PI3K/AKT赋予慢性淋巴细胞白血病患者对吡咯替尼的内在耐药性和获得性耐药性

IF 2.1 4区医学 Q3 HEMATOLOGY

Leukemia research Pub Date : 2024-07-07 DOI:10.1016/j.leukres.2024.107548

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引用次数: 0

摘要

目的皮罗布替尼是一种非共价布鲁顿酪氨酸激酶（BTK）抑制剂，已被批准作为克服共价BTK抑制剂（如伊布替尼、阿卡布替尼和扎努布替尼）耐药性的第一种药物。为了研究吡咯替尼的耐药性，我们通过 CRISPR-Cas9 敲除 BTK 或在 MEC-1 细胞中长期暴露于吡咯替尼，建立了耐药细胞模型。这些模型分别模拟了内在或获得性耐药性。然后，我们使用反相蛋白质微阵列（RPPA）分析了野生型（WT）和耐药 MEC-1 细胞之间的蛋白质表达差异，并通过 Western 印迹证实了这些发现。此外，我们还使用敏感和耐药细胞进行了细胞增殖试验、细胞凋亡研究和动物实验，评估了克服皮特鲁替尼耐药性的潜在药物。RPPA分析显示，耐药细胞中与PI3K/AKT通路相关的蛋白（包括AKT和S6）被显著激活。Western Blot证实，在对吡咯替尼耐药的MEC-1细胞中，AKT和S6的磷酸化增加。值得注意的是，PI3K 抑制剂（CAL101）和 AKT 抑制剂（MK2206）都能有效减少耐药细胞的增殖并诱导细胞凋亡。这些药物的抗肿瘤功效是通过抑制 PI3K/AKT 通路介导的。体内动物实验进一步证实，靶向 PI3K/AKT 有可能克服皮特鲁替尼的内在耐药性和获得性耐药性。以该通路为治疗靶点可能是克服皮特鲁替尼耐药性的一种有前途的策略。

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PI3K/AKT confers intrinsic and acquired resistance to pirtobrutinib in chronic lymphocytic leukemia

Purpose

Pirtobrutinib, a non-covalent Bruton’s tyrosine kinase (BTK) inhibitor, has been approved as the first agent to overcome resistance to covalent BTK inhibitors (such as ibrutinib, acalabrutinib, and zanubrutinib). However, the mechanisms of pirtobrutinib resistance in chronic lymphocytic leukemia (CLL) remain poorly understood.

Methods

To investigate pirtobrutinib resistance, we established resistant cell models using BTK knock-out via CRISPR-Cas9 or chronic exposure to pirtobrutinib in MEC-1 cells. These models mimicked intrinsic or acquired resistance, respectively. We then analyzed differential protein expression between wild-type (WT) and resistant MEC-1 cells using Revers Phase Protein microArray (RPPA) and confirmed the findings through Western Blot. Additionally, we evaluated potential drugs to overcome pirtobrutinib resistance by conducting cell proliferation assays, apoptosis studies, and animal experiments using both sensitive and resistant cells.

Results

MEC-1 cells developed resistance to pirtobrutinib either through BTK knock-out or prolonged drug exposure over three months. RPPA analysis revealed significant activation of proteins related to the PI3K/AKT pathway, including AKT and S6, in the resistant cells. Western Blot confirmed increased phosphorylation of AKT and S6 in pirtobrutinib-resistant MEC-1 cells. Notably, both the PI3K inhibitor (CAL101) and the AKT inhibitor (MK2206) effectively reduced cell proliferation and induced apoptosis in the resistant cells. The anti-tumor efficacy of these drugs was mediated by inhibiting the PI3K/AKT pathway. In vivo animal studies further supported the potential of targeting PI3K/AKT to overcome both intrinsic and acquired resistance to pirtobrutinib.

Conclusion

The PI3K/AKT pathway plays a crucial role in both intrinsic and acquired resistance to pirtobrutinib in CLL. Therapeutically targeting this pathway may offer a promising strategy to overcome pirtobrutinib resistance.

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来源期刊

Leukemia research 医学-血液学

CiteScore

4.00

自引率

3.70%

发文量

259

审稿时长

1 months

期刊介绍： Leukemia Research an international journal which brings comprehensive and current information to all health care professionals involved in basic and applied clinical research in hematological malignancies. The editors encourage the submission of articles relevant to hematological malignancies. The Journal scope includes reporting studies of cellular and molecular biology, genetics, immunology, epidemiology, clinical evaluation, and therapy of these diseases.