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在马拉维将磺胺多辛和乙胺嘧啶作为一线治疗药物引入七年之后,恶性疟原虫感染中五重突变的二氢蝶酸合酶/二氢叶酸还原酶基因的高流行率。

High prevalence of quintuple mutant dhps/dhfr genes in Plasmodium falciparum infections seven years after introduction of sulfadoxine and pyrimethamine as first line treatment in Malawi.

作者信息

Bwijo B, Kaneko A, Takechi M, Zungu I L, Moriyama Y, Lum J K, Tsukahara T, Mita T, Takahashi N, Bergqvist Y, Björkman A, Kobayakawa T

机构信息

Department of International Affairs and Tropical Medicine, Tokyo Women's Medical University, 8-1 Kawada-Cho, Shinjuku-Ku, Tokyo 162 8666, Japan.

出版信息

Acta Trop. 2003 Mar;85(3):363-73. doi: 10.1016/s0001-706x(02)00264-4.

Abstract

Malawi changed its national policy for malaria treatment in 1993, becoming the first country in Africa to replace chloroquine by sulfadoxine and pyrimethamine combination (SP) as the first-line drug for uncomplicated malaria. Seven years after this change, we investigated the prevalence of dihydropteroate synthase (dhps) and dihydrofolate reductase (dhfr) mutations, known to be associated with decreased sensitivity to SP, in 173 asymptomatic Plasmodium falciparum infections from Salima, Malawi. A high prevalence rate (78%) of parasites with triple Asn-108/Ile-51/Arg-59 dhfr and double Gly-437/Glu-540 dhps mutations was found. This 'quintuple mutant' is considered as a molecular marker for clinical failure of SP treatment of P. falciparum malaria. A total of 11 different dhfr and dhps combinations were detected, 3 of which were not previously reported. Nineteen isolates contained the single Glu-540 mutant dhps, while no isolate contained the single Gly-437 mutant dhps, an unexpected finding since Gly-437 are mostly assumed to be one of the first mutations commonly selected under sulfadoxine pressure. Two isolates contained the dhps single or double mutant coupled with dhfr wild-type. The high prevalence rates of the three dhfr mutations in our study were consistent with a previous survey in 1995 in Karonga, Malawi, whereas the prevalences of dhps mutations had increased, most probably as a result of the wide use of SP. A total of 52 P. falciparum isolates were also investigated for pyrimethamine and sulfadoxine/pyrimethamine activity against parasite growth according to WHO in vitro standard protocol. A pyrimethamine resistant profile was found. When pyrimethamine was combined with sulfadoxine, the mean EC(50) value decreased to less than one tenth of the pyrimethamine alone level. This synergistic activity may be explained by sulfadoxine inhibition of dhps despite the double mutations in the dhps genes, which would interact with pyrimethamine acting to block the remaining folate despite dhfr mutations in the low p-aminobenzoic acid and low folic acid medium mixed with blood.

摘要

1993年,马拉维改变了其疟疾治疗的国家政策,成为非洲首个用磺胺多辛与乙胺嘧啶合剂(SP)取代氯喹作为单纯性疟疾一线药物的国家。这一政策改变7年后,我们调查了来自马拉维萨利马的173例无症状恶性疟原虫感染中,已知与对SP敏感性降低相关的二氢蝶酸合酶(dhps)和二氢叶酸还原酶(dhfr)突变的流行情况。发现具有Asn-108/Ile-51/Arg-59三联dhfr和Gly-437/Glu-540双连dhps突变的寄生虫流行率很高(78%)。这种“五重突变体”被视为SP治疗恶性疟原虫疟疾临床失败的分子标志物。总共检测到11种不同的dhfr和dhps组合,其中3种以前未报告过。19个分离株含有单一的Glu-540突变型dhps,而没有分离株含有单一的Gly-437突变型dhps,这是一个意外发现,因为Gly-437大多被认为是在磺胺多辛压力下通常首先选择的突变之一。两个分离株含有dhps单突变或双突变与dhfr野生型的组合。我们研究中三种dhfr突变的高流行率与1995年在马拉维卡龙加进行的一项先前调查一致,而dhps突变的流行率有所增加,很可能是SP广泛使用的结果。还根据世界卫生组织的体外标准方案,对总共52株恶性疟原虫分离株进行了乙胺嘧啶以及磺胺多辛/乙胺嘧啶对寄生虫生长活性的研究。发现了乙胺嘧啶耐药情况。当乙胺嘧啶与磺胺多辛联合使用时,平均EC(50)值降至单独使用乙胺嘧啶时水平的十分之一以下。这种协同活性可能是由于尽管dhps基因存在双突变,但磺胺多辛对dhps的抑制作用,这将与乙胺嘧啶相互作用,在与血液混合的低对氨基苯甲酸和低叶酸培养基中,尽管存在dhfr突变,但仍能阻断剩余的叶酸。

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