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MYB转录因子在癌症耐药性中的新作用。

Emerging role of MYB transcription factors in cancer drug resistance.

作者信息

Biersack Bernhard, Höpfner Michael

机构信息

Organic Chemistry Laboratory, University of Bayreuth, Bayreuth 95440, Germany.

Institute for Physiology, Charité-Universitätsmedizin Berlin, Corporate Member of Freie Universität Berlin and Humboldt Universität zu Berlin, Berlin 10117, Germany.

出版信息

Cancer Drug Resist. 2024 Apr 30;7:15. doi: 10.20517/cdr.2023.158. eCollection 2024.

Abstract

Decades ago, the viral myeloblastosis oncogene - was identified as a gene responsible for the development of avian leukemia. However, the relevance of MYB proteins for human cancer diseases, in particular for solid tumors, remained basically unrecognized for a very long time. The human family of MYB transcription factors comprises MYB (c-MYB), MYBL2 (b-MYB), and MYBL1 (a-MYB), which are overexpressed in several cancers and are associated with cancer progression and resistance to anticancer drugs. In addition to overexpression, the presence of activated MYB-fusion proteins as tumor drivers was described in certain cancers. The identification of anticancer drug resistance mediated by MYB proteins and their underlying mechanisms are of great importance in understanding failures of current therapies and establishing new and more efficient therapy regimens. In addition, new drug candidates targeting MYB transcription factor activity and signaling have emerged as a promising class of potential anticancer therapeutics that could tackle MYB-dependent drug-resistant cancers in a more selective way. This review describes the correlation of MYB transcription factors with the formation and persistence of cancer resistance to various approved and investigational anticancer drugs.

摘要

几十年前,病毒成髓细胞增多症致癌基因被确定为一种导致禽类白血病发展的基因。然而,很长一段时间以来,MYB蛋白与人类癌症疾病,特别是实体瘤的相关性基本上未被认识。人类MYB转录因子家族包括MYB(c-MYB)、MYBL2(b-MYB)和MYBL1(a-MYB),它们在几种癌症中过度表达,并与癌症进展和抗癌药物耐药性相关。除了过度表达外,在某些癌症中还描述了作为肿瘤驱动因素的活化MYB融合蛋白的存在。确定由MYB蛋白介导的抗癌药物耐药性及其潜在机制对于理解当前治疗的失败以及建立新的、更有效的治疗方案非常重要。此外,靶向MYB转录因子活性和信号传导的新候选药物已成为一类有前景的潜在抗癌治疗药物,它们可以以更具选择性的方式治疗MYB依赖性耐药癌症。本综述描述了MYB转录因子与癌症对各种已批准和正在研究的抗癌药物耐药性的形成和持续存在之间的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/509d/11149108/5067c272bf55/cdr-7-15.fig.1.jpg

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