MAGNETIC RESONANCE AND DIFFUSION TENSOR IMAGING OF A MOUSE FASD MODEL U01

小鼠 FASD 模型 U01 的磁共振和扩散张量成像

• 批准号: 7502729
• 负责人: KATHLEEN K SULIK
• 金额: $ 23.42万
• 依托单位: UNIV OF NORTH CAROLINA CHAPEL HILL
• 依托单位国家: 美国
• 财政年份: 2007
• 资助国家: 美国
• 起止时间: 2007-09-30 至 2012-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7502729
• 关键词: 3-Dimensional; A Mouse; Acoustic Nerve; Acute; Address; Adolescent; Adverse effects; Affect; Africa; Alcohol consumption; Alcohol-Related Neurodevelopmental Disorder; Alcohols; Animal Model; Animals; Area; Back; Basic Science; Behavioral; Binding Sites; Biology; Brain; Brain imaging; Cell Death; Cells; Characteristics; Child; Choline; Chronic; Clinical; Clinical Research; Collaborations; Complement; Consult; Craniofacial Abnormalities; Data; Data Files; Data Storage and Retrieval; Databases; Defect; Development; Diagnosis; Diagnostic; Diagnostic tests; Diet; Dietary Intervention; Diffusion Magnetic Resonance Imaging; Dimensions; Disease model; Documentation; Dose; Drug Design; Dysmorphology; Early Diagnosis; Early Intervention; Elements; Embryo; Embryonic Development; Emotional; End Point; Ethanol; Ethnic group; Face; Female; Fertilization; Fetal Alcohol Exposure; Fetal Alcohol Spectrum Disorder; Fetal Alcohol Syndrome; Fetus; Fiber; First Pregnancy Trimester; Fostering; Frequencies; Future; Genetic Polymorphism; Goals; Hearing Tests; Human; Image; Image Analysis; Imagery; Incidence; Indiana; Individual; Infant; Infant Development; Informal Social Control; Informatics; Intervention; Investigation; Knowledge; Laboratories; Laboratory Animals; Labyrinth; Language; Language Development; Life; Liquid substance; Literature; Los Angeles; Machine Learning; Magnetic Resonance; Magnetic Resonance Imaging; Measurement; Measures; Menstruation; Methodology; Methods; Mission; Modeling; Morphology; Moscow; Mothers; Mus; Nasal septum structure; Neonatal; Neural Cell Adhesion Molecule L1; Neuraxis; Neurobiology; New Mexico; Optic Nerve; Optics; Outcome; Partner in relationship; Pattern; Performance; Personal Satisfaction; Phenotype; Photography; Pilot Projects; Play; Population; Pregnancy; Prevention; Principal Investigator; Prosencephalon; Public Health; Publishing; Range; Rattus; Recording of previous events; Reproduction; Request for Applications; Research; Research Design; Research Personnel; Research Project Grants; Resolution; Resources; Retrieval; Role; Scanning; Schools; Screening procedure; Sensitivity and Specificity; Severities; Sheep; Signal Pathway; Signal Transduction; Site; Specificity; Specimen; Staging; Structure; Sum; Supplementation; System; Technology; Testing; Therapeutic; Three-Dimensional Image; Three-Dimensional Imaging; Time; Toddler; Ukraine; Ultrasonography; Universities; Week; Woman; Work; alcohol effect; alcohol exposure; alcohol sensitivity; analog; base; brain behavior; brain morphology; cognitive control; computer generated; craniofacial; critical developmental period; data integration; day; design; dosage; drinking; fetal; follow-up; high throughput screening; human data; human study; human subject; improved; in utero; infancy; interest; intraperitoneal; literacy; malformation; member; membranous labyrinth; mouse model; multidisciplinary; neurobehavioral; northern plains; novel; prenatal; prenatal exposure; programs; prospective; reconstruction; response; sensory system; size; social; symposium; three dimensional structure

DESCRIPTION (provided by applicant): Fetal Alcohol Spectrum Disorders (FASD), significant components of which are Central Nervous System (CMS) and craniofacial abnormalities, are a major public health problem. While eliminating FASD is the ultimate goal for both clinical and basic FASD research, we recognize that in the near future, adverse effects from prenatal ethanol exposure will persist. To better diagnose and treat affected individuals, a more complete understanding of the full spectrum of the ethanol-induced abnormalities is needed. The proposed investigations are designed to integrate with those of other consortium members in meeting this need. For this work, both high resolution Magnetic Resonance Imaging (MRI), which can provide 29 micron (or less) isotropic scans and subsequent accurate 3-D reconstructions and segmental analyses, and Diffusion Tensor Imaging (DTI), which allows CMS fiber tract analyses, will be applied to the study of an FASD mouse model. Previous research utilizing this model has established critical exposure times that yield facial and CNS abnormalities that are consistent with full-blown Fetal Alcohol Syndrome, as well as other components of FASD. The proposed studies will employ this model and both acute and chronic ethanol treatment paradigms to test the overall hypothesis that in mice, ethanol induces structural abnormalities of the brain and face that are consistent with and informative for those in human FASD. To this end, utilizing MRI and DTI as high throughput screening platforms, we propose to address the following specific aims : 1) to provide comprehensive documentation and discovery of the ethanol-induced CNS dysmorphology that results from prenatal ethanol exposure at embryonic and early fetal stages of development; 2) to define the facial dysmorphology that results from prenatal ethanol exposure during embryonic and/or early fetal stages and to relate their character and severity to accompanying abnormalities of the brain; and 3) to identify regions other than the brain or face that may serve as diagnostic indicators of prenatal ethanol exposure. The results of the proposed studies will be compared to those of corresponding investigations by other consortium members. It is expected that the structural abnormalities of the brain and face that are induced by ethanol in mice will reflect the pattern of defects observed in children with FASD, will inform human diagnostic tests, and will provide new information that will be helpful in reducing the incidence of FASD.

描述（由申请人提供）：胎儿酒精谱系障碍（FASD），其重要组成部分是中枢神经系统（CMS）和颅面异常，是一个主要的公共卫生问题。虽然消除 FASD 是 FASD 临床和基础研究的最终目标，但我们认识到，在不久的将来，产前乙醇暴露带来的不利影响将持续存在。为了更好地诊断和治疗受影响的个体，需要更全面地了解乙醇引起的异常的全部范围。拟议的调查旨在与其他联盟成员的调查相结合，以满足这一需求。在这项工作中，高分辨率磁共振成像 (MRI)（可提供 29 微米（或更小）的各向同性扫描以及随后的精确 3-D 重建和分段分析）和扩散张量成像 (DTI)（可进行 CMS 纤维束分析）将应用于 FASD 小鼠模型的研究。先前利用该模型的研究已经确定了导致面部和中枢神经系统异常的关键暴露时间，这些异常与成熟的胎儿酒精综合症以及 FASD 的其他组成部分一致。拟议的研究将采用该模型以及急性和慢性乙醇治疗范例来检验总体假设，即在小鼠中，乙醇会引起大脑和面部的结构异常，这与人类 FASD 的异常一致并提供信息。为此，利用 MRI 和 DTI 作为高通量筛查平台，我们建议实现以下具体目标：1）提供全面的记录和发现乙醇诱导的中枢神经系统畸形，该畸形是由于胚胎和胎儿发育早期阶段的产前乙醇暴露所致； 2) 定义因胚胎和/或胎儿早期阶段产前乙醇暴露而导致的面部畸形，并将其特征和严重程度与伴随的大脑异常联系起来； 3) 识别大脑或面部以外的区域，这些区域可以作为产前乙醇暴露的诊断指标。拟议研究的结果将与其他联盟成员的相应调查结果进行比较。预计乙醇在小鼠体内引起的大脑和面部结构异常将反映在 FASD 儿童中观察到的缺陷模式，将为人类诊断测试提供信息，并提供有助于降低 FASD 发病率的新信息。