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Disseminated Intravascular Coagulation (DIC)

BSH Guidelines for the diagnosis and management of disseminated intravascular coagulation. Last revised: Jan 2012.

Article Last Updated:20/03/2026

Disclaimer:

The referenced guideline was last reviewed over 10 years ago. However, the core principles outlined remain relevant and appropriate for non-specialist level learning.

Definition

DIC is a clinicopathological syndrome that is characterised by systemic activation of the coagulation system, resulting in:

  • Widespread intravascular (microvascular) clot formation → organ failure
  • Consumption of platelets and clotting factors → serious bleeding
  • Often accompanied by secondary activation of fibrinolysis

Aetiology

DIC never occurs in isolation, it always arises as a secondary complication of an underlying disorder that triggers systemic activation of the coagulation system.

Common / important causes:

  • Sepsis – a common cause of DIC
  • Acute pancreatitis
  • Severe burns
  • Malignancy (classically APL)
  • Major trauma / severe burns
  • Obstetric causes (e.g. placental abruption, HELLP syndrome)
  • Toxins (e.g. snake bites, recreational drug use)
  • Immunological causes (e.g. acute haemolytic transfusion reaction, transplant rejection)

Clinical Manifestation

DIC paradoxically presents with BOTH bleeding and thrombosis, due to consumption of platelet and clotting factors (→ bleeding) and widespread microvascular thrombosis (→ thrombosis).

Bleeding manifestations
  • Easy bruising
  • Mucosal bleeding (e.g. epistaxis, bleeding gum)
  • Oozing from venepuncture / cannulation / wound sites
  • Severe haemorrhage (e.g. GI bleeding, intracranial haemorrhage)
Thrombotic manifestations
  • Venous / arterial thromboembolism
  • Acral ischaemia / skin necrosis (cold / pale / dusky skin, may progress to gangrene / necrosis)
  • Purpura fulminans (severe, rapidly progressive, painful skin haemorrhage and necrosis)
  • Microvascular thrombosis can compromise blood flow to multiple organs → organ dysfunction and/or failure (e.g. renal, respiratory, neurological dysfunction)

DIC = bleeding + thrombosis in a critically unwell patient

Investigation and Diagnosis

Typical findings in DIC:

Investigation Finding in DIC Rationale
Platelet count ↓ LOW Consumption of platelets due to widespread clot formation
Prothrombin time (PT) ↑ PROLONGED Consumption of clotting factors due to widespread activation of coagulation
Activated partial thromboplastin time (APTT) ↑ PROLONGED
Fibrinogen ↓ LOW Consumption in formation of fibrin clots
D-dimer ↑ HIGH Increased fibrinolysis → breakdown of fibrin clots
Blood film Schistocytes (not sensitive or specific to DIC) Microangiopathic haemolysis due to fibrin strands shearing RBCs

Diagnosis of DIC is based on the clinical context (i.e. underlying disorder associated with DIC) and supportive laboratory findings

  • No single test can definitively diagnose or exclude DIC, a combination of tests (see below) is necessary
  • DIC is a dynamic condition → laboratory tests should be repeated serially
  • Formal scoring systems (e.g. ISTH DIC score) and advanced markers (e.g. APTT biphasic waveform) may support diagnosis, but are out of scope at a non-specialist level

Management

Corestone of DIC management: treating the underlying disorder

In many cases, DIC will resolve spontaneously once the primary cause is properly managed

Blood Component Therapy

Supportive blood component therapy should NOT be given based on laboratory results only, they are indicated in patients with:

  • Active bleeding
  • Requiring invasive procedures
  • At high risk of bleeding complications

3 main types of blood components are used in DIC (if indicated):

Blood component Indication
Platelets Bleeding / high-risk patients with low platelet count
Fresh frozen plasma (FFP) Bleeding / procedures with prolonged PT / APTT
Cryoprecipitate Bleeding with low fibrinogen

PCC is not routinely used in DIC and is inferior to FFP. It should only be considered if FFP is not feasible (e.g. fluid overload), as it only partially corrects the coagulopathy and does not replace all depleted clotting factors (e.g. factor V).

In contrast, PCC is preferred over FFP for rapid reversal of warfarin in severe haemorrhage.

Anticoagulation Therapy

Therapeutic heparin is indicated when thrombosis predominates (e.g. severe purupa fulminas, arterial / venous thromboembolism)

  • UFH is often preferred in patients with a co-existing high risk of bleeding
  • Prophylactic heparin is recommended for critically ill, non-bleeding patients to prevent venous thromboembolism

Antifibrinolytic agents (e.g. tranexamic acid) should generally be avoided in DIC, as they may worsen fibrin deposition and microvascular thrombosis

Exception: it may be considered in rare cases with primary hyperfibrinolytic state (e.g. APL) with severe bleeding, however this is beyond the scope of a non-specialist level.

References

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