ETS转录因子家族
TMPRS2型
前列腺癌
转录因子
癌变
癌症研究
色丛
前列腺
融合基因
生物
医学
癌症
疾病
基因
内科学
遗传学
PCA3系列
传染病(医学专业)
2019年冠状病毒病(COVID-19)
作者
Taylor R. Nicholas,Brady G. Strittmatter,Peter C. Hollenhorst
标识
DOI:10.1007/978-3-030-32656-2_18
摘要
Prostate cancer is unique among carcinomas in that a fusion gene created by a chromosomal rearrangement is a common driver of the disease. The TMPRSS2/ERG rearrangement drives aberrant expression of the ETS family transcription factor ERG in 50% of prostate tumors. Similar rearrangements promote aberrant expression of the ETS family transcription factors ETV1 and ETV4 in another 10% of cases. Together, these three ETS factors are thought to promote tumorigenesis in the majority of prostate cancers. A goal of precision medicine is to be able to apply targeted therapeutics that are specific to disease subtypes. ETS gene rearrangement positive tumors represent the largest molecular subtype of prostate cancer, but to date there is no treatment specific to this marker. In this chapter we will review the latest findings regarding the molecular mechanisms of ETS factor function in the prostate. These molecular details may provide a path towards new therapeutic targets for this subtype of prostate cancer. Further, we will describe efforts to target the oncogenic functions of ETS family transcription factors directly as well as indirectly.
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