Understanding metabolic characteristics and molecular mechanisms of large to giant congenital melanocytic nevi: implications for melanoma risk and therapeutic targets†

IF 2.7 3区化学 Q2 CHEMISTRY, ANALYTICAL

Analytical Methods Pub Date : 2025-03-24 DOI:10.1039/D5AY00122F

Ge Song, Tao Dai, Yongqiang Ren, Yajie Chang, Pengfei Guo, Zhanwei Wang, Guiping Shen and Jianghua Feng

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Abstract

Large to giant congenital melanocytic nevi (LGCMN) present clinical challenges due to their complex phenotypic heterogeneity and increased melanoma risk. Molecular-level research is essential for understanding the pathogenic mechanisms of LGCMN and identifying potential therapeutic targets. Tissue samples from 67 LGCMN lesions and 49 matched controls were analyzed using metabolomics and transcriptomics to identify metabolic characteristics and gene expression differences. A protein–protein interaction network and a multi-layer network of key metabolites–genes-pathways were established to explore the metabolic characteristics and gene associations with LGCMN. Metabolic analysis revealed a consistent dysregulation in amino acid metabolisms, including arginine, alanine, aspartate, glutamate, phenylalanine, and tyrosine, across LGCMN lesions and subtypes. Compared to controls, 18 upregulated metabolites and 7 downregulated metabolites were identified in LGCMN lesions. Metabolic profiles varied among LGCMN subtypes, with the trunks subtype exhibiting significant alterations in branched-chain amino acids. Network analysis identified 23 genes related to melanogenesis and amino acid metabolism, including TYR, SOX10, and MITF, which showed strong correlation with tyrosine, phenylalanine, and branched-chain amino acids (r > 0.6). High centrality values for genes (e.g., EDNRB, TYR, MITF, SOX10, and MAPK3 > 0.300) and amino acids (e.g., tyrosine at 0.397 and phenylalanine at 0.374) emphasize their pivotal roles in melanogenesis. This study reveals significant metabolic and molecular differences between LGCMN lesions, normal skin, and across LGCMN subtypes, highlighting the deregulation of amino acid metabolism and key genes involved in melanogenesis. These insights enhance our understanding of LGCMN's biological heterogeneity and provide novel avenues for therapeutic intervention.

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了解大到巨大先天性黑素细胞痣的代谢特征和分子机制：对黑色素瘤风险和治疗靶点的影响。

大到巨大的先天性黑素细胞痣（LGCMN）由于其复杂的表型异质性和增加的黑色素瘤风险而面临临床挑战。分子水平的研究对于了解LGCMN的发病机制和确定潜在的治疗靶点至关重要。使用代谢组学和转录组学分析67例LGCMN病变组织样本和49例匹配对照，以确定代谢特征和基因表达差异。建立蛋白-蛋白相互作用网络和关键代谢产物-基因-通路的多层网络，探索LGCMN的代谢特征及其与基因的关联。代谢分析显示，在LGCMN病变和亚型中，氨基酸代谢一致失调，包括精氨酸、丙氨酸、天冬氨酸、谷氨酸、苯丙氨酸和酪氨酸。与对照组相比，在LGCMN病变中发现了18种上调代谢物和7种下调代谢物。不同LGCMN亚型的代谢谱不同，树干亚型在支链氨基酸方面表现出显著的变化。网络分析鉴定出23个与黑色素生成和氨基酸代谢相关的基因，包括TYR、SOX10和MITF，它们与酪氨酸、苯丙氨酸和支链氨基酸具有较强的相关性（r >.6）。基因（如EDNRB、TYR、MITF、SOX10和MAPK3 >.300）和氨基酸（如酪氨酸0.397和苯丙氨酸0.374）的高中心性值强调了它们在黑色素形成中的关键作用。本研究揭示了LGCMN病变、正常皮肤和不同LGCMN亚型之间显著的代谢和分子差异，突出了氨基酸代谢和参与黑素形成的关键基因的失调。这些见解增强了我们对LGCMN生物学异质性的理解，并为治疗干预提供了新的途径。

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