Assembly, dynamics and evolution of cell-cell and cell-matrix adhesions

细胞-细胞和细胞-基质粘附的组装、动力学和进化

基本信息

批准号：
8814966
负责人：
ROBERT Colin LIDDINGTON
金额：
$ 7.49万
依托单位：
SANFORD BURNHAM PREBYS MEDICAL DISCOVERY INSTITUTE
依托单位国家：
美国
项目类别：
财政年份：
2010
资助国家：
美国
起止时间：
2010-09-30 至 2015-06-30
项目状态：
已结题

来源：
https://reporter.nih.gov/project-details/8814966
关键词：
Actins Adhesions Affinity Area Binding Biochemistry Biological Cadherins Cell Adhesion Cell Shape Cell membrane Cell-Matrix Junction Cells Cellular biology Chemistry Complex Crystallization Cytoskeleton Defect Development Disease Electron Microscopy Environment Evolution Extracellular Matrix Face Gene Expression Genetic Genomics Goals Health Hereditary Disease Homeostasis Human Image Analysis In Situ In Vitro Individual Integrins Intermediate Filaments Life Link Location Malignant Neoplasms Maps Membrane Methods Microtubules Modeling Nature Normal Cell Normal tissue morphology Organ Output Phospholipids Phosphorylation Physiological Protein Analysis Protein Family Protein Structure Initiative Proteins Research Personnel Role Signal Transduction Signaling Protein Solutions Structure Techniques Tertiary Protein Structure Time X-Ray Crystallography body system cell motility cellular imaging new therapeutic target prevent programs protein complex protein protein interaction receptor reconstitution research study sensor stoichiometry structural biology tomography tool development

项目摘要

DESCRIPTION (provided by applicant): Cell adhesion complexes are a bio-medically important class of multi-protein assemblies. They are involved in sensing Interactions between cells and their external environment, and then initiating and regulating intracellular signals that control cell migration, cell shape and functional organization, proliferation and survival, and gene expression. They are evolutionarily old, critical for normal development and homeostasis, and are defective in genetic diseases and cancer. Currently, there is a lack of a concerted effort to integrate available genomic (evolutionary) and structural information to rigorously solve the hierarchical structural organization of these multi-protein complexes at the atomic, meso and macro scale. A further barrier to progress is the availability of large amounts of purified proteins for multi-protein complex reconstitution since classical approaches are not feasible due to the unstable nature of complex protein assemblies. The Consortium will leverage high-throughput expression and structures of large sets of target families of proteins and signaling networks to understand the structural and functional organization of both cell-cell and cell-ECM adhesion complexes. The Consortium will integrate expertise in structural biology (X-ray crystallography, electron microscopy of in situ complexes), biochemistry and cell biology (in vitro reconstitution), chemistry and live cell imaging (in situ bio-sensors and caged proteins) by: Specific Aim 1: Define multi-protein interactions, stoichiometries and affinities in solution (Liddington, Weis). Specific Aim 2: Reconstitute multi-protein complexes on biological membranes (Ginsberg, Nelson). Specific Aim 3: Define structures of multi-protein complexes in situ, at a physiological environment (Hanein, Volkmann). Specific Aim 4: Analyze dynamic protein-protein interactions and assembly in live cells (Hahn).

描述（由申请人提供）：细胞粘附复合物是生物医学上重要的一类多蛋白组装体。它们参与感知细胞与其外部环境之间的相互作用，然后启动和调节控制细胞迁移、细胞形状和功能组织、增殖和存活以及基因表达的细胞内信号。它们在进化上很古老，对正常发育和体内平衡至关重要，并且在遗传疾病和癌症中存在缺陷。目前，缺乏协调一致的努力来整合可用的基因组（进化）和结构信息，以严格解决这些多蛋白质复合物在原子、介观和宏观尺度上的层次结构组织。进展的另一个障碍是可用于多蛋白复合物重建的大量纯化蛋白，因为由于复杂蛋白组装体的不稳定性质，经典方法不可行。该联盟将利用大量目标蛋白质家族和信号网络的高通量表达和结构来了解细胞-细胞和细胞-ECM 粘附复合物的结构和功能组织。该联盟将整合结构生物学（X射线晶体学、原位复合物电子显微镜）、生物化学和细胞生物学（体外重构）、化学和活细胞成像（原位生物传感器和笼状蛋白）：具体目标 1：定义溶液中的多蛋白质相互作用、化学计量和亲和力（Liddington、Weis）。具体目标 2：在生物膜上重建多蛋白复合物（Ginsberg、Nelson）。具体目标 3：在生理环境中原位定义多蛋白复合物的结构（Hanein、Volkmann）。具体目标 4：分析活细胞中的动态蛋白质-蛋白质相互作用和组装 (Hahn)。