Abstract

BackgroundSepsis is a highly lethal disorder. Organ dysfunction in sepsis is not defined as a clinicopathological entity but rather by changes in clinical, physiological, or biochemical parameters. Pathogenesis and specific treatment of organ dysfunction in sepsis are unknown. The study of the histopathological correlate of organ dysfunction in sepsis will help understand its pathogenesis.MethodsWe searched in PubMed, EMBASE, and Scielo for original articles on kidney, brain, and liver dysfunction in human sepsis. A defined search strategy was designed, and pertinent articles that addressed the histopathological changes in sepsis were retrieved for review. Only studies considered relevant in the field were discussed.ResultsStudies on acute kidney injury (AKI) in sepsis reveal that acute tubular necrosis is less prevalent than other changes, indicating that kidney hypoperfusion is not the predominant pathogenetic mechanism of sepsis-induced AKI. Other more predominant histopathological changes are apoptosis, interstitial inflammation, and, to a lesser extent, thrombosis. Brain pathological findings include white matter hemorrhage and hypercoagulability, microabscess formation, central pontine myelinolysis, multifocal necrotizing leukoencephalopathy, metabolic changes, ischemic changes, and apoptosis. Liver pathology in sepsis includes steatosis, cholangiolitis and intrahepatic cholestasis, periportal inflammation, and apoptosis. There is no information on physiological or biochemical biomarkers of the histopathological findings.ConclusionsHistopathological studies may provide important information for a better understanding of the pathogenesis of organ dysfunction in sepsis and for the design of potentially effective therapies. There is a lack of clinically available biomarkers for the identification of organ dysfunction as defined by the histological analysis.

Highlights

  • Garofalo et al Intensive Care Medicine Experimental 2019, 7(Suppl 1):45. Why is it interesting to study the histopathology in sepsis-induced organ dysfunction? Sepsis is a highly lethal disorder that is responsible for the death of over 200,000 people annually in the USA alone [1]

  • Unlike classical disease entities, such as cancer and infectious or immunological conditions, organ dysfunction in the context of sepsis and acute respiratory failure is not defined as a clinicopathological entity but rather described by nonspecific clinical changes, physiological alterations or serum biomarkers of organ function

  • The aim of this study is to summarize the histopathological changes in the kidney, brain, and liver associated with sepsis-induced organ dysfunction in humans

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Summary

Introduction

Organ dysfunction in sepsis is not defined as a clinicopathological entity but rather by changes in clinical, physiological, or biochemical parameters. The study of the histopathological correlate of organ dysfunction in sepsis will help understand its pathogenesis. The aim of this study is to summarize the histopathological changes in the kidney, brain, and liver associated with sepsis-induced organ dysfunction in humans. The description of these pathological changes is of particular relevance in the face of conditions whose pathogenesis is not well defined and for which specific treatments are not available. Knowledge of pathological findings associated with sepsis could help with a better understanding of pathogenic mechanisms, a more precise knowledge on the reversibility of organ dysfunction, and a more effective design of potentially effective treatments

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