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通过CD40受体刺激B细胞期间转录因子NF-κB、AP-1和NF-AT的诱导。

Induction of the transcription factors NF-kappa B, AP-1 and NF-AT during B cell stimulation through the CD40 receptor.

作者信息

Francis D A, Karras J G, Ke X Y, Sen R, Rothstein T L

机构信息

Department of Pathology, Boston University Medical Center, MA 02118, USA.

出版信息

Int Immunol. 1995 Feb;7(2):151-61. doi: 10.1093/intimm/7.2.151.

Abstract

To address elements that might uniquely characterize CD40 mediated signaling, the nuclear expression of three transcription factors was evaluated following B cell stimulation by CD40L and by anti-Ig antibody. Cross-linked CD40L was found to induce nuclear expression of NF-kappa B, AP-1 and NF-AT with a time course and intensity similar to that produced by anti-Ig. Examination of NF-kappa B in more detail demonstrated that the CD40 mediated expression of DNA binding complexes correlated with induction of trans-activating activity which again attained similar levels following cross-linking of CD40 and slg. Despite the marked similarity in transcription factor induction triggered through CD40 and slg, differences in the intracellular signaling pathways utilized were apparent in that protein kinase C (PKC) depletion did not affect CD40 mediated induction of NF-kappa B even as induction by anti-Ig was abolished. These results suggest that a 'final common pathway' or convergence of transcription factor induction may exist for two distinct receptors, each of which is individually capable of triggering cell cycle progression, despite the use of separate intracellular signaling pathways that differ at the level of PKC. Although transcription factor induction was similar for CD40L and anti-Ig early on, subtle differences in expressed NF-kappa B and AP-1 nucleoprotein complexes were apparent at 24 h. Such differences may play a role in determining the variant effects on B cells of stimulation through these two receptors.

摘要

为了研究可能独特表征CD40介导信号传导的因素,在通过CD40L和抗Ig抗体刺激B细胞后,评估了三种转录因子的核表达情况。发现交联的CD40L诱导NF-κB、AP-1和NF-AT的核表达,其时间进程和强度与抗Ig产生的相似。对NF-κB的更详细检查表明,CD40介导的DNA结合复合物表达与反式激活活性的诱导相关,在CD40和表面免疫球蛋白交联后,反式激活活性再次达到相似水平。尽管通过CD40和表面免疫球蛋白触发的转录因子诱导存在明显相似性,但所利用的细胞内信号通路存在差异,表现为蛋白激酶C(PKC)耗竭不影响CD40介导的NF-κB诱导,而抗Ig诱导则被消除。这些结果表明,对于两种不同的受体可能存在转录因子诱导的“最终共同途径”或汇聚,尽管使用了在PKC水平不同的单独细胞内信号通路,但每种受体都能够单独触发细胞周期进程。虽然早期CD40L和抗Ig的转录因子诱导相似,但在24小时时,表达的NF-κB和AP-1核蛋白复合物存在细微差异。这些差异可能在决定通过这两种受体刺激对B细胞的不同影响中起作用。

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