Longitudinal SIT Trial Plasma Proteomic Biomarker Discovery and Validation in SCI

SCI 中的纵向 SIT 试验血浆蛋白质组生物标志物的发现和验证

• 批准号: 8005533
• 负责人: James F Casella
• 金额: $ 39.79万
• 依托单位: JOHNS HOPKINS UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2008
• 资助国家: 美国
• 起止时间: 2008-01-15 至 2013-12-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8005533
• 关键词: Age; Aging; Antibodies; Applications Grants; Area; Atherosclerosis; Biological Assay; Biological Markers; Brain; Brain Infarction; Brain Injuries; Brain Ischemia; Cardiovascular system; Cerebral Infarction; Cerebrum; Child; Chronic; Cognitive; Databases; Dementia; Development; Diabetes Mellitus; Diagnostic; Disease; Early treatment; Enrollment; Etiology; Evaluation; Fractionation; Genes; Goals; High Pressure Liquid Chromatography; Hypertension; Individual; Infarction; Infection; Institutes; Lesion; Life; Liquid Chromatography; Magnetic Resonance Imaging; Mass Spectrum Analysis; Migraine; Minority; Modeling; Morbidity - disease rate; Names; National Heart, Lung, and Blood Institute; Participant; Pathologic; Patients; Phase; Phenotype; Pilot Projects; Plasma; Plasma Proteins; Population; Principal Investigator; Proteins; Proteome; Proteomics; Public Health; Randomized; Research; Research Personnel; Resources; Risk; Sampling; Sampling Studies; Sickle Cell Anemia; Stream; Stroke; Structure; Symptoms; Systemic disease; Techniques; Technology; Therapeutic; Time; Transfusion; Treatment Efficacy; Validation; Western Blotting; abstracting; adverse outcome; arm; central nervous system injury; cognitive function; cohort; cost; design; insight; interest; patient population; prognostic; programs; protein expression; protein profiling; response; standard care; success; tv watching

DESCRIPTION (provided by applicant): Silent cerebral infarctions (SCI) occur in 22% of children with sickle cell disease (SCD) and are associated with decreased cognitive function. By definition, these children have MRI and pathologic evidence consistent with brain ischemia or infarction, without symptoms of overt stroke. As the etiology of SCI is unknown, we lack the means to identify children at risk for SCI, institute early therapy, or follow the success of therapy. The overall goal of this grant proposal is to identify diagnostic/prognostic plasma biomarkers of SCI in children ages 5-14 years with SCD. In our pilot studies, using a non-biased proteomic analysis of existing baseline plasma samples at enrollment in the Silent Infarct Transfusion (SIT) Trial from patients with or without SCI, we found differences in the protein profile and the presence of brain specific proteins in plasma of children with SCI. The SIT Trial represents a unique opportunity to: 1) extend these studies to serial plasma samples from study participants, which would be obtained as part of this proposal, but are not presently being obtained as part of the SIT Trial; 2) optimize sample procurement for deep proteomic analysis; and 3) assess biomarkers for prognostic value and therapeutic efficacy. We hypothesize that serial plasma samples optimized for proteomic studies from children with SCD and treated for SCI will contain diagnostic/prognostic biomarkers of SCI and treatment efficacy. The significance of the proposed studies is that identification of circulating markers of SCI could allow early intervention in these children, validate the efficacy of current therapy and provide insight into the design of new therapies. This proposal draws on the unique resources of the ongoing SIT Trial, the large and well phenotyped plasma samples in the SIT Trial Biologic Respository and the NHLBI Cardiovascular Proteomics Center at Johns Hopkins. In Specific Aim I, we will identify plasma biomarkers of SCI and evaluate differences in these biomarkers among 4 groups of patients: SCI patients randomly assigned to chronic transfusion (1) or standard care (2), patients without SCI (3), and patients with recent evidence of ischemic CNS injury (4), using state of the art, non-biased proteomic techniques (protein depletion, HPLC, ITRAQ and LC/MS/MS). In Specific Aim II, we will validate the efficacy of these biomarkers in predicting SCI and therapeutic response, using a combination of traditional western blotting and the development of high throughput multiplex antibody arrays. It is anticipated that these studies will provide new insights into the development of SCI and stroke in SCD and possibly ischemic CNS injury in other susceptible populations. This project has the potential to identify the protein biomarkers for the protection and evaluation of new and progressive silent cerebral infarcts. The identification of such circulating markers of SCI could allow early intervention in children who develop these lesions, help validate the efficacy of current therapy and provide insight into the design of new therapies. While we are studying a selected population of patients with a single gene disorder who develop silent cerebral infarction early in life, these results may generalize to the very large group of older individuals who develop silent cerebral infarctions as a presumed multi-factorial disorder (e.g., atherosclerosis, hypertension, diabetes, migraine, infection, other systemic diseases and aging), often associated with adverse outcomes such as dementia. Thus, the results of these studies could have a great deal of significance for public health in a variety of populations. (End of Abstract)

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