针对肺癌的新合成吖啶酮衍生物:毒性和异种移植模型研究。

IF 3.5 4区 医学 Q2 CHEMISTRY, MEDICINAL
Nilam Bhusare, Tanuja Yadav, Mukesh Nandave, Amruta Gadade, Vikas Dighe, Godefridus J. Peters, Maushmi S. Kumar, Mayur C. Yergeri
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引用次数: 0

摘要

AKT是非小细胞肺癌(NSCLC)中过度表达的靶点之一,在其进展过程中发挥着重要作用,是一个极具吸引力的治疗靶点。PI3K/AKT/mTOR通路在NSCLC中上调。吖啶酮是一种重要的杂环化合物,可通过各种机制治疗癌症,包括将 AKT 作为靶点。本研究旨在通过急性和重复剂量口服毒性评估三种吖啶酮衍生物(AC-2、AC-7 和 AC-26)的安全性。此外,我们还检测了这些衍生物在肿瘤异种移植模型中的 pAKT 过表达及其控制情况。急性和重复剂量毒性结果表明,这些化合物非常安全,没有任何毒性、死亡率或大鼠体重、食物和水摄入量的显著变化。在重复剂量毒性试验中,当剂量为 400 毫克/千克时,化合物在一些血液学参数上的变化可以忽略不计。组织病理学、生化和尿液参数保持不变。异种移植模型研究表明,AC-2 可通过显著降低 p-AKT1(Ser473)的表达来抑制 HOP-62 诱导的肿瘤。在免疫荧光染色中,AC-2 处理的组织切片显示 p-AKT1(Ser473)的表达降低了 2.5 倍。组织病理学研究显示,治疗后肿瘤细胞遭到破坏,坏死增加。研究认为,AC-2 通过阻断 p-AKT1 的表达导致肿瘤细胞坏死。这些发现为吖啶酮衍生物在 NSCLC 中的进一步临床应用提供了坚实的基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Newly synthesized acridone derivatives targeting lung cancer: A toxicity and xenograft model study

AKT is one of the overexpressed targets in nonsmall cell lung cancer (NSCLC) and plays an important role in its progression and offers an attractive target for the therapy. The PI3K/AKT/mTOR pathway is upregulated in NSCLC. Acridone is an important heterocycle compound which treats cancer through various mechanisms including AKT as a target. In the present work, the study was designed to evaluate the safety profile of three acridone derivatives (AC-2, AC-7, and AC-26) by acute and repeated dose oral toxicity. In addition to this, we also checked the pAKT overexpression and its control by these derivatives in tumor xenograft model. The results from acute and repeated dose toxicity showed these compounds to be highly safe and free from any toxicity, mortality, or significant alteration in body weight, food, and water intake in the rats. In the repeated dose toxicity, compounds showed negligible variations in a few hematological parameters at 400 mg/kg. The histopathology, biochemical, and urine parameters remained unchanged. The xenograft model study demonstrated AC-2 to be inhibiting HOP-62 induced tumor via reduction in p-AKT1 (Ser473) expression significantly. In immunofluorescence staining AC-2 treated tissue section showed 2.5 fold reduction in the expression of p-AKT1 (Ser473). Histopathology studies showed the destruction of tumor cells with increased necrosis after treatment. The study concluded that AC-2 causes cell necrosis in tumor cells via blocking the p-AKT1 expression. The findings may provide a strong basis for further clinical applications of acridone derivatives in NSCLC.

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来源期刊
CiteScore
6.40
自引率
2.60%
发文量
104
审稿时长
6-12 weeks
期刊介绍: Drug Development Research focuses on research topics related to the discovery and development of new therapeutic entities. The journal publishes original research articles on medicinal chemistry, pharmacology, biotechnology and biopharmaceuticals, toxicology, and drug delivery, formulation, and pharmacokinetics. The journal welcomes manuscripts on new compounds and technologies in all areas focused on human therapeutics, as well as global management, health care policy, and regulatory issues involving the drug discovery and development process. In addition to full-length articles, Drug Development Research publishes Brief Reports on important and timely new research findings, as well as in-depth review articles. The journal also features periodic special thematic issues devoted to specific compound classes, new technologies, and broad aspects of drug discovery and development.
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