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膜血红素作为降低双氢青蒿素疗效的宿主因素。

Membrane heme as a host factor in reducing effectiveness of dihydroartemisinin.

作者信息

Vattanaviboon Phantip, Siritanaratkul Noppadol, Ketpirune Jidapa, Wilairat Prapon, Yuthavong Yongyuth

机构信息

Faculty of Medical Technology, Department of Clinical Microscopy, Mahidol University, Siriraj Hospital, Bangkok, Thailand.

出版信息

Biochem Pharmacol. 2002 Jul 1;64(1):91-8. doi: 10.1016/s0006-2952(02)01060-2.

Abstract

Plasmodium falciparum infecting alpha-thalassemic erythrocytes are resistant to artemisinin and its derivatives. Binding of the drug to hemoglobin H resulting in drug inactivation was previously demonstrated. We now show that an additional host factor, membrane heme, significantly accounted for decreased antimalarial activity of artemisinin. The antimalarial activity of dihydroartemisinin in the presence of normal and thalassemic erythrocyte membranes showed a correlation with the heme content of the membrane (r(2)=0.466, P<0.01). The correlation was more clearly seen when the drug effectiveness was correlated with the heme content of alpha-thalassemic membrane (r(2)=0.636, P<0.01). However, the drug effectiveness showed no correlation to ferrozine-reactive (free or non-heme) iron content (r(2)=0.0001, P>0.05). alpha-Thalassemic erythrocytes contained higher amounts of membrane heme (11.04+/-8.96 nmol/mg membrane protein) than those from normal and beta-thalassemia/HbE erythrocytes (2.68+/-1.28 and 3.98+/-3.98 nmol/mg membrane protein, respectively, P<0.01). Loss of drug effectiveness was also correlated with increment of heme content in membrane prepared from normal erythrocytes treated with phenylhydrazine. It is concluded that heme in both normal and thalassemic erythrocyte membranes is an important factor in drug inactivation.

摘要

感染α地中海贫血红细胞的恶性疟原虫对青蒿素及其衍生物具有抗性。先前已证明药物与血红蛋白H结合会导致药物失活。我们现在表明,另一个宿主因子——膜血红素,在很大程度上导致了青蒿素抗疟活性的降低。在正常和地中海贫血红细胞膜存在的情况下,双氢青蒿素的抗疟活性与膜的血红素含量呈相关性(r(2)=0.466,P<0.01)。当将药物有效性与α地中海贫血膜的血红素含量相关联时,这种相关性更为明显(r(2)=0.636,P<0.01)。然而,药物有效性与亚铁嗪反应性(游离或非血红素)铁含量无相关性(r(2)=0.0001,P>0.05)。α地中海贫血红细胞所含的膜血红素量(11.04±8.96 nmol/mg膜蛋白)高于正常和β地中海贫血/HbE红细胞(分别为2.68±1.28和3.98±3.98 nmol/mg膜蛋白,P<0.01)从用苯肼处理的正常红细胞制备的膜中,药物有效性的丧失也与膜中血红素含量的增加相关。结论是,正常和地中海贫血红细胞膜中的血红素都是药物失活的重要因素。

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