Trauma-associated extracellular histones mediate inflammation via a MYD88-IRAK1-ERK signaling axis and induce lytic cell death in human adipocytes

脂肪组织 炎症 程序性细胞死亡 组蛋白 细胞生物学 生物 癌症研究 脂肪细胞 医学 免疫学 内分泌学 细胞凋亡 遗传学 基因
作者
Julian Roos,Julia Zinngrebe,Markus Huber‐Lang,Ludmila Lupu,Miriam A. Schmidt,Hannah A. Strobel,Mike‐Andrew Westhoff,Ulrich Stifel,Florian Gebhard,Martin Wabitsch,Tom Eirik Mollnes,Klaus‐Michael Debatin,Rebecca Halbgebauer,Pamela Fischer‐Posovszky
出处
期刊:Cell Death and Disease [Springer Nature]
卷期号:15 (4) 被引量:1
标识
DOI:10.1038/s41419-024-06676-9
摘要

Abstract Despite advances in the treatment and care of severe physical injuries, trauma remains one of the main reasons for disability-adjusted life years worldwide. Trauma patients often suffer from disturbances in energy utilization and metabolic dysfunction, including hyperglycemia and increased insulin resistance. White adipose tissue plays an essential role in the regulation of energy homeostasis and is frequently implicated in traumatic injury due to its ubiquitous body distribution but remains poorly studied. Initial triggers of the trauma response are mainly damage-associated molecular patterns (DAMPs) such as histones. We hypothesized that DAMP-induced adipose tissue inflammation contributes to metabolic dysfunction in trauma patients. Therefore, we investigated whether histone release during traumatic injury affects adipose tissue. Making use of a murine polytrauma model with hemorrhagic shock, we found increased serum levels of histones accompanied by an inflammatory response in white adipose tissue. In vitro, extracellular histones induced an inflammatory response in human adipocytes. On the molecular level, this inflammatory response was mediated via a MYD88-IRAK1-ERK signaling axis as demonstrated by pharmacological and genetic inhibition. Histones also induced lytic cell death executed independently of caspases and RIPK1 activity. Importantly, we detected increased histone levels in the bloodstream of patients after polytrauma. Such patients might benefit from a therapy consisting of activated protein C and the FDA-approved ERK inhibitor trametinib, as this combination effectively prevented histone-mediated effects on both, inflammatory gene activation and cell death in adipocytes. Preventing adipose tissue inflammation and adipocyte death in patients with polytrauma could help minimize posttraumatic metabolic dysfunction.

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