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全基因组甲基化分析揭示了翼状胬肉中甲基化谱改变的基因和通路。

Genome-wide methylation analysis unveils genes and pathways with altered methylation profiles in pterygium.

作者信息

L Mathan, Prasad Tejaswi, Aslam Mohammed Hameed, Gr Aadhithiya T, Devarajan Bharanidharan, Prajna N Venkatesh, Dharmalingam K, Banerjee Daipayan

机构信息

Aravind Medical Research Foundation, Madurai, Tamil Nadu, India.

Aravind Eye Hospital, Madurai, Tamil Nadu, India.

出版信息

Exp Eye Res. 2025 Jun;255:110353. doi: 10.1016/j.exer.2025.110353. Epub 2025 Mar 20.

Abstract

Pterygium is a highly prevalent ocular surface disease, particularly in equatorial regions, with no pharmaceutical intervention available and surgical excision remaining the only treatment option. Ultraviolet (UV) radiation from sunlight is widely recognized as the primary cause of pterygium. While chronic UV exposure induces epigenetic changes in the skin contributing to skin cancer, comprehensive studies on epigenetic alterations in pterygium remain unpublished, and causal relationships have yet to be established. This study aimed to investigate genome-wide methylation changes in pterygium using the Illumina Infinium Epic v2.0 Methylation array. We identified 1052 hypermethylated CpGs (499 genes) and 687 hypomethylated CpGs (340 genes) in pterygium tissue compared to control conjunctival tissue from patients undergoing cataract surgery (Δβ>|0.1|, P < 0.05). Hypomethylated genes were mainly associated with PI3K-Akt and MAPK pathways, while hypermethylated genes were enriched in pathways related to oxidative stress, autophagy, DNA repair, and Wnt signaling inhibition. Comparing these findings with transcriptomic datasets revealed 28 hypermethylated genes with downregulated transcripts and 74 hypomethylated genes with upregulated transcripts. qPCR validation confirmed upregulation of hypomethylated genes (MMP2, FBLN5, ZEB1) and downregulation of hypermethylated genes (SAMSN1, CBX4) at the transcript level. These findings suggest that dysregulated DNA methylation may contribute to pterygium pathogenesis by upregulating genes involved in cell proliferation, survival, angiogenesis, fibrosis, and extracellular matrix remodeling, while silencing genes associated with oxidative stress response, autophagy, and DNA damage repair. These insights into the global methylation landscape of pterygium open avenues for detailed functional analysis, potentially guiding targeted therapeutic strategies.

摘要

翼状胬肉是一种高度常见的眼表疾病,在赤道地区尤为普遍,目前尚无药物干预手段,手术切除仍是唯一的治疗选择。阳光中的紫外线(UV)辐射被广泛认为是翼状胬肉的主要病因。虽然长期紫外线暴露会诱导皮肤发生表观遗传变化,进而导致皮肤癌,但关于翼状胬肉表观遗传改变的全面研究尚未发表,因果关系也尚未确立。本研究旨在使用Illumina Infinium Epic v2.0甲基化芯片研究翼状胬肉全基因组甲基化变化。与白内障手术患者的对照结膜组织相比,我们在翼状胬肉组织中鉴定出1052个高甲基化的CpG(499个基因)和687个低甲基化的CpG(340个基因)(Δβ>|0.1|,P < 0.05)。低甲基化基因主要与PI3K-Akt和MAPK信号通路相关,而高甲基化基因则富集于与氧化应激、自噬、DNA修复和Wnt信号抑制相关的通路。将这些发现与转录组数据集进行比较,发现28个高甲基化基因的转录本下调,74个低甲基化基因的转录本上调。qPCR验证证实了低甲基化基因(MMP2、FBLN5、ZEB1)在转录水平上的上调以及高甲基化基因(SAMSN1、CBX4)的下调。这些发现表明,DNA甲基化失调可能通过上调参与细胞增殖、存活、血管生成、纤维化和细胞外基质重塑的基因,同时沉默与氧化应激反应、自噬和DNA损伤修复相关的基因,从而促进翼状胬肉的发病机制。这些对翼状胬肉整体甲基化格局的见解为详细的功能分析开辟了道路,有可能指导靶向治疗策略。

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