癌症细胞对紫杉醇的耐药性与miRNA-186和miRNA-7的低表达有关。

IF 4.6 Q1 ONCOLOGY
癌症耐药(英文) Pub Date : 2023-09-01 eCollection Date: 2023-01-01 DOI:10.20517/cdr.2023.19
Vera Apollonova, Daniil Plevako, Alexandr Garanin, Elena Sidina, Lidia Zabegina, Margarita Knyazeva, Viktoria Smirnova, Anna Artemyeva, Petr Krivorotko, Anastasia Malek
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引用次数: 0

摘要

目的:新辅助化疗是癌症(BC)复杂治疗的常用方法,紫杉醇(PTX)经常被纳入治疗方案。然而,基于PTX的治疗效果很难根据常规使用的标志物准确预测。由于微小RNA被认为是一类新的有前景的生物标志物,miRNA表达与BC细胞PTX抗性之间的联系需要深入研究。本研究旨在鉴定与BC细胞对PTX反应相关的miRNA。方法:在5个BC细胞系中测定固有PTX敏感性和miRNA图谱,以鉴定候选miRNA。通过实时定量聚合酶链反应(RT-qPCR)分析从诊断活检获得的BC组织样本(n.31)中选定的miRNA(n.15)表达。在两个周期的PTX效果和完成的新辅助治疗方案的效果的背景下分析结果。该研究的设计有助于评估PTX对细胞的影响,并鉴定仅与该药物敏感性相关的微小RNA表达谱的特征。结果:基于PTX的新辅助治疗效果较好的患者,BC组织中miR-186和miR-7的表达较高。结论:miR-186和miR-7的高表达与BC对PTX的良好反应有关,而它们的低表达可能与BC对PT的耐药性有关,这表明开发用于预测PTX反应的创新测试系统的可能性,该系统可在BC新辅助化疗开始前使用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Resistance of breast cancer cells to paclitaxel is associated with low expressions of miRNA-186 and miRNA-7.

Resistance of breast cancer cells to paclitaxel is associated with low expressions of miRNA-186 and miRNA-7.

Resistance of breast cancer cells to paclitaxel is associated with low expressions of miRNA-186 and miRNA-7.

Resistance of breast cancer cells to paclitaxel is associated with low expressions of miRNA-186 and miRNA-7.

Aim: Neo-adjuvant chemotherapy is a common approach for the complex treatment of breast cancer (BC) and paclitaxel (PTX) is frequently included in the therapeutic regimen. However, the effect of PTX-based treatment is hard to predict precisely based on routinely used markers. As microRNAs are considered a new promising class of biomarkers, the link between miRNA expression and PTX resistance of BC cells needs to be well investigated. This study aimed at the identification of miRNAs associated with responses of BC cells to PTX. Methods: Intrinsic PTX sensitivity and miRNA profiling were assayed in five BC cell lines to identify candidate miRNAs. Selected miRNA (n. 15) expressions were analyzed by real-time-quantitative polymerase chain reaction (RT-qPCR) in BC tissue samples (n. 31) obtained from a diagnostic biopsy. Results were analyzed in the context of the effect of two cycles of PTX and the effect of the completed scheme of neoadjuvant therapy. The study's design facilitated the evaluation of the effect of PTX on cells and the identification of features of the microRNA expression profiles associated exclusively with sensitivity to this drug. Results: miR-186 and miR-7 expression in BC tissues was higher in patients with better outcomes of PTX-based neoadjuvant therapy. Conclusion: High expressions of miR-186 and miR-7 are associated with good response to PTX, whereas their low expressions may be associated with resistance to PTX in BC, indicating the possibility of developing innovative test systems for the prediction of the PTX response, which can be used before the start of neo-adjuvant chemotherapy for BC.

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