1. Temporal–spatial organ response after blast‐induced experimental blunt abdominal trauma
- Author
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Alexander Maitz, Felix Haussner, Hans-Joachim Wilke, Peter Radermacher, Markus Huber-Lang, Thomas F. E. Barth, Andrea Hoffmann, Anita Ignatius, Ulrich Wachter, Rebecca Halbgebauer, Lucas Bettac, Morten Vogt, Christian Karl Braun, Annette Palmer, Sonja Braumüller, and Ludmila Lupu
- Subjects
Male ,Mean arterial pressure ,Pathology ,medicine.medical_specialty ,Hemodynamics ,Abdominal Injuries ,Biochemistry ,Mice ,Blunt ,Blast Injuries ,Genetics ,Animals ,Medicine ,Pancreas ,Molecular Biology ,Kidney ,Multiple Trauma ,business.industry ,Organ dysfunction ,Acute Kidney Injury ,medicine.disease ,Mice, Inbred C57BL ,medicine.anatomical_structure ,Liver ,Abdominal trauma ,Epigastrium ,medicine.symptom ,business ,Biotechnology - Abstract
Abdominal trauma (AT) is of major global importance, particularly with the increased potential for civil, terroristic, and military trauma. The injury pattern and systemic consequences of blunt abdominal injuries are highly variable and frequently underestimated or even missed, and the pathomechanisms remain still poorly understood. Therefore, we investigated the temporal-spatial organ and immune response after a standardized blast-induced blunt AT. Anesthetized mice were exposed to a single blast wave centered on the epigastrium. At 2, 6, or 24 h after trauma, abdominal organ damage was assessed macroscopically, microscopically, and biochemically. A higher degree of trauma severity, determined by a reduction of the distance between the epigastrium and blast inductor, was reflected by a reduced survival rate. The hemodynamic monitoring during the first 120 min after AT revealed a decline in the mean arterial pressure within the first 80 min, whereas the heart rate remained quite stable. AT induced a systemic damage and inflammatory response, evidenced by elevated HMGB-1 and IL-6 plasma levels. The macroscopic injury pattern of the abdominal organs (while complex) was consistent, with the following frequency: liver > pancreas > spleen > left kidney > intestine > right kidney > others > lungs and was reflected by microscopic liver and pancreas damages. Plasma levels of organ dysfunction markers increased during the first 6 h after AT and subsequently declined, indicating an early, temporal impairment of the function on a multi-organ level. The established highly reproducible murine blunt AT, with time- and trauma-severity-dependent organ injury patterns, systemic inflammatory response, and impairment of various organ functions, reflects characteristics of human AT. In the future, this model may help to study the complex immuno-pathophysiological consequences and innovative therapeutic approaches after blunt AT.
- Published
- 2021
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