研究miR-9作为喉癌健康差异的介导因子。

Investigating miR-9 as a mediator in laryngeal cancer health disparities.

作者信息

Gobin Christina, Inkabi Samuel, Lattimore Chayil C, Gu Tongjun, Menefee James N, Rodriguez Mayrangela, Kates Heather, Fields Christopher, Bian Tengfei, Silver Natalie, Xing Chengguo, Yates Clayton, Renne Rolf, Xie Mingyi, Fredenburg Kristianna M

机构信息

Department of Pathology, Immunology, and Laboratory Medicine, University of Florida, Gainesville, FL, United States.

College of Graduate Health Studies, A.T. Still University, Kirksville, MO, United States.

出版信息

Front Oncol. 2023 Apr 4;13:1096882. doi: 10.3389/fonc.2023.1096882. eCollection 2023.

DOI:10.3389/fonc.2023.1096882

PMID:37081981

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10112398/

Abstract

BACKGROUND

For several decades, Black patients have carried a higher burden of laryngeal cancer among all races. Even when accounting for sociodemographics, a disparity remains. Differentially expressed microRNAs have been linked to racially disparate clinical outcomes in breast and prostate cancers, yet an association in laryngeal cancer has not been addressed. In this study, we present our computational analysis of differentially expressed miRNAs in Black compared with White laryngeal cancer and further validate microRNA-9-5p (miR-9-5p) as a potential mediator of cancer phenotype and chemoresistance.

METHODS

Bioinformatic analysis of 111 (92 Whites, 19 Black) laryngeal squamous cell carcinoma (LSCC) specimens from the TCGA revealed miRNAs were significantly differentially expressed in Black compared with White LSCC. We focused on miR-9-5 p which had a significant 4-fold lower expression in Black compared with White LSCC (p<0.05). After transient transfection with either miR-9 mimic or inhibitor in cell lines derived from Black (UM-SCC-12) or White LSCC patients (UM-SCC-10A), cellular migration and cell proliferation was assessed. Alterations in cisplatin sensitivity was evaluated in transient transfected cells IC50 analysis. qPCR was performed on transfected cells to evaluate miR-9 targets and chemoresistance predictors, ABCC1 and MAP1B.

RESULTS

Northern blot analysis revealed mature miR-9-5p was inherently lower in cell line UM-SCC-12 compared with UM-SCC-10A. UM -SCC-12 had baseline increase in cellular migration (p < 0.01), proliferation (p < 0.0001) and chemosensitivity (p < 0.01) compared to UM-SCC-10A. Increasing miR-9 in UM-SCC-12 cells resulted in decreased cellular migration (p < 0.05), decreased proliferation (p < 0.0001) and increased sensitivity to cisplatin (p < 0.001). Reducing miR-9 in UM-SCC-10A cells resulted in increased cellular migration (p < 0.05), increased proliferation (p < 0.05) and decreased sensitivity to cisplatin (p < 0.01). A significant inverse relationship in ABCC1 and MAP1B gene expression was observed when miR-9 levels were transiently elevated or reduced in either UM-SCC-12 or UM-SCC-10A cell lines, respectively, suggesting modulation by miR-9.

CONCLUSION

Collectively, these studies introduce differential miRNA expression in LSCC cancer health disparities and propose a role for low miR-9-5p as a mediator in LSCC tumorigenesis and chemoresistance.

摘要

背景

几十年来，在所有种族中，黑人患者患喉癌的负担更高。即使考虑到社会人口统计学因素，差异仍然存在。差异表达的微小RNA与乳腺癌和前列腺癌中种族差异的临床结果有关，但喉癌中的关联尚未得到研究。在本研究中，我们展示了对黑人与白人喉癌中差异表达的微小RNA的计算分析，并进一步验证了微小RNA-9-5p（miR-9-5p）作为癌症表型和化疗耐药性的潜在调节因子。

方法

对来自TCGA的111例（92例白人，19例黑人）喉鳞状细胞癌（LSCC）标本进行生物信息学分析，发现与白人LSCC相比，黑人LSCC中的微小RNA存在显著差异表达。我们聚焦于miR-9-5p，与白人LSCC相比，其在黑人LSCC中的表达显著低4倍（p<0.05）。在用miR-9模拟物或抑制剂瞬时转染来自黑人（UM-SCC-12）或白人LSCC患者（UM-SCC-10A）的细胞系后，评估细胞迁移和细胞增殖。通过IC50分析评估瞬时转染细胞中顺铂敏感性的变化。对转染细胞进行qPCR以评估miR-9的靶标以及化疗耐药性预测因子ABCC1和MAP1B。

结果

Northern印迹分析显示，与UM-SCC-10A相比，细胞系UM-SCC-12中成熟miR-9-5p的固有水平较低。与UM-SCC-10A相比，UM-SCC-12在细胞迁移（p<0.01）、增殖（p<0.0001）和化疗敏感性（p<0.01）方面基线增加。在UM-SCC-12细胞中增加miR-9导致细胞迁移减少（p<0.05）、增殖减少（p<0.0001）和顺铂敏感性增加（p<0.001）。在UM-SCC-10A细胞中降低miR-9导致细胞迁移增加（p<0.05）、增殖增加（p<0.05）和顺铂敏感性降低（p<0.01）。当在UM-SCC-12或UM-SCC-10A细胞系中分别瞬时升高或降低miR-9水平时，观察到ABCC1和MAP1B基因表达存在显著的负相关关系，提示受miR-9调节。