JR-AB2-011 induces fast metabolic changes independent of mTOR complex 2 inhibition in human leukemia cells

IF 3.6 3区 医学 Q2 PHARMACOLOGY & PHARMACY Pharmacological Reports Pub Date : 2024-09-11 DOI:10.1007/s43440-024-00649-7
Tereza Kořánová, Lukáš Dvořáček, Dana Grebeňová, Kateřina Kuželová
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Abstract

Background

The mechanistic target of rapamycin (mTOR) is a crucial regulator of cell metabolic activity. It forms part of several distinct protein complexes, particularly mTORC1 and mTORC2. The lack of specific inhibitors still hampers the attribution of mTOR functions to these complexes. JR-AB2-011 has been reported as a specific mTORC2 inhibitor preventing mTOR binding to RICTOR, a unique component of mTORC2. We aimed to describe the effects of JR-AB2-011 in leukemia/lymphoma cells, where the mTOR pathway is often aberrantly activated.

Methods

The impact of JR-AB2-011 on leukemia/lymphoma cell metabolism was analyzed using the Seahorse platform. AKT phosphorylation at Ser473 was used as a marker of mTORC2 activity. mTOR binding to RICTOR was assessed by co-immunoprecipitation. RICTOR-null cells were derived from the Karpas-299 cell line using CRISPR/Cas9 gene editing.

Results

In leukemia/lymphoma cell lines, JR-AB2-011 induced a rapid drop in the cell respiration rate, which was variably compensated by an increased glycolytic rate. In contrast, an increase in the respiration rate due to JR-AB2-011 treatment was observed in primary leukemia cells. Unexpectedly, JR-AB2-011 did not affect AKT Ser473 phosphorylation. In addition, mTOR did not dissociate from RICTOR in cells treated with JR-AB2-011 under the experimental conditions used in this study. The effect of JR-AB2-011 on cell respiration was retained in RICTOR-null cells.

Conclusion

JR-AB2-011 affects leukemia/lymphoma cell metabolism via a mechanism independent of mTORC2.

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JR-AB2-011 在人类白血病细胞中诱导快速新陈代谢变化,与 mTOR 复合物 2 抑制无关
背景雷帕霉素机制靶标(mTOR)是细胞代谢活动的重要调节因子。它是几个不同蛋白质复合物的一部分,特别是 mTORC1 和 mTORC2。由于缺乏特异性抑制剂,mTOR 的功能仍无法归因于这些复合物。据报道,JR-AB2-011 是一种特异性 mTORC2 抑制剂,能阻止 mTOR 与 mTORC2 的独特成分 RICTOR 结合。我们的目的是描述 JR-AB2-011 在白血病/淋巴瘤细胞中的作用,因为在这些细胞中,mTOR 通路经常被异常激活。方法使用 Seahorse 平台分析了 JR-AB2-011 对白血病/淋巴瘤细胞代谢的影响。mTOR与RICTOR的结合通过共沉淀免疫法进行评估。结果在白血病/淋巴瘤细胞系中,JR-AB2-011诱导细胞呼吸速率迅速下降,而糖酵解速率的增加可不同程度地补偿这种下降。与此相反,在原代白血病细胞中观察到 JR-AB2-011 处理导致的呼吸速率增加。意外的是,JR-AB2-011 并未影响 AKT Ser473 磷酸化。此外,在本研究使用的实验条件下,用 JR-AB2-011 处理的细胞中,mTOR 没有与 RICTOR 分离。结论JR-AB2-011通过一种独立于mTORC2的机制影响白血病/淋巴瘤细胞的新陈代谢。
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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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