A quiescence-like/TGF-β1-specific CRISPRi screen reveals drug uptake transporters as secondary targets of kinase inhibitors in AML

IF 22 1区医学 Q1 PHARMACOLOGY & PHARMACY Drug Resistance Updates Pub Date : 2025-07-01 Epub Date: 2025-03-28 DOI:10.1016/j.drup.2025.101242

Elahe Rahimian , Masoud Koochak , Sofia Traikov , Michael Schroeder , Silke Brilloff , Silvia Schäfer , Vida Kufrin , Sandra Küchler , Alexander Krüger , Peter Mirtschink , Gustavo Baretton , Evelin Schröck , Denis M. Schewe , Claudia R. Ball , Martin Bornhäuser , Hanno Glimm , Marius Bill , Alexander A. Wurm

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Abstract

Relapse in acute myeloid leukemia (AML) is driven by resistant subclones that survive chemotherapy. It is assumed that these resilient leukemic cells can modify their proliferative behavior by entering a quiescent-like state, similar to healthy hematopoietic stem cells (HSCs). These dormant cells can evade the effects of cytostatic drugs that primarily target actively dividing cells. Although quiescence has been extensively studied in healthy hematopoiesis and various solid cancers, its role in AML has remained unexplored.

In this study, we applied an HSC-derived quiescence-associated gene signature to an AML patient cohort and found it to be strongly correlated with poor prognosis and active TGF-β signaling. In vitro treatment with TGF-β1 induces a quiescence-like phenotype, resulting in a G0 shift and reduced sensitivity to cytarabine. To find potential therapeutic targets that prevent AML-associated quiescence and improve response to cytarabine, we conducted a comprehensive CRISPR interference (CRISPRi) screen combined with TGF-β1 stimulation. This approach identified TGFBR1 inhibitors, like vactosertib, as effective agents for preventing the G0 shift in AML cell models. However, pretreatment with vactosertib unexpectedly induced complete resistance to cytarabine. To elucidate the underlying mechanism, we performed a multi-faceted approach combining a second CRISPRi screen, liquid chromatography-tandem mass spectrometry (LC-MS/MS), and in silico analysis. Our findings revealed that TGFBR1 inhibitors unintentionally target the nucleoside transporter SLC29A1 (ENT1), leading to reduced intracellular cytarabine levels. Importantly, we found that this drug interaction is not unique to TGFBR1 inhibitors, but extends to other clinically significant kinase inhibitors, such as the FLT3 inhibitor midostaurin. These findings may have important implications for optimizing combination therapies in AML treatment.

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静止样/TGF-β1特异性CRISPRi筛选显示药物摄取转运蛋白是AML中激酶抑制剂的次要靶点

急性髓性白血病（AML）的复发是由化疗后存活的耐药亚克隆驱动的。据推测，这些有弹性的白血病细胞可以通过进入类似于健康造血干细胞（hsc）的静息状态来改变其增殖行为。这些休眠细胞可以逃避主要针对活跃分裂细胞的细胞抑制剂的作用。尽管在健康造血和各种实体癌中已广泛研究了静息，但其在AML中的作用仍未被探索。在这项研究中，我们将hsc衍生的静止相关基因标记应用于AML患者队列，发现它与不良预后和活跃的TGF-β信号传导密切相关。TGF-β1在体外处理可诱导静止样表型，导致G0移位，降低对阿糖胞苷的敏感性。为了寻找潜在的治疗靶点，防止aml相关的静止，提高对阿糖胞苷的反应，我们进行了综合的CRISPR干扰（CRISPRi）筛选，并结合TGF-β1刺激。该方法确定TGFBR1抑制剂，如vactosertib，是防止AML细胞模型中G0转移的有效药物。然而，vactosertib预处理出人意料地诱导了对阿糖胞苷的完全耐药。为了阐明潜在的机制，我们进行了多方面的方法，结合了第二次CRISPRi筛选、液相色谱-串联质谱（LC-MS/MS）和硅分析。我们的研究结果表明，TGFBR1抑制剂无意中靶向核苷转运体SLC29A1 (ENT1)，导致细胞内阿糖胞苷水平降低。重要的是，我们发现这种药物相互作用并不是TGFBR1抑制剂所独有的，而是延伸到其他临床重要的激酶抑制剂，如FLT3抑制剂midostoin。这些发现可能对优化AML治疗中的联合疗法具有重要意义。

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来源期刊

Drug Resistance Updates 医学-药学

CiteScore

26.20

自引率

11.90%

发文量

审稿时长

29 days

期刊介绍： Drug Resistance Updates serves as a platform for publishing original research, commentary, and expert reviews on significant advancements in drug resistance related to infectious diseases and cancer. It encompasses diverse disciplines such as molecular biology, biochemistry, cell biology, pharmacology, microbiology, preclinical therapeutics, oncology, and clinical medicine. The journal addresses both basic research and clinical aspects of drug resistance, providing insights into novel drugs and strategies to overcome resistance. Original research articles are welcomed, and review articles are authored by leaders in the field by invitation. Articles are written by leaders in the field, in response to an invitation from the Editors, and are peer-reviewed prior to publication. Articles are clear, readable, and up-to-date, suitable for a multidisciplinary readership and include schematic diagrams and other illustrations conveying the major points of the article. The goal is to highlight recent areas of growth and put them in perspective. *Expert reviews in clinical and basic drug resistance research in oncology and infectious disease *Describes emerging technologies and therapies, particularly those that overcome drug resistance *Emphasises common themes in microbial and cancer research