The Features of Shared Genes among Transcriptomes Probed in Atopic Dermatitis, Psoriasis, and Inflammatory Acne: S100A9 Selection as the Target Gene.

IF 1 4区生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Protein and Peptide Letters Pub Date : 2024-01-01 DOI:10.2174/0109298665290166240426072642

Wei Wang, Sungbo Hwang, Daeui Park, Yong-Doo Park

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Abstract

Background: Atopic dermatitis (AD), psoriasis (PS), and inflammatory acne (IA) are well-known as inflammatory skin diseases. Studies of the transcriptome with altered expression levels have reported a large number of dysregulated genes and gene clusters, particularly those involved in inflammatory skin diseases.

Objective: To identify genes commonly shared in AD, PS, and IA that are potential therapeutic targets, we have identified consistently dysregulated genes and disease modules that overlap with AD, PS, and IA.

Methods: Microarray data from AD, PS, and IA patients were downloaded from Gene Expression Omnibus (GEO), and identification of differentially expressed genes from microarrays of AD, PS, and IA was conducted. Subsequently, gene ontology and gene set enrichment analysis, detection of disease modules with known disease-associated genes, construction of the protein-protein interaction (PPI) network, and PPI sub-mapping analysis of shared genes were performed. Finally, the computational docking simulations between the selected target gene and inhibitors were conducted.

Results: We identified 50 shared genes (36 up-regulated and 14 down-regulated) and disease modules for each disease. Among the shared genes, 20 common genes in PPI network were detected such as LCK, DLGAP5, SELL, CEP55, CDC20, RRM2, S100A7, S100A9, MCM10, AURKA, CCNB1, CHEK1, BTC, IL1F7, AGTR1, HABP4, SERPINB13, RPS6KA4, GZMB, and TRIP13. Finally, S100A9 was selected as the target gene for therapeutics. Docking simulations between S100A9 and known inhibitors indicated several key binding residues, and based on this result, we suggested several cannabinoids such as WIN-55212-2, JZL184, GP1a, Nabilone, Ajulemic acid, and JWH-122 could be potential candidates for a clinical study for AD, PS, and IA via inhibition of S100A9-related pathway.

Conclusion: Overall, our approach may become an effective strategy for discovering new disease candidate genes for inflammatory skin diseases with a reevaluation of clinical data.

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特应性皮炎、银屑病和炎症性痤疮转录组中共享基因的特征：选择 S100A9 作为目标基因。

背景：特应性皮炎（AD）、银屑病（PS）和炎症性痤疮（IA）是众所周知的炎症性皮肤病。对表达水平改变的转录组的研究报告了大量失调基因和基因簇，尤其是那些涉及炎症性皮肤病的基因：为了确定 AD、PS 和 IA 中常见的潜在治疗靶点基因，我们确定了与 AD、PS 和 IA 重叠的持续失调基因和疾病模块：从基因表达总库（Gene Expression Omnibus，GEO）中下载了AD、PS和IA患者的芯片数据，并对AD、PS和IA芯片中的差异表达基因进行了鉴定。随后，进行了基因本体和基因组富集分析、已知疾病相关基因的疾病模块检测、蛋白质相互作用（PPI）网络的构建以及共享基因的PPI子图谱分析。最后，对选定的靶基因和抑制剂进行了计算对接模拟：结果：我们为每种疾病确定了 50 个共有基因（36 个上调，14 个下调）和疾病模块。在共享基因中，我们发现了 20 个 PPI 网络中的常见基因，如 LCK、DLGAP5、SELL、CEP55、CDC20、RRM2、S100A7、S100A9、MCM10、AURKA、CCNB1、CHEK1、BTC、IL1F7、AGTR1、HABP4、SERPINB13、RPS6KA4、GZMB 和 TRIP13。最后，S100A9 被选为治疗药物的靶基因。S100A9与已知抑制剂之间的对接模拟显示了几个关键的结合残基，基于这一结果，我们认为WIN-55212-2、JZL184、GP1a、Nabilone、Ajulemic acid和JWH-122等几种大麻素可能成为通过抑制S100A9相关途径治疗AD、PS和IA的临床研究候选药物：总之，通过对临床数据的重新评估，我们的方法可能成为发现炎症性皮肤病新疾病候选基因的有效策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Protein and Peptide Letters 生物-生化与分子生物学

CiteScore

2.90

自引率

0.00%

发文量

审稿时长

2 months

期刊介绍： Protein & Peptide Letters publishes letters, original research papers, mini-reviews and guest edited issues in all important aspects of protein and peptide research, including structural studies, advances in recombinant expression, function, synthesis, enzymology, immunology, molecular modeling, and drug design. Manuscripts must have a significant element of novelty, timeliness and urgency that merit rapid publication. Reports of crystallization and preliminary structure determination of biologically important proteins are considered only if they include significant new approaches or deal with proteins of immediate importance, and preliminary structure determinations of biologically important proteins. Purely theoretical/review papers should provide new insight into the principles of protein/peptide structure and function. Manuscripts describing computational work should include some experimental data to provide confirmation of the results of calculations. Protein & Peptide Letters focuses on: Structure Studies Advances in Recombinant Expression Drug Design Chemical Synthesis Function Pharmacology Enzymology Conformational Analysis Immunology Biotechnology Protein Engineering Protein Folding Sequencing Molecular Recognition Purification and Analysis