TY - JOUR
T1 - Primary cilia suppress Ripk3-mediated necroptosis
AU - Kieckhöfer, Emilia
AU - Slaats, Gisela G
AU - Ebert, Lena K
AU - Albert, Marie-Christine
AU - Dafinger, Claudia
AU - Kashkar, Hamid
AU - Benzing, Thomas
AU - Schermer, Bernhard
N1 - Funding Information:
We would like to thank Stefanie Keller, Serena Greco-Torres, and Angelika Köser for expert technical assistance. We acknowledge the help of the CECAD imaging facility and the CECAD proteomics facility. We thank the FACS & IMAGING Core Facility at Max Plank Institute for Biology of Ageing, Cologne, for assisting with sorting cells for the generation mIMCD subclones. In addition, we would like to express our gratitude to all members of our laboratory and many members of the SFB1403 for helpful discussions and support. This study was supported by the German Research Foundation (DFG; SFB1403, project number 414786233, A09 to BS and TB). BS was also supported by the German Federal Ministry of Research and Education (BMBF grant 01GM1515; NEOCYST consortium). The CECAD proteomics facility was supported by the large instrument grant INST 1856/71–1 FUGG by the German Research Foundation (DFG Großgeräteantrag). GGS was supported by a Fritz Thyssen Foundation grant (project 10.20.1.012MN). We acknowledge support for the article processing charge from the DFG (German Research Foundation, 491454339).
Publisher Copyright:
© 2022, The Author(s).
PY - 2022/12/2
Y1 - 2022/12/2
N2 - Cilia are sensory organelles that project from the surface of almost all cells. Nephronophthisis (NPH) and NPH-related ciliopathies are degenerative genetic diseases caused by mutation of cilia-associated genes. These kidney disorders are characterized by progressive loss of functional tubular epithelial cells which is associated with inflammation, progressive fibrosis, and cyst formation, ultimately leading to end-stage renal disease. However, disease mechanisms remain poorly understood. Here, we show that targeted deletion of cilia in renal epithelial cells enhanced susceptibility to necroptotic cell death under inflammatory conditions. Treatment of non-ciliated cells with tumor necrosis factor (TNF) α and the SMAC mimetic birinapant resulted in Ripk1-dependent cell death, while viability of ciliated cells was almost not affected. Cell death could be enhanced and shifted toward necroptosis by the caspase inhibitor emricasan, which could be blocked by inhibitors of Ripk1 and Ripk3. Moreover, combined treatment of ciliated and non-ciliated cells with TNFα and cycloheximide induced a cell death response that could be partially rescued with emricasan in ciliated cells. In contrast, non-ciliated cells responded with pronounced cell death that was blocked by necroptosis inhibitors. Consistently, combined treatment with interferon-γ and emricasan induced cell death only in non-ciliated cells. Mechanistically, enhanced necroptosis induced by loss of cilia could be explained by induction of Ripk3 and increased abundance of autophagy components, including p62 and LC3 associated with the Ripk1/Ripk3 necrosome. Genetic ablation of cilia in renal tubular epithelial cells in mice resulted in TUNEL positivity and increased expression of Ripk3 in kidney tissue. Moreover, loss of Nphp1, the most frequent cause of NPH, further increased susceptibility to necroptosis in non-ciliated epithelial cells, suggesting that necroptosis might contribute to the pathogenesis of the disease. Together, these data provide a link between cilia-related signaling and cell death responses and shed new light on the disease pathogenesis of NPH-related ciliopathies.
AB - Cilia are sensory organelles that project from the surface of almost all cells. Nephronophthisis (NPH) and NPH-related ciliopathies are degenerative genetic diseases caused by mutation of cilia-associated genes. These kidney disorders are characterized by progressive loss of functional tubular epithelial cells which is associated with inflammation, progressive fibrosis, and cyst formation, ultimately leading to end-stage renal disease. However, disease mechanisms remain poorly understood. Here, we show that targeted deletion of cilia in renal epithelial cells enhanced susceptibility to necroptotic cell death under inflammatory conditions. Treatment of non-ciliated cells with tumor necrosis factor (TNF) α and the SMAC mimetic birinapant resulted in Ripk1-dependent cell death, while viability of ciliated cells was almost not affected. Cell death could be enhanced and shifted toward necroptosis by the caspase inhibitor emricasan, which could be blocked by inhibitors of Ripk1 and Ripk3. Moreover, combined treatment of ciliated and non-ciliated cells with TNFα and cycloheximide induced a cell death response that could be partially rescued with emricasan in ciliated cells. In contrast, non-ciliated cells responded with pronounced cell death that was blocked by necroptosis inhibitors. Consistently, combined treatment with interferon-γ and emricasan induced cell death only in non-ciliated cells. Mechanistically, enhanced necroptosis induced by loss of cilia could be explained by induction of Ripk3 and increased abundance of autophagy components, including p62 and LC3 associated with the Ripk1/Ripk3 necrosome. Genetic ablation of cilia in renal tubular epithelial cells in mice resulted in TUNEL positivity and increased expression of Ripk3 in kidney tissue. Moreover, loss of Nphp1, the most frequent cause of NPH, further increased susceptibility to necroptosis in non-ciliated epithelial cells, suggesting that necroptosis might contribute to the pathogenesis of the disease. Together, these data provide a link between cilia-related signaling and cell death responses and shed new light on the disease pathogenesis of NPH-related ciliopathies.
UR - http://www.scopus.com/inward/record.url?scp=85143377473&partnerID=8YFLogxK
U2 - 10.1038/s41420-022-01272-2
DO - 10.1038/s41420-022-01272-2
M3 - Article
C2 - 36460631
SN - 2058-7716
VL - 8
JO - Cell death discovery
JF - Cell death discovery
IS - 1
M1 - 477
ER -