作者
Thomas Efferth, Achille Benakis, Marta R Romero, Maja Tomicic, Rolf Rauh, Daniel Steinbach, Ralf Häfer, Thomas Stamminger, Franz Oesch, Bernd Kaina, Manfred Marschall
发表日期
2004/10/1
期刊
Free Radical Biology and Medicine
卷号
37
期号
7
页码范围
998-1009
出版商
Pergamon
简介
Iron(II) heme-mediated activation of the peroxide bond of artemisinins is thought to generate the radical oxygen species responsible for their antimalarial activity. We analyzed the role of ferrous iron in the cytotoxicity of artemisinins toward tumor cells. Iron(II)–glycine sulfate (Ferrosanol) and transferrin increased the cytotoxicity of free artesunate, artesunate microencapsulated in maltosyl-β-cyclodextrin, and artemisinin toward CCRF-CEM leukemia and U373 astrocytoma cells 1.5- to 10.3-fold compared with that of artemisinins applied without iron. Growth inhibition by artesunate and ferrous iron correlated with induction of apoptosis. Cell cycle perturbations by artesunate and ferrous iron were not observed. Treatment of p53 wild-type TK6 and p53 mutated WTK1 lymphoblastic cells showed that mutational status of the tumor suppressor p53 did not influence sensitivity to artesunate. The effect of ferrous iron and …
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T Efferth, A Benakis, MR Romero, M Tomicic, R Rauh… - Free Radical Biology and Medicine, 2004