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YRNA过表达及其在过敏中的潜在影响。

YRNAs overexpression and potential implications in allergy.

作者信息

Isidoro-García María, García-Sánchez Asunción, Sanz Catalina, Estravís Miguel, Marcos-Vadillo Elena, Pascual Marien, Roa Sergio, Marques-García Fernando, Triviño Juan Carlos, Dávila Ignacio

机构信息

Department of Clinical Biochemistry, University Hospital of Salamanca, Spain.

Institute for Biomedical Research of Salamanca, Spain.

出版信息

World Allergy Organ J. 2019 Jul 26;12(8):100047. doi: 10.1016/j.waojou.2019.100047. eCollection 2019 Aug.

Abstract

BACKGROUND

Small non-coding RNAs (snRNAs) develop important functions related to epigenetic regulation. YRNAs are snRNAs involved in the initiation of DNA replication and RNA stability that regulate gene expression. They have been related to autoimmune, cancer and inflammatory diseases but never before to allergy. In this work we described for the first time in allergic patients the differential expression profile of YRNAs, their regulatory mechanisms and their potential as new diagnostic and therapeutic targets.

METHODS

From a previous whole RNAseq study in B cells of allergic patients, differential expression profiles of coding and non-coding transcripts were obtained. To select the most differentially expressed non coding transcripts, fold change and p-values were analyzed. A validation of the expression differences detected was developed in an independent cohort of 304 individuals, 208 allergic patients and 96 controls by using qPCR. Potential binding and retrotransponibility capacity were characterized by structural analysis. Using a novel bioinformatics approach, RNA targets identification, functional enrichment and network analyses were performed.

RESULTS

We found that almost 70% of overexpressed non-coding transcripts in allergic patients corresponded to YRNAs. From the three more differentially overexpressed candidates, increased expression was independently confirmed in the peripheral blood of allergic patients. Structural analysis suggested a protein binding capacity decrease and an increase in retrotransponibility. Studies of RNA targets allowed the identification of sequences related to the immune mechanisms underlying allergy.

CONCLUSIONS

Overexpression of YRNAs is observed for the first time in allergic patients. Structural and functional information points to their implication on regulatory mechanisms of the disease.

摘要

背景

小非编码RNA(snRNA)发挥着与表观遗传调控相关的重要功能。YRNA是参与DNA复制起始和RNA稳定性从而调节基因表达的snRNA。它们与自身免疫性疾病、癌症和炎症性疾病有关,但此前从未与过敏相关联。在本研究中,我们首次描述了过敏患者中YRNA的差异表达谱、其调控机制及其作为新的诊断和治疗靶点的潜力。

方法

从先前对过敏患者B细胞进行的全RNA测序研究中,获得了编码和非编码转录本的差异表达谱。为了选择差异表达最显著的非编码转录本,分析了倍数变化和p值。通过qPCR在一个由304名个体组成的独立队列中进行了验证,其中包括208名过敏患者和96名对照,以检测所发现的表达差异。通过结构分析表征了潜在的结合和逆转录转座能力。使用一种新颖的生物信息学方法进行了RNA靶点鉴定、功能富集和网络分析。

结果

我们发现过敏患者中近70%过表达的非编码转录本对应于YRNA。在三个差异过表达最显著的候选基因中,过敏患者外周血中其表达增加得到了独立验证。结构分析表明其蛋白质结合能力下降,逆转录转座能力增加。RNA靶点研究使得能够鉴定与过敏潜在免疫机制相关的序列。

结论

首次在过敏患者中观察到YRNA的过表达。结构和功能信息表明它们参与了该疾病的调控机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c548/6664241/79e39135bcca/gr1.jpg

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