两种新型SKM13抗疟衍生物SKM13- meo和SKM13- f的体外评价

IF 16.4 1区 化学 Q1 CHEMISTRY, MULTIDISCIPLINARY
Thuy-Tien Thi Trinh, Young-Ah Kim, Hyelee Hong, Linh Thi Thuy Le, Hayoung Jang, Soon-Ai Kim, Hyun Park, Hak Sung Kim, Seon-Ju Yeo
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引用次数: 0

摘要

疟疾是一种由原虫疟原虫引起的致命疾病,抗疟药物在控制和治疗疟疾方面发挥着重要作用,迫切需要开发能有效对抗耐药疟原虫的新型抗疟药物。以SKM13为模板设计了SKM13- meo和SKM13-F衍生物,分别用供电子基(-OMe)或吸电子基(-F)取代苯基,从而逆转电子密度。采用比色法定量细胞毒性,并对恶性疟原虫3D7的3个不同血期(环、滋养体和分裂体)和D6同步后的环/混合期进行体外抑制试验。体外细胞毒性分析表明,2个新的SKM13衍生物降低了SKM13模板的细胞毒性。SKM13在环体和滋养体阶段维持IC50,而在分裂体阶段不维持IC50。恶性疟原虫滋养体期3D7和环/混合期D6的IC50值表明,2种SKM13衍生物的抗疟效果下降,尤其是SKM13- f衍生物。SKM13在环体和滋养体中可能同样有效,并且在SKM13修饰中,给电子基团(-OMe)可能比吸电子基团(-F)更能维持抗疟活性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

In Vitro Evaluation of Two Novel Antimalarial Derivatives of SKM13: SKM13-MeO and SKM13-F.

In Vitro Evaluation of Two Novel Antimalarial Derivatives of SKM13: SKM13-MeO and SKM13-F.

In Vitro Evaluation of Two Novel Antimalarial Derivatives of SKM13: SKM13-MeO and SKM13-F.

In Vitro Evaluation of Two Novel Antimalarial Derivatives of SKM13: SKM13-MeO and SKM13-F.

Antimalarial drugs play an important role in the control and treatment of malaria, a deadly disease caused by the protozoan parasite Plasmodium spp. The development of novel antimalarial agents effective against drug-resistant malarial parasites is urgently needed. The novel derivatives, SKM13-MeO and SKM13-F, were designed based on an SKM13 template by replacing the phenyl group with electron-donating (-OMe) or electron-withdrawing groups (-F), respectively, to reverse the electron density. A colorimetric assay was used to quantify cytotoxicity, and in vitro inhibition assays were performed on 3 different blood stages (ring, trophozoite, and schizonts) of P. falciparum 3D7 and the ring/mixed stage of D6 strain after synchronization. The in vitro cytotoxicity analysis showed that 2 new SKM13 derivatives reduced the cytotoxicity of the SKM13 template. SKM13 maintained the IC50 at the ring and trophozoite stages but not at the schizont stage. The IC50 values for both the trophozoite stage of P. falciparum 3D7 and ring/mixed stages of D6 demonstrated that 2 SKM13 derivatives had decreased antimalarial efficacy, particularly for the SKM13-F derivative. SKM13 may be comparably effective in ring and trophozoite, and electron-donating groups (-OMe) may be better maintain the antimalarial activity than electron-withdrawing groups (-F) in SKM13 modification.

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来源期刊
Accounts of Chemical Research
Accounts of Chemical Research 化学-化学综合
CiteScore
31.40
自引率
1.10%
发文量
312
审稿时长
2 months
期刊介绍: Accounts of Chemical Research presents short, concise and critical articles offering easy-to-read overviews of basic research and applications in all areas of chemistry and biochemistry. These short reviews focus on research from the author’s own laboratory and are designed to teach the reader about a research project. In addition, Accounts of Chemical Research publishes commentaries that give an informed opinion on a current research problem. Special Issues online are devoted to a single topic of unusual activity and significance. Accounts of Chemical Research replaces the traditional article abstract with an article "Conspectus." These entries synopsize the research affording the reader a closer look at the content and significance of an article. Through this provision of a more detailed description of the article contents, the Conspectus enhances the article's discoverability by search engines and the exposure for the research.
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