A Bioinformatics Analysis for Unveiling Novel Long Non-Coding RNAs and their Regulatory Impact on Key Genes Associated with Vitiligo

Mathematical Biology and Bioinformatics Pub Date : 2024-05-01 DOI:10.17537/2024.19.155

Safa Sadeq Fayez, Ahmed AbdulJabbar Suleiman

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Abstract

Vitiligo involves the gradual disappearance of melanocytes, causing skin depigmentation. Long noncoding RNAs (lncRNAs), a type of noncoding RNA, are important for regulating inflammation and immunity. Despite this significance, there needs to be more published research on how lncRNAs are expressed in vitiligo cases and their potential roles in the biology of this skin condition. This study aims to elucidate the molecular landscape of vitiligo by analyzing gene expression profiles of vitiligo skin and normal skin. Two datasets, RNA-seq and microarray, were thoroughly investigated to identify differentially expressed (DE) genes and lncRNAs associated with vitiligo development. Functional enrichment analysis revealed biological processes and pathways influenced by dysregulated genes, highlighting intricate processes such as melanin biosynthesis and melanogenesis, shedding light on the complex regulatory networks involved in pigmentation and immune responses. Protein-protein interaction analysis highlighted significantly downregulated hub genes, including TYRP1, MLANA, MC1R, SLC45A2, PAX3, TYR, DCT, OCA2, PMEL, and SOX10, revealing significant functional relationships among identified hub genes within the network. RNA-seq data analysis uncovered DE-lncRNAs, emphasizing the regulatory role of lncRNAs in vitiligo. Moreover, the correlation analysis between the expression of lncRNAs and key genes associated with melanogenesis (OCA2, TYRP1, and PMEL) unveiled novel upregulated lncRNAs such as CRTC3-AS1, LCMT1-AS1, LINC02178 contributing to vitiligo development. Additionally, lncRNA-gene networks constructed based on key melanocyte-related genes provided insights into the molecular relationships relevant to vitiligo. Overall, this study offers a comprehensive understanding of vitiligo pathogenesis, identifying potential therapeutic targets and laying the foundation for future research in this critical area.

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生物信息学分析揭示新型长非编码 RNA 及其对白癜风相关关键基因的调控影响

白癜风是指黑色素细胞逐渐消失，导致皮肤脱色。长非编码 RNA（lncRNA）是非编码 RNA 的一种，对调节炎症和免疫非常重要。尽管长非编码 RNA 具有重要意义，但仍需要发表更多关于长非编码 RNA 在白癜风病例中如何表达及其在这种皮肤病的生物学中的潜在作用的研究成果。本研究旨在通过分析白癜风皮肤和正常皮肤的基因表达谱，阐明白癜风的分子图谱。研究人员对RNA-seq和芯片两个数据集进行了深入研究，以确定与白癜风发病相关的差异表达（DE）基因和lncRNA。功能富集分析揭示了受失调基因影响的生物过程和通路，突出了黑色素生物合成和黑色素生成等复杂过程，揭示了色素沉着和免疫反应所涉及的复杂调控网络。蛋白-蛋白相互作用分析突出显示了明显下调的枢纽基因，包括TYRP1、MLANA、MC1R、SLC45A2、PAX3、TYR、DCT、OCA2、PMEL和SOX10，揭示了网络中已识别的枢纽基因之间的重要功能关系。RNA-seq数据分析发现了DE-lncRNAs，强调了lncRNAs在白癜风中的调控作用。此外，lncRNAs表达与黑色素生成相关关键基因（OCA2、TYRP1和PMEL）之间的相关性分析揭示了新的上调lncRNAs，如CRTC3-AS1、LCMT1-AS1、LINC02178等，这些lncRNAs有助于白癜风的发展。此外，基于关键黑色素细胞相关基因构建的lncRNA-基因网络为了解与白癜风相关的分子关系提供了见解。总之，这项研究提供了对白癜风发病机制的全面了解，确定了潜在的治疗靶点，并为这一关键领域的未来研究奠定了基础。

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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Mathematical Biology and Bioinformatics

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