Multiple organ dysfunction syndrome: Difference between revisions
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{{SK}} Multiorgan failure; multiorgan system failure; multisystem failure; MODS; multiple organ failure; MOF | {{SK}} Multiorgan failure; multiorgan system failure; multisystem failure; MODS; multiple organ failure; MOF; systemic inflammatory response syndrome; SIRS | ||
==Overview== | ==Overview== | ||
Multiple organ dysfunction syndrome is defined as altered [[organ (anatomy)|organ]] function in an acutely ill patient requiring [[medicine|medical]] intervention to perform [[homeostasis]]. The use of "multiple organ failure" should be avoided since that term was based upon physiologic parameters to determine whether or not a particular organ was failing.<ref name="Irwin-Rippe">[http://www.lww.com/product/?0-7817-3548-3 Intensive Care Medicine] by Irwin and Rippe</ref> | Multiple organ dysfunction syndrome is defined as altered [[organ (anatomy)|organ]] function in an acutely ill patient requiring [[medicine|medical]] intervention to perform [[homeostasis]]. The use of "multiple organ failure" should be avoided since that term was based upon physiologic parameters to determine whether or not a particular organ was failing.<ref name="Irwin-Rippe">[http://www.lww.com/product/?0-7817-3548-3 Intensive Care Medicine] by Irwin and Rippe</ref> Multiple organ dysfunction syndrome is the presence of altered organ function in acutely ill patients such that [[homeostasis]] cannot be maintained without intervention. It usually involves two or more organ systems.<ref name="Irwin-Rippe"/> | ||
== | ==Historical Perspective== | ||
Originally patients were classified as having sepsis or the sepsis syndrome. This resulted in two concepts: the systemic inflammatory response syndrome (SIRS) and multiple organ dysfunction syndrome (MODS).<ref name="Irwin-Rippe"/> | Originally patients were classified as having sepsis or the sepsis syndrome. This resulted in two concepts: the systemic inflammatory response syndrome (SIRS) and multiple organ dysfunction syndrome (MODS).<ref name="Irwin-Rippe"/> | ||
==Pathophysiology== | ==Pathophysiology== | ||
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===Integrated hypothesis=== | ===Integrated hypothesis=== | ||
Since in most cases no primary cause is found, the condition could be part of a compromised homeostasis involving the previous mechanisms.<ref name="Irwin-Rippe"/> | Since in most cases no primary cause is found, the condition could be part of a compromised homeostasis involving the previous mechanisms.<ref name="Irwin-Rippe"/> | ||
==Causes== | |||
he condition usually results from infection, injury (accident, surgery), hypoperfusion and hypermetabolism. The primary cause triggers an uncontrolled [[inflammation|inflammatory response]]. In operative and non-operative patients [[sepsis]] is the most common cause. Sepsis may result in [[septic shock]]. In the absence of infection a sepsis-like disorder is termed [[systemic inflammatory response syndrome]] (SIRS). Both SIRS and sepsis could ultimately progress to multiple organ dysfunction syndrome. However, in one-third of the patients no primary focus can be found.<ref name="Irwin-Rippe"/> | |||
==Natural History, Complications, Prognosis== | |||
Mortality varies from 30% to 100% where the chance of survival is diminished as the number of organs involved increases. Since the 1980s the mortality rate has not changed. | |||
==Diagnosis== | ==Diagnosis== | ||
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==Treatment== | ==Treatment== | ||
At present there is no agent that can reverse the established organ failure. Therapy therefore is limited to supportive care, i.e. safeguarding hemodynamics, and respiration. Maintaining adequate tissue oxygenation is a principal target. Starting enteral nutrition within 36 hours of admission to an [[Intensive care unit]] has reduced infectious complications. <ref name="Irwin-Rippe"/> | At present there is no agent that can reverse the established organ failure. Therapy therefore is limited to supportive care, i.e. safeguarding hemodynamics, and respiration. Maintaining adequate tissue oxygenation is a principal target. Starting enteral nutrition within 36 hours of admission to an [[Intensive care unit]] has reduced infectious complications. <ref name="Irwin-Rippe"/> | ||
==See also== | ==See also== |
Revision as of 22:08, 9 August 2012
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]
Synonyms and keywords: Multiorgan failure; multiorgan system failure; multisystem failure; MODS; multiple organ failure; MOF; systemic inflammatory response syndrome; SIRS
Overview
Multiple organ dysfunction syndrome is defined as altered organ function in an acutely ill patient requiring medical intervention to perform homeostasis. The use of "multiple organ failure" should be avoided since that term was based upon physiologic parameters to determine whether or not a particular organ was failing.[1] Multiple organ dysfunction syndrome is the presence of altered organ function in acutely ill patients such that homeostasis cannot be maintained without intervention. It usually involves two or more organ systems.[1]
Historical Perspective
Originally patients were classified as having sepsis or the sepsis syndrome. This resulted in two concepts: the systemic inflammatory response syndrome (SIRS) and multiple organ dysfunction syndrome (MODS).[1]
Pathophysiology
A definite explanation has not been found. Local and systemic responses are initiated by tissue damage. Respiratory failure is common in the first 72 hours after the original insult. Following this one might see hepatic failure (5-7 days), gastrointestinal bleeding (10-15 days), and renal failure (11-17 days)[1]
Gut hypothesis
The most popular theory to explain MODS in critically ill patients is the gut hypothesis. Due to splanchnic hypoperfusion and the subsequent mucosal ischaemia there are structural changes and alterations in cellular function. This results in increased gut permeability, changed immune function of the gut and increased translocation of bacteria. Hepatic dysfunction leads to toxins escaping into the systemic circulation and activating an immune response. This results in tissue injury and organ dysfunction.[1]
Endotoxin macrophage theory
Gram-negative infections in MODS patients are relatively common, hence endotoxins have been advanced as principal mediator in this disorder. It is thought that following the initial event cytokines are produced and released. The pro-inflammatory mediators are: tumor necrosis factor-alpha (TNF-α), interleukin-1, interleukin-6, thromboxane A2, prostacyclin, platelet activating factor, and nitric oxide.[1]
Tissue hypoxia-microvascular hypothesis
As a result of macro- and microvascular changes insufficient supply of oxygen occurs. Hypoxemia causes organ dysfuntion and cell death.[1]
Integrated hypothesis
Since in most cases no primary cause is found, the condition could be part of a compromised homeostasis involving the previous mechanisms.[1]
Causes
he condition usually results from infection, injury (accident, surgery), hypoperfusion and hypermetabolism. The primary cause triggers an uncontrolled inflammatory response. In operative and non-operative patients sepsis is the most common cause. Sepsis may result in septic shock. In the absence of infection a sepsis-like disorder is termed systemic inflammatory response syndrome (SIRS). Both SIRS and sepsis could ultimately progress to multiple organ dysfunction syndrome. However, in one-third of the patients no primary focus can be found.[1]
Natural History, Complications, Prognosis
Mortality varies from 30% to 100% where the chance of survival is diminished as the number of organs involved increases. Since the 1980s the mortality rate has not changed.
Diagnosis
The European Society of Intensive Care organized a consensus meeting in 1994 to create the "Sepsis-Related Organ Failure Assessment (SOFA)" score to describe and quantitate the degree of organ dysfunction in six organ systems. Using similar physiologic variables the Multiple Organ Dysfunction Score was developed.[1]
Four clinical phases have been suggested:
- Stage 1 the patient has increased volume requirements and mild respiratory alkalosis which is accompanied by oliguria, hyperglycemia and increased insulin requirements.
- Stage 2 the patient is tachypneic, hypocapnic and hypoxemic. Moderate liver dysfunction and possible hematologic abnormalities.
- Stage 3 the patient develops shock with azotemia and acid-base disturbances. Significant coagulation abnormalities.
- Stage 4 the patient is vasopressor dependent and oliguric or anuric. Ischemic colitis and lactic acidosis follow.
Treatment
At present there is no agent that can reverse the established organ failure. Therapy therefore is limited to supportive care, i.e. safeguarding hemodynamics, and respiration. Maintaining adequate tissue oxygenation is a principal target. Starting enteral nutrition within 36 hours of admission to an Intensive care unit has reduced infectious complications. [1]
See also
- Acute renal failure
- Acute respiratory distress syndrome
- Heart failure
- Intensive care
- Liver failure
- Respiratory insufficiency
- Shock
- systemic inflammatory response syndrome