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Br J Pharmacol Chemother. 1960 Mar;15(1):101-10. doi: 10.1111/j.1476-5381.1960.tb01216.x.
2
Derivatives of isatin beta-thiosemicarbazone with anti-viral chemotherapeutic activity against ectromelia infection.具有抗痘苗病毒感染的抗病毒化疗活性的异吲哚酮β-硫代半卡巴腙衍生物。
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本文引用的文献

1
The antiviral and synergic actions of isatin thiosemicarbazone and certain phenoxypyrimidines in vaccinia infection in mice.异吲哚酮硫代半卡巴腙和某些苯氧基嘧啶在小鼠痘苗病毒感染中的抗病毒及协同作用
Br J Exp Pathol. 1955 Feb;36(1):105-14.
2
Studies in enzyme cytochemistry. II. Synthesis of indigogenic substrates for esterases.酶细胞化学研究。II. 酯酶产色底物的合成。
Proc R Soc Lond B Biol Sci. 1958 Apr 8;148(933):481-94. doi: 10.1098/rspb.1958.0040.
3
The effect of thiocarbanidin and related compounds on Mycobacterium tuberculosis var. hominis in vitro and in vivo.硫卡巴腙及相关化合物对人型结核分枝杆菌的体内外作用
Am Rev Tuberc. 1958 Feb;77(2):301-10. doi: 10.1164/artpd.1958.77.2.301.
4
Antiviral activity of dicarbonyls and related compounds in embryonated eggs.二羰基化合物及相关化合物在鸡胚中的抗病毒活性。
J Immunol. 1957 Feb;78(2):104-11.
5
The chemotherapy of virus diseases, with brief consideration of the influence of dietary, hormonal and other factors in virus infections.
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The purine metabolism of a 6-mercaptopurine-resistant Lactobacillus casei.
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Effect of heterocyclic and other thiosemicarbazones on vaccinia infection in the mouse.杂环及其他硫代卡巴腙对小鼠痘苗感染的影响。
J Immunol. 1953 Mar;70(3):229-34.

异吲哚酮β-硫代半卡巴腙抗病毒化疗活性的构效关系。

The structure-activity relationships of the antiviral chemotherapeutic activity of isatin beta-thiosemicarbazone.

作者信息

BAUER D J, SADLER P W

出版信息

Br J Pharmacol Chemother. 1960 Mar;15(1):101-10. doi: 10.1111/j.1476-5381.1960.tb01216.x.

DOI:10.1111/j.1476-5381.1960.tb01216.x
PMID:13797622
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1481969/
Abstract

As part of an investigation devoted to the development of new antiviral agents a compound of established antiviral activity has been subjected to systematic structural modification. The structure-activity data so obtained have been used in the design of new compounds, some of which are described. The compound chosen was isatin beta-thiosemicarbazone, which has high activity against neurovaccinia infection in mice, and a 4-point parallel-line assay of in vivo chemotherapeutic activity has been developed, which has enabled the activity of the derivatives to be determined against isatin beta-thiosemicarbazone as a standard. The overall dimensions of the isatin beta-thiosemicarbazone molecule appear to be nearly maximal for the retention of high activity, as all substituents in the aromatic ring decrease the activity irrespective of their nature or position. The projection of the -CS.NH(2) group in relation to the ring nitrogen was found to be critical, as the alpha-thiosemicarbazone was inactive. A number of modifications of the side-chain were investigated:all led to reduction or loss of antiviral activity. The antiviral activity showed a positive correlation with chloroform solubility over a considerable range. The most active compound encountered was 1-ethylisatin beta-thiosemicarbazone, with an activity of 286 (isatin beta-thiosemicarbazone identical with100). Isatin beta-thiosemicarbazone showed no activity against 15 other viruses, and 20 related compounds showed on activity against ectromelia.

摘要

作为致力于开发新型抗病毒药物研究的一部分,一种具有确定抗病毒活性的化合物已进行了系统的结构修饰。由此获得的构效关系数据已用于新化合物的设计,其中一些化合物在此进行了描述。所选用的化合物是异烟肼β-硫代半卡巴腙,它对小鼠的神经痘苗感染具有高活性,并且已开发出一种体内化疗活性的四点平行线测定法,该方法能够以异烟肼β-硫代半卡巴腙为标准来测定衍生物的活性。异烟肼β-硫代半卡巴腙分子的整体尺寸对于保持高活性似乎几乎是最大的,因为芳环上的所有取代基无论其性质或位置如何都会降低活性。发现-CS.NH(2)基团相对于环氮的投影至关重要,因为α-硫代半卡巴腙没有活性。对侧链进行了多种修饰研究:所有修饰均导致抗病毒活性降低或丧失。在相当大的范围内,抗病毒活性与氯仿溶解度呈正相关。遇到的最具活性的化合物是1-乙基异烟肼β-硫代半卡巴腙,活性为286(异烟肼β-硫代半卡巴腙活性为100)。异烟肼β-硫代半卡巴腙对其他15种病毒无活性,20种相关化合物对痘苗病毒无活性。