RIPK1 is essential for Herpes Simplex Virus-triggered ZBP1-dependent necroptosis in human cells

Oluwamuyiwa T. Amusan, Shuqi Wang, Chaoran Yin, Heather S. Koehler, Yixun Li, Tencho Tenev, Rebecca Wilson, Benjamin Bellenie, Ting Zhang, Jian Wang, chang liu, kim seong, Seyedeh L. Poorbaghi, Joseph Yates, Yuchen Shen, Jason W. Upton, Pascal Meier, Siddharth Balachandra, Hongyan Guo
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Abstract

Necroptosis initiated by the host sensor Z-NA Binding Protein-1 (ZBP1) is essential for host defense against a growing number of viruses, including Herpes Simplex Virus-1 (HSV-1). Studies with HSV-1 and other necroptogenic stimuli in murine settings have suggested that ZBP1 triggers necroptosis by directly complexing with the kinase RIPK3. Whether this is also the case in human cells, or whether additional co-factors are needed for ZBP1-mediated necroptosis, is unclear. Here, we show that ZBP1-induced necroptosis in human cells requires RIPK1. We have found that RIPK1 is essential for forming a stable and functional ZBP1-RIPK3 complex in human cells, but is dispensable for the formation of the equivalent murine complex. The RIP Homology Interaction Motif (RHIM) in RIPK3 is responsible for this difference between the two species, because replacing the RHIM in human RIPK3 with the RHIM from murine RIPK3 is sufficient to overcome the requirement for RIPK1 in human cells. These observations describe a critical mechanistic difference between mice and humans in how ZBP1 engages in necroptosis, with important implications for treating human diseases.
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RIPK1 对人类细胞中由单纯疱疹病毒触发的 ZBP1 依赖性坏死至关重要
由宿主传感器 Z-NA 结合蛋白-1(ZBP1)引发的坏死对于宿主抵御越来越多的病毒(包括单纯疱疹病毒-1(HSV-1))至关重要。在小鼠体内使用 HSV-1 和其他致坏死刺激物进行的研究表明,ZBP1 通过直接与激酶 RIPK3 复合物触发坏死。在人体细胞中是否也是这种情况,或者 ZBP1 介导的坏死是否需要额外的辅助因子,目前还不清楚。在这里,我们发现 ZBP1 诱导的人体细胞坏死需要 RIPK1。我们发现,RIPK1 对于在人体细胞中形成稳定的、功能性的 ZBP1-RIPK3 复合物是必不可少的,但对于形成等效的鼠类复合物则是不可或缺的。RIPK3中的RIP同源相互作用元件(RIP Homology Interaction Motif,RHIM)是造成这两种生物之间差异的原因,因为用鼠RIPK3中的RHIM取代人RIPK3中的RHIM足以克服人体细胞对RIPK1的需要。这些观察结果描述了小鼠和人类在 ZBP1 如何参与坏死过程方面的关键机制差异,对治疗人类疾病具有重要意义。
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