Kawagoe Tatsukata, Sato Shintaro, Matsushita Kazufumi, Kato Hiroki, Matsui Kosuke, Kumagai Yutaro, Saitoh Tatsuya, Kawai Taro, Takeuchi Osamu, Akira Shizuo
Laboratory of Host Defense, World Premier International Research Center, 3-1 Yamada-oka, Suita, Osaka 565-0871, Japan.
Nat Immunol. 2008 Jun;9(6):684-91. doi: 10.1038/ni.1606. Epub 2008 Apr 27.
Members of the IRAK family of kinases mediate Toll-like receptor (TLR) signaling. Here we show that IRAK2 was essential for sustaining TLR-induced expression of genes encoding cytokines and activation of the transcription factor NF-kappaB, despite the fact that IRAK2 was dispensable for activation of the initial signaling cascades. IRAK2 was activated 'downstream' of IRAK4, like IRAK1, and TLR-induced cytokine production was abrogated in the absence of both IRAK1 and IRAK2. Whereas the kinase activity of IRAK1 decreased within 1 h of TLR2 stimulation, coincident with IRAK1 degradation, the kinase activity of IRAK2 was sustained and peaked at 8 h after stimulation. Thus, IRAK2 is critical in late-phase TLR responses, and IRAK1 and IRAK2 are essential for the initial responses to TLR stimulation.
白细胞介素-1受体相关激酶(IRAK)家族的成员介导Toll样受体(TLR)信号传导。我们在此表明,IRAK2对于维持TLR诱导的细胞因子编码基因的表达以及转录因子NF-κB的激活至关重要,尽管IRAK2对于初始信号级联的激活是可有可无的。与IRAK1一样,IRAK2在IRAK4的“下游”被激活,并且在同时缺失IRAK1和IRAK2的情况下,TLR诱导的细胞因子产生被消除。虽然IRAK1的激酶活性在TLR2刺激后1小时内下降,这与IRAK1的降解同时发生,但IRAK2的激酶活性得以维持并在刺激后8小时达到峰值。因此,IRAK2在TLR反应的后期阶段至关重要,而IRAK1和IRAK2对于TLR刺激的初始反应必不可少。
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