[A putative immunotherapy with biological response modifiers (BRM) against intractable pulmonary tuberculosis].

Kekkaku : [Tuberculosis] Pub Date : 2001-12-01
A Saito
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Abstract

The problem of tuberculosis is emerging again with increase in the population of aged people and immunocompromised patients in Japan. It has been well documented that cell-mediated immunity play a central role in host resistance to infection with Mycobacterium tuberculosis. Many recent studies have provided evidences suggesting that the Th1-Th2 cytokine balance may determine the outcome of some diseases: predominant production of Th1 cytokines may prevent the occurrence of infectious diseases caused by intracellularly growing pathogens and Th2 cytokines may be involved in the exacerbation of allergic diseases. On the other hand, IL-12 plays an essential role in the differentiation of Th1 cells from naive T cells, and IL-18 potentiates this effect although it does not show such effect by itself. In previous investigations using gene-disrupted mice, the essential roles for IFN-gamma, IL-12 and IL-18 have been demonstrated. There are several host factors which determines the outcome of mycobacterial infection. Among them, steroid treatment and AIDS are important factors. In this lecture, I addressed the effect of these pathological conditions on Th1-Th2 cytokine balance and outcome of mycobacterial infection using murine models. In both conditions, the exacerbated infection was well correlated with the reduced production of IFN-gamma. Furthermore, I also talked about the relationship between other host factors and balance in the production of Th1 and Th2 cytokines. Using a murine model of fatal infection with M. tuberculosis, we demonstrated the therapeutic effect of Th1-type cytokines against this infection and suggested that immunotherapy with these cytokines may be clinically effective in the intractable infection. We tried a combined therapy with anti-tuberculous agents and IFN-gamma in intractable pulmonary tuberculosis caused by multidrug-resistant pathogen in a patient with insulin-dependent diabetes mellitus. Although no report showing the clinical use of IL-12 in infectious diseases has been seen, clinical trials already commenced for the therapy of malignant neoplastic diseases. It may not be in far future that this cytokine is clinically used for the treatment of infectious diseases. IL-18 has not yet been under the clinical trials.

[用生物反应调节剂(BRM)治疗顽固性肺结核的假定免疫疗法]。
随着日本老年人口和免疫力低下患者的增加,结核病问题再次出现。大量文献表明,细胞介导免疫在宿主抵抗结核分枝杆菌感染的过程中发挥着核心作用。最近的许多研究表明,Th1-Th2 细胞因子的平衡可能会决定某些疾病的结局:Th1 细胞因子的主要分泌可能会阻止由细胞内生长的病原体引起的感染性疾病的发生,而 Th2 细胞因子则可能参与过敏性疾病的恶化。另一方面,IL-12 在从幼稚 T 细胞分化出 Th1 细胞的过程中起着至关重要的作用,IL-18 可增强这种作用,尽管它本身并不显示这种作用。以前利用基因缺失小鼠进行的研究表明,IFN-γ、IL-12 和 IL-18 发挥着重要作用。有几种宿主因素决定了分枝杆菌感染的结果。其中,类固醇治疗和艾滋病是重要因素。在本讲座中,我利用小鼠模型探讨了这些病理条件对 Th1-Th2 细胞因子平衡和霉菌感染结局的影响。在这两种情况下,感染的加重与 IFN-gamma 的产生减少密切相关。此外,我还谈到了其他宿主因素与 Th1 和 Th2 细胞因子产生平衡之间的关系。我们利用结核杆菌致命感染的小鼠模型,证明了 Th1 型细胞因子对这种感染的治疗效果,并提出使用这些细胞因子的免疫疗法可能对难治性感染有临床疗效。我们尝试用抗结核药物和 IFN-gamma 联合疗法治疗一名胰岛素依赖型糖尿病患者因耐多药病原体引起的难治性肺结核。虽然还没有报告显示 IL-12 在传染病中的临床应用,但用于治疗恶性肿瘤疾病的临床试验已经开始。也许在不久的将来,这种细胞因子才会在临床上用于治疗传染病。IL-18 尚未进行临床试验。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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