针对药靶基因PDCD10和MST4抑制剂体外筛选方法的建立及化合物的筛选
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国家高技术研究发展计划(863)“十一五”重大专项资助课题(2006AA02A305),重点项目资助课题(2006AA020501),“重点新药创制”科技重大专项资助课题(2009ZX09503-004)


The establishment of drug targets PDCD10 and MST4 inhibitors screening method in vitro and the compounds screening
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    目的:以人程序性细胞死亡分子10(homo sapiens programmed cell death 10, PDCD10)和Ste20激酶家族成员MST4(Mst3 and SOK1-related kinase)为靶标,建立体外小分子抑制剂筛选方法-方法:将PDCD10和MST4的开放读码框插入到原核表达载体pGEX4T-2,采用亲和层析纯化法纯化重组人GST-PDCD10和GST-MST4蛋白并通过Western blot进行鉴定-利用ELISA方法对重组蛋白进行活性检测-利用该ELISA方法对825个小分子化合物进行筛选,并通过其对Elk1通路的作用进行验证-结果:成功建立了针对药靶基因PDCD10和MST4抑制剂的体外筛选方法,筛选得到1个对PDCD10和MST4活性有抑制作用的化合物-结论:该方法具有较好的平行性和可重复性-筛选得到的化合物可以抑制PDCD10和MST4对Elk1通路的活化作用-

    Abstract:

    Objective:Taking PDCD10 (homo sapiens programmed cell death 10) and MST4 (Mst3 and SOK1-related kinase) as drug targets, to establish a low molecular weight inhibitors screening method in vitro. Methods:The open reading frames of PDCD10 and MST4 were reconstructed into the prokaryotic expressive vector pGEX4T-2. The recombinant proteins were purified using GST affinity chromatograph, and then analyzed using Western blot. ELISA assay was utilized to detect the activity of purified proteins of GST-PDCD10 and GST-MST4 and screen for the inhibitor in 825 compounds, which were verified by the dual luciferase reporter gene assay in Elk1 signaling pathway. Results:Drug targets PDCD10 and MST4 inhibitors screening method was established successfully in vitro. One compound screened by this method was confirmed to inhibit the activity of PDCD10 and MST4. Conclusion: The method is of better parallelism and stability. The screened compound could also inhibit the activity of PDCD10 and MST4 in Elk1 signaling pathway.

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张 慧,黄 卉,李 娜,杜培革,石太平.针对药靶基因PDCD10和MST4抑制剂体外筛选方法的建立及化合物的筛选[J].南京医科大学学报(自然科学版),2010,(11):1527-1532

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  • 收稿日期:2010-04-21
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