首页> 美国卫生研究院文献>Infection and Immunity >Depletion of interleukin-4 in BALB/c mice with established Leishmania major infections increases the efficacy of antimony therapy and promotes Th1-like responses.
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Depletion of interleukin-4 in BALB/c mice with established Leishmania major infections increases the efficacy of antimony therapy and promotes Th1-like responses.

机译:在已确定的利什曼原虫主要感染的BALB / c小鼠中白细胞介素4的消耗增加了锑治疗的功效并促进了Th1样反应。

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摘要

Whereas most inbred mouse strains mount a protective Th1 helper T-cell response following infection with Leishmania major, an ineffective Th2 response develops in BALB/c mice, leading to the development of disseminated, ultimately fatal disease. Interleukin-4 (IL-4) production is required for the initiation of the Th2 response, though little is known about the requirements for the long-term maintenance of this response. In order to investigate the role of the expanding parasite population on the Th2 response, mice infected for 2 weeks with L. major, which exhibited a Th2-like cytokine profile, were treated with a leishmanicidal agent (Pentostam) and/or various doses of anti-IL-4 antibody. Untreated mice, mice treated with Pentostam alone, or mice treated with 2.5 mg of anti-IL-4 antibody given at days 13 and 21 of infection developed progressive disease. However, in 8 of 10 mice treated with this dose of anti-IL-4 antibody plus Pentostam lesion development was arrested and lesions were either controlled or eventually healed. Healing was associated with the production of high levels of gamma interferon by spleen cells, and low levels of immunoglobulin E in serum compared with levels for control animals, indicating that a Th1-like response had developed in mice receiving both treatments. Thus, depletion of IL-4 only in combination with a reduction in the parasite burden allowed the expression of a Th1 response. When the dose of anti-IL-4 antibody was increased to 5 mg per injection, all mice treated with this dose of antibody, with or without Pentostam therapy, healed. However, combined therapy with Pentostam in mice treated with this dose of antibody had an additional protective effect. As expected, a Th1 response developed in mice treated with this dose of anti-IL-4 antibody with or without combined therapy with Pentostam, whereas a Th2 response developed in control mice. Thus, a significant effect on the course of disease is noted when mice with established L. major infections are treated with anti-IL-4 antibody in combination with Pentostam, suggesting that the combined effect of inhibiting IL-4 and reducing the parasite burden has a dramatic effect on the development of resistance to L. major.
机译:大多数自交系小鼠品系在感染大利什曼原虫后会产生保护性Th1辅助性T细胞应答,而BALB / c小鼠会产生无效的Th2应答,从而导致传播性疾病,最终导致致命性疾病的发展。 Th2应答的启动需要白细胞介素4(IL-4)的产生,尽管对这种应答的长期维持的要求知之甚少。为了研究不断扩大的寄生虫种群对Th2应答的作用,用利什曼杀菌剂(Pentostam)和/或不同剂量的Lethmanicidal agent(Pentostam)处理了感染L.major L. 2周的大型利什曼原虫感染的小鼠。抗IL-4抗体。未经治疗的小鼠,仅接受戊喷坦治疗的小鼠或在感染的第13和21天给予2.5 mg抗IL-4抗体治疗的小鼠会发展为疾病。但是,在用这种剂量的抗IL-4抗体加Pentostam治疗的10只小鼠中,有8只被阻止,病灶被控制或最终被治愈。与对照动物的水平相比,愈合与脾细胞高水平的γ-干扰素的产生以及血清中免疫球蛋白E的低水平相关,这表明接受两种治疗的小鼠均出现了类似Th1的应答。因此,仅通过减少IL-4与降低寄生虫负担相结合,就可以表达Th1应答。当抗IL-4抗体的剂量增加至每次注射5 mg时,所有接受该剂量抗体(接受或不接受Pentostam治疗)的小鼠均mice愈。但是,在用该剂量抗体治疗的小鼠中与戊喷坦联合治疗具有额外的保护作用。如预期的那样,在接受或未接受戊喷坦联合治疗的情况下,在用这种剂量的抗IL-4抗体治疗的小鼠中出现Th1反应,而在对照小鼠中出现Th2反应。因此,当用抗IL-4抗体和戊喷坦联合治疗已确立的重症梭状芽胞杆菌感染的小鼠时,对疾病进程具有显着影响,这表明抑制IL-4和减少寄生虫负担的综合作用具有对大麦芽孢杆菌的抗性发展有显着影响。

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