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Differentiation of Exudative Age-related Macular Degeneration and Polypoidal Choroidal Vasculopathy.

机译:渗出性年龄相关性黄斑变性和息肉样脉络膜血管病的鉴别。

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摘要

Age-related macular degeneration (AMD) is the leading cause of irreversible blindness for the elderly in developed countries. Its exudative subtype accounts for more than 80% of severe visual loss or legal blindness in AMD patients regardless of modified lifestyle and therapeutic treatments. Polypoidal choroidal vasculopathy (PCV) is a macular disorder characterized by typical polypoidal lesions on fundus angiography and sharing similar phenotype with exudative AMD. PCV was suggested as a distinct disease from exudative AMD based on different clinical features in ophthalmic imaging. Furthermore, PCV patients tend to be younger and more prevalent in Asian, and have different responses to photo-dynamic therapy and anti-vascular endothelial growth factor treatments, compared to exudative AMD patients. However, it has also been suggested that PCV could be a subtype of exudative AMD mainly because of their common genetic and environmental factors. Therefore, genetic differentiation between exudtive AMD and PCV might assist clinicians to determine the condition.;The complement factor H (CFH) gene, and age-related maculopathy susceptibility 2 (ARMS2)/high temperature requirement factor A1 (HTRA1) locus have been mapped for AMD by genome-wide association studies (GWAS) and subsequent molecular investigations. The formyl peptide receptor 1 (FPR1) gene, which mediates trafficking and activation of phagocytic leukocytes, is related to the AMD-associated inflammatory condition. This thesis aims to evaluate FPR1 as a novel disease gene for exudative AMD and PCV, to compare the genetic profiles of ARMS2, HTRA1, CFH, and FPR1 in exudative AMD and PCV, to investigate the correlation of ARMS2/HTRA1 genotypes with disease phenotypes, and to differentiate these two disorders through the genomic compositions.;Case-control association studies were conducted on ARMS2, HTRA1, CFH and FPR1 in exudative AMD and PCV patients of our Hong Kong Chinese cohort using polymerase chain reaction and direct sequencing. We observed different genotypic distributions (p < 0.05), association patterns and effect sizes between these two diseases.;This thesis attempts to dissect the genetic profiles of exudative AMD and PCV. Results in this thesis suggest FPR1 as a novel candidate gene for exudative AMD and PCV, reveal a significant and consistent association of ARMS2, HTRA1, CFH and FPR1 with both exudative AMD and PCV, provide evidences for genetic differentiation of these two disorders, demonstrate a significant correlation between ARMS2/HTRA1 genotypes and response to treatment, and indicate different influence of smoking in exudative AMD and PCV. However, definite differentiation between exudative AMD and PCV was limited because of the same trend of associations between these two disorders. Therefore, replication studies in other ethnic populations are necessary, and identification of PCV-specific genes/polymorphisms could further differentiate PCV from exudative AMD. (Abstract shortened by UMI.).
机译:与年龄有关的黄斑变性(AMD)是发达国家老年人不可逆性失明的主要原因。无论改变生活方式和治疗方法,其渗出亚型占AMD患者严重视力丧失或法盲的80%以上。息肉样脉络膜血管病(PCV)是一种黄斑疾病,其特征在于眼底血管造影上典型的息肉样病变,并且与渗出性AMD具有相似的表型。根据眼科影像学的不同临床特征,认为PCV是与渗出性AMD截然不同的疾病。此外,与渗出性AMD患者相比,PCV患者在亚洲更年轻,更普遍,并且对光动力疗法和抗血管内皮生长因子疗法的反应不同。但是,也有人提出PCV可能是渗出性AMD的一种亚型,主要是因为它们具有共同的遗传和环境因素。因此,渗出性AMD和PCV之间的遗传分化可能有助于临床医生确定病情。已经绘制了补体因子H(CFH)基因和年龄相关性黄斑病变易感性2(ARMS2)/高温需求因子A1(HTRA1)基因座通过全基因组关联研究(GWAS)和随后的分子研究对AMD进行研究。甲酰基肽受体1(FPR1)基因介导吞噬白细胞的运输和激活,与AMD相关的炎症有关。本文旨在评估FPR1作为渗出性AMD和PCV的新型疾病基因,以比较渗出性AMD和PCV中ARMS2,HTRA1,CFH和FPR1的遗传特征,研究ARMS2 / HTRA1基因型与疾病表型的相关性,并通过基因组组成区分这两种疾病。用聚合酶链反应和直接测序法对香港华裔队列性渗出性AMD和PCV患者的ARMS2,HTRA1,CFH和FPR1进行了病例对照关联研究。我们观察到了这两种疾病之间不同的基因型分布(p <0.05),关联模式和效应大小。;本论文试图剖析渗出性AMD和PCV的遗传特征。本论文的结果表明,FPR1是渗出性AMD和PCV的新候选基因,揭示了ARMS2,HTRA1,CFH和FPR1与渗出性AMD和PCV显着且一致的关联,为这两种疾病的遗传分化提供了证据,证明了ARMS2 / HTRA1基因型与治疗反应之间存在显着相关性,表明吸烟对渗出性AMD和PCV的影响不同。但是,由于这两种疾病之间的关联趋势相同,所以渗出性AMD与PCV之间的明确区分受到限制。因此,有必要在其他种族中进行复制研究,并且鉴定PCV特异性基因/多态性可以进一步将PCV与渗出性AMD区别开来。 (摘要由UMI缩短。)。

著录项

  • 作者

    Liang, Xiaoying.;

  • 作者单位

    The Chinese University of Hong Kong (Hong Kong).;

  • 授予单位 The Chinese University of Hong Kong (Hong Kong).;
  • 学科 Health Sciences Ophthalmology.;Biology Genetics.
  • 学位 Ph.D.
  • 年度 2012
  • 页码 171 p.
  • 总页数 171
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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