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异常的WNT/CTNNB1信号通路作为人类乳腺癌的治疗靶点:权衡证据

Aberrant WNT/CTNNB1 Signaling as a Therapeutic Target in Human Breast Cancer: Weighing the Evidence.

作者信息

van Schie Emma H, van Amerongen Renée

机构信息

University of Amsterdam, Amsterdam, Netherlands.

Section of Molecular Cytology and van Leeuwenhoek Centre for Advanced Microscopy, Swammerdam Institute for Life Sciences, University of Amsterdam, Amsterdam, Netherlands.

出版信息

Front Cell Dev Biol. 2020 Jan 31;8:25. doi: 10.3389/fcell.2020.00025. eCollection 2020.

Abstract

WNT signaling is crucial for tissue morphogenesis during development in all multicellular animals. After birth, WNT/CTNNB1 responsive stem cells are responsible for tissue homeostasis in various organs and hyperactive WNT/CTNNB1 signaling is observed in many different human cancers. The first link between WNT signaling and breast cancer was established almost 40 years ago, when was identified as a proto-oncogene capable of driving mammary tumor formation in mice. Since that discovery, there has been a dedicated search for aberrant WNT signaling in human breast cancer. However, much debate and controversy persist regarding the importance of WNT signaling for the initiation, progression or maintenance of different breast cancer subtypes. As the first drugs designed to block functional WNT signaling have entered clinical trials, many questions about the role of aberrant WNT signaling in human breast cancer remain. Here, we discuss three major research gaps in this area. First, we still lack a basic understanding of the function of WNT signaling in normal human breast development and physiology. Second, the overall extent and precise effect of (epi)genetic changes affecting the WNT pathway in different breast cancer subtypes are still unknown. Which underlying molecular and cell biological mechanisms are disrupted as a result also awaits further scrutiny. Third, we survey the current status of targeted therapeutics that are aimed at interfering with the WNT pathway in breast cancer patients and highlight the importance and complexity of selecting the subset of patients that may benefit from treatment.

摘要

WNT信号传导对于所有多细胞动物发育过程中的组织形态发生至关重要。出生后,WNT/CTNNB1反应性干细胞负责维持各个器官的组织内稳态,并且在许多不同类型的人类癌症中都观察到WNT/CTNNB1信号传导过度活跃。WNT信号传导与乳腺癌之间的首次联系是在大约40年前建立的,当时 被鉴定为一种原癌基因,能够在小鼠中驱动乳腺肿瘤形成。自该发现以来,人们一直在专门研究人类乳腺癌中异常的WNT信号传导。然而,关于WNT信号传导对不同乳腺癌亚型的起始、进展或维持的重要性,仍然存在许多争论和争议。随着首批旨在阻断功能性WNT信号传导的药物进入临床试验,关于异常WNT信号传导在人类乳腺癌中的作用仍有许多问题。在此,我们讨论该领域的三个主要研究空白。首先,我们仍然缺乏对WNT信号传导在正常人类乳腺发育和生理功能中的基本了解。其次,影响不同乳腺癌亚型中WNT通路的(表观)遗传变化的总体程度和精确作用仍然未知。由此导致哪些潜在的分子和细胞生物学机制被破坏也有待进一步研究。第三,我们调查了旨在干扰乳腺癌患者WNT通路的靶向治疗的现状,并强调了选择可能从治疗中受益的患者亚组的重要性和复杂性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c3a/7005411/fb4e391ca300/fcell-08-00025-g001.jpg

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