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首页> 外文期刊>Clinical and vaccine immunology: CVI >Reduced frequency of a CD14+ CD16+ monocyte subset with high toll-like receptor 4 expression in cord blood compared to adult blood contributes to lipopolysaccharide hyporesponsiveness in newborns
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Reduced frequency of a CD14+ CD16+ monocyte subset with high toll-like receptor 4 expression in cord blood compared to adult blood contributes to lipopolysaccharide hyporesponsiveness in newborns

机译:与成人血液相比,脐带血中具有高收费的受体4表达的CD14+ CD16+单核细胞子集的频率降低,导致新生儿的脂多糖低估

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The human innate immune response to pathogens is not fully effective and mature until well into childhood, as exemplified by various responses to Toll-like receptor (TLR) agonists in newborns compared to adults. To better understand the mechanistic basis for this age-related difference in innate immunity, we compared tumor necrosis factor alpha (TNF-α) production by monocytes from cord blood (CB) and adult blood (AB) in response to LAM (lipoarabinomannan from Mycobacterium tuberculosis, a TLR2 ligand) and LPS (lipopolysaccharide from Escherichia coli, a TLR4 ligand). LPS or LAM-induced TNF-α production was 5 to 18 times higher in AB than in CB monocytes, whereas interleukin-1α (IL-1α) stimulated similar levels of TNF-α in both groups, suggesting that decreased responses to LPS or LAM in CB are unlikely to be due to differences in the MyD88-dependent signaling pathway. This impaired signaling was attributable, in part, to lower functional TLR4 expression, especially on CD14+ CD16+ monocytes, which are the primary cell subset for LPS-induced TNF-α production. Importantly, the frequency of CD14+ CD16+ monocytes in CB was 2.5-fold lower than in AB (P 0.01). CB from Kenyan newborns sensitized to parasite antigens in utero had more CD14+ CD16+ monocytes (P = 0.02) and produced higher levels of TNF-α in response to LPS (P = 0.004) than CB from unsensitized Kenyan or North American newborns. Thus, a reduced CD14+ CD16+ activated/differentiated monocyte subset and a correspondingly lower level of functional TLR4 on monocytes contributes to the relatively low TNF-α response to LPS observed in immunologically naive newborns compared to the response in adults.
机译:与成年人相比,人类对病原体的先天免疫反应直到童年直到童年才完全有效和成熟,这是对新生儿的Toll样受体(TLR)激动剂的各种反应的例证。为了更好地理解这种与先天免疫相关的年龄相关差异的机理基础,我们比较了来自脐带血(CB)和成人血液(AB)的单核细胞的肿瘤坏死因子α(TNF-α)的生产,以响应LAM(脂肪肉虫杆菌中的脂肪肉芽菌群。结核病,TLR2配体)和LPS(来自Escherichia Coli,TLR4配体的脂多糖)。在AB中,LPS或LAM诱导的TNF-α的产生比CB单核细胞高5至18倍,而两组的白介素1α(IL-1α)刺激了类似的TNF-α水平,这表明对LPS或LAM的反应降低了。在CB中,不太可能是由于MYD88依赖性信号通路的差异所致。这种受损的信号传导部分归因于降低功能性TLR4表达,尤其是在CD14+ CD16+单核细胞上,这是LPS诱导的TNF-α产生的主要细胞子集。重要的是,CB中CD14+ CD16+单核细胞的频率比AB低2.5倍(P< 0.01)。来自肯尼亚新生儿的CB对子宫内的寄生虫抗原的敏感性更高的CD14+ CD16+单核细胞(P = 0.02)多于对LPS的CD14+ CD16+单核细胞(p = 0.02),而TNF-α水平高于LPS(p = 0.004)(p = 0.004)(p = 0.004)。因此,与成年人相比,与单核细胞的CD14+ CD16+激活/分化的单核细胞子集和单核细胞上相应较低的功能性TLR4水平相比,与成年人的反应相比,在免疫天真新生儿中观察到的LPS对LPS的TNF-α反应相对较低。

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