Homing and Differentiation of Adult Stem Cells to Lung

成体干细胞向肺的归巢和分化

基本信息

批准号：
7098050
负责人：
DARWIN Johnson PROCKOP
金额：
$ 179.57万
依托单位：
TULANE UNIVERSITY OF LOUISIANA
依托单位国家：
美国
项目类别：
财政年份：
2005
资助国家：
美国
起止时间：
2005-07-18 至 2010-05-31
项目状态：
已结题

来源：
https://reporter.nih.gov/project-details/7098050
关键词：
cell differentiation cell migration clinical research interdisciplinary collaboration lung respiratory disease /disorder therapy stem cells

项目摘要

DESCRIPTION (provided by applicant): This application is to foster collaborative research among four groups of investigators at two neighboring institutions that will develop definitive data about the potential usefulness of adult stem cells to treat important pulmonary diseases. The staff includes one group of investigators with expertise in the preparation and characterization of adult stem cells, two groups of investigators with expertise in animal models for diseases such as fibrosis and emphysema, and a fourth group with expertise in the development of viral vectors for correction of the genetic disease cystic fibrosis (CF). The research will focus on the special class of adult stem cells that can be isolated from a patient's own bone marrow and that are referred to as mesenchymal stem cells or marrow stromal cells (MSCs). The program project format will allow the investigators to advance the field by performing collaborative work that cannot be carried out with individual research grants. Three sub-populations of MSCs that are well characterized will be tested in an innovative co-culture system that assays quantitatively their potential for repairing damaged pulmonary cells. We will also explore the possibility that cell fusion may play a role in the repair of pulmonary cells by MSCs. In addition, it will use a new assay for competitive engraftment to determine which sub-population of MSCs engrafts most efficiently in lungs of immunodeficient mice. The three sub-populations of cells will be assayed for engraftment and differentiation in a model for lung damage by asbestos and in a tracheal explant model. The three sub-populations of cells will be tested for their effectiveness in repairing lung damage in an elastase model for emphysema. In addition, we will attempt to define the mechanisms by which MSCs engraft in lung. MSCs from patients with CF will be engineered to correct the gene defect and then tested to determine whether they can become functional ciliated epithelial cells. Of necessity, the investigators will have to quickly share data as their experiment progresses. For example, data will suggest which sub-populations of MSC should be tested in the other three projects. As another example, the experience developed with lentiviruses will make it possible to use viruses for tracking MSCs.

描述（由申请人提供）：该应用程序旨在促进两个邻近机构的四组研究人员之间的合作研究，这些研究人员将开发有关成体干细胞治疗重要肺部疾病的潜在用途的明确数据。工作人员包括一组在成体干细胞制备和表征方面具有专业知识的研究人员，两组在纤维化和肺气肿等疾病动物模型方面具有专业知识的研究人员，以及第四组在开发用于校正的病毒载体方面具有专业知识的研究人员遗传病囊性纤维化（CF）。该研究将重点关注可以从患者自身骨髓中分离出来的特殊类别的成体干细胞，这些细胞被称为间充质干细胞或骨髓基质细胞（MSC）。该计划的项目格式将允许研究人员通过开展单独研究资助无法开展的协作工作来推进该领域的发展。三个经过充分表征的 MSC 亚群将在创新的共培养系统中进行测试，该系统定量分析它们修复受损肺细胞的潜力。我们还将探讨细胞融合在间充质干细胞修复肺细胞中发挥作用的可能性。此外，它将使用一种新的竞争性移植测定法来确定哪些 MSC 亚群在免疫缺陷小鼠的肺部移植最有效。将在石棉肺损伤模型和气管外植体模型中分析这三个细胞亚群的植入和分化。将测试这三个细胞亚群在肺气肿弹性蛋白酶模型中修复肺损伤的有效性。此外，我们将尝试确定间充质干细胞植入肺部的机制。来自 CF 患者的 MSC 将被改造以纠正基因缺陷，然后进行测试以确定它们是否可以成为功能性纤毛上皮细胞。不可避免的是，随着实验的进展，研究人员必须快速共享数据。例如，数据将建议哪些 MSC 亚群应在其他三个项目中进行测试。另一个例子，慢病毒开发的经验将使利用病毒追踪间充质干细胞成为可能。