双链 RNA 上的 ADAR1 dsRBD3-PKR 激酶结构域相互作用抑制 PKR 激活。
An ADAR1 dsRBD3-PKR kinase domain interaction on dsRNA inhibits PKR activation.
机构信息
Central European Institute for Technology at Masaryk University (CEITEC MU), Building E35, Kamenice 735/5, 625 00 Brno, Czechia; National Centre for Biomolecular Research, Faculty of Science, Masaryk University, Kamenice 5, 625 00 Brno, Czechia.
Central European Institute for Technology at Masaryk University (CEITEC MU), Building E35, Kamenice 735/5, 625 00 Brno, Czechia.
出版信息
Cell Rep. 2024 Aug 27;43(8):114618. doi: 10.1016/j.celrep.2024.114618. Epub 2024 Aug 14.
Adar null mutant mouse embryos die with aberrant double-stranded RNA (dsRNA)-driven interferon induction, and Adar Mavs double mutants, in which interferon induction is prevented, die soon after birth. Protein kinase R (Pkr) is aberrantly activated in Adar Mavs mouse pup intestines before death, intestinal crypt cells die, and intestinal villi are lost. Adar Mavs Eifak2 (Pkr) triple mutant mice rescue all defects and have long-term survival. Adenosine deaminase acting on RNA 1 (ADAR1) and PKR co-immunoprecipitate from cells, suggesting PKR inhibition by direct interaction. AlphaFold studies on an inhibitory PKR dsRNA binding domain (dsRBD)-kinase domain interaction before dsRNA binding and on an inhibitory ADAR1 dsRBD3-PKR kinase domain interaction on dsRNA provide a testable model of the inhibition. Wild-type or editing-inactive human ADAR1 expressed in A549 cells inhibits activation of endogenous PKR. ADAR1 dsRNA binding is required for, but is not sufficient for, PKR inhibition. Mutating the ADAR1 dsRBD3-PKR contact prevents co-immunoprecipitation, ADAR1 inhibition of PKR activity, and co-localization of ADAR1 and PKR in cells.
Adar 缺失突变体小鼠胚胎在双链 RNA (dsRNA) 驱动的干扰素诱导下死亡,而 Adar Mavs 双突变体,其中干扰素诱导被阻止,出生后不久即死亡。蛋白激酶 R (Pkr) 在 Adar Mavs 小鼠幼仔肠道死亡前异常激活,肠隐窝细胞死亡,肠绒毛丢失。Adar Mavs Eifak2 (Pkr) 三重突变体小鼠挽救了所有缺陷,并具有长期存活。来自细胞的腺苷脱氨酶作用于 RNA 1 (ADAR1) 和 PKR 的共免疫沉淀表明,PKR 抑制是通过直接相互作用实现的。在结合 dsRNA 之前,对抑制性 PKR dsRNA 结合域 (dsRBD)-激酶域相互作用以及对结合 dsRNA 上的抑制性 ADAR1 dsRBD3-PKR 激酶域相互作用的 AlphaFold 研究提供了抑制作用的可测试模型。在 A549 细胞中表达的野生型或编辑失活的人 ADAR1 抑制内源性 PKR 的激活。ADAR1 dsRNA 结合是 PKR 抑制所必需的,但不是充分的。突变 ADAR1 dsRBD3-PKR 接触会阻止共免疫沉淀、ADAR1 对 PKR 活性的抑制以及 ADAR1 和 PKR 在细胞中的共定位。
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