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[疟疾的当前治疗与预防及未来展望]

[Current therapy and prevention of malaria and perspectives for the future].

作者信息

Markwalder K

出版信息

Schweiz Med Wochenschr. 1982 Mar 13;112(11):362-8.

PMID:7041253
Abstract

At present the basic antimalarial drugs are still the 4-aminoquinolines chloroquine and amodiaquine, the combinations of antifol compounds (such as pyrimethamine and sulfadoxine = Fansidar), and quinine. In South East Asia and parts of Latin America Plasmodium falciparum has become highly resistant to chloroquine, and increasingly so to the antifol combinations. By selecting the antimalarials bearing the lowest risk of resistance, or combinations of them, an attempt can be made to avoid failures of treatment and chemoprophylaxis. The other areas endemic for malaria tropica may still be generally considered "chloroquine sensitive", although sporadic low-grade resistance to chloroquine is reported. It would be a mistake to replace chloroquine systematically by antifol combinations in those parts of the world now as well. The questions when drug resistance is to be suspected, and how individual treatment can be adjusted to it, are likewise discussed. Mefloquine is the best known new compound, with excellent activity against multiresistant Plasmodium falciparum. A combination with Fansidar is now being developed to prevent the former from inducing resistant strains. Despite considerable experimental advances a malaria vaccine is unlikely to be generally available before the end of this decade.

摘要

目前,基本的抗疟药物仍然是4-氨基喹啉类的氯喹和氨酚喹、抗叶酸化合物组合(如乙胺嘧啶和磺胺多辛= Fansidar)以及奎宁。在东南亚和拉丁美洲部分地区,恶性疟原虫已对氯喹产生高度耐药性,对抗叶酸组合的耐药性也日益增强。通过选择耐药风险最低的抗疟药物或其组合,可以尝试避免治疗和化学预防失败。其他热带疟疾流行地区尽管有零星的对氯喹低度耐药的报告,但总体上仍可被视为“氯喹敏感”地区。现在在世界这些地区也系统性地用抗叶酸组合取代氯喹将是错误的。文中同样讨论了何时应怀疑耐药性以及如何针对耐药性调整个体治疗的问题。甲氟喹是最知名的新化合物,对多重耐药的恶性疟原虫具有出色的活性。目前正在研发一种与Fansidar的组合,以防止前者诱导耐药菌株产生。尽管在实验方面取得了相当大的进展,但在本世纪末之前,疟疾疫苗不太可能普遍可用。

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