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免疫功能低下的微小巴贝斯虫感染患者对阿奇霉素-阿托伐醌耐药的出现。

Emergence of resistance to azithromycin-atovaquone in immunocompromised patients with Babesia microti infection.

机构信息

Divisions of 1Infectious Diseases, Departments of Medicine and 3Pathology, New York Medical College, Valhalla, NY 10595, USA.

出版信息

Clin Infect Dis. 2010 Feb 1;50(3):381-6. doi: 10.1086/649859.

Abstract

BACKGROUND

Babesiosis is an emerging tickborne malaria-like infection principally caused by Babesia microti. This infection typically resolves either spontaneously or after administration of a 7-10-day course of azithromycin plus atovaquone or clindamycin plus quinine. Although certain highly immunocompromised patients may respond suboptimally to these drug regimens, unlike the situation with malaria there has been no reported evidence that the cause of treatment failure is infection with drug-resistant strains of B. microti.

METHODS

Emergence of drug resistance in B. microti was defined as the development of a microbiologic relapse (recurrent parasitemia or a marked increase in parasitemia) in association with both clinical and laboratory abnormalities indicative of active babesiosis in a patient after 28 days of uninterrupted antibabesia drug therapy and while still receiving treatment.

RESULTS

The clinical case histories of 3 highly immunocompromised patients who received a subcurative course of azithromycin-atovaquone associated with the eventual development of resistance to this drug regimen are described. One of the 3 patients died of complications related to babesiosis.

CONCLUSIONS

B. microti may become resistant to azithromycin-atovaquone during the treatment of babesiosis with this combined drug regimen in highly immunocompromised patients. Although research is needed to determine the optimal therapy for highly immunocompromised patients with babesiosis, reducing the level of immunosuppression when possible would appear to be a desirable strategy.

摘要

背景

巴贝斯虫病是一种新兴的蜱传疟疾样感染,主要由微小巴贝斯虫引起。这种感染通常会自行解决,或者在服用 7-10 天的阿奇霉素加阿托伐醌或克林霉素加奎宁后解决。虽然某些高度免疫功能低下的患者可能对这些药物方案反应不佳,但与疟疾不同,没有报道证据表明治疗失败的原因是感染了对药物有抵抗力的微小巴贝斯虫株。

方法

微小巴贝斯虫的耐药性出现定义为在不间断的抗巴贝斯虫药物治疗 28 天后,仍在接受治疗的情况下,患者出现临床和实验室异常,表明存在活动性巴贝斯虫病,同时出现微生物学复发(复发性寄生虫血症或寄生虫血症明显增加)。

结果

描述了 3 名高度免疫功能低下的患者接受亚治疗剂量的阿奇霉素-阿托伐醌治疗后,最终对该药物方案产生耐药性的临床病例。3 名患者中的 1 名因与巴贝斯虫病相关的并发症而死亡。

结论

在高度免疫功能低下的患者中,使用这种联合药物方案治疗巴贝斯虫病时,微小巴贝斯虫可能对阿奇霉素-阿托伐醌产生耐药性。虽然需要研究确定高度免疫功能低下的巴贝斯虫病患者的最佳治疗方法,但在可能的情况下降低免疫抑制水平似乎是一种理想的策略。

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