盘尾丝虫病患者服用伊维菌素后不良临床事件可能的致病途径。

Charles D Mackenzie, Timothy G Geary, John A Gerlach
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引用次数: 58

摘要

背景:反应通常与盘尾丝虫病的化疗有关。然而,当使用伊维菌素(Mectizan(R))治疗这种感染时,难以控制的反应并不常见,这种药物已被证明比以前使用的药物有很大的改进。然而,严重的不良事件(SAE)已经发生,人们对这些事件可能对大规模药物给药计划产生的负面影响相当关注。本文综述了化疗药物破坏微丝蚴的基本致病机制。丝虫化疗的一个主要挑战是需要从生物敏感组织中清除寄生虫,这是一个比从胃肠道中清除线虫更困难的医学挑战。由于缺乏具体的病理病例资料,对伊维菌素治疗发生的严重不良反应的病因解释受到阻碍,这些地区同时存在严重的罗阿罗阿感染。本文回顾了调查这些可能性的方法。可能的致病机制包括栓塞性血管病理伴局部炎症、血脑屏障mdr1异常和过度炎症反应的遗传易感性。结论:将伊维菌素及其相关的临床不良事件与许多其他常用化疗药物进行比较是很重要的,其中许多化疗药物产生的严重不良事件甚至比伊维菌素更频繁。目前已有证据表明,loa相关不良反应的发病机制可能与特定组织对微丝虫的炎症反应有关。然而,也应该考虑到遗传因素对病理的影响。
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Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.

BACKGROUND: Reactions are commonly associated with the chemotherapy of onchocerciasis. However unmanageable reactions are uncommon when ivermectin (Mectizan(R)) is used for the treatment of this infection, and this drug has proved to be a great improvement over previously used agents. Serious adverse events (SAE) nevertheless have occurred, and there is considerable concern about the negative effect such events may have on mass drug administration programs.This paper reviews the basic pathogenic mechanisms that can be involved in the destruction of microfilaria by chemotherapeutic agents. A central challenge to filarial chemotherapy is the need to remove parasites from biologically sensitive tissues, a more difficult medical challenge than eliminating nematodes from the gastrointestinal tract.Explanations for the etiology of the serious adverse reactions occurring with ivermectin treatment in specific geographic areas where there is coincident heavy Loa loa infections are hampered by a lack of specific pathological case material. Ways to investigate these possibilities are reviewed. Possible pathogenic mechanisms include embolic vascular pathology accompanied by local inflammation, blood brain barrier mdr1 abnormalities, and genetic predisposition to excessive inflammatory responses. CONCLUSION: It is important to keep ivermectin, and all its associated adverse clinical events, in perspective with the many other chemotherapeutic agents in general use - many of which produce serious adverse events even more frequently than does ivermectin. Currently available evidence indicates that the pathogenesis of the Loa-associated adverse reactions are probably related to inflammatory responses to microfilariae in specific tissues. However, the possibility of genetic predispositions to pathology should also be considered.

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