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乳腺癌内分泌耐药:雌激素受体稳定性的作用。

Endocrine Resistance in Breast Cancer: The Role of Estrogen Receptor Stability.

机构信息

Centre for Circulating Tumour Cells Diagnostics & Research, Ingham Institute of Applied Medical Research, Liverpool NSW 2170, Australia.

School of Medicine, Western Sydney University, Campbelltown NSW 2560, Australia.

出版信息

Cells. 2020 Sep 11;9(9):2077. doi: 10.3390/cells9092077.

Abstract

Therapy of hormone receptor positive breast cancer (BCa) generally targets estrogen receptor (ER) function and signaling by reducing estrogen production or by blocking its interaction with the ER. Despite good long-term responses, resistance to treatment remains a significant issue, with approximately 40% of BCa patients developing resistance to ET. Mutations in the gene encoding ERα, , have been identified in BCa patients and are implicated as drivers of resistance and disease recurrence. Understanding the molecular consequences of these mutations on ER protein levels and its activity, which is tightly regulated, is vital. ER activity is in part controlled via its short protein half-life and therefore changes to its stability, either through mutations or alterations in pathways involved in protein stability, may play a role in therapy resistance. Understanding these connections and how alterations could affect protein stability may identify novel biomarkers of resistance. This review explores the current reported data regarding posttranslational modifications (PTMs) of the ER and the potential impact of known resistance associated mutations on ER regulation by affecting these PTMs in the context of ET resistance.

摘要

激素受体阳性乳腺癌 (BCa) 的治疗通常通过降低雌激素的产生或阻断其与 ER 的相互作用来靶向雌激素受体 (ER) 的功能和信号。尽管长期反应良好,但对治疗的耐药性仍然是一个重大问题,大约 40%的 BCa 患者对 ET 产生耐药性。在 BCa 患者中已经鉴定出编码 ERα 的基因中的突变,并且被认为是耐药性和疾病复发的驱动因素。了解这些突变对 ER 蛋白水平及其活性的分子后果至关重要,因为 ER 活性受到其短蛋白半衰期的严格调控,因此其稳定性的变化,无论是通过突变还是参与蛋白质稳定性的途径的改变,都可能在治疗耐药性中发挥作用。了解这些联系以及这些改变如何影响蛋白质稳定性,可能有助于确定耐药性的新型生物标志物。这篇综述探讨了目前关于 ER 的翻译后修饰 (PTMs) 的报道数据,以及在 ET 耐药性的背景下,已知的耐药相关突变通过影响这些 PTMs 对 ER 调节的潜在影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a2b/7564140/59561ba80cec/cells-09-02077-g001.jpg

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