取代的1,3,4-恶二唑衍生物的抗血管生成和抗增殖作用是通过下调血管内皮生长因子（VEGF）以及抑制艾氏腹水瘤细胞中缺氧诱导因子-1α（HIF-1α）的转位来介导的。

Antiangiogenic and antiproliferative effects of substituted-1,3,4-oxadiazole derivatives is mediated by down regulation of VEGF and inhibition of translocation of HIF-1alpha in Ehrlich ascites tumor cells.

作者信息

Kumar Akhilesh, D'Souza Saritha S, Nagaraj Sachin Raj Mysore, Gaonkar S L, Salimath Bharathi P, Rai K M Lokanatha

机构信息

Department of Studies in Biotechnology, University of Mysore, Manasagangotri, Mysore 570006, Karnataka, India.

出版信息

Cancer Chemother Pharmacol. 2009 Nov;64(6):1221-33. doi: 10.1007/s00280-009-0992-y. Epub 2009 Apr 16.

DOI:10.1007/s00280-009-0992-y

PMID:19370348

Abstract

PURPOSE

1,3,4-Oxadiazoles are an important class of heterocyclic compounds, which play a pivotal role in various pharmaceutical applications. Here, we investigated the antiangiogenic and antiproliferative effects of the derivatives and explored its mechanism of action on EAT cells.

METHODS

The cytotoxic effect of the derivatives on EAT and HEK293 cells was assessed by MTT assay. Effect of the derivatives on ALP activity and proliferation was measured. Swiss albino mice transplanted with EAT cells were used as a model system to study the effect of the derivatives in vivo. Inhibition of angiogenesis in mice peritoneum, CAM and Cornea of the rat were studied. Finally, the effects on VEGF gene expression, HIF-1alpha translocation and cell cycle arrest were determined.

RESULTS

The IC50 range for growth inhibition of EAT cells was found to be 140-175 microM. In contrast normal HEK293 cells were resistant to the derivatives at this range. Treatment with derivatives in vivo was demonstrated by the down regulation of VEGF in EAT cells and inhibition of blood vessels formation in mice peritoneum, CAM and cornea of rat, indicating the potent angioinhibitory effect of the derivatives. VEGF promoter-luciferase reporter gene expression analysis showed suppression of VEGF gene expression in vitro. The derivatives proved to be potent antiproliferative agents as shown by FACS analysis and decreased ALP activity. Furthermore, expression of HIF-1alpha was also down regulated by derivatives by repressing its nuclear translocation.

CONCLUSIONS

Oxadiazole derivatives are strong bioactive compounds with antiangiogenic and antiproliferative potential both in vitro and in vivo. We postulate that diminished HIF-1alpha nuclear presence in oxadiazole treated EAT cells could be responsible for decreased VEGF expression and antiangiogenic effects.

摘要

目的

1,3,4-恶二唑是一类重要的杂环化合物，在各种药物应用中发挥着关键作用。在此，我们研究了这些衍生物的抗血管生成和抗增殖作用，并探讨了其对艾氏腹水癌细胞（EAT细胞）的作用机制。

方法

通过MTT法评估衍生物对EAT细胞和人胚肾293细胞（HEK293细胞）的细胞毒性作用。测定衍生物对碱性磷酸酶（ALP）活性和增殖的影响。以移植了EAT细胞的瑞士白化小鼠作为模型系统，研究衍生物在体内的作用。研究了衍生物对小鼠腹膜、鸡胚绒毛尿囊膜（CAM）和大鼠角膜血管生成的抑制作用。最后，确定了其对血管内皮生长因子（VEGF）基因表达、缺氧诱导因子-1α（HIF-1α）转位和细胞周期阻滞的影响。

结果

发现EAT细胞生长抑制的半数抑制浓度（IC50）范围为140 - 175微摩尔。相比之下，正常HEK293细胞在该浓度范围内对这些衍生物具有抗性。体内用衍生物处理表现为EAT细胞中VEGF下调以及小鼠腹膜、CAM和大鼠角膜血管生成受到抑制，表明这些衍生物具有强大的血管生成抑制作用。VEGF启动子-荧光素酶报告基因表达分析表明其在体外抑制了VEGF基因表达。流式细胞术分析和ALP活性降低表明这些衍生物是有效的抗增殖剂。此外，衍生物通过抑制HIF-1α的核转位，使其表达也下调。

结论

恶二唑衍生物是具有强大生物活性的化合物，在体外和体内均具有抗血管生成和抗增殖潜力。我们推测，恶二唑处理的EAT细胞中HIF-1α核内含量减少可能是VEGF表达降低和抗血管生成作用的原因。

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取代的1,3,4-恶二唑衍生物的抗血管生成和抗增殖作用是通过下调血管内皮生长因子（VEGF）以及抑制艾氏腹水瘤细胞中缺氧诱导因子-1α（HIF-1α）的转位来介导的。

Antiangiogenic and antiproliferative effects of substituted-1,3,4-oxadiazole derivatives is mediated by down regulation of VEGF and inhibition of translocation of HIF-1alpha in Ehrlich ascites tumor cells.

作者信息

机构信息

出版信息

PURPOSE

METHODS

RESULTS

CONCLUSIONS

目的

方法

结果

结论

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