首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >Expression profile of cord blood neutrophils and dysregulation of HSPA1A and OLR1 upon challenge by bacterial peptidoglycan
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Expression profile of cord blood neutrophils and dysregulation of HSPA1A and OLR1 upon challenge by bacterial peptidoglycan

机译:细菌肽聚糖攻击后脐血中性粒细胞的表达谱和HSPA1A和OLR1的异常表达

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In newborn infants, the innate cellular system plays a crucial role in the first line of defense against pathogens. Neutrophils are the most abundant leukocytes, and their response to the commonly encountered nos-ocomial bacterial (Gram positive) infection in newborns remains largely unclear. In this study, a genome-wide expression array analysis was performed on CB neutrophils after challenge by PGN in vitro and compared with neutrophils in CTL cultures without PGN. We investigated responses of neutrophils to PGN and LPS, with respect to cytokine synthesis, chemotaxis, ROS production, cell death, and pathways of HSP response. Our results provide the first comprehensive expres-sional profile of neonatal neutrophils stimulated by PGN. mRNA levels of 16 up-regulated genes and 6 down-regulated genes were validated by qPCR. Their regulatory networks were identified downstream of TLR-2 and NOD-2, which work in concert toward signals of death, cytoprotection, inflammation, and stress responses. Members of the HSP family were significantly up-regulated in PGN-stimulated neutrophils, compared with those in LPS-stimulated cells. We confirmed protein co-precipitation of HSPA1A and OLR1 in stimulated neutrophils, and their transcription, induced by NF-kappaB but not by MAPK signals. We found increased CD11b, chemotaxis, TNF-alpha, and IL-8 in neutrophils stimulated by PGN or LPS. PGN, but not LPS, increased ROS production. We conclude that neonatal neutrophils are capable of vigorous molecular and functional responses to PGN and suggest that HSP plays a critical role in the host defense mechanism, possibly involving proinflam-matory OLR1 and CD11b-facilitated chemotaxis.
机译:在新生儿中,先天细胞系统在抵抗病原体的第一道防线中起着至关重要的作用。中性粒细胞是最丰富的白细胞,它们对新生儿中常见的no-ocomial细菌(革兰氏阳性)感染的反应仍不清楚。在这项研究中,在体外受到PGN攻击后,对CB中性粒细胞进行了全基因组表达阵列分析,并与无PGN的CTL培养物中的中性粒细胞进行了比较。我们研究了中性粒细胞对PGN和LPS的反应,涉及细胞因子合成,趋化性,ROS产生,细胞死亡和HSP反应途径。我们的结果提供了由PGN刺激的新生儿嗜中性粒细胞的第一个全面的表达概况。通过qPCR验证了16个上调基因和6个下调基因的mRNA水平。在TLR-2和NOD-2的下游确定了它们的调控网络,它们协同作用于死亡,细胞保护,炎症和应激反应的信号。与LPS刺激的细胞相比,PGN刺激的中性粒细胞的HSP家族成员明显上调。我们证实了受刺激的中性粒细胞中HSPA1A和OLR1的蛋白共沉淀及其转录,是由NF-κB而非由MAPK信号诱导的。我们发现由PGN或LPS刺激的嗜中性粒细胞CD11b,趋化性,TNF-α和IL-8含量增加。 PGN(而非LPS)增加了ROS的产生。我们得出的结论是,新生儿嗜中性粒细胞能够对PGN进行强烈的分子和功能反应,并暗示HSP在宿主防御机制中起关键作用,可能涉及促炎性OLR1和CD11b促进的趋化性。

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