首页> 外文期刊>Journal of biomolecular screening: The official journal of the Society for Biomolecular Screening >An efficient high-throughput screening method for MYST family acetyltransferases, a new class of epigenetic drug targets
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An efficient high-throughput screening method for MYST family acetyltransferases, a new class of epigenetic drug targets

机译:一种有效的高通量筛选方法,用于筛选新型表观遗传药物靶点MYST家族的乙酰转移酶

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摘要

Epigenetic aberrations are increasingly regarded as key factors in cancer progression. Recently, deregulation of histone acetyltransferases (HATs) has been linked to several types of cancer. Monocytic leukemia zinc finger protein (MOZ) is a member of the MYST family of HATs, which regulate gene expression in cell proliferation and differentiation. Deregulation of these processes through constitutively active MOZ fusion proteins gives rise to the formation of leukemic stem cells, rendering MOZ an excellent target for treating myeloid leukemia. The authors implemented a hit discovery campaign to identify small-molecule inhibitors of MOZ-HAT activity. They developed a robust, homogeneous assay measuring the acetylation of synthetic histone peptides. In a primary screening campaign testing 243 000 lead-like compounds, they identified inhibitors from several chemical classes. Secondary assays were used to eliminate assay-interfering compounds and prioritize confirmed hits. This study establishes a new high-throughput assay for HAT activity and could provide the foundation for the development of a new class of drugs for the treatment of leukemias.
机译:表观遗传畸变越来越被认为是癌症进展的关键因素。最近,组蛋白乙酰转移酶(HATs)的失调与几种类型的癌症有关。单核细胞白血病锌指蛋白(MOZ)是HAT的MYST家族的成员,该家族调节细胞增殖和分化中的基因表达。通过组成型活性的MOZ融合蛋白使这些过程失控会导致白血病干细胞的形成,使MOZ成为治疗骨髓性白血病的极佳靶标。作者开展了一项命中发现活动,以识别MOZ-HAT活性的小分子抑制剂。他们开发了一种强大的,均质的测定方法,可测量合成组蛋白肽的乙酰化程度。在一次初筛活动中,测试了243 000种铅样化合物,他们从几种化学类别中鉴定了抑制剂。二级检测用于消除干扰检测的化合物并确定已确认的匹配数据的优先级。这项研究为HAT活性建立了一种新的高通量测定方法,并可以为开发用于治疗白血病的新型药物奠定基础。

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