导致 HbSC 视网膜病变的分子机制可能取决于血管生成相关基因 ROBO1 和 SLC38A5 的作用

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
S. M. da Silva Costa, M. T. Ito, Pedro Rodrigues Sousa da Cruz, B. B. de Souza, V. M. Rios, V. D. H. E. Bertozzo, Ana Carolina Lima Camargo, M. Viturino, C. Lanaro, D. M. de Albuquerque, Amanda M. do Canto, Sara Teresinha Olalla Saad, Stephanie Ospina-Prieto, M. Ozelo, F. F. Costa, M. B. de Melo
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引用次数: 0

摘要

增殖性镰状细胞性视网膜病变(HbSC)是镰状细胞病的一种不太严重的形式,它对视网膜的影响更为频繁,患者发生增殖性视网膜病变的几率更高,可发展为视力丧失。本研究旨在确定与增殖性镰状细胞视网膜病变(PSCR)病理生理学相关的内皮细胞衍生分子的表达差异。研究人员利用 RNAseq 比较了镰状细胞血红蛋白病和增殖性视网膜病变患者(5 人)与无视网膜病变的镰状细胞患者(3 人)的循环内皮集落形成细胞的基因表达谱。实时聚合酶链反应(qRT-PCR)用于验证 RNAseq 结果。共发现 134 个差异表达基因(DEGs)。DEGs主要与血管扩张、I型干扰素信号转导、先天免疫和血管生成有关。在已发现的 DEGs 中,我们特别强调了上调最多的基因 ROBO1(log2FoldChange = 4.32,FDR = 1.35E-11)和 SLC38A5(log2FoldChange = 3.36,FDR = 1.59E-07)。ROBO1是一种轴突引导的受体,能促进内皮细胞迁移,有助于视网膜血管生成和病理性眼部新生血管的发展。内皮细胞 SLC38A5 是一种氨基酸(AA)转运体,它通过控制 AA 营养物质的摄取来调节发育期和病理性视网膜血管生成,AA 营养物质可作为内皮细胞(ECs)增殖的代谢燃料,从而促进血管生成。我们的数据为阐明 PSCR 的分子病理生理学迈出了重要一步,这可能解释了血红蛋白病个体间眼部表现的差异,并为抑制病理性血管生成的新替代策略提供了启示。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The molecular mechanism responsible for HbSC retinopathy may depend on the action of the angiogenesis-related genes ROBO1 and SLC38A5
HbSC disease, a less severe form of sickle cell disease, affects the retina more frequently and patients have higher rates of proliferative retinopathy that can progress to vision loss. This study aimed to identify differences in the expression of endothelial cell-derived molecules associated with the pathophysiology of proliferative sickle cell retinopathy (PSCR). RNAseq was used to compare the gene expression profile of circulating endothelial colony-forming cells from patients with SC hemoglobinopathy and proliferative retinopathy (n = 5), versus SC patients without retinopathy (n = 3). Real-time polymerase chain reaction (qRT-PCR) was used to validate the RNAseq results. A total of 134 differentially expressed genes (DEGs) were found. DEGs were mainly associated with vasodilatation, type I interferon signaling, innate immunity and angiogenesis. Among the DEGs identified, we highlight the most up-regulated genes ROBO1 (log2FoldChange = 4.32, FDR = 1.35E-11) and SLC38A5 (log2FoldChange = 3.36 FDR = 1.59E-07). ROBO1, an axon-guided receptor, promotes endothelial cell migration and contributes to the development of retinal angiogenesis and pathological ocular neovascularization. Endothelial SLC38A5, an amino acid (AA) transporter, regulates developmental and pathological retinal angiogenesis by controlling the uptake of AA nutrient, which may serve as metabolic fuel for the proliferation of endothelial cells (ECs) and consequent promotion of angiogenesis. Our data provide an important step towards elucidating the molecular pathophysiology of PSCR that may explain the differences in ocular manifestations between individuals with hemoglobinopathies and afford insights for new alternative strategies to inhibit pathological angiogenesis.
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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