Enhanced induction of apoptosis in chronic myeloid leukemia cells through synergistic effect of telomerase inhibitor MST-312 and imatinib.

IF 2.6 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular Biology Reports Pub Date : 2024-11-17 DOI:10.1007/s11033-024-10074-x
Najibe Karami, Amir Abbas Navidinia, Mohsen Ehsan, Alireza Farsinejad, Ahmad Fatemi
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Abstract

Background: Chronic Myeloid Leukemia (CML), accounting for 15-20% of adult leukemia cases, is marked by the Philadelphia chromosome, resulting from the t(9;22)(q34;q11) translocation. This leads to uncontrolled cell proliferation and survival. Imatinib therapy lowers BCR-ABL levels, influencing telomere-associated proteins and increasing telomerase accessibility, indirectly boosting its activity. This study investigates the effects of MST-312 and imatinib, both individually and combined, on a CML cell line.

Methods: The K562 cells were subjected to different doses of MST-312 and imatinib, including four combination concentrations. Cell viability and metabolic activity were measured using trypan blue and MTT assays at 24-, 36-, and 48-h post-treatment. Flow cytometry (AnnexinV/PI) assessed cell apoptosis after 36 h of treatment with MST-312 and imatinib, both individually and in combination. The expression levels of Bax, Bcl-2, hTERT, P21, P53, and c-Myc were determined via qRT-PCR.

Results: Both MST-312 and imatinib independently reduced cell viability in a dose- and time-dependent manner. Their combination further decreased cell viability compared to monotherapy. Treatment of K562 cells with MST-312 and imatinib for 36 h increased Bax expression and the Bax/Bcl-2 ratio while decreasing Bcl-2 expression. Combined treatment significantly reduced hTERT ansd P21 gene expression compared to imatinib alone.

Conclusions: The combination of MST-312 and imatinib shows potential as a CML therapy. However, further research and clinical trials are necessary to validate these findings and determine their clinical relevance.

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端粒酶抑制剂MST-312和伊马替尼的协同作用增强了对慢性髓性白血病细胞凋亡的诱导。
背景:慢性粒细胞白血病(CML)占成人白血病病例的 15-20%,其特征是费城染色体由 t(9;22)(q34;q11)易位产生。这导致细胞增殖和存活失控。伊马替尼疗法可降低BCR-ABL水平,影响端粒相关蛋白,增加端粒酶的可及性,间接提高端粒酶的活性。本研究探讨了MST-312和伊马替尼单独或联合使用对CML细胞系的影响:方法:对 K562 细胞使用不同剂量的 MST-312 和伊马替尼,包括四种组合浓度。在处理后 24、36 和 48 小时,使用胰蓝和 MTT 检测法测量细胞活力和代谢活性。流式细胞术(AnnexinV/PI)评估了单独或联合使用 MST-312 和伊马替尼治疗 36 小时后的细胞凋亡情况。通过 qRT-PCR 测定 Bax、Bcl-2、hTERT、P21、P53 和 c-Myc 的表达水平:结果:MST-312和伊马替尼均以剂量和时间依赖的方式降低了细胞活力。与单药治疗相比,这两种药物联合使用可进一步降低细胞活力。用MST-312和伊马替尼处理K562细胞36小时后,Bax表达和Bax/Bcl-2比值增加,而Bcl-2表达减少。与单独使用伊马替尼相比,联合治疗可明显降低hTERT和P21基因的表达:结论:MST-312和伊马替尼的联合治疗显示了作为CML疗法的潜力。结论:MST-312和伊马替尼的联合治疗显示出作为CML疗法的潜力,但还需要进一步的研究和临床试验来验证这些发现并确定其临床相关性。
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来源期刊
Molecular Biology Reports
Molecular Biology Reports 生物-生化与分子生物学
CiteScore
5.00
自引率
0.00%
发文量
1048
审稿时长
5.6 months
期刊介绍: Molecular Biology Reports publishes original research papers and review articles that demonstrate novel molecular and cellular findings in both eukaryotes (animals, plants, algae, funghi) and prokaryotes (bacteria and archaea).The journal publishes results of both fundamental and translational research as well as new techniques that advance experimental progress in the field and presents original research papers, short communications and (mini-) reviews.
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