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T-cell receptor early signalling complex activation in response to interferon-alpha receptor stimulation

  作者 Stevens, CN; Simeone, AM; John, S; Ahmed, Z; Lucherini, OM; Baldari, CT; Ladbury, JE  
  选自 期刊  Biochemical Journal;  卷期  2010年428-Part 3;  页码  429-437  
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[摘要]Signalling through the IFN alpha R (interferon-alpha receptor) and TCR (T-cell receptor) in Jurkat T lymphocytes results in distinct immune responses. Despite this both receptors elicit ERK (extracellular-signal-regulated kinase)/MAPK (mitogen-activated protein kinase) phosphorylation. Vav and Slp76 are shown to be required for IFN alpha (interferon-alpha)-stimulated ERK activity. These form a subset of proteins which behave identically on stimulation of both receptors. TCR deletion abrogates IFN alpha R-stimulated MAPK activity, whereas the canonical JAK/STAT (Janus kinase/signal transducer and activator of transcription) pathway is unaffected. Thus recruitment of the intact TCR ESC (early signalling complex) is necessary for this downstream MAPK response. Despite using a common ESC, stimulation of the IFN alpha R does not produce the transcriptional response associated with TCR. Up-regulation of the MAPK pathway by IFN alpha R might be important to ensure that the cell responds to only one stimulant.

 
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