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Novel regulatory functions for Toll-like receptor-activated B cells during intracellular bacterial infection

机译:细胞内细菌感染过程中Toll样受体激活的B细胞的新型调节功能。

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Infections by intracellular bacterial pathogens remain a major cause of human diseases worldwide. Despite intensive efforts, the development of effective vaccines or immunotherapies against these diseases has largely remained unsuccessful, asking for the exploration of new aspects of the host response to these pathogens. Genetic studies have demonstrated beyond doubt that cell-mediated mechanisms of host defense involving innate immunity and T cells are of crucial importance for the control of these diseases. By contrast, the role of B cells during intracellular bacterial infection has so far received little attention besides their role as antibody-producing cells. However, the general knowledge of B-cell immunology and in particular of their antibody-independent functions has greatly increased during the last years. Recently, it was found in a model of Salmonella typhimurium infection that Toll-like receptor triggering on B cells resulted through interleukin-10 secretion in a marked suppression of innate defense mechanisms ultimately leading to uncontrolled growth of the bacteria and earlier death from the disease during both primary and secondary infections. This article reviews the protective and deleterious roles of B cells during intracellular bacterial infections and discusses how manipulating their antibody-independent functions may be a powerful means to therapeutically improve host resistance against these diseases.
机译:细胞内细菌病原体的感染仍然是全世界人类疾病的主要原因。尽管付出了巨大的努力,但针对这些疾病的有效疫苗或免疫疗法的开发仍基本上没有成功,要求探索宿主对这些病原体反应的新方面。遗传学研究毫无疑问地表明,涉及先天免疫和T细胞的细胞介导的宿主防御机制对于控制这些疾病至关重要。相比之下,到目前为止,B细胞在细胞内细菌感染中的作用除了作为抗体产生细胞的作用外,几乎没有受到关注。然而,在最近几年中,B细胞免疫学的常识,尤其是其不依赖抗体的功能有了很大的提高。最近,在鼠伤寒沙门氏菌感染的模型中发现,白细胞介素10的分泌可导致Toll样受体触发B细胞,从而显着抑制先天防御机制,最终导致细菌不受控制的生长和疾病早期死亡。原发和继发感染。本文回顾了B细胞在细胞内细菌感染过程中的保护作用和有害作用,并讨论了如何操纵其抗体非依赖性功能可能是治疗上改善宿主抵抗这些疾病的有效方法。

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