A noncanonical IRAK4-IRAK1 pathway counters DNA damage-induced apoptosis independently of TLR/IL-1R signaling.

IF 7.3 1区 生物学
Yuanyuan Li, Richa B Shah, Samanta Sarti, Alicia L Belcher, Brian J Lee, Andrej Gorbatenko, Francesca Nemati, Honglin Yu, Zoe Stanley, Mahbuba Rahman, Zhengping Shao, Jose M Silva, Shan Zha, Samuel Sidi
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Abstract

Interleukin-1 receptor (IL-1R)-associated kinases (IRAKs) are core effectors of Toll-like receptors (TLRs) and IL-1R in innate immunity. Here, we found that IRAK4 and IRAK1 together inhibited DNA damage-induced cell death independently of TLR or IL-1R signaling. In human cancer cells, IRAK4 was activated downstream of ATR kinase in response to double-strand breaks (DSBs) induced by ionizing radiation (IR). Activated IRAK4 then formed a complex with and activated IRAK1. The formation of this complex required the E3 ubiquitin ligase Pellino1, acting structurally but not catalytically, and the activation of IRAK1 occurred independently of extracellular signaling, intracellular TLRs, and the TLR/IL-1R signaling adaptor MyD88. Activated IRAK1 translocated to the nucleus in a Pellino2-dependent manner. In the nucleus, IRAK1 bound to the PIDD1 subunit of the proapoptotic PIDDosome and interfered with platform assembly, thus supporting cell survival. This noncanonical IRAK signaling pathway was also activated in response to other DSB-inducing agents. The loss of IRAK4, of IRAK4 kinase activity, of either Pellino protein, or of the nuclear localization sequence in IRAK1 sensitized p53-mutant zebrafish to radiation. Thus, the findings may lead to strategies for overcoming tumor resistance to conventional cancer treatments.

独立于 TLR/IL-1R 信号的非经典 IRAK4-IRAK1 通路可对抗 DNA 损伤诱导的细胞凋亡。
白细胞介素-1受体(IL-1R)相关激酶(IRAK)是先天性免疫中Toll样受体(TLR)和IL-1R的核心效应因子。在这里,我们发现IRAK4和IRAK1共同抑制DNA损伤诱导的细胞死亡,而不受TLR或IL-1R信号转导的影响。在人类癌细胞中,当电离辐射(IR)诱导双链断裂(DSB)时,IRAK4在ATR激酶下游被激活。活化的 IRAK4 随后与 IRAK1 形成复合物并活化 IRAK1。该复合物的形成需要E3泛素连接酶Pellino1,Pellino1在结构上起作用而不是催化作用,IRAK1的活化不受细胞外信号、细胞内TLR和TLR/IL-1R信号适配体MyD88的影响。活化的 IRAK1 以 Pellino2 依赖性方式转位到细胞核。在细胞核中,IRAK1 与促凋亡 PIDDosome 的 PIDD1 亚基结合,干扰平台组装,从而支持细胞存活。这种非经典的IRAK信号通路在其他DSB诱导剂的作用下也会被激活。IRAK4、IRAK4激酶活性、Pellino蛋白或IRAK1核定位序列的缺失使p53突变斑马鱼对辐射敏感。因此,这些发现可能会为克服肿瘤对常规癌症治疗的抗药性提供策略。
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来源期刊
Science Signaling
Science Signaling Biochemistry, Genetics and Molecular Biology-Molecular Biology
自引率
0.00%
发文量
148
期刊介绍: Science Signaling is a weekly, online multidisciplinary journal dedicated to the life sciences. Our editorial team's mission is to publish studies that elucidate the fundamental mechanisms underlying biological processes across various organisms. We prioritize research that offers novel insights into physiology, elucidates aberrant mechanisms leading to disease, identifies potential therapeutic targets and strategies, and characterizes the effects of drugs both in vitro and in vivo.
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