Tristetraprolin可影响三阴性乳腺癌模型中侵袭相关基因的表达和细胞运动。

Anastasiia Hubiernatorova, Josef Novak, Michaela Vaskovicova, David Sekac, Serhii Kropyvko, Zdenek Hodny
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摘要

Tristetraprolin(TTP)是一种 RNA 结合蛋白,可对其靶 mRNA 进行负调控,并被证明可抑制肿瘤的进展和侵袭。肿瘤侵袭需要细胞骨架成分的精确调控,细胞骨架相关基因的失调可显著改变细胞的运动性和侵袭能力。包括 SH3PXD2A、SH3PXD2B、CTTN、WIPF1 和 WASL 在内的一些基因是细胞骨架重组机制的重要组成部分,对细胞的充分运动至关重要。这些基因还参与侵袭过程,其中 SH3PXD2A、SH3PXD2B、WIPF1 和 CTTN 是促进侵袭的侵袭灶特化结构的关键组成部分。然而,人们对这些基因的调控还不甚了解。本研究表明,在 MDA-MB-231 细胞中异位表达 TTP 会导致 CTTN 和 SH3PXD2A 的 mRNA 水平下降,以及细胞运动和肌动蛋白丝组织的缺陷。此外,多柔比星会显著增加 TTP 的表达,降低细胞骨架相关基因的 mRNA 水平,从而加深我们对多柔比星如何影响细胞转录谱的理解。然而,多柔比星对靶标 mRNA 的影响不同于 TTP 的异位表达,这表明它可能不是多柔比星治疗乳腺癌(BC)的主要机制。TTP的高表达被认为是包括乳腺癌在内的多种癌症的阳性预后标志。鉴于多柔比星是治疗三阴性乳腺癌的常用药物,在这组患者中使用TTP作为预后标志物可能会受到限制,因为要了解TTP的高表达是由于患者的良好生理状态还是治疗的结果可能会很困难。
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Tristetraprolin affects invasion-associated genes expression and cell motility in triple-negative breast cancer model.

Tristetraprolin (TTP) is an RNA-binding protein that negatively regulates its target mRNAs and has been shown to inhibit tumor progression and invasion. Tumor invasion requires precise regulation of cytoskeletal components, and dysregulation of cytoskeleton-associated genes can significantly alter cell motility and invasive capability. Several genes, including SH3PXD2A, SH3PXD2B, CTTN, WIPF1, and WASL, are crucial components of the cytoskeleton reorganization machinery and are essential for adequate cell motility. These genes are also involved in invasion processes, with SH3PXD2A, SH3PXD2B, WIPF1, and CTTN being key components of invadopodia-specialized structures that facilitate invasion. However, the regulation of these genes is not well understood. This study demonstrates that ectopic expression of TTP in MDA-MB-231 cells leads to decreased mRNA levels of CTTN and SH3PXD2A, as well as defects in cell motility and actin filament organization. Additionally, doxorubicin significantly increases TTP expression and reduces the mRNA levels of cytoskeleton-associated genes, enhancing our understanding of how doxorubicin may affect the transcriptional profile of cells. However, doxorubicin affects target mRNAs differently than TTP ectopic expression, suggesting it may not be the primary mechanism of doxorubicin in breast cancer (BC) treatment. High TTP expression is considered as a positive prognostic marker in multiple cancers, including BC. Given that doxorubicin is a commonly used drug for treating triple-negative BC, using TTP as a prognostic marker in this cohort of patients might be limited since it might be challenging to understand if high TTP expression occurred due to the favorable physiological state of the patient or as a consequence of treatment.

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