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剪接调控异常、microRNA 异常和 Notch 异常:三管齐下克服恶性间皮瘤的药物耐药性。

Splicing deregulation, microRNA and notch aberrations: fighting the three-headed dog to overcome drug resistance in malignant mesothelioma.

机构信息

Department of Medical Oncology, VU University Medical Center, Cancer Center Amsterdam, Amsterdam, Netherlands.

Department of Oncology, University of Torino, Orbassano, Italy.

出版信息

Expert Rev Clin Pharmacol. 2022 Mar;15(3):305-322. doi: 10.1080/17512433.2022.2074835. Epub 2022 May 15.

Abstract

INTRODUCTION

Malignant mesothelioma (MMe) is an aggressive rare cancer of the mesothelium, associated with asbestos exposure. MMe is currently an incurable disease at all stages mainly due to resistance to treatments. It is therefore necessary to elucidate key mechanisms underlying chemoresistance, in an effort to exploit them as novel therapeutic targets.

AREAS COVERED

Chemoresistance is frequently elicited by microRNA (miRNA) alterations and splicing deregulations. Indeed, several miRNAs, such as miR-29c, have been shown to exert oncogenic or oncosuppressive activity. Alterations in the splicing machinery might also be involved in chemoresistance. Moreover, the Notch signaling pathway, often deregulated in MMe, plays a key role in cancer stem cells formation and self-renewal, leading to drug resistance and relapses.

EXPERT OPINION

The prognosis of MMe in patients varies among different tumors and patient characteristics, and novel biomarkers and therapies are warranted. This work aims at giving an overview of MMe, with a special focus on state-of-the-art treatments and new therapeutic strategies against vulnerabilities emerging from studies on epigenetics factors. Besides, this review is also the first to discuss the interplay between miRNAs and alternative splicing as well as the role of Notch as new promising frontiers to overcome drug resistance in MMe.

摘要

简介

恶性间皮瘤(MMe)是一种与石棉暴露有关的间皮恶性罕见癌症。由于对治疗的耐药性,MMe 在所有阶段目前都是一种无法治愈的疾病。因此,有必要阐明化疗耐药的关键机制,努力将其作为新的治疗靶点加以利用。

涵盖领域

化疗耐药性通常是由 microRNA(miRNA)改变和剪接失调引起的。事实上,已经有几种 miRNA,如 miR-29c,被证明具有致癌或抑癌活性。剪接机制的改变也可能与化疗耐药性有关。此外, Notch 信号通路在 MMe 中经常失调,在癌症干细胞的形成和自我更新中发挥关键作用,导致耐药性和复发。

专家意见

不同肿瘤和患者特征的 MMe 患者的预后存在差异,需要新的生物标志物和治疗方法。这项工作旨在概述 MMe,特别关注最先进的治疗方法和针对表观遗传因素研究中出现的脆弱性的新治疗策略。此外,这篇综述也是第一篇讨论 miRNA 和可变剪接之间的相互作用以及 Notch 作为克服 MMe 药物耐药性的新的有前途的前沿的文章。

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