Exploring the toxicological network in diabetic microvascular disease: The Role of Endocrine Disrupting Chemicals.

IF 12.5 2区医学 Q1 SURGERY

International journal of surgery Pub Date : 2025-04-11 DOI:10.1097/JS9.0000000000002394

Siyuan Song, Liji Huang, Xiqiao Zhou, Jiangyi Yu

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引用次数: 0

Abstract

Purpose: This study investigates how endocrine-disrupting chemicals contribute to diabetic microvascular disease.

Methods: This study assessed endocrine-disrupting chemical toxicity using PubChem, ProTox 3.0, and ChEMBL. Relevant EDC targets were identified via SwissTargetPrediction and Similarity Ensemble Approach. Gene targets for diabetic microvascular diseases (diabetic kidney disease, retinopathy, and sensory polyneuropathy) were retrieved from CTD, GeneCards, and OMIM. Candidate targets were identified by intersecting EDC and disease-related targets. A protein-protein interaction network was built using STRING to identify hub genes. Functional enrichment analysis was conducted via Metascape. Molecular docking of EDC compounds with hub targets was performed using Discovery Studio and CDOCKER. Hub targets were validated through immunohistochemical staining, single-cell distribution, subcellular localization assays, and gene expression analysis in external HPA and GEO datasets.

Results: A total of 843, 474, and 623 potential toxic targets were identified for diabetic kidney disease, diabetic retinopathy, and diabetic sensory polyneuropathy, respectively. KEGG pathway analysis linked EDC toxicity in diabetic kidney disease to key pathways such as cancer, chemokine signaling, apoptosis, calcium signaling, and drug metabolism (cytochrome P450), with hub targets including EGFR, ALB, MYC, ESR1, and HSP90AA1. Diabetic retinopathy was associated with MAPK, ERBB, NOD-like receptor signaling, and renal cell carcinoma pathways, with ALB, EGFR, MYC, BCL2, and CD4 identified as hub targets. For diabetic sensory polyneuropathy, EDCs may influence chemokine, apoptosis, ERBB, VEGF, and JAK-STAT signaling pathways, with ALB, EGFR, MYC, ESR1, and BCL2 as key targets. Molecular docking confirmed strong binding activity between EDC components and hub targets.

Conclusion: This study offers a theoretical basis for identifying toxic targets and mechanisms by which endocrine-disrupting chemicals contribute to diabetic microvascular diseases.

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探讨糖尿病微血管疾病的毒理学网络：内分泌干扰物的作用。

目的：探讨内分泌干扰物在糖尿病微血管疾病中的作用机制。方法：本研究使用PubChem、ProTox 3.0和ChEMBL评估内分泌干扰化学物质的毒性。通过SwissTargetPrediction和相似集成方法识别相关EDC目标。从CTD、GeneCards和OMIM中检索糖尿病微血管疾病（糖尿病肾病、视网膜病变和感觉多发性神经病变）的基因靶点。候选靶点是通过交叉EDC和疾病相关靶点来确定的。利用STRING构建蛋白互作网络，识别中心基因。通过metscape进行功能富集分析。利用Discovery Studio和CDOCKER进行EDC化合物与枢纽靶点的分子对接。Hub靶点通过免疫组织化学染色、单细胞分布、亚细胞定位分析以及外部HPA和GEO数据集的基因表达分析进行验证。结果：共鉴定出843、474和623个潜在毒性靶点，分别用于糖尿病肾病、糖尿病视网膜病变和糖尿病感觉多发性神经病变。KEGG通路分析将糖尿病肾病中的EDC毒性与癌症、趋化因子信号、凋亡、钙信号和药物代谢（细胞色素P450）等关键通路联系起来，中心靶点包括EGFR、ALB、MYC、ESR1和HSP90AA1。糖尿病视网膜病变与MAPK、ERBB、nod样受体信号通路和肾细胞癌通路相关，ALB、EGFR、MYC、BCL2和CD4被确定为枢纽靶点。对于糖尿病感觉多发性神经病变，EDCs可能影响趋化因子、凋亡、ERBB、VEGF和JAK-STAT信号通路，其中ALB、EGFR、MYC、ESR1和BCL2是关键靶点。分子对接证实了EDC组分与hub靶点之间具有很强的结合活性。结论：本研究为确定内分泌干扰物致糖尿病微血管病变的毒性靶点和机制提供了理论依据。

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来源期刊

International journal of surgery SURGERY-

CiteScore

17.70

自引率

3.30%

发文量

审稿时长

6-12 weeks

期刊介绍： The International Journal of Surgery (IJS) has a broad scope, encompassing all surgical specialties. Its primary objective is to facilitate the exchange of crucial ideas and lines of thought between and across these specialties.By doing so, the journal aims to counter the growing trend of increasing sub-specialization, which can result in "tunnel-vision" and the isolation of significant surgical advancements within specific specialties.