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用抗体-蒜氨酸酶缀合物和蒜氨酸治疗鼠肺曲霉病。

Therapy of murine pulmonary aspergillosis with antibody-alliinase conjugates and alliin.

机构信息

Department of Biological Chemistry, Weizmann Institute of Science, Rehovot 76100, Israel.

出版信息

Antimicrob Agents Chemother. 2010 Feb;54(2):898-906. doi: 10.1128/AAC.01267-09. Epub 2009 Nov 30.

Abstract

Aspergillus fumigatus is an opportunistic fungal pathogen responsible for invasive aspergillosis in immunocompromised individuals. The high morbidity and mortality rates as well as the poor efficacy of antifungal agents remain major clinical concerns. Allicin (diallyl-dithiosulfinate), which is produced by the garlic enzyme alliinase from the harmless substrate alliin, has been shown to have wide-range antifungal specificity. A monoclonal antibody (MAb) against A. fumigatus was produced and chemically ligated to the enzyme alliinase. The purified antibody-alliinase conjugate bound to conidia and hyphae of A. fumigatus at nanomolar concentrations. In the presence of alliin, the conjugate produced cytotoxic allicin molecules, which killed the fungus. In vivo testing of the therapeutical potential of the conjugate was carried out in immunosuppressed mice infected intranasally with conidia of A. fumigatus. Intratracheal (i.t.) instillation of the conjugate and alliin (four treatments) resulted in 80 to 85% animal survival (36 days), with almost complete fungal clearance. Repetitive intratracheal administration of the conjugate and alliin was also effective when treatments were initiated at a more advanced stage of infection (50 h). The fungi were killed specifically without causing damage to the lung tissue or overt discomfort to the animals. Intratracheal instillation of the conjugate without alliin or of the unconjugated monoclonal antibody significantly delayed the death of the infected mice, but only 20% of the animals survived. A limitation of this study is that the demonstration was achieved in a constrained setting. Other routes of drug delivery will be investigated for the treatment of pulmonary and extrapulmonary aspergillosis.

摘要

烟曲霉是一种机会性真菌病原体,可导致免疫功能低下个体发生侵袭性曲霉病。高发病率和死亡率以及抗真菌药物疗效不佳仍然是主要的临床关注点。大蒜酶蒜氨酸酶从无害的底物蒜氨酸中产生的大蒜素(二烯丙基二硫代亚磺酸酯)已被证明具有广泛的抗真菌特异性。针对烟曲霉产生了一种单克隆抗体(MAb),并用化学方法将其连接到酶蒜氨酸酶上。纯化的抗体-蒜氨酸酶缀合物在纳摩尔浓度下结合到烟曲霉的分生孢子和菌丝上。在蒜氨酸存在的情况下,该缀合物产生细胞毒性的大蒜素分子,从而杀死真菌。在免疫抑制的小鼠中进行了该缀合物的治疗潜力的体内测试,这些小鼠通过鼻腔感染了烟曲霉的分生孢子。气管内(i.t.)滴注缀合物和蒜氨酸(四次治疗)导致 80-85%的动物存活(36 天),几乎完全清除了真菌。在感染的更晚期(50 小时)开始进行重复气管内给药时,该缀合物和蒜氨酸的重复给药也是有效的。该真菌被特异性杀死,而不会对肺组织造成损害或使动物感到明显不适。气管内滴注没有蒜氨酸的缀合物或未缀合的单克隆抗体会明显延迟感染小鼠的死亡,但只有 20%的动物存活。这项研究的局限性在于,在有限的环境中进行了证明。将研究其他药物输送途径以治疗肺部和肺外曲霉病。

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