Burns Flashcards
Describe the local response to burn in terms of 3 zones
- Zone of coagulation –> This is the region that has experienced maximal damage. Proteins have undergone coagulation. Coagulative necrosis. Irreversible/ non-viable. Requires debridement or grafting.
- Zone of stasis –> Characterized by ischemia caused by reduced blood flow/ vasoconstriction. Accounts for the systemic effects of burn injury. Potentially salvageable with prompt fluid therapy to re-perfuse tissue.
- Zone of hyperemia –> Characterized by vasodilation and inreased blood flow. The tissue is fully viable as long as there are no secondary insults or infection.
Explain the primary systemic response in severe burn
The primary systemic response to burn injury is driven by a massive release of inflammatory cytokines (TNF-a, IL-1, IL-6) and vasoactive mediators (histamine, NO, prostaglandins), leading to increased vascular permeability. This causes significant fluid loss into the interstitial space, resulting in intravascular hypovolemia and edema. While vasodilation may occur, the dominant issue in the acute phase is capillary leak and subsequent burn shock.
The initial 48-hour “ebb” phase is characterized by a hypometabolic state. Cardiac output drops due to a combination of myocardial depression (caused by cytokine release) and reduced preload (due to fluid shifts out of the intravascular space). Despite compensatory catecholamine release, perfusion remains inadequate. Aggressive fluid resuscitation is critical to restoring intravascular volume and preventing organ failure.
By approximately 48 hours, the “flow” phase begins, characterized by a hypermetabolic state that can persist for months—or even over a year in severe burns. This phase is driven by increased catecholamine and cortisol release, resulting in tachycardia, hyperglycemia, massive catabolism, muscle wasting (due to proteolysis), insulin resistance, and immunosuppression, increasing the risk of infection and sepsis. Splanchnic vasoconstriction, which can impair gut barrier function and promote bacterial translocation, should be mitigated with early enteral feeding to maintain gut integrity and reduce septic complications.
Outline 4 causes of anemia in a burns patient
- Acute blood loss from the injury itself and/or surgical intervention.
- Inflammatory cytokines suppress erythropoeisis by inhibiting erythoid precursor proliferation and inhibiting EPO synthesis in kidney.
- Depletion of iron, folate, B12 due to hypermetabolic state.
- Increased hepcidin production in liver in response to inflammation; inhibits iron absorption from the gut and release of iron from intracellular stores –> further hinders erythropoeisis.
- Increased RBC sequestration in damaged tissue and haemophagocytosis.
- Hemodilutional anemia due to fluid replacement therapy
Outline 4 reasons why burns victims may be predisposed to infection
- Effect on Lymphocytes
–> T and B cell proliferation is inhibited, particularly due to excessive release of TGF-β, which suppresses immune cell function post-burn.
–>A shift from a Th1 to a Th2-dominated response impairs pathogen clearance. IL-4 and IL-10 promote Th2 responses, which suppress cytotoxic T-cell and macrophage activation, weakening cell-mediated immunity and increasing susceptibility to infections. - Effect on Innate Immune Response
–>Initial hyperinflammatory phase (cytokine storm) with TNF-α, IL-1, and IL-6 leads to immune dysregulation, followed by compensatory anti-inflammatory response syndrome (CARS), which causes immune suppression.
–>Neutrophils, macrophages, and dendritic cells exhibit impaired chemotaxis, phagocytosis, and antigen presentation, reducing pathogen clearance.
–> Complement dysfunction weakens opsonization, further impairing innate immune defense. - Hormonal and Metabolic Changes
–> Elevated cortisol and catecholamines contribute to immunosuppression by downregulating pro-inflammatory cytokines and impairing leukocyte function.
–> These stress-induced changes weaken both adaptive and innate immune responses, making infections more likely. - Loss of Skin Barrier
- Burn-induced gut permeability
–>Splanchnic vasoconstriction and elevated systemic inflammatory mediators contribute to gut mucosal atrophy and increased permeability.
–>This allows bacterial translocation from the gut into the bloodstream, leading to sepsis and systemic infections.