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Destabilization of Bcr-Abl/Jak2 Network by a Jak2/Abl Kinase Inhibitor ON044580 Overcomes Drug Resistance in Blast Crisis Chronic Myelogenous Leukemia (CML)

机译：Jak2 / Abl激酶抑制剂ON044580破坏Bcr-Abl / Jak2网络的稳定性克服了爆炸性危机慢性粒细胞性白血病（CML）中的耐药性

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Bcr-Abl is the predominant therapeutic target in chronic myeloid leukemia (CML), and tyrosine kinase inhibitors (TKIs) that inhibit Bcr-Abl have been successful in treating CML. With progression of CML disease especially in blast crisis stage, cells from CML patients become resistant to imatinib mesylate (IM) and other TKIs, resulting in relapse. Because Bcr-Abl is known to drive multiple signaling pathways, the study of the regulation of stability of Bcr-Abl in IM-resistant CML cells is a critical issue as a possible therapeutic strategy. Here, we report that a new dual-kinase chemical inhibitor, ON044580, induced apoptosis of Bcr-Abl+ IM-sensitive, IM-resistant cells, including the gatekeeper Bcr-Abl mutant, T315I, and also cells from blast crisis patients. In addition, IM-resistant K562-R cells, cells from blast crisis CML patients, and all IM-resistant cell lines tested had reduced ability to form colonies in soft agar in the presence of 0.5 µM ON044580. In in vitro kinase assays, ON044580 inhibited the recombinant Jak2 and Abl kinase activities when the respective Jak2 and Abl peptides were used as substrates. Incubation of the Bcr-Abl+ cells with ON044580 rapidly reduced the levels of the Bcr-Abl protein and also reduced the expression of HSP90 and its client protein levels. Lysates of Bcr-Abl+ cell lines were found to contain a large signaling network complex composed of Bcr-Abl, Jak2, HSP90, and its client proteins as detected by a gel filtration column chromatography, which was rapidly disrupted by ON044580. Therefore, targeting Jak2 and Bcr-Abl kinases is an effective way to destabilize Bcr-Abl and its network complex, which leads to the onset of apoptosis in IM-sensitive and IM-resistant Bcr-Abl+ cells. This inhibitory strategy has potential to manage all types of drug-resistant CML cells, especially at the terminal blast crisis stage of CML, where TKIs are not clinically useful.

机译：Bcr-Abl是慢性粒细胞白血病（CML）的主要治疗靶标，抑制Bcr-Abl的酪氨酸激酶抑制剂（TKIs）已成功治疗CML。随着CML疾病的发展，尤其是在原始危机时期，来自CML患者的细胞对甲磺酸伊马替尼（IM）和其他TKI产生抗性，导致复发。由于已知Bcr-Abl可以驱动多个信号通路，因此对IM耐药性CML细胞中Bcr-Abl稳定性的调节研究作为可能的治疗策略是一个至关重要的问题。在这里，我们报道了一种新型的双激酶化学抑制剂ON044580诱导了Bcr-Abl + IM敏感，IM耐药细胞的凋亡，包括Gatekeeper Bcr-Abl突变体T315I，以及来自高危危机患者的细胞。此外，在存在0.5 µM ON044580的情况下，耐IM的K562-R细胞，来自原始危机CML患者的细胞以及所有经过测试的耐IM的细胞系在软琼脂中形成菌落的能力均降低。在体外激酶测定中，当将各自的Jak2和Abl肽用作底物时，ON044580抑制了重组Jak2和Abl激酶的活性。将Bcr-Abl +细胞与ON044580一起孵育会迅速降低Bcr-Abl蛋白的水平，并且还会降低HSP90的表达及其客户蛋白的水平。发现Bcr-Abl +细胞系的裂解物含有由Bcr-Abl，Jak2，HSP90及其客户蛋白质组成的大型信号网络复合物，通过凝胶过滤柱色谱法检测到，该复合物被ON044580迅速破坏。因此，靶向Jak2和Bcr-Abl激酶是使Bcr-Abl及其网络复合物不稳定的有效方法，这会导致IM敏感和IM抵抗Bcr-Abl +细胞凋亡的开始。这种抑制策略具有处理所有类型的耐药性CML细胞的潜力，尤其是在TML在临床上无用的CML的细胞爆炸初期阶段。

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Samanta, Ajoy K.; Chakraborty, Sandip N.; Wang, Yan; Schlette, Ellen; Reddy, E. Premkumar; Arlinghaus, Ralph B.;
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2. Activation of Jak2 in patients with blast crisis chronic myelogenous leukemia: inhibition of Jak2 inactivates Lyn kinase [J] . S Chakraborty, Y-H Lin, X Leng, Blood cancer journal. . 2013,第9期

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3. Graft-versus-Leukemia (GVL) against Mouse Blast-Crisis Chronic Myelogenous Leukemia (BC-CML) and Chronic-Phase Chronic Myelogenous Leukemia (CP-CML): Shared Mechanisms of T Cell Killing, but Programmed Death Ligands Render CP-CML and Not BC-CML GVL Resistant [J] . Catherine Matte-Martone, Srividhya Venkatesan, Hung Sheng Tan, The journal of immunology . 2011,第4期

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4. Controlled Cellular Delivery of Bcr-Abl Coiled-Coil Domain for Apoptosis of Chronic Myelogenous Leukemia Cells [C] . Mudit Kakar, James R. Davis, Carol S. Lim Controlled Release Society Annual Meeting and Exposition . 2007

机译：慢性骨髓性白血病细胞凋亡的Bcr-Abl螺旋线圈结构域的受控细胞传递。
5. Transcriptional and Proteomic Changes Associated with the Sensitivity and Resistance to JAK2 Inhibitors: Implications for the Treatment of BCR-ABL (-) Myeloproliferative Neoplasms (MPNs). [D] . McDevitt, Theresa Marie. 2012

机译：与JAK2抑制剂的敏感性和抗性相关的转录和蛋白质组学变化：对BCR-ABL（-）骨髓增生性肿瘤（MPNs）的治疗意义。
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机译：Jak2 / Abl激酶抑制剂ON044580破坏Bcr-Abl / Jak2网络的稳定性克服了爆炸性危机慢性粒细胞性白血病（CML）中的耐药性
7. Multiple BCR-ABL kinase domain mutations confer polyclonal resistance to the tyrosine kinase inhibitor imatinib (STI571) in chronic phase and blast crisis chronic myeloid leukemia [O] . Shah Neil P., Nicoll John M., Nagar Bhushan, 2002

机译：多个BCR-ABL激酶结构域突变在慢性期和胚芽危机性慢性粒细胞白血病中赋予酪氨酸激酶抑制剂伊马替尼（STI571）多克隆耐药性
8. BCR-ABL Kinase Activity-Independent Signaling Pathway in Chronic Myelogenous Leukemia; Final rept. 1 Feb 2006-31 Jan 2008 [R] . Li, S. 2008

机译：BCR-aBL激酶活性独立信号通路在慢性粒细胞白血病中的作用;最终报告2006年2月1日至2008年1月31日

Destabilization of Bcr-Abl/Jak2 Network by a Jak2/Abl Kinase Inhibitor ON044580 Overcomes Drug Resistance in Blast Crisis Chronic Myelogenous Leukemia (CML)

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