Hepatocellular senescence induces multi-organ senescence and dysfunction via TGFβ

IF 17.3 1区 生物学 Q1 CELL BIOLOGY
Christos Kiourtis, Maria Terradas-Terradas, Lucy M. Gee, Stephanie May, Anastasia Georgakopoulou, Amy L. Collins, Eoin D. O’Sullivan, David P. Baird, Mohsin Hassan, Robin Shaw, Ee Hong Tan, Miryam Müller, Cornelius Engelmann, Fausto Andreola, Ya-Ching Hsieh, Lee H. Reed, Lee A. Borthwick, Colin Nixon, William Clark, Peter S. Hanson, David Sumpton, Gillian Mackay, Toshiyasu Suzuki, Arafath K. Najumudeen, Gareth J. Inman, Andrew Campbell, Simon T. Barry, Alberto Quaglia, Christopher M. Morris, Fiona E. N. LeBeau, Owen J. Sansom, Kristina Kirschner, Rajiv Jalan, Fiona Oakley, Thomas G. Bird
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Abstract

Cellular senescence is not only associated with ageing but also impacts physiological and pathological processes, such as embryonic development and wound healing. Factors secreted by senescent cells affect their microenvironment and can induce spreading of senescence locally. Acute severe liver disease is associated with hepatocyte senescence and frequently progresses to multi-organ failure. Why the latter occurs is poorly understood. Here we demonstrate senescence development in extrahepatic organs and associated organ dysfunction in response to liver senescence using liver injury models and genetic models of hepatocyte-specific senescence. In patients with severe acute liver failure, we show that the extent of hepatocellular senescence predicts disease outcome, the need for liver transplantation and the occurrence of extrahepatic organ failure. We identify the TGFβ pathway as a critical mediator of systemic spread of senescence and demonstrate that TGFβ inhibition in vivo blocks senescence transmission to other organs, preventing liver senescence induced renal dysfunction. Our results highlight the systemic consequences of organ-specific senescence, which, independent of ageing, contributes to multi-organ dysfunction.

Abstract Image

肝细胞衰老通过 TGFβ诱导多器官衰老和功能障碍
细胞衰老不仅与衰老有关,还会影响胚胎发育和伤口愈合等生理和病理过程。衰老细胞分泌的因子会影响其微环境,并可诱导衰老在局部扩散。急性重症肝病与肝细胞衰老有关,并经常发展为多器官衰竭。人们对后者发生的原因知之甚少。在这里,我们利用肝损伤模型和肝细胞特异性衰老遗传模型证明了衰老在肝外器官的发展以及与肝衰老相关的器官功能障碍。在严重急性肝衰竭患者中,我们发现肝细胞衰老的程度可预测疾病的结局、肝移植的需要以及肝外器官衰竭的发生。我们发现 TGFβ 通路是衰老向全身扩散的关键介质,并证明在体内抑制 TGFβ 可阻断衰老向其他器官的传播,防止肝衰老诱发肾功能障碍。我们的研究结果突显了器官特异性衰老的系统性后果,衰老与老化无关,会导致多器官功能障碍。
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来源期刊
Nature Cell Biology
Nature Cell Biology 生物-细胞生物学
CiteScore
28.40
自引率
0.90%
发文量
219
审稿时长
3 months
期刊介绍: Nature Cell Biology, a prestigious journal, upholds a commitment to publishing papers of the highest quality across all areas of cell biology, with a particular focus on elucidating mechanisms underlying fundamental cell biological processes. The journal's broad scope encompasses various areas of interest, including but not limited to: -Autophagy -Cancer biology -Cell adhesion and migration -Cell cycle and growth -Cell death -Chromatin and epigenetics -Cytoskeletal dynamics -Developmental biology -DNA replication and repair -Mechanisms of human disease -Mechanobiology -Membrane traffic and dynamics -Metabolism -Nuclear organization and dynamics -Organelle biology -Proteolysis and quality control -RNA biology -Signal transduction -Stem cell biology
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