Profiling of the serum MiRNAome in pediatric egyptian patients with wilms tumor.

IF 3.9 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Frontiers in Molecular Biosciences Pub Date : 2024-10-15 eCollection Date: 2024-01-01 DOI:10.3389/fmolb.2024.1453562

Fatma S Mohamed, Deena Jalal, Youssef M Fadel, Samir F El-Mashtoly, Wael Z Khaled, Ahmed A Sayed, Mohamed A Ghazy

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引用次数: 0

Abstract

Wilms tumor (WT) is a pediatric kidney cancer associated with poor outcomes in patients with unfavorable histological features such as anaplasia. Small non-coding RNAs, such as miRNAs, are known to be involved in WT pathogenesis. However, research on the clinical potential of blood-based miRNAs is limited. This study aimed to profile aberrantly expressed miRNAs in WT serum samples, evaluate their potential to differentiate standard-risk patients with favorable histology from those with anaplastic WTs, and assess their clinical value as minimally invasive biomarkers for WT detection. The study used next-generation sequencing (NGS) to analyze miRNA expressions in serum samples from 37 Egyptian children, including 10 healthy individuals, 14 with non-anaplastic WTs (favorable histology FH-WTs), and 13 with anaplastic WTs (unfavorable histology UnFH-WTs). Functional enrichment analysis was conducted to identify critical pathways and biological processes affected by dysregulated miRNAs, and a network was created for the most promising miRNA-target interactions linked to WT. The study identified a distinct miRNA expression signature of 45 miRNAs (3 upregulated and 42 downregulated) in WT serum samples compared to healthy controls, with 29 miRNAs exclusively dysregulated in FH-WTs and 6 miRNAs dysregulated solely in UnFH-WTs. These dysregulated miRNAs displayed significant enrichment in cancer-related pathways, such as PI3K/AKT, FOXO, and MAPK signaling. In relation to WT clinicopathological features, decreased levels of hsa-miR-2355-3p showed a significant positive correlation with clinical stage (r = 0.6597, p = 0.0006) and WT metastasis (r = 0.439, p = 0.021). The ROC curve analysis revealed that multiple dysregulated miRNAs in WT, specifically hsa-miR-7-5p, hsa-miR-146a-5p, hsa-miR-378a-3p, and hsa-miR-483-5p, exhibited high diagnostic potential for WT, with AUC values exceeding 0.86. Among WT histopathology types, the hsa-miR-1180-3p showed a 2.3 log2fold difference in expression between UnFH-WTs and FH-WTs, indicating its potential as a biomarker with 92% sensitivity and 85% specificity for identifying UnFH-WTs. Its target genes were enriched in pathways related to cell division and cell cycle regulation. In conclusion, hsa-miR-1180-3p could be a reliable blood-based biomarker for distinguishing WT histopathological types, and further research is needed to validate its clinical value.

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埃及儿科威尔姆斯肿瘤患者血清 MiRNA 组分析。

Wilms瘤（WT）是一种小儿肾癌，具有无细胞增生等不利组织学特征的患者预后较差。已知小非编码 RNA（如 miRNA）参与了 WT 的发病机制。然而，基于血液的 miRNAs 的临床潜力研究还很有限。本研究旨在分析 WT 血清样本中异常表达的 miRNA，评估它们在区分组织学良好的标准风险患者和无细胞 WT 患者方面的潜力，并评估它们作为 WT 检测的微创生物标记物的临床价值。该研究利用新一代测序技术（NGS）分析了 37 名埃及儿童血清样本中 miRNA 的表达，其中包括 10 名健康人、14 名非无弹性 WTs 患者（有利组织学 FH-WTs）和 13 名无弹性 WTs 患者（不利组织学 UnFH-WTs）。研究人员进行了功能富集分析，以确定受失调 miRNA 影响的关键通路和生物过程，并为与 WT 相关的最有希望的 miRNA-靶点相互作用创建了一个网络。研究发现，与健康对照组相比，WT血清样本中有45个miRNA表达特征（3个上调，42个下调），其中29个miRNA在FH-WT中完全失调，6个miRNA在UnFH-WT中完全失调。这些失调的 miRNA 在癌症相关通路（如 PI3K/AKT、FOXO 和 MAPK 信号转导）中表现出明显的富集。就 WT 临床病理特征而言，hsa-miR-2355-3p 水平的降低与临床分期（r = 0.6597，p = 0.0006）和 WT 转移（r = 0.439，p = 0.021）呈显著正相关。ROC曲线分析表明，WT中多个失调的miRNA，特别是hsa-miR-7-5p、hsa-miR-146a-5p、hsa-miR-378a-3p和hsa-miR-483-5p，对WT具有很高的诊断潜力，AUC值超过0.86。在 WT 组织病理学类型中，hsa-miR-1180-3p 在 UnFH-WTs 和 FH-WTs 之间的表达量相差 2.3 log2 倍，这表明它具有作为生物标记物的潜力，对鉴别 UnFH-WTs 的灵敏度为 92%，特异性为 85%。其靶基因富集在与细胞分裂和细胞周期调控相关的通路中。总之，hsa-miR-1180-3p 是一种可靠的血液生物标记物，可用于鉴别 WT 组织病理学类型。

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

Frontiers in Molecular Biosciences Biochemistry, Genetics and Molecular Biology-Biochemistry

CiteScore

7.20

自引率

4.00%

发文量

1361

审稿时长

14 weeks

期刊介绍： Much of contemporary investigation in the life sciences is devoted to the molecular-scale understanding of the relationships between genes and the environment — in particular, dynamic alterations in the levels, modifications, and interactions of cellular effectors, including proteins. Frontiers in Molecular Biosciences offers an international publication platform for basic as well as applied research; we encourage contributions spanning both established and emerging areas of biology. To this end, the journal draws from empirical disciplines such as structural biology, enzymology, biochemistry, and biophysics, capitalizing as well on the technological advancements that have enabled metabolomics and proteomics measurements in massively parallel throughput, and the development of robust and innovative computational biology strategies. We also recognize influences from medicine and technology, welcoming studies in molecular genetics, molecular diagnostics and therapeutics, and nanotechnology. Our ultimate objective is the comprehensive illustration of the molecular mechanisms regulating proteins, nucleic acids, carbohydrates, lipids, and small metabolites in organisms across all branches of life. In addition to interesting new findings, techniques, and applications, Frontiers in Molecular Biosciences will consider new testable hypotheses to inspire different perspectives and stimulate scientific dialogue. The integration of in silico, in vitro, and in vivo approaches will benefit endeavors across all domains of the life sciences.