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前列腺癌作为去分化器官:雄激素受体、癌症干细胞和癌症干性。

Prostate cancer as a dedifferentiated organ: androgen receptor, cancer stem cells, and cancer stemness.

机构信息

Department of Pharmacology & Therapeutics, Roswell Park Comprehensive Cancer Center, Buffalo, NY 14263, U.S.A.

Experimental Therapeutics (ET) Graduate Program, Roswell Park Comprehensive Cancer Center and the University at Buffalo, Buffalo, NY 14263, U.S.A.

出版信息

Essays Biochem. 2022 Sep 16;66(4):291-303. doi: 10.1042/EBC20220003.

Abstract

Cancer progression is characterized and driven by gradual loss of a differentiated phenotype and gain of stem cell-like features. In prostate cancer (PCa), androgen receptor (AR) signaling is important for cancer growth, progression, and emergence of therapy resistance. Targeting the AR signaling axis has been, over the decades, the mainstay of PCa therapy. However, AR signaling at the transcription level is reduced in high-grade cancer relative to low-grade PCa and loss of AR expression promotes a stem cell-like phenotype, suggesting that emergence of resistance to AR-targeted therapy may be associated with loss of AR signaling and gain of stemness. In the present mini-review, we first discuss PCa from the perspective of an abnormal organ with increasingly deregulated differentiation, and discuss the role of AR signaling during PCa progression. We then focus on the relationship between prostate cancer stem cells (PCSCs) and AR signaling. We further elaborate on the current methods of using transcriptome-based stemness-enriched signature to evaluate the degree of oncogenic dedifferentiation (cancer stemness) in pan-cancer datasets, and present the clinical significance of scoring transcriptome-based stemness across the spectrum of PCa development. Our discussions highlight the importance to evaluate the dynamic changes in both stem cell-like features (stemness score) and AR signaling activity across the PCa spectrum.

摘要

癌症的进展以逐渐丧失分化表型和获得干细胞样特征为特征和驱动。在前列腺癌 (PCa) 中,雄激素受体 (AR) 信号对癌症的生长、进展和治疗耐药性的出现很重要。靶向 AR 信号轴几十年来一直是 PCa 治疗的主要方法。然而,与低级别 PCa 相比,高级别癌症中 AR 信号在转录水平上降低,并且 AR 表达的丧失促进了干细胞样表型,这表明 AR 靶向治疗的耐药性的出现可能与 AR 信号的丧失和干性的获得有关。在本综述中,我们首先从分化失调日益严重的异常器官的角度讨论 PCa,并讨论 AR 信号在 PCa 进展过程中的作用。然后,我们将重点放在前列腺癌干细胞 (PCSC) 和 AR 信号之间的关系上。我们进一步详细阐述了目前使用基于转录组的干性富集特征来评估泛癌数据集癌基因去分化程度 (癌症干性) 的方法,并提出了在整个 PCa 发展过程中基于转录组的干性评分的临床意义。我们的讨论强调了评估整个 PCa 谱中干细胞样特征 (干性评分) 和 AR 信号活性的动态变化的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a0b6/9484140/a8f0f647586a/ebc-66-ebc20220003-g1.jpg

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