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对称和不对称取代的1,4-双[(氨基烷基)氨基]蒽-9,10-二酮及1,4-双[(氨基烷基)氨基]-5,8-二羟基蒽-9,10-二酮的合成与抗肿瘤评估

Synthesis and antitumor evaluations of symmetrically and unsymmetrically substituted 1,4-bis[(aminoalkyl)amino]anthracene-9,10-diones and 1,4-bis[(aminoalkyl)amino]-5,8-dihydroxyanthracene-9,10-diones.

作者信息

Krapcho A P, Getahun Z, Avery K L, Vargas K J, Hacker M P, Spinelli S, Pezzoni G, Manzotti C

机构信息

Department of Chemistry, University of Vermont, Burlington 05405.

出版信息

J Med Chem. 1991 Aug;34(8):2373-80. doi: 10.1021/jm00112a009.

Abstract

The ipso bis displacements of fluoride from 1,4-difluoroanthracene-9,10-dione (3) and 1,4-difluoro-5,8-dihydroxyanthracene-9,10-dione (4) by excess of a diamine (or a monoamine) in pyridine at room temperature lead to the symmetrically substituted 1,4-bis-substituted analogues 5 and 6, respectively. The ipso monodisplacements of fluoride from 3 and 4 can be accomplished by treatment with less than 1 molar equiv of a diamine (or a monoamine) to yield 7 and 8, respectively. Treatment of 7 or 8 with a different diamine leads to the unsymmetrically substituted 1,4-bis[(aminoalkyl)amino]anthracene-9,10-diones 9 and 10, respectively. Many of the synthetic unsymmetrical analogues have been evaluated for their antitumor activity against L1210 in vitro and in vivo. Cross resistance of analogue 10a with mitoxantrone (2) and doxorubicin was evaluated against MDR lines in vitro against human colon carcinoma LOVO and its subline resistant to DOXO (LOVO/DOXO). Potential mechanisms for the observed cytotoxicity are presented and discussed.

摘要

在室温下,于吡啶中,1,4 - 二氟蒽 - 9,10 - 二酮(3)和1,4 - 二氟 - 5,8 - 二羟基蒽 - 9,10 - 二酮(4)中的氟通过过量的二胺(或单胺)进行本位双取代,分别生成对称取代的1,4 - 双取代类似物5和6。3和4的氟本位单取代可通过用小于1摩尔当量的二胺(或单胺)处理来实现,分别得到7和8。用不同的二胺处理7或8,分别得到不对称取代的1,4 - 双[(氨基烷基)氨基]蒽 - 9,10 - 二酮9和10。许多合成的不对称类似物已在体外和体内针对L1210进行了抗肿瘤活性评估。在体外针对人结肠癌LOVO及其对多柔比星耐药的亚系(LOVO/DOXO)的多药耐药细胞系评估了类似物10a与米托蒽醌(2)和多柔比星的交叉耐药性。提出并讨论了观察到的细胞毒性的潜在机制。

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