Abnormal vascular repair in lupus: a link to premature atherosclerosis

狼疮血管修复异常：与过早动脉粥样硬化的联系

• 批准号: 8284343
• 负责人: Mariana J Kaplan
• 金额: $ 37.43万
• 依托单位: UNIVERSITY OF MICHIGAN AT ANN ARBOR
• 依托单位国家: 美国
• 财政年份: 2009
• 资助国家: 美国
• 起止时间: 2009-08-01 至 2013-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8284343
• 关键词: Accounting; Affect; Animal Model; Apoptosis; Area; Atherosclerosis; Blood Vessels; Bone Marrow; Cardiovascular Diseases; Cardiovascular system; Cell Count; Cells; Characteristics; Complication; Data; Development; Disease; Endothelial Cells; Endothelium; Equilibrium; Event; Functional disorder; Generations; Genes; Health; Human; Immune; In Vitro; Incidence; Inflammatory Infiltrate; Interferon Type I; Interferons; Knockout Mice; Lead; Link; Lupus; Maintenance; Medial; Michigan; Microarray Analysis; Modeling; Molecular; Mus; Outcome; Pathogenesis; Pathway interactions; Patients; Phenotype; Play; Prevention; Recombinant Interferon; Risk; Risk Factors; Role; Secondary to; Serum; Severities; Stem cells; Structure; System; Systemic Lupus Erythematosus; Testing; Therapeutic Intervention; Thick; Thromboplastin; Universities; Work; atherogenesis; cell injury; cohort; coronary artery calcification; cytokine; design; improved; in vivo; interest; intima media; mortality; patient population; premature; premature atherosclerosis; prevent; repaired; therapy design; treatment strategy; vascular endothelial dysfunction; vasculogenesis

DESCRIPTION (provided by applicant): Systemic lupus erythematosus (SLE) is associated with up to a 50-fold increase in the incidence of cardiovascular (CV) events secondary to premature atherosclerosis. Framingham risk factors do not account for this increased propensity and the exact responsible mechanisms remain uncharacterized. We have recently proposed that accelerated CV damage in SLE is due to an imbalance of endothelial cell damage (apoptosis) and repair. We hypothesize that type I interferons (IFNs) play a crucial role in the induction of abnormal vascular repair in SLE and, potentially in the development of vascular damage and premature atherosclerosis in this disease. SPECIFIC AIMS: 1. Characterize the role of type I IFNs on endothelial dysfunction, vascular repair and atherosclerosis development in lupus murine systems. This will be tested by comparing the murine lupus model NZM2328 with the same strain crossed to type I IFNR knock-out (KO) mice (NZM2318/IFNRKO). Endothelium-dependent and independent vascular function and development of arterial inflammatory infiltrates will be evaluated in these mice. Whether administration of recombinant IFN-1 accelerates endothelial dysfunction and promotes atherosclerosis in NZM2328 mice will also be evaluated. 2. Characterize the angiogenenic pathways affected by type I IFNs in murine SLE. The role of type I IFNs on phenotype and function of endothelial progenitor cells (EPCs) will be studied by comparing vasculogenesis in vitro and in vivo on NZM2318 and NZM2318/IFNRKO mice. This will be performed by quantifying EPCs, assessing their capacity to become mature ECs, form and incorporate into vascular structures, and synthesize proangiogenic factors. Microarray analysis will assess the EPC genes affected by type I IFNs in NZM2328 and NZM2318/IFNRKO in specific cellular compartments. Vascular repair molecular pathways that are affected by type I IFNs will be identified. 3. Characterize the role of type I IFNs in endothelial dysfunction and atherosclerosis risk in SLE. The University of Michigan has established a Cardiovascular Lupus Cohort which follows SLE patients prospectively to examine functional, anatomical, cellular and soluble markers of vascular damage and atherosclerotic risk, and the development of CV events. To assess the role of type I IFNs in the development of premature CVD in SLE, the association of type I IFN signatures and IFN-1 expression with endothelial function (FMD/NMD), carotid intimal medial thickness (CIMT), coronary calcification, serum and cellular markers of vascular damage/ repair will be established in this cohort. PUBLIC HEALTH RELEVANCE: The results from this study will characterize mechanisms that promote early cardiovascular disease in patients with lupus and could contribute to the design of therapeutic interventions aimed at decreasing the risk of this potentially fatal complication.

描述（由申请人提供）：系统性红斑狼疮（SLE）与继发于过早动脉粥样硬化的心血管（CV）事件发生率增加高达50倍相关。弗雷明汉风险因素不能解释这种增加的倾向，确切的负责机制仍未确定。我们最近提出SLE中加速的CV损伤是由于内皮细胞损伤（凋亡）和修复的不平衡。我们假设I型干扰素（ifn）在SLE的异常血管修复诱导中发挥关键作用，并可能在该疾病的血管损伤和过早动脉粥样硬化的发展中发挥关键作用。具体目标：1；表征I型ifn在狼疮小鼠系统内皮功能障碍、血管修复和动脉粥样硬化发展中的作用。这将通过将小鼠狼疮模型NZM2328与与I型IFNR敲除（KO）小鼠（NZM2318/IFNRKO）杂交的相同菌株进行比较来进行测试。内皮依赖和独立血管功能和动脉炎症浸润的发展将在这些小鼠中进行评估。我们还将评估重组IFN-1是否会加速NZM2328小鼠内皮功能障碍并促进动脉粥样硬化。2. 表征受I型ifn影响的小鼠SLE血管生成途径。通过比较NZM2318和NZM2318/IFNRKO小鼠体外和体内血管生成，研究I型IFNs对内皮祖细胞（EPCs）表型和功能的作用。这将通过量化内皮细胞、评估其成为成熟内皮细胞、形成并融入血管结构以及合成促血管生成因子的能力来实现。微阵列分析将评估特定细胞区室中NZM2328和NZM2318/IFNRKO中I型IFNs影响的EPC基因。将确定受I型ifn影响的血管修复分子途径。3. 描述I型干扰素在SLE患者内皮功能障碍和动脉粥样硬化风险中的作用。密歇根大学建立了一个心血管狼疮队列，对SLE患者进行前瞻性随访，以检查血管损伤和动脉粥样硬化风险的功能、解剖、细胞和可溶性标志物，以及心血管事件的发展。为了评估I型IFN在SLE早期CVD发展中的作用，将在本队列中建立I型IFN特征和IFN-1表达与内皮功能（FMD/NMD）、颈动脉内膜内侧厚度（CIMT）、冠状动脉钙化、血管损伤/修复的血清和细胞标志物的关联。公共卫生相关性：本研究的结果将描述狼疮患者早期心血管疾病的机制，并有助于设计旨在降低这一潜在致命并发症风险的治疗干预措施。