Disseminated intravascular coagulation
Disseminated intravascular coagulation (DIC) is a serious and potentially life-threatening disorder characterized by the abnormal activation of the blood coagulation system, resulting in widespread formation of small blood clots throughout the body's blood vessels.[1] This hypercoagulable state consumes clotting factors and platelets, paradoxically leading to simultaneous bleeding tendencies due to depleted hemostatic resources.[2] DIC is not a primary disease but a secondary syndrome triggered by underlying conditions, often developing acutely in critical illnesses.[3] The pathophysiology of DIC involves systemic activation of the coagulation cascade, primarily through the release of tissue factor from damaged endothelial cells or inflammatory mediators, generating excessive thrombin that promotes fibrin clot formation in microvasculature.[2] This process is compounded by impaired fibrinolysis and anticoagulation pathways, leading to microvascular thrombosis, organ ischemia, and depletion of procoagulant and anticoagulant factors.[4] In severe cases, the ensuing coagulopathy manifests as both thrombotic and hemorrhagic complications, contributing to multi-organ dysfunction.[1] Common causes of DIC include severe infections such as sepsis, malignancy (particularly acute promyelocytic leukemia), major trauma, obstetric complications like amniotic fluid embolism or placental abruption, and other conditions such as severe pancreatitis or liver failure.[5] Risk factors encompass blood transfusion reactions, snake bites, and heatstroke, with sepsis being the most frequent trigger in clinical settings.[2] Epidemiologically, DIC occurs in approximately 1-3% of hospitalized patients but is far more prevalent in intensive care units, affecting up to 50% of septic patients.[3] Clinically, DIC presents with a spectrum of symptoms including unexplained bleeding from multiple sites (e.g., gums, nose, or surgical wounds), easy bruising, petechiae, and ecchymoses, alongside signs of organ hypoperfusion such as hypotension, shortness of breath, confusion, and fever.[5] Diagnosis relies on clinical context combined with laboratory findings like prolonged prothrombin time, elevated fibrin degradation products (D-dimer), low fibrinogen levels, and thrombocytopenia, scored using the updated International Society on Thrombosis and Haemostasis (ISTH) overt DIC criteria (2025), which incorporate phase-based classification (pre-DIC, early-phase DIC, overt DIC).[4][6] Recent 2025 updates emphasize disease-specific scoring for improved early detection in conditions like sepsis.[7] Management of DIC focuses primarily on treating the underlying disorder to halt the coagulopathic process, supplemented by supportive measures such as fresh frozen plasma transfusions for bleeding patients or, rarely, anticoagulants like heparin for predominant thrombosis.[5] Blood product replacement (platelets, cryoprecipitate) is tailored to the hemorrhagic risk, while complications like organ failure may require intensive care interventions.[2] Prognosis varies widely depending on the inciting condition, with mortality rates exceeding 40% in severe cases, underscoring the need for early recognition and intervention.[1]Overview
Definition
Disseminated intravascular coagulation (DIC) is an acquired syndrome defined as a widespread activation of the coagulation system throughout the vasculature, leading to the formation of microvascular thrombi, consumptive coagulopathy, and subsequent risk of hemorrhage.[2] This process disrupts normal hemostasis, resulting in the paradoxical occurrence of both excessive clotting and bleeding tendencies.[1] The core characteristics of DIC include systemic thrombin generation that consumes platelets and coagulation factors, such as fibrinogen and factors V and VIII, thereby impairing the body's ability to form clots at sites of injury while promoting diffuse thrombosis in small vessels.[8] This depletion often culminates in a hemorrhagic phase, where bleeding from multiple sites—such as mucous membranes, wounds, or intravenously—becomes prominent due to insufficient hemostatic reserves.[2] DIC was first recognized as a distinct clinical entity in the early 20th century, particularly in association with obstetric complications, with more comprehensive understanding of its mechanisms emerging in the mid-20th century through studies on sepsis and trauma-related cases.[9] Unlike localized clotting disorders, such as deep vein thrombosis, which involve thrombus formation confined to a single large vessel, DIC represents a systemic disorder with multi-organ involvement and dual thrombotic-hemorrhagic features.[1] Typically, DIC arises secondary to an underlying trigger that initiates uncontrolled coagulation activation.[2]Classification
Disseminated intravascular coagulation (DIC) is primarily classified into acute and chronic forms based on the rapidity of onset and underlying clinical context. Acute DIC manifests with rapid activation of coagulation, often within hours to days, and is typically life-threatening due to overwhelming consumptive coagulopathy that leads to severe bleeding and organ dysfunction.[2] In contrast, chronic DIC develops insidiously over weeks to months, frequently compensating through increased production of clotting factors, and is commonly associated with underlying malignancies or vascular abnormalities.[10][2] Subtypes of DIC are further categorized by their primary triggers, which influence clinical management and prognosis. Sepsis-related DIC, the most prevalent subtype (accounting for 30-50% of cases), arises from systemic infection, particularly gram-negative bacteria, leading to endothelial damage and procoagulant release.[2] Trauma-induced DIC occurs in severe injuries, exacerbated by tissue factor exposure and hypoperfusion, contributing to high mortality rates.[2] Obstetric DIC is triggered by complications such as placental abruption or amniotic fluid embolism, often presenting peripartum.[2] Cancer-associated DIC, seen in up to 20% of metastatic adenocarcinomas, involves tumor-derived procoagulants and is more common in solid tumors (1-5% incidence).[2] Severity in DIC is graded using the International Society on Thrombosis and Haemostasis (ISTH) scoring system, which assesses overt DIC through laboratory parameters and requires an underlying disorder for application. The system evaluates four key criteria: platelet count, elevated fibrin-related markers (e.g., D-dimer), prolonged prothrombin time (PT), and fibrinogen levels. A total score of ≥5 indicates overt DIC, with daily reassessment recommended to monitor progression.[11][12]| Parameter | Score |
|---|---|
| Platelet count (×10⁹/L) | ≥100: 0 50–<100: 1 <50: 2 |
| Elevated fibrin-related marker (e.g., D-dimer) | No increase: 0 Moderate increase: 2 Strong increase (>4× upper limit): 3 |
| Prolonged PT | <3 s or <1.2× normal: 0 ≥3 s but <6 s or ≥1.2× but <1.4× normal: 1 ≥6 s or ≥1.4× normal: 2 |
| Fibrinogen (g/L) | >1: 0 ≤1: 1 |
Etiology
Causes
Disseminated intravascular coagulation (DIC) is invariably a secondary disorder triggered by underlying medical conditions or events that provoke systemic activation of the coagulation cascade. The primary initiators include widespread endothelial injury, exposure of tissue factor (TF), or release of procoagulant substances, leading to uncontrolled thrombin generation.[13] Infections represent one of the most common causes of DIC, particularly severe sepsis induced by bacterial pathogens such as Gram-negative organisms (e.g., Escherichia coli) or Gram-positive bacteria (e.g., Staphylococcus aureus). These infections lead to endothelial damage and release of microbial components like lipopolysaccharide, which, in conjunction with inflammatory cytokines, expose TF on damaged cells and monocytes, initiating coagulation. Viral infections such as malaria or hemorrhagic fevers (e.g., Ebola) can similarly trigger DIC through endothelial disruption and procoagulant release. DIC develops in approximately 35% of patients with severe sepsis, highlighting its high prevalence in this setting.[13] Trauma is another major precipitant, often seen in cases of severe injury, including multitrauma, head trauma, or extensive burns. The mechanism involves direct release of TF from damaged tissues into the bloodstream and endothelial injury from hypoperfusion or shock, promoting widespread fibrin formation. Approximately 20-30% of patients with severe trauma may develop DIC, particularly when associated with massive transfusion or prolonged hypotension.[13] Malignancies frequently underlie DIC, with acute promyelocytic leukemia (APL) being a classic example due to the release of procoagulants from leukemic promyelocytes, causing rapid TF expression and consumptive coagulopathy. Solid tumors, such as adenocarcinomas of the lung, pancreas, or prostate, can also initiate DIC through tumor cell expression of TF or mucin-associated procoagulants, especially in advanced or metastatic disease. DIC occurs in about 15% of acute leukemia cases and up to 20% of patients with metastatic solid tumors.[13] Obstetric complications are significant triggers, including placental abruption, amniotic fluid embolism, and retained dead fetus syndrome. These conditions cause DIC via leakage of TF-bearing amniotic fluid or placental tissue into the maternal circulation, leading to acute endothelial activation and procoagulant exposure. Such events account for a notable proportion of peripartum coagulopathies, with DIC developing in approximately 80% of cases of amniotic fluid embolism.[13] Less common causes encompass envenomations, such as snake bites from viper species that release prothrombin activators or direct procoagulants into the bloodstream, resulting in endothelial damage and TF-mediated coagulation. Vascular disorders like giant hemangiomas (Kasabach-Merritt syndrome) trap platelets and activate coagulation locally through stagnant blood flow and procoagulant release. Heatstroke can also precipitate DIC by inducing severe endothelial injury from hyperthermia and cytokine storm. These rarer etiologies typically involve localized or systemic procoagulant overload but share the core mechanism of overwhelming the anticoagulant systems.[2]Risk Factors
Patient-related factors significantly influence the susceptibility to disseminated intravascular coagulation (DIC) in the presence of underlying triggers. Advanced age, particularly in the elderly, heightens risk due to a chronic low-grade pro-inflammatory state that exacerbates coagulation disturbances. Comorbidities such as liver disease impair the synthesis of clotting factors, thereby amplifying the potential for coagulopathy when combined with precipitating events. Genetic predispositions, including heterozygous protein C deficiency, confer an elevated thrombotic risk that can predispose individuals to DIC development.[14] Environmental and iatrogenic factors also play a key role in increasing DIC likelihood. Recent surgery is associated with approximately 15.5% of DIC cases, often through complications involving systemic inflammation or tissue injury.[2] Use of extracorporeal circuits, such as extracorporeal membrane oxygenation (ECMO), promotes DIC via consumption of coagulation factors, acquired von Willebrand syndrome, and thrombocytopenia.[15] Certain chemotherapeutic agents can induce DIC as a complication, particularly in patients with underlying malignancies, by triggering rapid tumor lysis and release of procoagulant substances.[16] Disease-specific amplifiers further elevate risk in affected individuals. Disseminated cancers contribute to DIC by increasing circulating procoagulant microparticles, which express tissue factor and enhance thrombin generation.[17] Quantifiable risks highlight the impact in specific scenarios, such as trauma. Patients with an injury severity score greater than 15 face a substantially heightened DIC risk, with incidences reported in 20-30% of severe cases, correlating with higher mortality and transfusion needs.[18]Pathophysiology
Coagulation Activation
Disseminated intravascular coagulation (DIC) begins with the widespread activation of the coagulation system, primarily triggered by the exposure or expression of tissue factor (TF), a transmembrane glycoprotein normally absent from circulating blood but present in subendothelial tissues and certain cells like monocytes and fibroblasts. In pathological states, such as sepsis or trauma, TF is aberrantly expressed on the surface of endothelial cells or blood cells, initiating the extrinsic coagulation pathway. The TF binds circulating factor VII or its activated form, factor VIIa, forming the TF-factor VIIa complex, which potently activates factor X to factor Xa and factor IX to factor IXa, thereby catalyzing the conversion of prothrombin to thrombin.[19][2] This initial activation is amplified through the intrinsic and common pathways, leading to explosive thrombin generation that exceeds the capacity of natural anticoagulants. The intrinsic pathway, involving factors XII, XI, and VIII, is recruited via positive feedback from thrombin, which activates factor XI and factor V, further enhancing the activation of factor X and prothrombin. The common pathway then proceeds with factor Xa, in complex with factor Va on phospholipid surfaces, converting prothrombin to thrombin at an accelerated rate. Thrombin not only cleaves fibrinogen to form fibrin but also sustains the cascade by activating additional factors, creating a self-perpetuating loop of coagulation.[2][3] Endothelial dysfunction plays a central role in sustaining this hypercoagulable state by impairing anticoagulant mechanisms and promoting procoagulant activity. Damaged or activated endothelium downregulates thrombomodulin expression, a key cofactor that normally binds thrombin to activate protein C, thereby inhibiting the natural anticoagulant pathway and allowing unchecked thrombin activity. Concurrently, endothelial cells release increased levels of von Willebrand factor (vWF), which facilitates platelet adhesion to the subendothelium and promotes the formation of platelet-rich thrombi in the microvasculature.[2][20] In sepsis-associated DIC, proinflammatory cytokines such as tumor necrosis factor-alpha (TNF-α) and interleukin-6 (IL-6) are pivotal in driving coagulation activation. These cytokines, released by activated immune cells, induce TF expression on monocytes and endothelial cells through signaling pathways like NF-κB, thereby initiating the extrinsic pathway in a dysregulated manner. TNF-α, in particular, enhances endothelial permeability and procoagulant activity while suppressing anticoagulant proteins, amplifying the systemic response. IL-6 further contributes by stimulating acute-phase reactants that support coagulation. Neutrophils also play a crucial role, releasing neutrophil extracellular traps (NETs) upon activation by pathogens or inflammatory signals. NETs, composed of decondensed chromatin and antimicrobial proteins, provide procoagulant surfaces that promote thrombin generation and fibrin formation, exacerbating microvascular thrombosis in DIC.[19][21][8] Feedback loops involving platelets exacerbate the process, as thrombin-generated fibrin strands and exposed collagen activate platelets, leading to their aggregation and release of additional procoagulant factors like polyphosphates. Activated platelets provide phospholipid surfaces that assemble coagulation complexes, accelerating thrombin formation and contributing to the deposition of microvascular thrombi throughout the circulation. This platelet involvement creates localized sites of intense coagulation activity, propagating the disseminated nature of the disorder.[2][3]Consumptive Coagulopathy and Secondary Effects
In disseminated intravascular coagulation (DIC), the initial widespread activation of coagulation leads to the consumption of essential hemostatic components, resulting in a phase of hypocoagulability known as consumptive coagulopathy. This process depletes platelets, fibrinogen, and key clotting factors such as II, V, and VIII, as they are incorporated into widespread fibrin thrombi throughout the microvasculature. The exhaustion of these elements impairs the body's ability to form stable clots at sites of vascular injury, predisposing patients to severe hemorrhagic complications.[2][8][22] A secondary consequence of this coagulopathy is the activation of fibrinolysis, where plasmin is generated to degrade the excess fibrin deposits. This enzymatic breakdown produces elevated levels of fibrin degradation products, including D-dimers, which further contribute to the bleeding diathesis by interfering with normal clot stabilization. The imbalance between ongoing thrombus formation and this compensatory lysis exacerbates the systemic hemostatic failure.[8][22][2] The microvascular thrombi formed during the hypercoagulable phase also induce ischemia in vital organs, leading to profound secondary effects. For instance, glomerular and tubular microthrombosis can cause renal hypoperfusion and acute kidney injury, while pulmonary thrombi impair gas exchange, contributing to acute respiratory distress syndrome (ARDS). Hepatic involvement similarly results in dysfunction, with reduced synthetic capacity for clotting factors amplifying the coagulopathy. These ischemic insults compound the systemic derangements in DIC.[8][22] DIC's consumptive phase synergizes with inflammation, where proinflammatory cytokines such as tumor necrosis factor and interleukin-6 promote endothelial damage and tissue factor expression, intensifying coagulation activation. Neutrophil-derived NETs further bridge inflammation and thrombosis by releasing histones and DNA that activate coagulation factors and impair fibrinolysis, contributing to organ damage. This interplay exacerbates multi-organ dysfunction syndrome (MODS), as the coagulopathy fuels a proinflammatory cascade that impairs organ perfusion and repair mechanisms across multiple systems.[8][22] The resulting hemorrhage from hypocoagulability perpetuates a vicious cycle, as blood loss and tissue exposure to procoagulant materials trigger further thrombin generation and consumption of remaining hemostatic reserves. This self-reinforcing loop sustains the dual thrombotic and bleeding phenotypes of DIC, worsening prognosis in affected patients.[2][8]Clinical Features
Signs and Symptoms
Disseminated intravascular coagulation (DIC) manifests through a combination of bleeding and thrombotic symptoms due to widespread activation of the coagulation system. Patients often present with signs of both microvascular and macrovascular involvement, reflecting the dual nature of consumptive coagulopathy and fibrin deposition.[2] Bleeding symptoms are prominent and include petechiae, which appear as small red or purple spots on the skin caused by capillary bleeding, and ecchymoses, larger purple bruises from subcutaneous hemorrhage. Mucosal bleeding from the gums, nose, or mouth is common, along with prolonged oozing from venipuncture or surgical sites, and hematuria or blood in the stool. These manifestations arise from depletion of clotting factors and platelets.[2][1] Thrombotic signs may coexist or predominate, such as acrocyanosis with bluish discoloration of the extremities due to microvascular thrombosis, and digital ischemia leading to pain or gangrene in the fingers or toes. Organ-specific thrombosis can cause stroke-like symptoms including confusion, headaches, or focal neurological deficits from cerebral vessel occlusion.[2][8] Systemic symptoms include fever, often linked to underlying infection, and hypotension in sepsis-associated cases, contributing to overall hemodynamic instability. Fatigue and shortness of breath may result from anemia secondary to blood loss or hemolytic processes.[1][8] In acute DIC, bleeding symptoms dominate and develop rapidly over hours to days following the triggering event, such as severe infection or trauma. Chronic DIC, by contrast, presents more insidiously with recurrent thrombosis over weeks to months, often with subtler bleeding.[23][2]Complications
Disseminated intravascular coagulation (DIC) can precipitate severe hemorrhagic complications due to the consumptive coagulopathy that depletes clotting factors and platelets, leading to widespread bleeding. Intracranial hemorrhage represents a critical risk, often manifesting as the initial presentation in some cases and contributing to high morbidity through neurological deficits or rapid deterioration.[24] Gastrointestinal bleeding is another frequent hemorrhagic event, arising from mucosal erosions exacerbated by microvascular thrombosis and subsequent ischemia, which can result in significant blood loss and hemodynamic instability.[25] Adrenal hemorrhage, particularly in the context of bacterial sepsis, may culminate in Waterhouse-Friderichsen syndrome, characterized by bilateral adrenal infarction and acute adrenal insufficiency, further compounding shock and multi-organ involvement.[26] Thrombotic complications in DIC stem from the initial hypercoagulable state, where microvascular occlusion predominates before the shift to hemorrhage. Purpura fulminans is a hallmark thrombotic manifestation, involving extensive dermal vascular thrombosis that leads to purpuric lesions, skin necrosis, and potential amputation, often triggered by severe infections.[27] Limb gangrene, including symmetrical peripheral gangrene and venous limb gangrene, occurs due to distal microvascular thrombosis despite preserved large-vessel pulses, resulting in tissue ischemia and necrosis that may necessitate surgical intervention. Multi-organ failure frequently arises as a direct sequela of DIC through combined thrombotic and ischemic insults to vital organs. Acute kidney injury, often progressing to cortical necrosis, results from renal microvascular occlusion and hypoperfusion, severely impairing renal function in up to a significant proportion of severe cases.[28] Shock liver, or ischemic hepatitis, develops from hepatic hypoperfusion and microvascular damage, leading to elevated transaminases and potential acute liver failure.[29] Additionally, DIC can exacerbate acute respiratory distress syndrome (ARDS) by promoting pulmonary microvascular thrombosis and inflammation, worsening gas exchange and respiratory failure.[30] Survivors of advanced DIC may experience long-term sequelae from residual organ damage incurred during the acute phase. Chronic organ impairment, such as persistent renal dysfunction or hepatic fibrosis, can ensue from ischemic insults that were not fully reversible.[2] In cases linked to sepsis-induced DIC, post-sepsis cognitive impairment is a recognized outcome, involving deficits in memory, executive function, and attention due to cerebral microvascular injury and systemic inflammation.[31] In severe DIC, particularly when associated with sepsis, complications contribute to mortality rates approaching 40-50%, underscoring the life-threatening nature of unchecked disease progression.[32]Diagnosis
Clinical Assessment
Clinical assessment of disseminated intravascular coagulation (DIC) begins with a thorough history to identify potential underlying triggers, as DIC rarely occurs in isolation and is almost always secondary to an acute systemic insult. Clinicians should inquire about recent severe trauma, such as major injuries or surgery, which can activate widespread coagulation through tissue factor release.[2] Similarly, a history of severe infection, particularly sepsis from bacterial sources like gram-negative organisms, is a common precipitant, often presenting with fever, hypotension, or organ dysfunction.[2] Malignancy, especially acute promyelocytic leukemia or solid tumors like prostate adenocarcinoma, should be explored through reports of unexplained weight loss, night sweats, or prior cancer diagnoses.[2] Obstetric complications, including placental abruption, amniotic fluid embolism, or postpartum hemorrhage, warrant specific attention in reproductive-age patients, as these can rapidly trigger consumptive coagulopathy.[2] Physical examination focuses on detecting signs of microvascular bleeding and thrombosis, alongside systemic instability, to heighten suspicion for DIC. Bleeding manifestations may include petechiae, purpura, or ecchymoses on the skin and mucous membranes, such as conjunctival hemorrhages, alongside oozing from venipuncture sites or surgical wounds.[33] Thrombotic features can present as limb swelling suggestive of deep vein thrombosis or acral cyanosis from digital ischemia, though these may be subtle in acute settings.[2] Vital signs often reveal instability, including tachycardia, hypotension, and tachypnea, particularly in sepsis- or trauma-associated cases, reflecting the underlying disorder's severity.[33] In intensive care unit (ICU) patients, DIC should be suspected when unexplained coagulopathy emerges in the context of these triggers, such as progressive bleeding without prior hemostatic defects.[34] The 2025 ISTH update recognizes DIC as a dynamic process with phases (pre-DIC, early-phase DIC, overt DIC), emphasizing early suspicion to prevent progression to advanced coagulopathy and organ dysfunction.[35] To aid early clinical suspicion, especially in sepsis, the modified Japanese Association for Acute Medicine (JAAM-2) DIC score (2025) can be applied as a bedside tool, using platelet count, fibrin degradation products (FDP), and prothrombin time (PT) ratio for rapid identification aligned with Sepsis-3 definitions.[36] A score of 4 or greater indicates DIC, with high sensitivity for early coagulopathy in critically ill patients and utility in guiding anticoagulation.[36] Differential diagnosis requires distinguishing DIC from primary coagulopathies; unlike hemophilia, which presents with isolated joint or muscle bleeds in a hereditary pattern without systemic triggers, DIC involves consumptive thrombocytopenia and is linked to acute illnesses like infection or trauma.[37] Thrombotic thrombocytopenic purpura (TTP) and hemolytic uremic syndrome (HUS) may mimic DIC with microangiopathic hemolytic anemia and thrombocytopenia but typically occur in non-septic settings, such as autoimmune or Shiga toxin-related etiologies, without the broad consumptive features of DIC.[38]Laboratory Tests and Criteria
Diagnosis of disseminated intravascular coagulation (DIC) relies on laboratory testing to identify abnormalities in coagulation parameters, platelet count, and fibrin degradation products, which reflect the underlying consumptive process.[39] Key laboratory findings include thrombocytopenia, typically with platelet counts below 100 × 10^9/L, prolonged prothrombin time (PT) and activated partial thromboplastin time (aPTT), decreased fibrinogen levels often less than 1.5 g/L, and elevated levels of D-dimer or fibrin degradation products (FDPs), usually exceeding 10 times the upper limit of normal.[40] These changes arise from widespread activation and consumption of clotting factors and platelets.[2] The International Society on Thrombosis and Haemostasis (ISTH) provides a standardized scoring system updated in 2025 for diagnosing overt DIC, integrating platelet count, D-dimer, PT international normalized ratio (INR), and fibrinogen level, with a total score of 5 or greater compatible with overt DIC.[35] The 2025 update introduces phase-based classification, including early-phase DIC assessed via sepsis-induced coagulopathy (SIC) scoring for timely intervention. Scoring should be repeated daily to monitor progression.[35] The overt DIC scoring is as follows:| Parameter | Score |
|---|---|
| Platelet count (×10^9/L) | |
| ≥100 | 0 |
| 50–<100 | 1 |
| <50 | 2 |
| D-dimer | |
| No increase | 0 |
| >3× but ≤7× upper limit | 2 |
| >7× upper limit | 3 |
| Prothrombin time INR | |
| ≤1.2 | 0 |
| >1.2 to ≤1.4 | 1 |
| >1.4 | 2 |
| Fibrinogen (g/L) | |
| >1.0 | 0 |
| ≤1.0 | 1 |