首页> 美国卫生研究院文献>Marine Drugs >Chemistry of Renieramycins. Part 19: Semi-Syntheses of 22-O-Amino Ester and Hydroquinone 5-O-Amino Ester Derivatives of Renieramycin M and Their Cytotoxicity against Non-Small-Cell Lung Cancer Cell Lines
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Chemistry of Renieramycins. Part 19: Semi-Syntheses of 22-O-Amino Ester and Hydroquinone 5-O-Amino Ester Derivatives of Renieramycin M and Their Cytotoxicity against Non-Small-Cell Lung Cancer Cell Lines

机译:Renieramycins的化学。第19部分:12-O-氨基酯和氢醌5-O-氨基酯衍生物的半合成素霉素M及其对非小细胞肺癌细胞系的细胞毒性

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摘要

Two new series of synthetic renieramycins including 22- -amino ester and hydroquinone 5- -amino ester derivatives of renieramycin M were semi-synthesized and evaluated for their cytotoxicity against the metastatic non-small-cell lung cancer H292 and H460 cell lines. Interestingly, the series of 22- -amino ester derivatives displayed a potent cytotoxic activity greater than the hydroquinone derivatives. The most cytotoxic derivative of the series was the 22- -( -Boc- -glycine) ester of renieramycin M ( : IC 3.56 nM), which showed 7-fold higher potency than renieramycin M (IC 24.56 nM) and 61-fold more than jorunnamycin A (IC 217.43 nM) against H292 cells. In addition, exhibited a significantly higher cytotoxic activity than doxorubicin (ca. 100 times). The new semi-synthetic renieramycin derivatives will be further studied and developed as potential cytotoxic agents for non-small-cell lung cancer treatment.
机译:包括22--氨基酯和氢醌的两种新的合成renieramycins,Renieramycinm的羟基氨基氨基氨基胺M是半合成的,并针对转移性非小细胞肺癌H292和H460细胞系评估其细胞毒性。有趣的是,22- amino酯衍生物的系列呈现出高于氢醌衍生物的有效细胞毒性活性。该系列的最多细胞毒性衍生物是Renieramycin M(:IC 3.56nm)的22-(聚甘氨酸)酯,其表现出比Renieramycin M(IC 24.56nm)和61倍以下的效力高7倍比jorunnamycin a(Ic 217.43nm)对抗H292细胞。此外,表现出比多柔比星(约100次)显着更高的细胞毒性活性。将进一步研究新的半合成雷诺霉素衍生物,并开发为用于非小细胞肺癌治疗的潜在细胞毒性剂。

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