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Limited Activity of Clofazimine as a Single Drug in a Mouse Model of Tuberculosis Exhibiting Caseous Necrotic Granulomas

机译:克洛他明作为单一药物在结核性干酪样坏死性肉芽肿的小鼠模型中的有限活性

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摘要

New drugs and drugs with a novel mechanism of action are desperately needed to shorten the duration of tuberculosis treatment, to prevent the emergence of drug resistance, and to treat multiple-drug-resistant strains of Mycobacterium tuberculosis. Recently, there has been renewed interest in clofazimine (CFZ). In this study, we utilized the C3HeB/FeJ mouse model, possessing highly organized, hypoxic pulmonary granulomas with caseous necrosis, to evaluate CFZ monotherapy in comparison to results with BALB/c mice, which form only multifocal, coalescing cellular aggregates devoid of caseous necrosis. While CFZ treatment was highly effective in BALB/c mice, its activity was attenuated in the lungs of C3HeB/FeJ mice. This lack of efficacy was directly related to the pathological progression of disease in these mice, since administration of CFZ prior to the formation of hypoxic, necrotic granulomas reconstituted bactericidal activity in this mouse strain. These results support the continued use of mouse models of tuberculosis infection which exhibit a granulomatous response in the lungs that more closely resembles the pathology found in human disease.
机译:迫切需要新药和具有新颖作用机制的药物,以缩短结核病的治疗时间,防止耐药性的出现以及治疗结核分枝杆菌的多重耐药菌株。最近,人们对氯氟嗪明(CFZ)产生了新的兴趣。在这项研究中,我们利用具有高度组织性,缺氧性肺肉芽肿伴干酪样坏死的C3HeB / FeJ小鼠模型,评估CFZ单一疗法与BALB / c小鼠的结果相比,后者仅形成多灶,合并的细胞聚集体,没有干酪样坏死。虽然CFZ治疗在BALB / c小鼠中非常有效,但其活性在C3HeB / FeJ小鼠的肺中减弱了。这种功效的缺乏与这些小鼠的疾病病理进展直接相关,因为在缺氧,坏死性肉芽肿形成之前施用CFZ可以使该小鼠品系恢复杀菌活性。这些结果支持继续使用结核感染的小鼠模型,该模型在肺部表现出肉芽肿反应,与人类疾病中发现的病理更为相似。

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