Pseudofracture: An Acute Peripheral Tissue Trauma Model

Darwiche, Sophie S.; Kobbe, Philipp; Pfeifer, Roman; Kohut, Lauryn; Pape, Hans-Christian; Billiar, Timothy R.

doi:10.3791/2074

Cited by 29 publications

(46 citation statements)

References 40 publications

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“…23,24 We demonstrate that LPS acting through TLR4 promotes Mϕ necroptosis, as expected. However, release of HMGB1 from damaged tissue signals via RAGE signaling to upregulate caveolin-1 expression and so induces Mϕ surface TLR4 internalization, which results in amelioration of LPS-TLR4-induced Mϕ necroptosis.…”

Section: Figure 1 Continuedsupporting

confidence: 82%

“…The PF model consists of two parts: a musclecrush injury to the hind limbs, followed by injection of a bone solution into these injured muscles. 24 In the current study, we used the PF model to elucidate the influence of tissue damage on LPS-induced Mϕ necroptosis, and revealed that HMGB1 within the BCM acts through RAGE signaling and is a major component mediating tissue damage-suppressed Mϕ necroptosis in response to LPS. Necroptosis is a regulated form of inflammatory cell death.…”

Section: Discussionmentioning

confidence: 93%

“…To determine Mϕ death response to posttrauma infection, wild-type (WT) mice were first subjected to PF, a validated model of long-bone fracture. 23,24 To further confirm that necroptosis was occurring in the Mϕ/ monocytes, cells were double stained with the RIPK1 and RIPK3. 26 Colocalization of RIPK1 and RIPK3 was visualized by confocal microscopy and represents the RIPK1 and RIPK3 association to form the necrosome.…”

Section: Resultsmentioning

confidence: 99%

“…PF is a reproducible murine model of sterile musculoskeletal trauma that allows for evaluation of post-traumatic immune responses. 24 The challenges in experimental murine trauma modeling include technical difficulties in fracture fixation in mice and reproducibility. The PF model overcomes these difficulties by immunologically mimicking an extremity fracture environment, whereas allowing freedom of movement in the animals and long-term survival without continual, prolonged use of anesthesia.…”

Section: Discussionmentioning

confidence: 99%

“…The recipient mouse was anesthetized with ketamine (50 mg/kg BW) and xylazine (5 mg/kg BW) and the thighs were squeezed with a hemostat for 30 s to induce a soft-tissue lesion, followed by injection of 0.15 ml of the BCM in the tissue lesion area. 24 Sham animals underwent the same anesthesia procedure and injection of 0.15 ml of normal saline at the thighs. In some animals, at 12 h after the injection of BCM or saline, were intraperitoneally administered LPS (2 mg/kg BW in 0.2 ml of PBS).…”

Section: Methodsmentioning

confidence: 99%

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Tissue damage negatively regulates LPS-induced macrophage necroptosis

Scott

Fan

et al. 2016

Cell Death Differ

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Infection is a common clinical complication following tissue damage resulting from surgery and severe trauma. Studies have suggested that cell pre-activation by antecedent trauma/tissue damage profoundly impacts the response of innate immune cells to a secondary infectious stimulus. Cell necroptosis, a form of regulated inflammatory cell death, is one of the mechanisms that control cell release of inflammatory mediators from important innate immune executive cells such as macrophages (Mϕ), which critically regulate the progress of inflammation. In this study, we investigated the mechanism and role of trauma/tissue damage in the regulation of LPS-induced Mϕ necroptosis using a mouse model simulating long-bone fracture. We demonstrate that LPS acting through Toll-like receptor (TLR) 4 promotes Mϕ necroptosis. However, necroptosis is ameliorated by high-mobility group box 1 (HMGB1) release from damaged tissue. We show that HMGB1 acting through cell surface receptor for advanced glycation end products (RAGE) upregulates caveolin-1 expression, which in turn induces caveolae-mediated TLR4 internalization and desensitization to decrease Mϕ necroptosis. We further show that RAGE-MyD88 activation of Cdc42 and subsequent activation of transcription factor Sp1 serves as a mechanism underlying caveolin-1 transcriptional upregulation. These results reveal a previous unidentified protective role of damage-associated molecular pattern (DAMP) molecules in restricting inflammation in response to exogenous pathogen-associated molecular pattern molecules.

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Section: Figure 1 Continuedsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 93%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 3 more Smart Citations

Tissue damage negatively regulates LPS-induced macrophage necroptosis

Scott

Fan

et al. 2016

Cell Death Differ

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A rat model of multicompartmental traumatic injury and hemorrhagic shock induces bone marrow dysfunction and profound anemia

Kelly,

Munley,

Pons

et al. 2024

Anim Models and Exp Med

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BackgroundSevere trauma is associated with systemic inflammation and organ dysfunction. Preclinical rodent trauma models are the mainstay of postinjury research but have been criticized for not fully replicating severe human trauma. The aim of this study was to create a rat model of multicompartmental injury which recreates profound traumatic injury.MethodsMale Sprague–Dawley rats were subjected to unilateral lung contusion and hemorrhagic shock (LCHS), multicompartmental polytrauma (PT) (unilateral lung contusion, hemorrhagic shock, cecectomy, bifemoral pseudofracture), or naïve controls. Weight, plasma toll‐like receptor 4 (TLR4), hemoglobin, spleen to body weight ratio, bone marrow (BM) erythroid progenitor (CFU‐GEMM, BFU‐E, and CFU‐E) growth, plasma granulocyte colony‐stimulating factor (G‐CSF) and right lung histologic injury were assessed on day 7, with significance defined as p values <0.05 (*).ResultsPolytrauma resulted in markedly more profound inhibition of weight gain compared to LCHS (p = 0.0002) along with elevated plasma TLR4 (p < 0.0001), lower hemoglobin (p < 0.0001), and enlarged spleen to body weight ratios (p = 0.004). Both LCHS and PT demonstrated suppression of CFU‐E and BFU‐E growth compared to naïve (p < 0.03, p < 0.01). Plasma G‐CSF was elevated in PT compared to both naïve and LCHS (p < 0.0001, p = 0.02). LCHS and PT demonstrated significant histologic right lung injury with poor alveolar wall integrity and interstitial edema.ConclusionsMulticompartmental injury as described here establishes a reproducible model of multicompartmental injury with worsened anemia, splenic tissue enlargement, weight loss, and increased inflammatory activity compared to a less severe model. This may serve as a more effective model to recreate profound traumatic injury to replicate the human inflammatory response postinjury.

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Polymorphonuclear myeloid-derived suppressor cells link inflammation and damage response after trauma

Liu

Xing

et al. 2021

Journal of Leukocyte Biology

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Elimination of the posttraumatic inflammatory response and recovery of homeostasis are crucial for the positive prognosis of trauma patients. Myeloid‐derived suppressor cells (MDSCs) are known to play a regulatory role in the posttraumatic immune response in mice, but their induction source and involved potential mechanism are poorly understood. Here, we report that polymorphonuclear MDSCs (PMN‐MDSCs) are activated after trauma and are closely associated with the progression of the posttraumatic inflammatory response. In humans, lectin‐type oxidized LDL receptor 1 (LOX1) was used to specifically characterize LOX1+ PMN‐MDSCs. Trauma patients showed high intracellular reactive oxygen species (ROS) production, as well as activation of LOX1+ PMN‐MDSCs. These MDSCs contribute to the anti‐inflammatory immune response by regulating the Treg/Th17 and Th2/Th1 balances after trauma, increasing the levels of anti‐inflammatory factors, and decreasing the levels of proinflammatory factors. The number of LOX1+ PMN‐MDSCs was positively correlated with the positive clinical prognosis of trauma patients with infection. Activation of LOX1+ PMN‐MDSCs is mediated by NF‐κB signal, and TGF‐β1 may be as an important inducer for LOX1+ PMN‐MDSCs in the posttraumatic cytokine environment. In a pseudofracture trauma mouse model, we also observed the activation of PMN‐MDSCs, accompanying high levels of intracellular ROS production, NF‐κB phosphorylation, and changes in the inflammatory environment, in particularly by regulating the Treg/Th17 and Th2/Th1 balance. And more significantly, posttraumatic inflammation was alleviated in mice after transferring trauma‐derived PMN‐MDSCs, but aggravated after injecting with Gr1 agonistic antibody. These findings provide evidence for the specific role of PMN‐MDSCs in the regulation of posttraumatic inflammation.

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Pseudofracture: An Acute Peripheral Tissue Trauma Model

Cited by 29 publications

References 40 publications

Tissue damage negatively regulates LPS-induced macrophage necroptosis

Tissue damage negatively regulates LPS-induced macrophage necroptosis

A rat model of multicompartmental traumatic injury and hemorrhagic shock induces bone marrow dysfunction and profound anemia

Polymorphonuclear myeloid-derived suppressor cells link inflammation and damage response after trauma

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