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首页> 外文期刊>Investigative ophthalmology & visual science >Proteomic Analysis of Embryonic and Young Human Vitreous
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Proteomic Analysis of Embryonic and Young Human Vitreous

机译:胚胎和年轻玻璃体的蛋白质组学分析

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Purpose: The proteomic profile of vitreous from second-trimester human embryos and young adults was characterized using mass spectrometry and analyzed for changes in protein levels that may relate to structural changes occurring during this time. This vitreous proteome was compared to previous reports to confirm proteins already identified and reveal novel ones. Methods: Vitreous from 17 human embryos aged 14 to 20 weeks gestation (WG) and from a 12-, a 14-, a 15-, and a 28-year-old was individually analyzed using tandem mass spectrometrya??based proteomics. Peptide spectral count associations with embryonic age were assessed using a general linear model of fold changes and Spearman's rank correlation. Differences between embryonic and young adult vitreous proteomes were also compared. Immunohistochemistry was used to evaluate three proteins in five additional fetal (10a??18 WG) human eyes. Results: There were 1217 proteins identified in fetal and young adult human vitreous, 206 after quantile normalization and variance filtering. In embryos, the peptide counts of 37 proteins changed significantly from 14 to 20 WG: 75.7% increased, 24.3% decreased. Immunohistochemistry confirmed the absence of clusterin and cadherin in 10 and 14 WG eyes and their presence at 18 WG. Comparing embryonic to young adult vitreous, 47 proteins were significantly higher or lower. A total of 768 proteins not previously identified in the literature are presented. Conclusions: Proteins previously unreported in the human vitreous were identified. The human vitreous proteome undergoes significant changes during embryogenesis and young adulthood. A number of protein levels change considerably during the second trimester, with the majority decreasing.
机译:目的:使用质谱仪对来自孕中期人胚胎和年轻成年人的玻璃体的蛋白质组学特征进行表征,并分析可能与此期间发生的结构变化有关的蛋白质水平变化。将该玻璃体蛋白质组与以前的报道进行了比较,以确认已经鉴定出的蛋白质并揭示出新的蛋白质。方法:使用基于串联质谱的蛋白质组学技术,分别分析了17个年龄在14至20周(WG),12岁,14岁,15岁和28岁的人类胚胎的玻璃体。使用倍数变化和Spearman秩相关的通用线性模型评估了肽谱数与胚胎年龄的关系。还比较了胚胎和年轻成人的玻璃体蛋白质组之间的差异。免疫组织化学用于评估另外五只胎儿(10a ?? 18 WG)人眼中的三种蛋白质。结果:经分位数归一化和方差过滤后,在胎儿和年轻成人玻璃体中鉴定出1217种蛋白质,其中206种。在胚胎中,37种蛋白质的肽数从14 WG显着变化为20 WG:增加了75.7%,减少了24.3%。免疫组织化学证实,在10和14 WG的眼中不存在簇蛋白和钙黏着蛋白,而在18 WG的眼中则存在。与胚胎和年轻成人玻璃体相比,有47种蛋白质明显更高或更低。总共提供了768种蛋白质,以前在文献中未发现。结论:鉴定出先前未在人玻璃体内报道的蛋白质。人类玻璃体蛋白质组在胚胎发生和成年后会发生重大变化。在孕中期,许多蛋白质水平发生了很大变化,而大多数蛋白质水平下降。

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