New Uracil Analog with Exocyclic Methylidene Group Can Reverse Resistance to Taxol in MCF-7 Cancer Cells.

IF 5.3 Q1 MEDICINE, RESEARCH & EXPERIMENTAL Biologics : Targets & Therapy Pub Date : 2023-01-01 DOI:10.2147/BTT.S405080
Angelika Długosz-Pokorska, Renata Perlikowska, Tomasz Janecki, Anna Janecka
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Abstract

Introduction: Taxol (Tx), a microtubule-stabilizing drug, has been widely used as a chemotherapeutic in several types of cancer. However, the development of resistance limited its application. One of the strategies used to prevent the emergence of drug resistance is combination treatment, involving at least two drugs. The aim of the current study was to assess if a new uracil analog, 3-p-bromophenyl-1-ethyl-5-methylidenedihydrouracil (U-359) can prevent the development of Tx resistance in breast cancer cells.

Methods: The cytotoxicity of the new drug was tested in MCF-7 (hormone receptor (ER, PR) positive cell-line) and MCF-10A cell lines using MTT method. For the detection of apoptosis and necrosis, the Wright and Giemsa staining was used. Gene expression was measured by real-time PCR, and changes in the protein levels were evaluated by ELISA and bioluminescent method.

Results: We investigated the effect of Tx and U-359 on cancer MCF-7 and normal MCF-10A cells alone and in combination. Tx co-administered with U-359 inhibited proliferation of MCF-7 cells to 7% while the level of ATPase drastically decreased to 14%, compared with effects produced by Tx alone. The apoptosis process was induced through the mitochondrial pathway. These effects were not seen in MCF-10A cells, showing the wide safety margin. The obtained results have shown that U-359 produced a synergistic effect with Tx probably by reducing Tx resistance in MCF-7 cells. To elucidate the possible mechanism of resistance, expression of tubulin III (TUBIII), responsible for microtubule stabilization and tau and Nlp proteins, responsible for microtubule dynamics, was assessed.

Conclusion: Combination of Tx with U-359 reduced overexpression of TUBIII and Nlp. Thus, U-359 may stand for a potential reversal agent for the treatment of MDR in cancer cells.

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含有外环亚甲基的新型尿嘧啶类似物可逆转MCF-7癌细胞对紫杉醇的耐药性。
紫杉醇(Tx)是一种微管稳定药物,已被广泛用于多种癌症的化疗。然而,耐药性的发展限制了其应用。用于防止耐药性出现的策略之一是联合治疗,涉及至少两种药物。目前研究的目的是评估一种新的尿嘧啶类似物,3-对溴苯基-1-乙基-5-甲基二氢尿嘧啶(U-359)是否可以预防乳腺癌细胞中Tx耐药性的发展。方法:采用MTT法在MCF-7(激素受体(ER, PR)阳性细胞系)和MCF-10A细胞系中检测新药的细胞毒性。采用Wright和Giemsa染色法检测细胞凋亡和坏死。实时荧光定量PCR检测基因表达,ELISA和生物荧光法检测蛋白水平变化。结果:我们研究了Tx和U-359对肿瘤MCF-7和正常MCF-10A细胞单独和联合作用的影响。与单独使用Tx相比,Tx与U-359联合使用对MCF-7细胞的增殖抑制率为7%,而atp酶水平则急剧下降至14%。凋亡过程是通过线粒体途径诱导的。这些影响在MCF-10A细胞中未见,显示出较宽的安全范围。结果表明,U-359可能通过降低MCF-7细胞对Tx的抗性而与Tx产生协同作用。为了阐明可能的耐药机制,我们评估了负责微管稳定的微管蛋白III (TUBIII)和负责微管动力学的tau和Nlp蛋白的表达。结论:Tx联合U-359可降低TUBIII和Nlp的过表达。因此,U-359可能代表着一种潜在的逆转剂,用于治疗癌症细胞中的耐多药。
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来源期刊
Biologics : Targets & Therapy
Biologics : Targets & Therapy MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
8.30
自引率
0.00%
发文量
22
审稿时长
16 weeks
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