Jitender Singh, Krishan Lal Khanduja, Divya Dahiya, Pramod K Avti
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Gene and protein expression analysis in the normal vs BC and across age groups and major subclasses reveals divergent patterns as EGFR and HER-2 levels are reduced in tumors versus normal tissue, while ER and PR levels are higher, particularly in luminal subtypes. However, there was no significant difference in survival rates among high and low/medium expression levels of EGFR and PR receptors. Conversely, patients with high HER-2 and ER expression exhibited poorer survival rates compared to low or medium expression levels. The in vitro findings indicate that Dabrafenib exhibits greater effectiveness than Palbociclib in suppressing various BC cells such as MCF-7 (Luminal), MDA-MB-231 (Triple-Negative), SKBR-3 (HER-2 + ) proliferation, promoting cell death, (IC<sub>50</sub> of Dab < Pal) at 24 and 48 h, ROS production, and reduced ER and PR, elevated HER-2 with no change in EGFR expression. Molecular simulation studies revealed Dabrafenib's thermodynamically stable interactions (ΔG), tighter binding, and less structural deviation in the order EGFR > HER-2 > ER > PR as compared to Palbociclib (HER-2 > ER > PR = EGFR). 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引用次数: 0
摘要
乳腺癌(BC)中生长因子(表皮生长因子受体、HER-2)和激素(ER、PR)受体的差异表达模式对于评估和调整治疗干预措施至关重要。本研究调查了乳腺癌患者体内激素和生长因子受体的不同表达谱,以及不同年龄组、主要亚类、疾病分期、肿瘤组织学和生存率、新兴临床试验药物(Dabrafenib 和 Palbociclib)的疗效,并阐明其分子相互作用机制,以制定有效的治疗策略。正常组织与 BC 组织的基因和蛋白质表达分析,以及不同年龄组和主要亚类的基因和蛋白质表达分析,揭示了不同的模式,即肿瘤组织中表皮生长因子受体(EGFR)和 HER-2 水平较正常组织低,而 ER 和 PR 水平较高,尤其是在管腔亚型中。不过,表皮生长因子受体和 PR 受体的高表达水平和低/中等表达水平的患者在生存率方面没有明显差异。相反,HER-2和ER高表达患者的存活率比低或中等表达水平的患者低。体外研究结果表明,Dabrafenib比Palbociclib更能抑制MCF-7(Luminal)、MDA-MB-231(Triple-Negative)、SKBR-3(HER-2 +)等多种BC细胞的增殖,促进细胞死亡(Dab的IC50小于Pal)(24小时和48小时)、ROS产生、降低ER和PR、升高HER-2,而EGFR表达无变化。分子模拟研究显示,与 Palbociclib(HER-2 > ER > PR = EGFR)相比,Dabrafenib 的相互作用(ΔG)热力学稳定,结合更紧密,EGFR > HER-2 > ER > PR 的结构偏差更小。这些结果表明,与 Palbociclib 相比,Dabrafenib 能通过与激素和生长因子受体的特异性相互作用,更有效地调节乳腺癌细胞的增殖,从而实现再利用。
Mechanistic Regulation of Epidermal Growth Factor and Hormonal Receptors by Kinase Inhibitors and Organofluorines in Breast Cancer Therapy.
Differential expression patterns of growth factor (EGFR, HER-2) and hormonal (ER, PR) receptors in breast cancer (BC) remain crucial for evaluating and tailoring therapeutic interventions. This study investigates differential expression profiles of hormonal and growth factor receptors in BC patients and across age groups, major subclasses, disease stages and tumor histology and survival rates, the efficacy of emerging clinical trial drugs (Dabrafenib and Palbociclib) and elucidating their molecular interaction mechanisms for efficient therapeutic strategies. Gene and protein expression analysis in the normal vs BC and across age groups and major subclasses reveals divergent patterns as EGFR and HER-2 levels are reduced in tumors versus normal tissue, while ER and PR levels are higher, particularly in luminal subtypes. However, there was no significant difference in survival rates among high and low/medium expression levels of EGFR and PR receptors. Conversely, patients with high HER-2 and ER expression exhibited poorer survival rates compared to low or medium expression levels. The in vitro findings indicate that Dabrafenib exhibits greater effectiveness than Palbociclib in suppressing various BC cells such as MCF-7 (Luminal), MDA-MB-231 (Triple-Negative), SKBR-3 (HER-2 + ) proliferation, promoting cell death, (IC50 of Dab < Pal) at 24 and 48 h, ROS production, and reduced ER and PR, elevated HER-2 with no change in EGFR expression. Molecular simulation studies revealed Dabrafenib's thermodynamically stable interactions (ΔG), tighter binding, and less structural deviation in the order EGFR > HER-2 > ER > PR as compared to Palbociclib (HER-2 > ER > PR = EGFR). These results indicate that Dabrafenib, compared to Palbociclib, more effectively regulates breast cancer cell proliferation through specific interactions with hormonal and growth factor receptors towards a repurposing approach.
期刊介绍:
Cell Biochemistry and Biophysics (CBB) aims to publish papers on the nature of the biochemical and biophysical mechanisms underlying the structure, control and function of cellular systems
The reports should be within the framework of modern biochemistry and chemistry, biophysics and cell physiology, physics and engineering, molecular and structural biology. The relationship between molecular structure and function under investigation is emphasized.
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