Genetic Studies of POAG in Ghana, West Africa

西非加纳的 POAG 遗传学研究

• 批准号: 6804091
• 负责人: Robert RAND ALLINGHAM
• 金额: $ 15.4万
• 依托单位: DUKE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2003
• 资助国家: 美国
• 起止时间: 2003-09-30 至 2006-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6804091
• 关键词: African; clinical research; disease /disorder etiology; family genetics; genetic disorder; genetic registry /resource /referral center; genetic screening; genetic susceptibility; glaucoma; health disparity; human subject; linkage mapping; medically underserved population; molecular biology information system; parents; phenotype; quantitative trait loci; siblings; single nucleotide polymorphism; urban poverty area

DESCRIPTION (provided by applicant): Primary Open Angle Glaucoma (POAG) is the leading cause of blindness among African Americans living in the United States. Within this patient population, it has a prevalence that is 4-6 times greater, clinically more severe, and more likely to lead to blindness than in white Americans. The objective of this research is to determine the genetic basis of this complex inherited disease. With this vital information, future methods of diagnosis, treatment and possible prevention will be elucidated. POAG is highly prevalent and is a leading cause of blindness in West Africa. A large portion of the African American population living in the United States has its origins in West Africa. The study of genetics of POAG in the West African population offers several advantages to similar studies being conducted in the United States. Glaucoma is highly prevalent in West Africa and POAG is the dominant form. Families are larger in West Africa are mobile. These qualities greatly assist identifying and then locating families and family members that meet study criteria. Disease phenotype is generally more severe, at least in part due to shortages in health care delivery. Therefore, families with multiple affected members are more common, a critical element for any genetic study. Finally, the populations on West Africa are more homogeneous than similar populations in the U.S. and elsewhere. There has been very little population emigration to Ghana or West Africa thus resulting in reduced genetic admixture. Genetic admixture is very common in the U.S. and elsewhere. This is very important since greater genetic homogeneity increases the power to detect and identify genetic sources of inherited diseases. The specific aims of this study are to 1) screen glaucoma patient populations in Ghana, West Africa and identify 150 discordant sib pairs with POAG and 2) create a West African POAG clinical and DNA association dataset to evaluate current and future candidate loci for POAG. Candidate genes within regions that demonstrate association will be screened using SNP and gene sequencing strategies. The clinical and genetic dataset created by proposal will be invaluable for future investigations of glaucoma in this population. This dataset can also serve as a foundation for genetic linkage dataset for genome-wide screen to identify new candidate genes and loci in this important population.

描述(申请人提供)：原发性开角型青光眼(POAG)是居住在美国的非裔美国人致盲的主要原因。在这些患者中，它的患病率是美国白人的4-6倍，临床上更严重，更有可能导致失明。这项研究的目的是确定这种复杂遗传病的遗传基础。有了这些重要的信息，未来的诊断、治疗和可能的预防方法将被阐明。开角型青光眼非常普遍，是西非失明的主要原因。居住在美国的非洲裔美国人有很大一部分起源于西非。与美国正在进行的类似研究相比，在西非人群中进行的POAG遗传学研究具有几个优势。青光眼在西非非常普遍，POAG是主要形式。在西非，家庭规模更大，而且是流动的。这些素质极大地有助于识别和定位符合研究标准的家庭和家庭成员。疾病表型通常更严重，至少部分原因是卫生保健服务短缺。因此，有多个受影响成员的家庭更为常见，这是任何基因研究的关键因素。最后，西非的人口比美国和其他地方的类似人口更同质化。移民到加纳或西非的人口很少，因此减少了遗传混合。基因混合在美国和其他地方很常见。这一点非常重要，因为更大的遗传同质性增加了检测和识别遗传性疾病的遗传源的能力。这项研究的具体目标是1)在加纳和西非筛选青光眼患者群体，并确定150对与POAG不一致的同胞对；2)创建西非POAG临床和DNA关联数据集，以评估当前和未来POAG的候选基因座。将使用SNP和基因测序策略筛选显示关联的区域内的候选基因。Proposal创建的临床和基因数据集将对未来该人群中青光眼的研究具有无价的价值。该数据集也可以作为全基因组筛选的遗传连锁数据集的基础，以在这个重要的群体中识别新的候选基因和基因座。