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孕期抗疟药物的安全性、有效性及有效性的决定因素:对撒哈拉以南非洲恶性疟原虫流行地区预防项目的启示

Safety, efficacy and determinants of effectiveness of antimalarial drugs during pregnancy: implications for prevention programmes in Plasmodium falciparum-endemic sub-Saharan Africa.

作者信息

Newman Robert D, Parise Monica E, Slutsker Laurence, Nahlen Bernard, Steketee Richard W

机构信息

Malaria Epidemiology Branch, Division of Parasitic Diseases, NCID, CDC, Atlanta, GA 30341, USA.

出版信息

Trop Med Int Health. 2003 Jun;8(6):488-506. doi: 10.1046/j.1365-3156.2003.01066.x.

Abstract

Plasmodium falciparum malaria in pregnancy poses substantial risk to a pregnant woman and her neonate through anaemia and low birth weight (LBW), respectively, and is responsible for up to 35% of preventable LBW in malaria-endemic areas. Chemoprophylaxis or intermittent preventive treatment (IPT) with an effective antimalarial can ameliorate the adverse effects of malaria during pregnancy. Current guidelines from the WHO recommend that women in highly malarious areas receive IPT with an effective antimalarial. Two central considerations in evaluating drugs for use during pregnancy are safety for the mother and her foetus and effectiveness, which is determined by efficacy, cost, availability, deliverability and acceptability of the drug. These factors may be scored and potential drugs or drug combinations ranked in order of potential effectiveness for use in prevention programmes. The seven most promising regimens are all IPT, primarily because they are more easily delivered and less expensive than chemoprophylaxis. Currently, IPT with sulphadoxine-pyrimethamine (SP) is more likely to have the best overall effectiveness in preventing adverse outcomes associated with malaria in pregnancy. Its low cost, wide availability, easy deliverability and acceptability make it the clear choice in countries where efficacy of the drug remains good. For countries where resistance to SP is rising or already high, amodiaquine (alone or in combination with SP or artesunate) artesunate + SP, chlorproguanil-dapsone (with and without artesunate) and artemether-lumefantrine require urgent evaluation for use in pregnancy.

摘要

孕期感染恶性疟原虫疟疾会分别通过贫血和低出生体重对孕妇及其新生儿构成重大风险,在疟疾流行地区,这一疾病导致的低出生体重占可预防低出生体重病例的35%。使用有效的抗疟药物进行化学预防或间歇性预防治疗(IPT)可改善孕期疟疾的不良影响。世界卫生组织目前的指南建议,疟疾高发地区的妇女应接受有效的抗疟药物进行间歇性预防治疗。评估孕期用药时的两个核心考量因素是对母亲及其胎儿的安全性以及有效性,有效性由药物的疗效、成本、可及性、可交付性和可接受性决定。可以对这些因素进行评分,并根据预防项目中潜在的有效性对潜在药物或药物组合进行排序。最有前景的七种方案均为间歇性预防治疗,主要是因为它们比化学预防更易于实施且成本更低。目前,使用周效磺胺-乙胺嘧啶(SP)进行间歇性预防治疗在预防孕期疟疾相关不良后果方面最有可能具有最佳的总体效果。其低成本、广泛可及、易于实施和可接受性使其在该药物疗效仍然良好的国家成为明确选择。对于对周效磺胺-乙胺嘧啶耐药性正在上升或已经很高的国家,阿莫地喹(单独使用或与周效磺胺-乙胺嘧啶或青蒿琥酯联合使用)、青蒿琥酯+周效磺胺-乙胺嘧啶、氯胍-氨苯砜(含或不含青蒿琥酯)以及蒿甲醚-本芴醇需要紧急评估其在孕期的使用情况。

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