Genetic modifiers of Duchenne Muscular Dystrophy

杜氏肌营养不良症的遗传修饰

• 批准号: 9057628
• 负责人: KEVIN M FLANIGAN
• 金额: $ 77.48万
• 依托单位: RESEARCH INST NATIONWIDE CHILDREN'S HOSP
• 依托单位国家: 美国
• 财政年份: 2014
• 资助国家: 美国
• 起止时间: 2014-05-15 至 2019-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9057628
• 关键词: 20 year old; Affect; Age; Becker Muscular Dystrophy; Birth; C-terminal; Candidate Disease Gene; Cardiac; Cardiomyopathies; Cessation of life; Chicago; Clinical; Clinical Data; Clinical Trials; Code; Collaborations; Complement; DNA; Data; Data Set; Databases; Diagnosis; Disease; Disease Progression; Duchenne muscular dystrophy; Dystrophin; Enrollment; Europe; Evaluation; Event; Family; Fatty acid glycerol esters; Fibrosis; Funding; Gene Mutation; Gene-Modified; Genes; Genetic; Genetic Polymorphism; Genome; Genomic Segment; Genomics; Goals; Haplotypes; Health; Individual; Life; Link; Maps; Medical Care Costs; Methodology; Mus; Muscle Fibers; Muscular Dystrophies; Mutation; Myopathy; Natural History; Necrosis; Open Reading Frames; Other Genetics; Outcome; Parents; Pathway interactions; Patients; Pediatric Hospitals; Phenotype; Principal Investigator; Proteins; Recontacts; Research; Research Personnel; Resources; Sample Size; Sampling; Severities; Severity of illness; Siblings; Single Nucleotide Polymorphism; Skeletal Muscle; Stratification; Testing; Therapeutic Intervention; Therapeutic Trials; Time; United States National Institutes of Health; Universities; Update; Utah; Variant; Vital capacity; Walking; Work; career; cohort; data archive; density; disability; exome sequencing; gene discovery; genome wide association study; genotyping technology; male; mouse model; muscle strength; next generation; novel; novel therapeutics; opportunity cost; patient stratification; phenotypic data; programs; psychologic; rare variant; socioeconomics; trait; validation studies

DESCRIPTION (provided by applicant): Duchenne muscular dystrophy (DMD) is a degenerative muscle disorder that affects approximately 1:3500 to 1:5200 live male births caused by mutations in the X-linked DMD gene. DMD gene mutations result in absence of the dystrophin protein in muscle fibers, leading to myofiber necrosis, endomysial fibrosis, and fat replacement. It is a devastating disorder, leading to loss of ambulation by age 12, and historically to death by age 20. The psychological and socioeconomic effects on families are enormous; these include but are not limited to the costs of medical care, opportunity costs for career and work, and the psychological toll taken on parents and siblings. Our long-term goal is to understand which genes modify disease progression and severity of DMD. Confirming a hypothesis derived from a genetic modifier of muscular dystrophies in mice, we have recently used data from patients enrolled in the United Dystrophinopathy Project (UDP) to demonstrate that polymorphisms in the LTBP4 gene influence age at loss of ambulation. Our objective in this project is to identify additional genetic modifiers of skeletal muscle, cardiac, and ventilatory function, and our central hypothesis is that such modifiers can be identified by use of the UDP database, a unique resource that contains detailed phenotypic data and archived DNA samples from over 900 DMD patients. Our specific aims are to 1) update and analyze phenotypic data within the UDP cohort, 2) map modifier traits by high-density single nucleotide polymorphism arrays, 3) perform exome sequencing of individuals with extreme outlier phenotypes, and 4) validate newly identified putative genetic modifiers. These aims will be achieved by the combined expertise and efforts from a consortium of researchers at Nationwide Children's Hospital, the University of Utah and UCLA. Collaborators for validating putative modifier genes include investigators at the University of Chicago who have pioneered modifier gene discovery in dystrophic mouse models, and two collaborating networks of investigators in the US and Europe, who have additional natural history cohorts of DMD patients. At the conclusion of these Aims, we will have gained new information about modifier genes associated with the severity and progression of DMD.

描述（由申请人提供）：杜氏肌营养不良症（DMD）是一种退行性肌肉疾病，由X连锁DMD基因突变引起，影响约1：3500至1：5200的活产男婴。DMD基因突变导致肌纤维中肌营养不良蛋白的缺失，导致肌纤维坏死、肌内膜纤维化和脂肪替代。这是一种毁灭性的疾病，导致12岁时失去记忆力，历史上20岁时死亡。对家庭的心理和社会经济影响是巨大的;这些影响包括但不限于医疗保健费用、职业和工作的机会成本以及对父母和兄弟姐妹的心理影响。我们的长期目标是了解哪些基因改变DMD的疾病进展和严重程度。为了证实一个来自小鼠肌营养不良症遗传修饰基因的假设，我们最近使用了来自联合肌营养不良症项目（UDP）患者的数据来证明LTBP 4基因的多态性影响失肌年龄。我们在这个项目中的目标是确定骨骼肌，心脏和排泄功能的其他遗传修饰剂，我们的中心假设是，这些修饰剂可以通过使用UDP数据库来识别，UDP数据库是一个独特的资源，包含详细的表型数据和900多名DMD患者的存档DNA样本。我们的具体目标是：1）更新和分析UDP队列中的表型数据，2）通过高密度单核苷酸多态性阵列绘制修饰子性状，3）对具有极端离群表型的个体进行外显子组测序，以及4）验证新鉴定的推定遗传修饰子。这些目标将通过全国儿童医院、犹他州大学和加州大学洛杉矶分校的研究人员联合起来的专业知识和努力来实现。验证假定修饰基因的合作者包括芝加哥大学的研究人员，他们在营养不良小鼠模型中率先发现了修饰基因，以及美国和欧洲的两个合作研究人员网络，他们有额外的DMD患者自然史队列。在这些目标的结论中，我们将获得与DMD的严重程度和进展相关的修饰基因的新信息。