Preclinical In Vitro Investigation of MDM2 Inhibition in Combination with Antiangiogenic Therapy for Breast Cancer Treatment

IF 2.3 Q3 PHARMACOLOGY & PHARMACY Scientia Pharmaceutica Pub Date : 2023-02-20 DOI:10.3390/scipharm91010012
A. Alaseem, Khalid Alhazzani, A. Z. Alanazi, Yasser Alqarni, M. Algahtani, A. Alhamed, Glowi A Alasiri, Fahad T. Alotaibi, Talha Jawaid, J. Aldali
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引用次数: 2

Abstract

Background: Combining antiangiogenic drugs with other chemotherapeutic drugs has been found to produce superior therapeutic outcomes and prevent drug resistance in a variety of cancers. Methods: Experimental assays such as the MTT assay, flow cytometry, western blotting, and qPCR have been used to evaluate the efficacy of combination therapy. Results: When compared to controls and monotherapies, the combination treatment of axitinib and idasanutlin demonstrated a substantial decrease in cell viability at lower doses, a significant decrease in migration, and a shift toward early and late apoptosis. This study examined major apoptotic, metastatic, and angiogenic factors, including MDM2, p21, BCL-2, BCL-XL, and MMP9, which have showed differential expressions at the protein and mRNA levels after combination. Axitinib and idasanutlin decreased tumorigenesis and migration in vitro in the MCF-7 cell line when compared to other chemotherapeutic medications. The suggested mechanisms of the antitumorigenic effect of the combination therapy may depend on its capacity to promote the production of apoptotic markers and reduce antiapoptotic markers. Conclusions: Treatments with axitinib and idasanutlin demonstrated effective therapeutic targeting of the primary angiogenic growth factor and, consequently, the pro-metastatic arbitrators. This will not only eliminate cancer cells but also stop other malignant processes and ultimately reduce the metastatic cascade.
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MDM2抑制联合抗血管生成治疗乳腺癌的临床前体外研究
背景:抗血管生成药物与其他化疗药物相结合已被发现可产生优越的治疗效果,并可预防各种癌症的耐药性。方法:采用MTT比色法、流式细胞术、免疫印迹法和qPCR等实验方法评价联合治疗的疗效。结果:与对照组和单一疗法相比,阿西替尼和伊达那素的联合治疗显示,在较低剂量下,细胞活力显著降低,迁移显著减少,并向早期和晚期凋亡转变。本研究检测了主要的凋亡、转移和血管生成因子,包括MDM2、p21、BCL-2、BCL-XL和MMP9,这些因子在组合后在蛋白质和mRNA水平上表现出差异表达。与其他化疗药物相比,Axitinib和idasanutlin在体外降低了MCF-7细胞系中的肿瘤发生和迁移。联合治疗的抗肿瘤作用的机制可能取决于其促进凋亡标志物产生和减少抗凋亡标志物的能力。结论:阿西替尼和伊达那素治疗显示出对原发性血管生成生长因子的有效治疗靶向性,从而对促转移仲裁者具有治疗作用。这不仅可以消灭癌症细胞,还可以阻止其他恶性过程,最终减少转移级联。
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来源期刊
Scientia Pharmaceutica
Scientia Pharmaceutica Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science
CiteScore
4.60
自引率
4.00%
发文量
67
审稿时长
10 weeks
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