恶性疟原虫细胞色素b基因的突变与接受阿托伐醌-氯胍治疗的疟疾患者中寄生虫复发延迟有关。
Mutations in the Plasmodium falciparum cytochrome b gene are associated with delayed parasite recrudescence in malaria patients treated with atovaquone-proguanil.
作者信息
Sutherland Colin J, Laundy Matt, Price Nicholas, Burke Martina, Fivelman Quinton L, Pasvol Geoffrey, Klein John L, Chiodini Peter L
机构信息
Department of Clinical Parasitology, Hospital for Tropical Diseases, Mortimer Market, Capper St, London, WC1E 6AU, UK.
出版信息
Malar J. 2008 Nov 20;7:240. doi: 10.1186/1475-2875-7-240.
BACKGROUND
Fixed-dose combination antimalarial drugs have played an increasingly important role in the treatment and chemoprophylaxis of falciparum malaria since the worldwide failure of monotherapy with chloroquine. Atovaquone-proguanil is one such combination drug used both for prophylaxis in travellers, and for treatment of acute malaria cases in European hospitals and clinics.
METHODS
A series of eight atovaquone-proguanil treatment failures and two prophylaxis breakthroughs from four UK hospitals from 2004-2008 were analysed for evidence of mutations in the pfcyt-b gene, previously found to be associated with failure of the atovaquone component.
RESULTS
Parasites carrying pfcyt-b mutations were found in five falciparum malaria patients with recrudescent parasitaemia occurring weeks after apparently successful treatment of a primary infection with atovaquone-proguanil. Four of these cases carried parasites with the Tyr268Cys mutation in pfcyt-b, previously reported in two French patients with malaria. In contrast, mutations in pfcyt-b were not found in three patients treated with atovaquone-proguanil who exhibited delayed clearance of the primary infection, nor in two returning travellers with malaria who had used the combination for prophylaxis. Using current and previously published data, mean time to recrudescence of parasites carrying pfcytb codon 268 mutations was estimated as 28.0 days after treatment (95% C.I. 23.0 - 33.0 days), whereas treatment failures without codon 268 mutations received rescue treatment an average of 4.71 days after initial AP treatment (95% C.I. 1.76 - 7.67 days).
CONCLUSION
Genetically-determined parasite resistance to atovaquone is associated with delayed recrudescence of resistant parasites three weeks or more after initial clearance of parasitaemia by atovaquone/proguanil therapy. The 268-Cys allele of pfcyt-b may have been overlooked in previous studies of atovaquone-proguanil treatment failure as it is not detected by current RFLP methods.
背景
自从氯喹单一疗法在全球范围内失效以来,固定剂量复方抗疟药物在恶性疟的治疗和化学预防中发挥着越来越重要的作用。阿托伐醌-氯胍就是这样一种复方药物,用于旅行者预防用药,以及在欧洲医院和诊所治疗急性疟疾病例。
方法
分析了2004年至2008年期间来自英国四家医院的一系列八例阿托伐醌-氯胍治疗失败病例和两例预防用药突破病例,以寻找pfcyt-b基因中突变的证据,该基因先前被发现与阿托伐醌成分治疗失败有关。
结果
在五例恶性疟患者中发现携带pfcyt-b突变的疟原虫,这些患者在初次感染用阿托伐醌-氯胍治疗看似成功数周后出现寄生虫血症复发。其中四例病例携带的疟原虫在pfcyt-b中有Tyr268Cys突变,此前在两名法国疟疾病例中曾有报道。相比之下,在用阿托伐醌-氯胍治疗的三例患者中未发现pfcyt-b突变,这三例患者初次感染清除延迟,在两名使用该复方进行预防的回国旅行者疟疾病例中也未发现突变。利用当前和先前发表的数据,估计携带pfcytb密码子268突变的疟原虫复发的平均时间为治疗后28.0天(95%可信区间23.0 - 33.0天),而没有密码子268突变的治疗失败病例在初次阿托伐醌-氯胍治疗后平均4.71天接受挽救治疗(95%可信区间1.76 - 7.67天)。
结论
基因决定的疟原虫对阿托伐醌的耐药性与在用阿托伐醌/氯胍疗法初次清除寄生虫血症三周或更长时间后耐药性疟原虫的延迟复发有关。pfcyt-b的268-Cys等位基因可能在先前阿托伐醌-氯胍治疗失败的研究中被忽视,因为目前的限制性片段长度多态性方法无法检测到它。
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