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INHIBITORS OF INV(16) LEUKEMIA

机译:INV(16)白血病的抑制剂

摘要

This invention describes the development of targeted small molecule inhibitors of the inv(16) fusion, the causative agent in ˜12% of acute myeloid leukemia (AML). The inv(16) fusion results in expression of the CBFβ-SMMHC fusion protein in the blood cells of afflicted patients. The present invention provides compounds which inhibit the function of both CBFβ and the CBFβ-SMMHC fusion. These compounds block the growth of an inv(16) leukemia cell line as well as increase its apoptosis, while showing minimal effects against non inv(16) cell lines. As a mechanism to develop inhibitors with selectivity for the CBFβ-SMMHC fusion protein, the present invention further provides dimeric derivatives of these compounds which show both increased potency as well as selectivity for CBFβ-SMMHC. These compounds show potent inhibition of an inv(16) leukemia cell line with minimal effects on non inv(16) cell lines. Analysis of the pharmacokinetics of the developed compounds has made it possible to improve the lifetime of the compound in the plasma of mice to a level commensurate with long-term treatment.
机译:本发明描述了inv(16)融合的靶向小分子抑制剂的开发,inv(16)融合是〜约12%的急性髓细胞性白血病(AML)的病原体。 inv(16)融合导致CBFβ-SMMHC融合蛋白在患病患者的血细胞中表达。本发明提供了抑制CBFβ和CBFβ-SMMHC融合两者的功能的化合物。这些化合物可阻止inv(16)白血病细胞系的生长并增加其凋亡,同时对非inv(16)细胞系的影响最小。作为开发对CBFβ-SMMHC融合蛋白具有选择性的抑制剂的机制,本发明进一步提供了这些化合物的二聚衍生物,其显示出对CBFβ-SMMHC的增强的效力以及选择性。这些化合物显示出对inv(16)白血病细胞系的有效抑制作用,对非inv(16)细胞系的影响最小。对已开发化合物的药代动力学的分析使得可以将化合物在小鼠血浆中的寿命提高到与长期治疗相当的水平。

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