c-Myc 抑制和 p21 调节有助于非对称双吖啶诱导胰腺癌细胞凋亡和衰老。

IF 3.6 3区 医学 Q2 PHARMACOLOGY & PHARMACY
Agnieszka Kurdyn, Monika Pawłowska, Ewa Paluszkiewicz, Mirosława Cichorek, Ewa Augustin
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引用次数: 0

摘要

背景:胰腺癌(PC)是侵袭性最强的癌症之一,也是全球第七大癌症致死原因。胰腺癌的特点是进展迅速和对常规治疗产生抗药性。KRAS、CDKN2A、TP53、SMAD4/DPC4 和 MYC 基因突变是与 PC 患者治疗效果不佳相关的主要基因改变。因此,优化 PC 治疗是一项巨大的挑战。我们小组合成的不对称双吖啶(UAs)是一种新的有前途的化合物,对包括胰腺癌在内的多种实体瘤具有很高的细胞毒性和抗肿瘤活性:方法:通过 MTT 试验(细胞生长抑制)、流式细胞术、荧光和光学显微镜(细胞周期分布、细胞凋亡和衰老检测)评估 UAs 对 PC 细胞的细胞效应。用 Western 印迹法分析了 UAs 对蛋白质(c-Myc、p53、SMAD4、p21 和 p16)水平的影响:c-Myc是UAs的分子靶标之一,能以与p53无关的方式参与诱导细胞死亡。此外,UAs 还能通过 p21 的上调诱导加速衰老。值得注意的是,衰老细胞在长期接触 UAs 后可通过凋亡死亡:UAs已成为一种有效的抗癌剂,它通过抑制c-Myc蛋白诱导细胞凋亡,并通过提高p21水平以剂量依赖的方式引发细胞衰老。因此,UAs 具有理想的特性,有望成为未来胰腺癌抗癌疗法的候选药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
c-Myc inhibition and p21 modulation contribute to unsymmetrical bisacridines-induced apoptosis and senescence in pancreatic cancer cells.

Background: Pancreatic cancer (PC) is one of the most aggressive cancers and is the seventh leading cause of cancer-related death worldwide. PC is characterized by rapid progression and resistance to conventional treatments. Mutations in KRAS, CDKN2A, TP53, SMAD4/DPC4, and MYC are major genetic alterations associated with poor treatment outcomes in patients with PC. Therefore, optimizing PC therapy is a tremendous challenge. Unsymmetrical bisacridines (UAs), synthesized by our group, are new promising compounds that have exhibited high cytotoxicity and antitumor activity against several solid tumors, including pancreatic cancer.

Methods: The cellular effects induced by UAs in PC cells were evaluated by MTT assay (cell growth inhibition), flow cytometry, and fluorescence and light microscopy (cell cycle distribution, apoptosis, and senescence detection). Analysis of the effects of UAs on the levels of proteins (c-Myc, p53, SMAD4, p21, and p16) was performed by Western blotting.

Results: Apoptosis was the main triggered mechanism of death after UAs treatment, and induction of the SMAD4 protein can facilitate this process. c-Myc, which is one of the molecular targets of UAs, can participate in the induction of cell death in a p53-independent manner. Moreover, UAs can also induce accelerated senescence through the upregulation of p21. Notably, senescent cells can die via apoptosis after prolonged exposure to UAs.

Conclusions: UAs have emerged as potent anticancer agents that induce apoptosis by inhibiting c-Myc protein and triggering cellular senescence in a dose-dependent manner by increasing p21 levels. Thus, UAs exhibit desirable features as promising candidates for future pancreatic anticancer therapies.

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来源期刊
Pharmacological Reports
Pharmacological Reports 医学-药学
CiteScore
8.40
自引率
0.00%
发文量
91
审稿时长
6 months
期刊介绍: Pharmacological Reports publishes articles concerning all aspects of pharmacology, dealing with the action of drugs at a cellular and molecular level, and papers on the relationship between molecular structure and biological activity as well as reports on compounds with well-defined chemical structures. Pharmacological Reports is an open forum to disseminate recent developments in: pharmacology, behavioural brain research, evidence-based complementary biochemical pharmacology, medicinal chemistry and biochemistry, drug discovery, neuro-psychopharmacology and biological psychiatry, neuroscience and neuropharmacology, cellular and molecular neuroscience, molecular biology, cell biology, toxicology. Studies of plant extracts are not suitable for Pharmacological Reports.
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