Basic mechanisms in arteriovenous fistula maturation for hemodialysis
血液透析动静脉内瘘成熟的基本机制
基本信息
- 批准号:8143186
- 负责人:
- 金额:--
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2011
- 资助国家:美国
- 起止时间:2011-10-01 至 2014-09-30
- 项目状态:已结题
- 来源:
- 关键词:AdhesionsAffectAnimal ModelAreaArteriovenous fistulaBiological AssayBiological MarkersBiometryBloodBlood CellsBlood Flow VelocityBlood VesselsBlood flowCaringCase Report FormCathetersCell AdhesionCell Adhesion MoleculesCell CommunicationCellsClinical TrialsCoupledDataDiabetes MellitusDialysis patientsDialysis procedureDoctor of PhilosophyEnd stage renal failureEndothelial CellsEnvironmentEpidemicFailureFellowshipFistulaForearmFoundationsFunctional disorderGelatinasesGoalsGrantGrowthGrowth FactorGuidelinesHemodialysisHumanHyperplasiaHypertensionIncidenceInfectionInfiltrationInflammatoryInjuryInterventionKidneyKidney DiseasesKidney FailureLeadLeukocytesMaintenanceManuscriptsMatrix MetalloproteinasesMeasurementMedicalMedical centerMolecularMolecular TargetMultivariate AnalysisNational Research Service AwardsObesityOperative Surgical ProceduresOutcomePathologicPathologyPatient CarePatientsPeer ReviewPermeabilityPopulationPrevalenceProceduresProcessProductionProteinsPublicationsPublishingRegulationRepeat SurgeryResearchResearch TrainingResistanceRisk FactorsRoleStenosisSurgeonSurgical InjuriesSurvival AnalysisTechniquesTestingThickThrombosisTraining ProgramsUltrasonographyUnited States Centers for Medicare and Medicaid ServicesUnited States National Institutes of HealthVascular remodelingVeinsVenousVeteransWestern BlottingWorkabstractingbasecareercostcytokineelectric impedanceimprovedinsightinterestintima mediamigrationmonocytemortalitynovel diagnosticsperipheral bloodresponseshear stressstemsuccesstooltranslational approachvascular inflammation
项目摘要
DESCRIPTION (provided by applicant):
Project Summary/Abstract NOMINEE: This proposal describes a three year training program to develop a candidate's academic career in Vascular Surgery centered at a VA medical center. The candidate spent 3 years in formal research training at the Minneapolis VA with an NIH F32 NRSA fellowship grant working on intimal hyperplasia, a pathologic form of vascular remodeling after surgical injury. From the fellowship, the candidate published 15 peer-reviewed publications, 8 as first author and 6 directly related to the NRSA project. The fellowship led to the successful defense of a PhD thesis. The candidate has continued his research interests through a translational approach to vascular remodeling assessing the mechanisms of vein remodeling after arteriovenous fistula (AVF) construction for renal failure patients. In the past year, the candidate has published 3 peer-reviewed manuscripts related to this area, 1 as first author. HYPOTHESIS: The candidate plans to test the hypothesis that monocyte-endothelial cell adhesion followed by transmigration induces endothelial barrier injury and impairs Matrix Metalloproteinase (MMP) production and activity, leading to the failure of AVF maturation. SPECIFIC OBJECTIVES: (1) To evaluate the biomarker role of MMPs and monocyte adhesion molecules in the blood and vein segment of hemodialysis patients for predicting AVF maturation. (2) To investigate the molecular mechanisms of monocyte-endothelial cell interactions in endothelial barrier dysfunction and MMP dysregulation, leading to fistula failure. RELEVANCE: A vascular procedure where failure is more common (30-60% failure rate) than success is the surgical construction of a mature autogenous AVF for hemodialysis access. This project emphasizes the interactive roles of blood cells and endothelial cells in vascular injury, with a practical view on the identification of new diagnostic tools and molecular targets for improved AVF outcome. SUBJECT POPULATION: All Veteran patients with renal insufficiency or renal failure. PROCEDURES TO BE USED: Molecular analyses will be performed in vein segments and blood from patients undergoing hemodialysis access surgery. The following experimental procedures will be used to test the stated hypothesis: 7 Isolation and purification of monocyte isolation from peripheral blood. 7 Gelatinase zymography and Western immunoblot quantification of protein (MMPs) expression. 7 Flow cytometric measurement of adhesion molecules 7 Electric Cell-substrate Impedance Sensing (ECIS) technique 7 Transwell assays of monocyte transendothelial migration and endothelial permeability 7 Biostatistics: Multivariate analysis and survival analysis (vein maturation and duration) 7 Patient management and case report form management. SIGNIFICANCE OF POTENTIAL NEW FINDINGS: Important insight can be gained in describing the mechanism for vein remodeling after AVF construction. If reliable biomarkers can be developed, certain patients could potentially be selected for alternative hemodialysis access such as a primary bridge graft. Furthermore, greater insight into the mechanism could lead to clinical trials evaluating medical therapies that decrease monocyte-endothelial cell interactions, such as statins. If successful, maturation rates for AVF would improve and the need for repeat surgery minimized.
描述(由申请人提供):
项目摘要/摘要提名者:该提案描述了一项为期三年的培训计划,旨在发展候选人在以退伍军人管理局医疗中心为中心的血管外科学术生涯。该候选人在明尼阿波利斯退伍军人管理局接受了 3 年的正式研究培训,并获得了 NIH F32 NRSA 奖学金,研究内膜增生(手术损伤后血管重塑的一种病理形式)。通过该奖学金,该候选人发表了 15 篇同行评审出版物,其中 8 篇作为第一作者,6 篇与 NRSA 项目直接相关。该奖学金促成了博士论文的成功答辩。该候选人通过血管重塑的转化方法继续他的研究兴趣,评估肾衰竭患者动静脉瘘(AVF)构建后静脉重塑的机制。在过去的一年里,候选人发表了3篇与该领域相关的同行评审论文,其中1篇作为第一作者。假设:候选人计划检验以下假设:单核细胞-内皮细胞粘附和迁移会诱导内皮屏障损伤并损害基质金属蛋白酶 (MMP) 的产生和活性,从而导致 AVF 成熟失败。具体目标:(1)评估血液透析患者血液和静脉段中MMP和单核细胞粘附分子对预测AVF成熟的生物标志物作用。 (2)探讨单核细胞-内皮细胞相互作用导致内皮屏障功能障碍和MMP失调导致内瘘失败的分子机制。相关性:失败比成功更常见(失败率 30-60%)的血管手术是通过外科手术构建成熟的自体 AVF 以进行血液透析通路。该项目强调血细胞和内皮细胞在血管损伤中的相互作用,并以实用的观点来确定新的诊断工具和分子靶点以改善 AVF 的结果。受试者人群:所有患有肾功能不全或肾衰竭的退伍军人患者。使用的程序:将对接受血液透析通路手术的患者的静脉段和血液进行分子分析。以下实验程序将用于检验所述假设: 7 从外周血中分离和纯化单核细胞。图 7 蛋白质 (MMP) 表达的明胶酶酶谱和蛋白质免疫印迹定量。 7 粘附分子的流式细胞术测量 7 电细胞基质阻抗传感 (ECIS) 技术 7 单核细胞跨内皮迁移和内皮通透性的 Transwell 测定 7 生物统计学:多变量分析和生存分析(静脉成熟度和持续时间) 7 患者管理和病例报告表管理。潜在新发现的意义:在描述 AVF 构建后静脉重塑的机制方面可以获得重要的见解。如果能够开发出可靠的生物标志物,某些患者可能会被选择进行替代性血液透析,例如初次桥接移植。此外,对该机制的更深入了解可能会导致临床试验评估减少单核细胞与内皮细胞相互作用的药物疗法,例如他汀类药物。如果成功,AVF 的成熟率将会提高,并且重复手术的需要将降至最低。
项目成果
期刊论文数量(0)
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Eugene Sangkeu Lee其他文献
Eugene Sangkeu Lee的其他文献
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{{ truncateString('Eugene Sangkeu Lee', 18)}}的其他基金
Basic mechanisms in arteriovenous fistula maturation for hemodialysis
血液透析动静脉内瘘成熟的基本机制
- 批准号:
8391101 - 财政年份:2011
- 资助金额:
-- - 项目类别:
Basic mechanisms in arteriovenous fistula maturation for hemodialysis
血液透析动静脉内瘘成熟的基本机制
- 批准号:
8595287 - 财政年份:2011
- 资助金额:
-- - 项目类别:
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