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首页> 外文期刊>Antiviral chemistry & chemotherapy >Design, synthesis and structure relationships of new N,N',N',N''-tetrakis (omega-amino alkyl) tetraazamacrocycles.
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Design, synthesis and structure relationships of new N,N',N',N''-tetrakis (omega-amino alkyl) tetraazamacrocycles.

机译:新的N,N',N“,N”'-四(ω-氨基烷基)四氮杂大环的设计,合成和结构关系。

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摘要

A number of N,N',N",N"'-tetrakis (omega-aminoalkyl) tetraazamacrocycles and related compounds were synthesized and evaluated for their inhibitory effects on human immunodeficiency virus type 1 (HIV-1) and duck hepatitis B virus (DHBV) replication. The activity of these compounds was found to be highly dependent upon structural features: (i) the length of the alkyl linker connecting the nitrogen atoms of the macrocyclic ring to the exocyclic nitrogen atoms of the terminal amino groups (five methylenes favoured antiviral activity); (ii) substitution of the terminal amino groups of the linker reduced antiviral activity; and (iii) the size of the tetraazamacrocyclic ring (14 or 15 atoms) did not markedly affect the antiviral activity. Some analogues were potent inhibitors of HIV-1 replication, with anti-HIV activity similar to that of biscyclam (JM 2763). In contrast, other analogues were found to be highly toxic in duck hepatocyte primary culture, the 2.2.15 cell line and to a lesser extent in MT-4 cells. Structural parameters, macrocyclic ring size and metal-chelating ability have been used to develop a structure-activity relationship model in order to aid the design of antiviral molecules derived from N,N',N",N"'-tetrakis (omega-aminoalkyl) tetraazamacrocycles.
机译:合成了许多N,N',N“,N”-四(ω-氨基烷基)四氮杂大环和相关化合物,并评估了它们对人1型免疫缺陷病毒(HIV-1)和鸭乙型肝炎病毒( DHBV)复制。发现这些化合物的活性高度依赖于结构特征:(i)连接大环的氮原子与末端氨基的环外氮原子的烷基连接基团的长度(五个亚甲基有利于抗病毒活性); (ii)接头的末端氨基的取代降低了抗病毒活性; (iii)四氮杂大环环的大小(14或15个原子)没有显着影响抗病毒活性。一些类似物是有效的HIV-1复制抑制剂,其抗HIV活性类似于双环素(JM 2763)。相反,发现其他类似物在鸭肝细胞原代培养物,2.2.15细胞系中毒性很高,而在MT-4细胞中毒性较小。结构参数,大环尺寸和金属螯合能力已用于开发结构-活性关系模型,以帮助设计衍生自N,N',N“,N”'-四(ω-氨基烷基)的抗病毒分子)tetraazamacrocycles。

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