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Participation of Monocyte Subpopulations in Progression of Experimental Endotoxemia (EE) and Systemic Inflammation

机译:单核细胞亚流量在实验内毒血症(EE)和全身炎症进展中的参与

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Systemic inflammation plays a crucial role in formation of various pathological conditions, including sepsis, burns, and traumas. The main effector cells participating in progression of systemic inflammation response and sepsis are monocytes, which regulate both innate and acquired immunity via phagocytosis, synthesis of cytokines and chemokines, antigen presentation, and lymphocyte activation. Thus, the monocytes are considered as a link between innate and acquired immunity. The monocyte subpopulations taken into consideration in the study essentially determine the progression of systemic inflammation and could serve as targets for therapeutic intervention. The complexity of the analysis of pathophysiology of systemic inflammation lies in its high variability conditioned by individual peculiarities of the patients and inflammation progression specifications. To overcome these limitation, model of experimental endotoxemia (EE) is used. The results of EE, in turn, cannot be directly extrapolated on patients with the systemic inflammatory response. This review is dedicated to discussing the role of monocyte subpopulations in progression of systemic inflammation/sepsis and EE.
机译:全身炎症在形成各种病理条件下发挥至关重要的作用,包括败血症,烧伤和创伤。参与全身炎症反应和败血症进展的主要效应细胞是单核细胞,其通过吞噬作用,合成细胞因子和趋化因子,抗原呈递和淋巴细胞活化来调节先天性和获得的免疫。因此,单核细胞被认为是先天性和获得的免疫之间的联系。在该研究中考虑的单核细胞群基本上确定了系统性炎症的进展,可以作为治疗干预的目标。全身炎症病理生理学分析的复杂性在于患者单个特殊性的高可变性和炎症进展规范。为了克服这些限制,使用实验内毒血症(EE)的模型。反过来,EE的结果不能直接推断出全身炎症反应的患者。本综述致力于讨论单核细胞群在全身炎症/败血症和ee进展中的作用。

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