通过诱导 PERK/eIF2 介导的细胞凋亡，靶向 NLRP3 可抑制急性髓细胞白血病的进展。

IF 8.2 2区生物学 Q1 CELL BIOLOGY

Cell Communication and Signaling Pub Date : 2024-09-02 DOI:10.1186/s12964-024-01777-6

Michela Luciano, Helene Sieberer, Peter W Krenn, Hieu-Hoa Dang, Julia Vetter, Theresa Neuper, Diana Amend, Constantin Blöchl, Christian X Weichenberger, Anna Eglseer, Michael S Unger, Ancuela Andosch, Philip Steiner, Daniel Neureiter, Renate Bauer, Laura Hummer, Suzana Tesanovic, Stephanie Binder, Dominik P Elmer, Helen Strandt, Susanne Schaller, Dirk Strunk, Lisa Pleyer, Richard Greil, Stephan Winkler, Tanja N Hartmann, Dirk Schmidt-Arras, Christian G Huber, Fritz Aberger, Jutta Horejs-Hoeck

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引用次数: 0

摘要

背景：急性髓性白血病（AML）以髓系前体细胞异常增殖为特征，由于其异质性，给治疗带来了巨大挑战。最近，NLRP3 炎性体已成为急性髓性白血病发病机制的一个潜在因素，尽管人们对其确切机制仍知之甚少：方法：利用公共基因组数据集评估急性髓细胞性白血病患者与健康人相比NLRP3炎性体相关基因（IL-1β、IL-18、ASC和NLRP3）的表达情况。研究人员采用CRISPR/Cas9技术生成了NLRP3缺陷的MOLM-13 AML细胞，然后利用实时PCR、Western印迹、FACS分析、透射电子显微镜和免疫荧光显微镜进行了全面鉴定。通过蛋白质组学分析，确定了 NLRP3 依赖性蛋白水平的变化，重点是 eIF2 激酶 PERK 介导的信号通路。此外，还利用白血病小鼠模型进行了体内研究，以阐明NLRP3在急性髓细胞性白血病中的致病作用：结果：NLRP3的表达升高与急性髓细胞性白血病患者总生存期的缩短有明显关系。通过基因缺失、药物抑制和 RNA 干扰沉默 NLRP3 可诱导细胞凋亡，从而降低 AML 细胞的存活率。蛋白质组分析发现，NLRP3依赖性改变了蛋白质的翻译，其特征是在NLRP3缺陷的AML细胞中eIF2α磷酸化增强。此外，抑制 PERK 介导的 eIF2α 磷酸化可通过下调促凋亡的 Bcl-2 家族成员来减少细胞凋亡。体内研究表明，NLRP3基因敲除AML细胞接种小鼠的白血病负担减轻，白血病症状减轻就是证明：我们的研究结果阐明了NLRP3/PERK/eIF2轴是AML细胞存活的新型驱动因素。针对NLRP3诱导的信号通路，特别是通过PERK/eIF2轴，是一种很有前景的急性髓细胞性白血病干预治疗策略。这些关于 NLRP3 炎性体作用的见解为改善急性髓细胞性白血病患者的预后和治疗效果提供了潜在的途径。

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Targeting NLRP3 inhibits AML progression by inducing PERK/eIF2-mediated apoptosis.

Background: Acute myeloid leukemia (AML) is characterized by the abnormal proliferation of myeloid precursor cells and presents significant challenges in treatment due to its heterogeneity. Recently, the NLRP3 inflammasome has emerged as a potential contributor to AML pathogenesis, although its precise mechanisms remain poorly understood.

Methods: Public genome datasets were utilized to evaluate the expression of NLRP3 inflammasome-related genes (IL-1β, IL-18, ASC, and NLRP3) in AML patients compared to healthy individuals. CRISPR/Cas9 technology was employed to generate NLRP3-deficient MOLM-13 AML cells, followed by comprehensive characterization using real-time PCR, western blotting, FACS analysis, and transmission electron and immunofluorescence microscopy. Proteomic analyses were conducted to identify NLRP3-dependent alterations in protein levels, with a focus on the eIF2 kinase PERK-mediated signaling pathways. Additionally, in vivo studies were performed using a leukemic mouse model to elucidate the pathogenic role of NLRP3 in AML.

Results: Elevated expression of NLRP3 was significantly associated with diminished overall survival in AML patients. Genetic deletion, pharmacological inhibition and silencing by RNA interference of NLRP3 led to decreased AML cell survival through the induction of apoptosis. Proteomic analyses uncovered NLRP3-dependent alterations in protein translation, characterized by enhanced eIF2α phosphorylation in NLRP3-deficient AML cells. Moreover, inhibition of PERK-mediated eIF2α phosphorylation reduced apoptosis by downregulating pro-apoptotic Bcl-2 family members. In vivo studies demonstrated reduced leukemic burden in mice engrafted with NLRP3 knockout AML cells, as evidenced by alleviated leukemic symptoms.

Conclusion: Our findings elucidate the involvement of the NLRP3/PERK/eIF2 axis as a novel driver of AML cell survival. Targeting NLRP3-induced signaling pathways, particularly through the PERK/eIF2 axis, presents a promising therapeutic strategy for AML intervention. These insights into the role of the NLRP3 inflammasome offer potential avenues for improving the prognosis and treatment outcomes of AML patients.

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来源期刊

Cell Communication and Signaling CELL BIOLOGY-

CiteScore

11.00

自引率

0.00%

发文量

180

期刊介绍： Cell Communication and Signaling (CCS) is a peer-reviewed, open-access scientific journal that focuses on cellular signaling pathways in both normal and pathological conditions. It publishes original research, reviews, and commentaries, welcoming studies that utilize molecular, morphological, biochemical, structural, and cell biology approaches. CCS also encourages interdisciplinary work and innovative models, including in silico, in vitro, and in vivo approaches, to facilitate investigations of cell signaling pathways, networks, and behavior. Starting from January 2019, CCS is proud to announce its affiliation with the International Cell Death Society. The journal now encourages submissions covering all aspects of cell death, including apoptotic and non-apoptotic mechanisms, cell death in model systems, autophagy, clearance of dying cells, and the immunological and pathological consequences of dying cells in the tissue microenvironment.