain; in vivo; insight; nervous system development; protein function; response; transcription factor

The overall goal is to understand the roles that specific LIM homeodomain (Lhx) transcription factors play in expression of the glycoprotein hormone subunit genes in thyrotropes and gonadotropes of the pituitary and to determine the mechanism of action of Lhx factors. We have shown that Lhx2 and Lhx3 can interact with a specific DNA element designated the PGBE to activate transcription of the glycoprotein hormone alpha-subunit gene. These findings raise the possibility that Lhx2 and Lhx3 may play an interchangeable role in regulating alpha-subunit gene expression. However, recent findings from this and other laboratories suggest specificity in Lhx factor action. We have recently performed a mutational study that offers evidence for distinct mechanisms mediating transcriptional responses to Lhx2 and Lhx3. The possibility of distinct actions of individual Lhx factors is consistent with recent studies of the role of specific Lhx factors in central nervous system development. Although the Lhx2 and Lhx3 genes have been disrupted in mice, the genetic manipulations result in developmental defects so that adult populations of pituitary cells are not available. To address these issues and explore the mechanism of Lhx factor action the specific aims include: 1) Map the site of GnRH-induced phosphorylation of Lhx2 and Lhx3 and evaluate the function of this phosphorylation. The possibility of GnRH-induced phosphorylation of SLB will also be evaluated. 2) Use a genetic screen to identify mutations that disrupt the interaction between Lhx3 and the putative adapter/coactivator, SLB, to examine structurefunction relationships for this complex in alpha-subunit gene expression. 3) Directly test the requirement for Lhx2, Lhx3 and SLB for alpha-subunit gene expression in vivo. 4) Search for Lhx2 and Lhx3 target genes. These studies should define the role of specific Lhx factors in gonadotropin and thyrotropin biosynthesis as well as provide new insights into more general issues about specificity and mechanisms mediating Lhx actions to regulate gene expression and development.

总的目标是了解特定的LIM同源结构域(LHX)转录因子在垂体促甲状腺激素和促性腺激素的糖蛋白激素亚单位基因表达中所起的作用，并确定LHX因子的作用机制。我们已经证明，LHX2和Lhx3可以与一种称为PGBE的特定DNA元件相互作用，激活糖蛋白激素α亚单位基因的转录。这些发现提出了LHX2和Lhx3可能在调节阿尔法亚单位基因表达方面发挥互换作用的可能性。然而，来自该实验室和其他实验室的最新发现表明，lhx因子的作用具有特异性。我们最近进行了一项突变研究，为调节LHX2和Lhx3转录反应的不同机制提供了证据。单个lhx因子发挥不同作用的可能性与最近关于特定lhx因子在中枢神经系统发育中的作用的研究一致。虽然LHX2和Lhx3基因已经在小鼠身上被破坏，但遗传操作会导致发育缺陷，因此无法获得成年群体的垂体细胞。为了解决这些问题并探索Lhx因子的作用机制，具体目的包括：1)定位GnRH诱导的LHX2和Lhx3的磷酸化位置，并评价这种磷酸化的功能。GnRH诱导SLB磷酸化的可能性也将被评估。2)使用基因筛查来确定破坏Lhx3与可能的接头/辅活化子SLB之间相互作用的突变，以检查该复合体在阿尔法亚单位基因表达中的结构-功能关系。3)在体内直接检测LHX2、LHX3和SLB对α亚基基因表达的要求。4)寻找LHX2和Lhx3靶基因。这些研究应该明确特定的lhx因子在促性腺激素和促甲状腺激素生物合成中的作用。 并为更一般的问题提供了新的见解，这些问题涉及调节LHX调控基因表达和发育的特异性和机制。