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Innate immune system favors emergency monopoiesis at the expense of DC-differentiation to control systemic bacterial infection in mice

机译:先天免疫系统支持紧急monopoiesis以牺牲DC-differentiation控制系统性细菌感染的老鼠

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DCs are professional APCs playing a crucial role in the initiation of T-cell responses to combat infection. However, systemic bacterial infection with various pathogens leads to DC-depletion in humans and mice. The mechanisms of pathogen-induced DC-depletion remain poorly understood. Previously, we showed that mice infected with Yersinia enterocolitica (Ye) had impaired de novo DC-development, one reason for DC-depletion. Here, we extend these studies to gain insight into the molecular mechanisms of DC-depletion and the impact of different bacteria on DC-development. We show that the number of bone marrow (BM) hematopoietic progenitors committed to the DC lineage is reduced following systemic infection with different Gram-positive and Gram-negative bacteria. This is associated with a TLR4- and IFN--signaling dependent increase of committed monocyte progenitors in the BM and mature monocytes in the spleen upon Ye-infection. Adoptive transfer experiments revealed that infection-induced monopoiesis occurs at the expense of DC-development. Our data provide evidence for a general response of hematopoietic progenitors upon systemic bacterial infections to enhance monocyte production, thereby increasing the availability of innate immune cells for pathogen control, whereas impaired DC-development leads to DC-depletion, possibly driving transient immunosuppression in bacterial sepsis.
机译:DCs是专业装甲运兵车在其中扮演着重要的角色在t细胞反应的起始战斗感染。各种病原体导致DC-depletion人类和老鼠。pathogen-induced DC-depletion仍然很差理解。感染鼠疫的enterocolitica(你们)新创DC-development受损的原因之一DC-depletion。洞察的分子机制DC-depletion和不同的细菌的影响DC-development。骨髓造血祖细胞(BM)致力于减少直流血统系统性感染不同的革兰氏阳性和革兰氏阴性细菌。与TLR4和干扰素信号相关的增加的承诺单核细胞祖细胞BM和成熟单核细胞在脾脏Ye-infection。表明,侵染诱导monopoiesis发生在DC-development为代价的。提供证据的一般反应造血祖细胞在系统性细菌感染增强单核细胞生产,从而增加先天的可用性为控制病原体的免疫细胞,而DC-development受损导致DC-depletion,可能开车瞬态免疫抑制细菌性败血症。

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