首页> 外文期刊>Blood: The Journal of the American Society of Hematology >IL-15 regulates immature B-cell homing in an Ly49D-, IL-12 , and IL-18 dependent manner.
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IL-15 regulates immature B-cell homing in an Ly49D-, IL-12 , and IL-18 dependent manner.

机译:IL-15以Ly49D-,IL-12和IL-18依赖性方式调节未成熟B细胞归巢。

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摘要

To complete their maturation and participate in the humoral immune response, immature B cells that leave the bone marrow are targeted to specific areas in the spleen, where they differentiate into mature cells. Previously, we showed that immature B cells actively down-regulate their integrin-mediated migration to lymph nodes or to sites of inflammation, enabling their targeting to the spleen for final maturation. This inhibition is mediated by IFN-gamma, which is transcribed and secreted at low levels by these immature B cells; IFN-gamma expression is extinguished following B-cell maturation. Stimulation of the MHC class I receptor, Ly49D, triggers a signaling cascade that increases transcription of both IL-12 (p40) and IL-18; these, in turn, induce the secretion of IFN-gamma. In the present study, we demonstrate that Ly49D-dependent secretion of IL-12 and IL-18 induces IL-15 expression by immature B cells, and that these 3 factors together regulate IFN-gamma production that inhibits their ability to home to the lymph nodes or to sites of inflammation. Thus, IL-15 controls immature B-cell homing, resulting in shaping the B-cell repertoire to enable an efficient immune response.
机译:为了完成它们的成熟并参与体液免疫反应,离开骨髓的未成熟B细胞靶向脾脏中的特定区域,在那里它们分化为成熟细胞。以前,我们发现未成熟的B细胞会主动下调其整合素介导的迁移至淋巴结或炎症部位,从而使其靶向脾脏以达到最终成熟。这种抑制作用是由IFN-γ介导的,它们被这些未成熟的B细胞转录并以低水平分泌。 B细胞成熟后,IFN-γ表达消失。 MHC I类受体Ly49D的刺激触发信号级联反应,从而增加IL-12(p40)和IL-18的转录;这些反过来会诱导IFN-γ的分泌。在本研究中,我们证明了IL-12和IL-18的Ly49D依赖性分泌可诱导未成熟B细胞表达IL-15,并且这3个因子共同调节IFN-γ的产生,从而抑制了它们归巢于淋巴的能力。结或发炎部位。因此,IL-15控制着未成熟的B细胞归巢,从而使B细胞库成形,从而实现了有效的免疫反应。

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