Antiproliferation and apoptosis studies of estrone pharmacophores in triple-negative breast cancer

Felix Acheampong, Trevor Ostlund, Mater Mahnashi, Fathi Halaweish
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引用次数: 1

Abstract

Triple-negative breast cancer (TNBC) is an aggressive subtype of breast cancer that shows high metastatic capability and poor prognosis. The aggressive behavior of TNBC may involve amplified EGFR expression. Currently, no targeted therapy has been approved for treating TNBC, which urgently needs novel treatment options. In this study, we report that estrone analogs with novel pharmacophores exhibited high potency toward TNBC cells through multiple mechanisms, inhibition of cell proliferation via EGFR receptor, and induction of mitochondrial apoptosis. Molecular docking studies revealed that hit analogs MMA307 and MMA321 were potent against the EGFR receptor (pdb code: 1M17) in silico and were over 10-fold more potent than sorafenib (positive control) when dosed against MDA-MB-468 cells in vitro. MMA307 and MMA321 induced mitochondrial apoptosis as characterized by condensed nuclei with fragmented chromatin, phosphatidylserine flip and modulated expressions of Apaf1, cytochrome c, and caspases 3 and 9. MMA307 and MMA321 inhibited TNBC proliferation through suppression of EGFR and activated EGFR (Y1068) expressions. Similarly, EGFR signaling pathways, RAF/ERK and AKT/mTOR, were inhibited as pARaf, pERK1/2 (characterizes RAF/ERK pathway) and pAKT, pmTOR, p70S6Kα (characterizes AKT/mTOR pathway) were all suppressed. Moreover, MMA307 and MMA321 inhibited TNBC cell growth through downregulation of cyclin D1 expression and arresting TNBC cells in the G1 phase of cell cycle. This study reports for the first time that estrone congeners with novel pharmacophores may be an effective therapy for TNBC. Findings from this research provide a solid foundation for further preclinical and clinical studies in developing estrone derivatives as novel TNBC therapeutics.

Abstract Image

雌激素药效团在癌症三阴性乳腺癌中的抗增殖和凋亡研究。
癌症三阴性(TNBC)是癌症的一种侵袭性亚型,表现出高转移能力和不良预后。TNBC的攻击性行为可能涉及EGFR表达的扩增。目前,尚未批准靶向治疗TNBC,这迫切需要新的治疗方案。在本研究中,我们报道了具有新药效团的雌酮类似物通过多种机制对TNBC细胞表现出高效力,通过EGFR受体抑制细胞增殖,并诱导线粒体凋亡。分子对接研究表明,hit类似物MMA307和MMA21在体外对MDA-MB-468细胞给药时,对EGFR受体(pdb代码:1M17)的效力是索拉非尼(阳性对照)的10倍以上。MMA307和MMA21诱导线粒体凋亡,其特征是具有碎片化染色质的浓缩细胞核、磷脂酰丝氨酸翻转和调节Apaf1、细胞色素c以及胱天蛋白酶3和9的表达。MMA307和MMA21通过抑制EGFR和激活EGFR(Y1068)表达来抑制TNBC增殖。类似地,EGFR信号通路RAF/ERK和AKT/mTOR被抑制,因为pARaf、pERK1/2(表征RAF/ERK通路)和pAKT、pmTOR、p70S6Kα(表征AKT/mTOR通路)都被抑制。此外,MMA307和MMA21通过下调细胞周期蛋白D1的表达并将TNBC细胞阻滞在细胞周期的G1期来抑制TNBC细胞的生长。本研究首次报道具有新药效团的雌酮同源物可能是治疗TNBC的有效方法。这项研究的发现为进一步开发雌酮衍生物作为新型TNBC疗法的临床前和临床研究奠定了坚实的基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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