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Targeting the mitochondrial apoptosis pathway by a newly synthesized COX-2 inhibitor in pediatric ALL lymphocytes

机译:靶向细胞凋亡途径通过新合成的COX-2抑制剂在儿科所有淋巴细胞中

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Aim: Acute lymphoblastic leukemia (ALL) is known as a barely curable malignancy. Particular mutations involved in apoptosis may have a main role in the onset of ALL in the pediatric patients. It has been proven that cycloxygenase-2 is capable of impairing the apoptosis pathway through mitochondria in tumor cells. Methodology: In this study, we investigated selective toxicity of a newly synthesized chalconeferrocenyl derivative as a selective cycloxygenase-2 inhibitor in ALL and healthy B-lymphocytes, and also isolated mitochondria obtained from them. For this purpose, we evaluated the cellar parameters like viability, apoptosis/necrosis, caspase-3 activation and ATP content, and also mitochondrial parameters like mitochondrial membrane potential decline, reactive oxygen species formation, cytochrome C release and mitochondrial swelling. Conclusion: Our results implied that this compound can selectively induce cellular and mitochondrial toxicity in cancerous ALL B-lymphocytes and obtained mitochondria from them without any detrimental effects on healthy subjects.
机译:目的:急性淋巴细胞白血病(全部)被称为勉强可治愈的恶性肿瘤。参与细胞凋亡的特殊突变可能在儿科患者的发作中具有主要作用。已证明环氧基酶-2能够通过肿瘤细胞中的线粒体损害细胞凋亡途径。方法论:在本研究中,我们研究了新合成的核心酮转胶衍生物作为所有和健康B淋巴细胞的选择性环氧基酶-2抑制剂的选择性毒性,以及从它们中获得的分离的线粒体。为此目的,我们评估了可存活率,凋亡/坏死,Caspase-3激活和ATP含量等地窖参数,以及线粒体膜电位下降,反应性氧物种形成,细胞色素C释放和线粒体溶胀等线粒体参数。结论:我们的结果暗示,该化合物可以在癌症所有B淋巴细胞中选择性地诱导细胞和线粒体毒性,并从它们中获得线粒体,对健康受试者没有任何不利影响。

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