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首页> 美国卫生研究院文献>Frontiers in Medicine >In silico Analysis of Gamma-Secretase-Complex Mutations in Hidradenitis Suppurativa Demonstrates Disease-Specific Substrate Recognition and Cleavage Alterations
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In silico Analysis of Gamma-Secretase-Complex Mutations in Hidradenitis Suppurativa Demonstrates Disease-Specific Substrate Recognition and Cleavage Alterations

机译:在化脓性汗腺炎中γ分泌酶复合突变的计算机分析表明特定疾病的基质识别和分裂改变。

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>Background: Familial Hidradenitis Suppurativa and Familial Alzheimer's Disease are both associated with Gamma-Secretase Complex mutations; however, the two diseases are not epidemiologically associated. Understanding the molecular differences between the two diseases may aid in the development of hypotheses for differing pathogenesis and ultimately, targets for detection.>Aims: To characterize the in silico structural and functional alterations to the Gamma Secretase Complex in documented mutations in Familial Hidradenitis Suppurativa, along with comparison of downstream substrate recognition and cleavage.>Methods: In silico analysis of publicly available genomic data, assessment of protein structure and binding affinity using Swiss-model and Dynamut was undertaken. Differential Expression was expressed using Log Fold Change using the general framework for linear models in R. Differentially expressed genes (DEGs) were defined by FCH ≥1.5 or ≤−1.5 and false discovery rate (FDR ≤ 0.05).>Results: Twenty three of 39 mutations in HS are degraded via nonsense mediated decay with altered substrate and binding affinity of substrates identified in the remaining mutations. Significant differential expression of ErbB4, SCNB1, and Tie1 in lesional skin was specific to Hidradenitis Suppurativa and EphB2, EPHB4, KCNE1, LRP6, MUSK, SDC3, Sortilin1 in blood specific to Familial Alzheimer's Disease.>Discussion and Conclusions: We present the first in silico evidence as to the impact of documented mutations in Familial Hidradenitis Suppurativa. We also demonstrate unique substrate recognition and cleavage between Hidradenitis Suppurativa and Familial Alzheimer's Disease, providing a potential explanation as to why the two diseases do not occur within the same pedigree. These proteomic signatures may be a first step in identifying reliable biomarkers for Familial Hidradenitis Suppurativa.
机译:>背景:家族性化脓性汗腺炎和家族性阿尔茨海默氏病均与γ-分泌酶复合物突变有关;但是,这两种疾病在流行病学上并不相关。了解两种疾病之间的分子差异可能有助于建立不同发病机理的假说,并最终成为检测靶标。>目的:表征文献中记载的伽马分泌酶复合物的计算机结构和功能改变>方法:对公开获得的基因组数据进行计算机分析,使用Swiss-model和Dynamut对蛋白质结构和结合亲和力进行评估。在R中使用线性模型的通用框架,使用对数倍数变化来表达差异表达。差异表达基因(DEG)由FCH≥1.5或≤-1.5和错误发现率(FDR≤0.05)定义。>结果:< / strong> HS中39个突变中的23个是通过无义介导的衰变降解的,这些衰变具有改变的底物和在其余突变中鉴定的底物的结合亲和力。 ErbB4,SCNB1和Tie1在病变皮肤中的显着差异是特异于化脓性足底炎和EphB2,EPHB4,KCNE1,LRP6,MUSK,SDC3,Sortilin1在家族性阿尔茨海默氏病特异性血液中的表现。>讨论和结论:我们提供了第一个计算机上的证据,证明有记载的突变对家族性汗腺上皮炎有影响。我们还证明了化脓性汗腺炎和家族性阿尔茨海默氏病之间独特的底物识别和分裂,为为什么这两种疾病不在同一谱系中发生提供了可能的解释。这些蛋白质组学特征可能是鉴定家族性汗腺上皮炎的可靠生物标志物的第一步。

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