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논문 기본 정보

자료유형
학술저널
저자정보
Thuy-Tien Thi Trinh (Seoul National University) Young-ah Kim (Wonkwang University) Hyelee Hong (Seoul National University) Linh Thi Thuy Le (Seoul National University) Hayoung Jang (Seoul National University) Soon-Ai Kim (Wonkwang University) Hyun Park (Wonkwang University) Hak Sung Kim (Wonkwang University) Seon-Ju Yeo (Seoul National University)
저널정보
대한기생충학열대의학회 Parasites, Hosts and Diseases The Korean Journal of Parasitology Vol.60 No.6
발행연도
2022.12
수록면
401 - 407 (7page)

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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 IC<SUB>50</SUB> at the ring and trophozoite stages but not at the schizont stage. The IC<SUB>50</SUB> 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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Abstract
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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