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脐血T细胞上CD40配体的表达无效可能导致新生儿免疫球蛋白产生不足。

Ineffective expression of CD40 ligand on cord blood T cells may contribute to poor immunoglobulin production in the newborn.

作者信息

Brugnoni D, Airò P, Graf D, Marconi M, Lebowitz M, Plebani A, Giliani S, Malacarne F, Cattaneo R, Ugazio A G

机构信息

Clinical Immunology Service, University of Brescia, Italy.

出版信息

Eur J Immunol. 1994 Aug;24(8):1919-24. doi: 10.1002/eji.1830240831.

Abstract

A major feature of the immature immune system in the newborn is its inability to produce significant levels of immunoglobulins other than IgM in response to antigens. It has recently been demonstrated that interaction of the CD40 molecule on B cells with the CD40 ligand (CD40L) on activated T cells is pivotal for immunoglobulin switching. In view of these findings, we have tested cord blood mononuclear cells (CBMC) for expression of CD40L. Our data clearly demonstrate that freshly isolated CBMC do not express significant levels of CD40L upon in vitro activation; this defect is intrinsic to CD4+ cord blood lymphocytes. In vitro priming of CBMC with phytohemagglutinin and interleukin-2 for several days induced a conversion from the "naive" to the "memory" phenotype (as assessed by expression of CD45 isoforms) and led to substantial CD40L expression upon appropriate restimulation. These data indicate that ineffective CD40L expression might represent a major factor for reduced immunoglobulin production in the neonate, and suggest that antigenic exposure in vivo leads to changes in the genetic program, enabling T cells to express CD40L.

摘要

新生儿未成熟免疫系统的一个主要特征是,其在对抗原作出反应时,除了IgM之外,无法产生大量的免疫球蛋白。最近有研究表明,B细胞上的CD40分子与活化T细胞上的CD40配体(CD40L)之间的相互作用对于免疫球蛋白类别转换至关重要。鉴于这些发现,我们检测了脐血单个核细胞(CBMC)中CD40L的表达情况。我们的数据清楚地表明,新鲜分离的CBMC在体外活化后并不会表达大量的CD40L;这种缺陷是CD4+脐血淋巴细胞所固有的。用植物血凝素和白细胞介素-2对CBMC进行体外致敏处理数天,可诱导其从“初始”表型转变为“记忆”表型(通过CD45同工型的表达进行评估),并在适当的再刺激后导致大量CD40L表达。这些数据表明,CD40L表达无效可能是新生儿免疫球蛋白产生减少的一个主要因素,并提示体内的抗原暴露会导致基因程序发生变化,使T细胞能够表达CD40L。

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