首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Low expression of the interleukin (IL)-4 receptor alpha chain and reduced signalling via the IL-4 receptor complex in human neonatal B cells.
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Low expression of the interleukin (IL)-4 receptor alpha chain and reduced signalling via the IL-4 receptor complex in human neonatal B cells.

机译:在人类新生儿B细胞中白介素(IL)-4受体α链的低表达和通过IL-4受体复合物的信号减少。

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摘要

Diminished neonatal antibody responses following infection or immunization may stem in part from intrinsic characteristics of neonatal B cells. In this study, we used B-cell subset sorting combined with gene expression assays to investigate major differences in the expression of host genes in neonatal and adult naive B cells. We discovered significantly reduced expression of the interleukin (IL)-4 receptor alpha chain and reduced IL-4-induced signalling in neonatal B cells. Neonatal naive B cells were susceptible to more rapid and more profound levels of apoptosis when cultured in vitro. They also exhibited a limited response to IL-4 treatment compared with adult cells. The expression level of the IL-13 receptor alpha 1 chain, a key component of the IL-13 receptor/IL-4 type II receptor, and the response to IL-13 treatment for protection against apoptosis in neonatal B cells were similar to those of the adult B cells. These studies suggest a possible mechanism underlying the limited magnitude and durability of neonatal antibody responses.
机译:感染或免疫后新生儿抗体反应减弱可能部分源于新生儿B细胞的固有特征。在这项研究中,我们使用B细胞亚群分类与基因表达分析相结合,研究了新生儿和成年幼稚B细胞中宿主基因表达的主要差异。我们发现新生儿B细胞中白介素(IL)-4受体α链的表达明显减少,并且IL-4诱导的信号减少。当在体外培养时,新生幼稚B细胞对更快速和更深远的凋亡水平敏感。与成年细胞相比,它们对IL-4处理的反应也有限。 IL-13受体α1链的表达水平,IL-13受体/ IL-4 II型受体的关键成分以及对IL-13治疗以防止新生B细胞凋亡的反应与那些相似成人B细胞的数量这些研究提示了新生儿抗体反应的有限幅度和持久性的潜在机制。

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