Retinopathy of prematurity: contribution of inflammatory and genetic factors

被引:0
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作者
Mariza Fevereiro-Martins
Hercília Guimarães
Carlos Marques-Neves
Manuel Bicho
机构
[1] Faculdade de Medicina,Laboratório de Genética and Grupo Ecogenética e Saúde Humana, Instituto de Saúde Ambiental
[2] Universidade de Lisboa,Departamento de Oftalmologia
[3] Instituto de Investigação Científica Bento da Rocha Cabral,Centro de Estudos das Ciências da Visão
[4] Hospital Cuf Descobertas,Departamento de Ginecologia
[5] Faculdade de Medicina, Obstetrícia e Pediatria
[6] Universidade de Lisboa,undefined
[7] Faculdade de Medicina,undefined
[8] Universidade do Porto,undefined
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关键词
Retinopathy of prematurity; Inflammation; Polymorphism; Genetic; Angiogenesis; Preterm infant;
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摘要
Retinopathy of prematurity (ROP) is a retinal vasoproliferative disorder that represents an important cause of childhood visual impairment and blindness. Although oxidative stress has long been implicated in ROP etiology, other prenatal and perinatal factors are also involved. This review focuses on current research involving inflammation and genetic factors in the pathogenesis of ROP. Increasing evidence suggests that perinatal inflammation or infection contributes to ROP pathogenesis. Cytokines and chemokines with a fundamental role in inflammatory responses and that significantly contributing to angiogenesis are analyzed. Microglia cells, the retinal-resident macrophages, are crucial for retinal homeostasis, however, under sustained pathological stimuli release exaggerated amounts of inflammatory mediators and can promote pathological neovascularization. Current modulation of angiogenic cytokines, such as treatment with antibodies to vascular endothelial growth factor (anti-VEGF), has shown efficacy in the treatment of ocular neovascularization; however, some patients are refractory to anti-VEGF agents, suggesting that other angiogenic or anti-angiogenic cytokines need to be identified. Much evidence suggests that genetic factors contribute to the phenotypic variability of ROP. Several studies have implicated the involvement of candidate genes from different signaling pathways in the development of ROP. However, a genetic component with a major impact on ROP has not yet been discovered. Most studies have limitations and did not replicate results. Future research involving bioinformatics, genomics, and proteomics may contribute to finding more genes associated with ROP and may allow discovering better solutions in the management and treatment of ROP.
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页码:1739 / 1763
页数:24
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