What does abdominal tenderness indicate in dengue?

Abdominal pain or tenderness is a WHO warning sign and may reflect dengue hepatitis, ascites from plasma leakage into the abdominal cavity, or retroperitoneal fluid accumulation. It warrants prompt assessment and often hospitalisation, particularly when combined with rising haematocrit and falling platelets.

What monitoring should be performed in a dengue patient managed at home?

Daily clinical review including vital signs, oral intake adequacy, warning sign assessment, and full blood count (haematocrit and platelets). Home monitoring includes temperature twice daily, fluid intake and urine output tracking, and immediate emergency attendance if any warning sign develops.

What dengue vaccines are available?

Two vaccines are approved: Dengvaxia (Sanofi Pasteur) for previously infected individuals aged 9 and above, requiring pre-vaccination serotesting. Qdenga (Takeda) approved in the EU, Indonesia, Brazil, and other countries for ages 4 and above, showing 84% reduction in dengue hospitalisation regardless of prior serostatus.

Dengue Severity Calculator- Free WHO 2009 Warning Signs and Classification Tool

Dengue Severity Calculator – Free WHO 2009 Warning Signs and Classification Tool | Super-Calculator.com

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This dengue severity calculator requires JavaScript to assess WHO 2009 dengue warning signs, classify dengue severity, and generate management guidance for dengue fever. Please enable JavaScript in your browser to use this free dengue clinical assessment tool.

Important Medical Disclaimer

This calculator is provided for informational and educational purposes only. It is not intended to replace professional medical advice, diagnosis, or treatment. Always consult with a qualified healthcare professional before making any medical decisions. The results from this calculator should be used as a reference guide only and not as the sole basis for clinical decisions. Dengue is a dynamic illness – this assessment reflects the clinical state at one point in time and must be repeated as the illness progresses.

Dengue Severity Calculator

Structured clinical assessment tool based on WHO 2009 revised dengue classification. Evaluate all 7 dengue warning signs, assess severe dengue criteria including dengue shock syndrome and organ impairment, and receive evidence-based management guidance for dengue fever triage and hospital admission decisions.

Dengue Severity Classification

WHO 2009 Classification

Complete Assessment

Enter clinical details to classify dengue severity

Laboratory Parameters

Platelet Count (x10^3/uL)100

Current Haematocrit (%)40

Baseline Haematocrit (%) pre-illness or normal40

Platelet Count

100

x10^3/uL

Haematocrit Rise

above baseline

Management Guidance

Assessment Required

Complete the clinical assessment to receive management guidance

WHO 2009 Dengue Severity Classification Reference

Classification	Key Criteria	Management	Risk Level
Dengue (No Warning Signs)	Fever plus 2 or more: nausea/vomiting, rash, aches, positive tourniquet test, leukopenia. No warning signs present.	Home care with daily follow-up. Oral rehydration, paracetamol (not NSAIDs). Written warning sign instructions.	Low Risk
Dengue with Warning Signs	Any dengue case with one or more of the 7 WHO warning signs present.	Hospital admission. IV fluid therapy. Close monitoring of vitals and haematocrit every 4-6 hours. Platelet count monitoring.	Moderate-High Risk
Severe Dengue	Severe plasma leakage (shock or respiratory distress), severe bleeding, or severe organ impairment (liver, CNS, heart, kidney).	Emergency hospital care. Immediate IV fluid resuscitation for shock. ICU-level monitoring. Specialist team involvement.	Critical – Emergency
Dengue Shock Syndrome	Pulse pressure below 20 mmHg (systolic minus diastolic), or age-appropriate hypotension, with rising haematocrit confirming plasma leakage.	Isotonic crystalloid 10 ml/kg bolus over 15-30 minutes. Reassess every 15-30 minutes. Repeat bolus if no improvement. Escalate to colloid if unresponsive.	Critical – Emergency

Source: WHO (2009). Dengue: Guidelines for Diagnosis, Treatment, Prevention and Control (New edition). World Health Organization, Geneva. All classifications should be applied by trained healthcare professionals.

All 7 WHO Dengue Warning Signs – Clinical Criteria Detail

Warning Sign	Clinical Description	Pathophysiological Basis
1. Abdominal Pain or Tenderness	Persistent or severe abdominal pain, or tenderness on palpation of the abdomen, especially the right upper quadrant and epigastrium	Dengue hepatitis causing hepatic pain; ascites from plasma leakage into the peritoneal cavity; retroperitoneal fluid accumulation
2. Persistent Vomiting	Vomiting that prevents adequate oral fluid intake; clinically defined as inability to keep fluids down due to repeated vomiting episodes	Gastric irritation from dengue-related gastritis; dehydration exacerbating nausea; direct effect of dengue viraemia on the gastrointestinal tract
3. Clinical Fluid Accumulation	Clinical or radiological evidence of fluid in body cavities: ascites (abdominal fluid), pleural effusion (fluid around lungs), or pericardial effusion (fluid around heart)	Increased vascular permeability causing plasma leakage from the intravascular to extravascular compartment, accumulating in potential body spaces
4. Mucosal Bleeding	Spontaneous bleeding from mucosal surfaces: gum bleeding on minimal provocation, epistaxis (nosebleed), conjunctival haemorrhage (bleeding in the eye)	Dengue-associated thrombocytopenia and platelet dysfunction combined with capillary fragility from vascular endothelial damage
5. Lethargy or Restlessness	Marked lethargy, unusual drowsiness, difficulty waking, or paradoxical agitation or restlessness, particularly in children	Reduced cerebral perfusion from plasma leakage and early circulatory compromise; direct dengue effect on the central nervous system; hepatic encephalopathy from dengue hepatitis
6. Liver Enlargement greater than 2 cm	Hepatomegaly with the liver palpable more than 2 cm below the right costal margin on clinical examination	Dengue hepatitis causing hepatocyte injury and liver swelling; Kupffer cell activation from dengue viraemia; hepatic inflammation
7. Rising Haematocrit with Rapid Platelet Drop	Concurrent 20% or more rise in haematocrit above baseline AND a rapid fall in platelet count, often to below 100,000 per microlitre	The haematocrit rise reflects plasma leakage causing haemoconcentration; the platelet drop reflects bone marrow suppression from dengue viraemia and peripheral platelet consumption

Note: Any single warning sign warrants hospital admission. Multiple warning signs indicate higher risk of progression to severe dengue. Warning signs most commonly appear during the critical defervescence period, approximately days 3-7 of illness.

Dengue Laboratory Reference Values and Severity Thresholds

Parameter	Value / Range	Clinical Significance in Dengue	Status
Platelet Count	Above 100,000 x10^3/uL	Normal range; dengue may show mild reduction. Monitor trend.	Normal
Platelet Count	50,000 – 100,000 x10^3/uL	Mild to moderate thrombocytopenia. Increased monitoring frequency. Dengue with warning signs if concurrent with haematocrit rise.	Mild-Moderate
Platelet Count	20,000 – 50,000 x10^3/uL	Moderate to severe thrombocytopenia. High risk of bleeding with trauma or procedures. Consider inpatient monitoring.	Severe
Platelet Count	Below 20,000 x10^3/uL	Profound thrombocytopenia. Risk of spontaneous bleeding. Platelet transfusion only if active significant bleeding – not prophylactically.	Critical
Haematocrit Rise	Below 10% above baseline	Minimal plasma leakage. Monitor closely if approaching defervescence.	Minimal
Haematocrit Rise	10% – 20% above baseline	Moderate haemoconcentration. Increasing risk of plasma leakage. Ensure adequate oral hydration and close follow-up.	Moderate
Haematocrit Rise	20% or more above baseline	Significant plasma leakage – WHO Warning Sign. Requires hospitalisation and IV fluid management.	Warning Sign
White Cell Count (WBC)	Below 4,000 x10^3/uL	Leukopenia is a diagnostic criterion for dengue (not a severity marker). Common in the febrile phase.	Low (expected)
Liver Enzymes (AST/ALT)	Normal to 5 times upper limit	Mild elevation common in dengue. Monitor trend.	Mild
Liver Enzymes (AST/ALT)	Above 1000 IU/L	Severe dengue hepatitis – this alone meets Severe Dengue criteria regardless of other features.	Severe Dengue
Pulse Pressure	Below 20 mmHg	Dengue Shock Syndrome – compensated shock with plasma leakage. Urgent fluid resuscitation required.	Shock

Note: Reference ranges may vary with age, sex, altitude, and laboratory methods. Paediatric normal values differ from adult values – use age-appropriate reference ranges. All laboratory results must be interpreted in the context of the full clinical picture by a qualified healthcare professional.

About This Dengue Severity Calculator

This dengue severity calculator is designed for healthcare professionals, medical students, and trained clinicians who need a structured, systematic tool for classifying dengue severity at the point of care. It computes WHO 2009 dengue severity classification by guiding the user through evaluation of dengue diagnostic criteria, all seven WHO dengue warning signs, severe dengue features including dengue shock syndrome, and laboratory parameters including haematocrit rise and platelet count severity – producing an evidence-based severity classification and management guidance in real time.

The calculator applies the World Health Organization 2009 revised dengue guidelines, which classify dengue into three actionable tiers: dengue without warning signs (suitable for home management with daily follow-up), dengue with warning signs (requires hospital admission and IV fluid monitoring), and severe dengue (requires emergency hospital treatment). The severe dengue tier is further subdivided by pathway: severe plasma leakage (dengue shock syndrome with pulse pressure below 20 mmHg or hypotension, or fluid accumulation with respiratory distress), severe bleeding, and severe organ impairment (liver AST or ALT 1000 IU/L or above, impaired consciousness from dengue encephalopathy or encephalitis, or other organ failure). The haematocrit rise calculator identifies the 20% threshold that constitutes a dengue warning sign for plasma leakage.

Using this dengue clinical assessment tool reduces the risk of missing warning signs during high-volume triage, particularly during the critical defervescence period when patients may appear clinically stable while plasma leakage is progressing. The Dengue Severity Reference tab provides a complete WHO 2009 classification table; the Warning Signs Clinical Criteria tab details the pathophysiological basis of each of the seven warning signs; and the Lab Values Reference tab displays dengue thrombocytopenia severity thresholds and haematocrit rise interpretation ranges. All assessments should be performed by a qualified clinician and repeated as the illness evolves – dengue is a dynamic disease, and a single assessment does not substitute for continuous clinical monitoring.

Dengue Severity Calculator – Complete Clinical Guide to WHO 2009 Classification, Warning Signs, and Patient Management

Dengue fever is one of the most significant mosquito-borne viral diseases in the world, affecting an estimated 390 million people annually across more than 100 countries. The disease is caused by any of four serotypes of the dengue virus (DENV-1 through DENV-4), transmitted primarily by the Aedes aegypti and Aedes albopictus mosquitoes. Accurate severity assessment is critical because dengue can progress rapidly from a mild febrile illness to severe dengue with life-threatening complications including plasma leakage, haemorrhage, and organ impairment.

This dengue severity calculator is built on the World Health Organization (WHO) 2009 revised classification system, which replaced the older 1997 classification and is now widely used in clinical practice globally. Understanding how to apply this classification – and recognising the warning signs that require immediate medical attention – can be the difference between safe outpatient monitoring and timely hospital admission that saves a life.

The WHO 2009 Dengue Classification System

The WHO 2009 guidelines introduced a three-tier classification of dengue that better reflects the clinical spectrum of the disease and guides management decisions at each stage. The three categories are: Dengue (without warning signs), Dengue with Warning Signs, and Severe Dengue.

This revised classification was developed following extensive field experience showing that the older categories (dengue fever, dengue haemorrhagic fever grades I-IV, and dengue shock syndrome) did not adequately guide clinical decision-making, particularly in identifying patients at risk of deterioration before they developed severe disease. The 2009 framework emphasises prospective monitoring for warning signs as the key triage tool.

WHO 2009 Dengue Severity Classification

Dengue – No Warning Signs – Dengue with Warning Signs – Severe Dengue

Dengue (No Warning Signs): Fever plus two or more of: nausea/vomiting, rash, aches and pains, positive tourniquet test, leukopenia. May be managed at home with close monitoring.

Dengue with Warning Signs: Any dengue case with one or more of the seven WHO warning signs. Requires inpatient observation and intravenous fluid support in many cases.

Severe Dengue: Severe plasma leakage with shock or fluid accumulation with respiratory distress, severe bleeding, or severe organ impairment. Requires emergency treatment in a hospital with intensive care capability.

The Seven WHO Dengue Warning Signs

Recognising the seven warning signs defined by the WHO is the cornerstone of dengue triage. These signs typically appear around the time of defervescence – when the fever breaks, usually between days 3 and 7 of illness. This is a critical and deceptive period because patients may appear to be improving while actually entering the most dangerous phase of disease.

The seven warning signs are: abdominal pain or tenderness; persistent vomiting; clinical fluid accumulation (ascites, pleural effusion, or pericardial effusion detected clinically or on imaging); mucosal bleeding; lethargy or restlessness; liver enlargement greater than 2 cm; and a rise in haematocrit concurrent with a rapid decrease in platelet count. Each of these signs reflects a specific pathophysiological process that increases the risk of progression to severe dengue.

Key Point: The Critical Defervescence Period

Warning signs most commonly appear when the fever breaks, typically between days 3 and 7 of illness. Paradoxically, patients may feel subjectively better as the fever subsides, masking the onset of plasma leakage. Clinicians and caregivers must be vigilant during this period even when the patient appears to be improving.

Understanding Severe Dengue Criteria

Severe dengue is defined by the presence of one or more of three major categories of severe manifestation. The first is severe plasma leakage leading to dengue shock syndrome (narrowed pulse pressure below 20 mmHg, or hypotension for age) or respiratory distress from fluid accumulation in the pleural space or abdomen. The second is severe bleeding as assessed by the treating clinician. The third is severe organ involvement – including liver injury (AST or ALT of 1000 IU/L or above), central nervous system manifestations such as impaired consciousness, or other organ failures affecting the heart, kidneys, or other systems.

Understanding that these three pathways represent distinct clinical syndromes helps guide both diagnosis and management. A patient in dengue shock requires aggressive but carefully measured fluid resuscitation, whereas a patient with impaired consciousness requires neurological assessment and investigation for dengue encephalitis or encephalopathy. One-size-fits-all management is inappropriate in severe dengue.

Severe Dengue Diagnostic Criteria

Severe Plasma Leakage OR Severe Bleeding OR Severe Organ Involvement

Severe Plasma Leakage: Dengue shock syndrome (pulse pressure less than 20 mmHg, or hypotension) OR fluid accumulation with respiratory distress (pleural effusion, ascites causing respiratory compromise).

Severe Bleeding: Clinically significant haemorrhage judged by the treating physician to require intervention or that is haemodynamically significant.

Severe Organ Impairment: Liver: AST or ALT 1000 IU/L or above. CNS: Impaired consciousness, dengue encephalitis or encephalopathy. Heart: myocarditis. Kidneys: acute kidney injury.

Dengue Shock Syndrome and Haemodynamic Assessment

Dengue shock syndrome (DSS) results from massive plasma leakage caused by increased vascular permeability, a hallmark of dengue pathophysiology. Unlike septic shock, which involves vasodilation, DSS is a distributive shock characterised by leakage of plasma proteins and fluid into the extravascular compartment. This creates haemoconcentration (rising haematocrit) even as intravascular volume falls.

The hallmark haemodynamic finding in early DSS is a narrowing of the pulse pressure to below 20 mmHg, which occurs as diastolic blood pressure rises (compensatory peripheral vasoconstriction) while systolic blood pressure falls. Blood pressure may remain within the normal range until decompensation occurs, making pulse pressure a more sensitive early indicator than systolic blood pressure alone. In children, normal blood pressure values vary with age, and age-appropriate reference ranges must be applied.

Key Point: Pulse Pressure as an Early Shock Indicator

A pulse pressure below 20 mmHg indicates compensated shock even when blood pressure appears within normal limits. In clinical practice, calculate pulse pressure by subtracting diastolic from systolic blood pressure. Early identification of compensated shock allows fluid resuscitation before the patient decompensates to profound hypotension.

Haematocrit and Platelet Count in Dengue Assessment

Serial monitoring of haematocrit (PCV) and platelet count is essential in managing dengue patients. A rising haematocrit of 20% or more above the patient’s baseline (or above age- and sex-appropriate normal values) is a reliable indicator of plasma leakage and signals the onset of the critical phase. It is important to use the trend – a single haematocrit value is less informative than the rate of change.

Thrombocytopenia (low platelet count) is nearly universal in dengue and worsens during the febrile and critical phases. Platelet counts below 100,000 per microlitre are common; below 20,000 increases the risk of spontaneous bleeding. However, it is critical to understand that platelet count alone does not reliably predict bleeding risk in dengue. Significant haemorrhage is uncommon even with profound thrombocytopenia in the absence of other coagulopathy or vascular injury. Prophylactic platelet transfusion is not routinely recommended in the absence of active significant bleeding.

Haematocrit Rise Calculation

% Rise = ((Current HCT – Baseline HCT) / Baseline HCT) x 100

A rise of 20% or more above baseline indicates significant plasma leakage. In the absence of baseline values, use age- and sex-appropriate reference ranges: adult males approximately 40-50%, adult females approximately 36-44%. Apply this formula to serial readings taken every 4-6 hours during the critical phase.

The Tourniquet Test in Dengue Diagnosis

The tourniquet test (Rumpel-Leede test) is a bedside capillary fragility test that supports the diagnosis of dengue when positive. It is performed by inflating a blood pressure cuff to a point midway between the systolic and diastolic blood pressure and maintaining it for five minutes, then counting the number of petechiae (pinpoint haemorrhages) in a 2.5 cm x 2.5 cm (one square inch) area on the forearm below the cuff.

A result of 10 or more petechiae per square inch is considered positive. The sensitivity of the tourniquet test for dengue varies widely (40 to 90%) across studies, but its specificity is reasonable when interpreted in the correct clinical context. A positive tourniquet test in a febrile patient with headache, retro-orbital pain, myalgia, and arthralgia in an area where dengue is endemic is a clinically useful finding that increases diagnostic probability and supports the decision to perform dengue serology or NS1 antigen testing.

Clinical Phases of Dengue Fever

Dengue illness follows three distinct clinical phases that every clinician managing dengue should understand. These phases guide expectations for disease progression and the timing of investigations and interventions.

The febrile phase typically lasts two to seven days. Patients present with sudden onset high fever (often 39 to 40 degrees Celsius), severe headache, retro-orbital pain, myalgia, arthralgia, and sometimes a maculopapular rash. Facial flushing, nausea, and vomiting are common. The full blood count may show early leukopenia (low white cell count) and a normal or mildly reduced platelet count. NS1 antigen testing has the highest sensitivity during this phase (typically days one to five).

The critical phase occurs around defervescence (fever breaking), typically between days three and seven. This is the period of plasma leakage and highest risk. Haematocrit rises, platelets fall rapidly, and warning signs may emerge. Most patients who will develop severe dengue do so during this phase. Intensive monitoring is required even for patients who appear to be improving clinically as their temperature normalises.

The recovery phase begins when plasma leakage stops and fluid reabsorption starts, typically 48 to 72 hours after the start of the critical phase. Appetite returns, haematocrit normalises or may fall slightly as reabsorbed fluid dilutes the blood, platelets begin to recover, and the patient develops a characteristic convalescent rash. During recovery, fluid overload is a risk – particularly in patients who received large-volume intravenous fluids during the critical phase.

Key Point: Managing the Recovery Phase

During recovery, reabsorption of leaked plasma back into the intravascular compartment can cause fluid overload, pulmonary oedema, and haemodynamic strain. Intravenous fluids should be reduced or stopped early in recovery. Patients should be monitored for signs of fluid overload: increasing respiratory distress, decreasing heart rate, or worsening blood pressure after initial improvement.

Dengue in Special Populations

Certain patient groups face higher risk of severe dengue and require heightened clinical vigilance. These include infants, elderly patients, pregnant women, and individuals with comorbid conditions such as obesity, diabetes mellitus, hypertension, chronic kidney disease, or haematological disorders.

In infants, dengue can be particularly severe. The normal physiological polycythaemia of infancy makes haematocrit interpretation more complex, and clinical dehydration may be difficult to distinguish from plasma leakage. Infants have less physiological reserve and may deteriorate more rapidly than older children or adults.

Pregnant women with dengue face risks of maternal haemorrhage, premature labour, and vertical transmission to the foetus. The physiological anaemia of pregnancy complicates haematocrit interpretation, and fluid management must account for the increased circulating volume of pregnancy.

Patients with concurrent conditions such as peptic ulcer disease, haemolytic conditions, or those on anticoagulant therapy face substantially elevated bleeding risk in dengue. Non-steroidal anti-inflammatory drugs (NSAIDs) and aspirin must be avoided in dengue due to their antiplatelet effects and risk of gastric bleeding.

Dengue Serology and Diagnostics

Laboratory diagnosis of dengue is confirmed by one or more of the following: isolation of the dengue virus from serum; detection of dengue viral RNA by reverse transcription polymerase chain reaction (RT-PCR); detection of dengue NS1 antigen by rapid test or enzyme-linked immunosorbent assay (ELISA); or detection of dengue-specific IgM or IgG antibodies.

The timing of infection significantly affects which test is most appropriate. During days one to five of illness (the early febrile phase), NS1 antigen testing and RT-PCR have the highest sensitivity. After day five, as the immune response matures, dengue IgM serology becomes positive. In secondary dengue infections (where a person has been previously infected with a different dengue serotype), IgG may rise more rapidly and become the predominant antibody. Negative dengue serology in the first five days does not exclude dengue – repeat testing or NS1 testing should be performed.

Clinical Example: Correct Application of the Severity Assessment

A 28-year-old woman presents on day four of fever (39.2 degrees Celsius), with severe myalgia, retro-orbital pain, and a maculopapular rash. She has mild nausea but no vomiting. Her tourniquet test shows 12 petechiae per square inch. Full blood count shows WBC 2.8 x 10^9/L, platelets 65,000, haematocrit 38%. She has no warning signs: no abdominal pain, no mucosal bleeding, no lethargy, no fluid accumulation, and liver is not enlarged. No severe dengue features.

Classification: Dengue without warning signs. She requires dengue serology/NS1 testing, oral hydration, paracetamol for fever and pain (not NSAIDs), and clear return instructions for warning signs – particularly as she is approaching the critical defervescence period. Daily follow-up review is appropriate.

Fluid Management in Dengue

Fluid management is the cornerstone of dengue treatment. There are no antiviral agents with proven efficacy against dengue, and platelet transfusion is reserved for patients with significant active bleeding. The primary therapeutic intervention is careful fluid replacement to compensate for plasma leakage while avoiding fluid overload.

For patients with dengue without warning signs and adequate oral intake, oral rehydration at home with clear instructions to return if warning signs develop is appropriate. For patients with warning signs or who cannot tolerate oral fluids, intravenous fluid therapy using isotonic crystalloid solutions (normal saline or Ringer’s lactate) is the standard approach. Fluid rates are guided by clinical response – vital signs, haematocrit trends, urine output (target 0.5 to 1 ml/kg per hour), and capillary refill time.

In dengue shock syndrome, fluid resuscitation begins with an intravenous isotonic crystalloid bolus of 10 ml/kg over 15 to 30 minutes with immediate clinical reassessment. This approach differs from septic shock management, where larger initial boluses are commonly used. Excessive fluid resuscitation in dengue can precipitate pulmonary oedema during the recovery phase when leaked plasma is reabsorbed.

Global Epidemiology and Transmission

Dengue is endemic in more than 100 countries across tropical and subtropical regions of the world, with highest burden in Southeast Asia, the Western Pacific, the Americas (particularly the Caribbean and South America), and parts of Africa and South Asia. The global incidence of dengue has increased dramatically over the past five decades, driven by rapid urbanisation, population growth, inadequate vector control, and climate change expanding the geographical range of Aedes mosquitoes.

The four dengue serotypes co-circulate in endemic areas, and immunity to one serotype does not provide protection against the others. Secondary infection with a different serotype is associated with a higher risk of severe dengue due to antibody-dependent enhancement (ADE), in which pre-existing cross-reactive antibodies from the first infection facilitate viral entry into monocytes and macrophages during the second infection, amplifying viral replication. This mechanism partly explains why severe dengue is more common in individuals experiencing their second dengue infection.

Key Point: Secondary Infection and Severe Disease Risk

Individuals experiencing their second dengue infection with a different serotype face an elevated risk of severe dengue, partly due to antibody-dependent enhancement. In endemic regions, severe dengue disproportionately affects children aged 5 to 15 years who are experiencing secondary infections. This risk profile differs in populations newly exposed to dengue, where primary infection in adults can also result in severe disease.

Dengue Prevention and Vector Control

Prevention of dengue relies primarily on control of the Aedes aegypti mosquito, which breeds in small accumulations of clean standing water around human habitation – flower pots, discarded tyres, water storage containers, and drains. Vector control measures include source reduction (eliminating breeding sites), larviciding, and adult mosquito control using insecticides. Personal protective measures include the use of insect repellents containing DEET, picaridin, or IR3535, wearing long-sleeved clothing, and using mosquito nets and window screens.

A dengue vaccine (Dengvaxia, CYD-TDV, manufactured by Sanofi Pasteur) is licensed in several countries for use in individuals aged nine years and above who have had a confirmed prior dengue infection. It is not recommended for dengue-naive individuals, as it may increase the risk of severe dengue upon subsequent natural infection in that group. A second-generation dengue vaccine (TAK-003, Qdenga, manufactured by Takeda) has received regulatory approval in the European Union and several other countries and demonstrates efficacy against all four serotypes regardless of serostatus, though post-licensure safety monitoring is ongoing.

Differential Diagnosis of Dengue

Dengue must be distinguished from other febrile illnesses that share clinical features. Important differential diagnoses include malaria (which can cause similar fever patterns, thrombocytopenia, and severe disease), chikungunya (which is also transmitted by Aedes mosquitoes and causes fever and severe arthralgia), Zika virus infection (generally milder, with conjunctivitis and rash as distinctive features), leptospirosis, typhoid fever, and other viral haemorrhagic fevers.

In non-endemic regions or in returned travellers, the clinical presentation of dengue may be unfamiliar to clinicians, and a travel history is essential. Any febrile patient who has returned from a dengue-endemic region within 14 days should have dengue included in the differential diagnosis, and appropriate diagnostic testing should be performed promptly.

Monitoring Parameters During Hospital Admission

For patients admitted with dengue with warning signs or severe dengue, a structured monitoring protocol is essential. Vital signs (blood pressure, heart rate, respiratory rate, temperature) should be monitored every one to four hours depending on clinical severity. Haematocrit and platelet count should be checked every four to six hours during the critical phase. Urine output should be measured and charted – a minimum output of 0.5 ml/kg per hour indicates adequate perfusion.

The decision to discharge a patient should be based on meeting all of the following criteria: no fever for at least 48 hours without the use of antipyretics; improvement in clinical status with good appetite; adequate urine output; stable or rising platelet count above 50,000; stable haematocrit without ongoing intravenous fluid support; and at least 48 hours elapsed since defervescence.

Clinical Example: Dengue with Warning Signs – Management Approach

A 35-year-old male presents on day five of illness. Fever has just broken (current temperature 37.1 degrees Celsius). He complains of severe abdominal pain and has vomited four times in the past six hours. On examination, the liver is palpable 3 cm below the right costal margin. Haematocrit is 52% (his known baseline is 42%, representing a 24% rise). Platelet count is 35,000. No active bleeding is observed.

Classification: Dengue with Warning Signs (abdominal pain, persistent vomiting, liver enlargement, and significant haematocrit rise with rapid platelet drop). This patient requires hospital admission, intravenous fluid therapy, close monitoring of vitals and haematocrit, and assessment for progression to severe dengue. He should not be discharged until all discharge criteria are met.

Medications to Avoid in Dengue

Several commonly used medications are contraindicated or carry significant risk in dengue and must be avoided. Non-steroidal anti-inflammatory drugs (NSAIDs) such as ibuprofen, naproxen, and diclofenac inhibit platelet function and increase the risk of gastric bleeding, which can be catastrophic in a patient with dengue-associated thrombocytopenia. Aspirin shares these antiplatelet properties and should be similarly avoided.

Intramuscular injections should be avoided in dengue patients with thrombocytopenia due to the risk of intramuscular haematoma. Corticosteroids and intravenous immunoglobulin have been studied in dengue but are not recommended in routine management based on current evidence. Paracetamol (acetaminophen) at appropriate doses is the analgesic and antipyretic of choice in dengue, as it does not affect platelet function. High doses of paracetamol should also be avoided due to hepatotoxicity risk, particularly if dengue-related hepatitis is present.

Paediatric Dengue Considerations

Dengue in children shares the same fundamental pathophysiology as in adults but has several important clinical differences. Children may be unable to verbalise symptoms accurately, and non-specific signs such as refusal to feed, irritability, or lethargy may be the presenting features. Vital sign interpretation must use age-appropriate reference ranges – tachycardia and blood pressure norms differ substantially between infants, toddlers, school-age children, and adolescents.

Haematocrit reference ranges are also age-dependent, and the 20% rise criterion must be applied relative to the child’s appropriate baseline. Fluid calculations are based on body weight. The WHO recommends weight-based fluid resuscitation protocols specifically calibrated for paediatric patients. Clinicians should use paediatric dengue management protocols, particularly for young infants in whom dengue can be especially life-threatening.

Key Point: When to Seek Emergency Care Immediately

The following features indicate a medical emergency requiring immediate hospital attendance: severe abdominal pain that is constant or worsening; repeated vomiting (three or more times in the past hour); bleeding from the nose, gums, or in vomit or stool; drowsiness, confusion, or difficulty waking; pale, cold, or clammy skin; rapid breathing; or fainting. These are not symptoms to manage at home while waiting for a scheduled clinic appointment.

Role of This Calculator in Clinical Practice

This dengue severity calculator is designed as a structured clinical decision support tool that guides healthcare workers through the systematic assessment of dengue severity according to the WHO 2009 classification. By prompting evaluation of each diagnostic criterion – including the presence of warning signs and severe dengue features – it reduces the risk of overlooking critical findings in a busy clinical environment.

The calculator is intended to support, not replace, clinical judgement. Dengue is a dynamic illness that evolves over days, and a single assessment reflects the clinical state at one point in time. Repeat assessment is essential as the illness progresses, particularly around defervescence. All clinical findings must be interpreted in the context of the individual patient, local epidemiology, available laboratory results, and the clinical experience of the treating team.

Frequently Asked Questions

What is the WHO 2009 dengue classification and why was it introduced?

The WHO 2009 revised dengue classification replaced the older 1997 system that used the categories of dengue fever, dengue haemorrhagic fever (grades I to IV), and dengue shock syndrome. The 2009 system was introduced because field experience showed that the older classification was difficult to apply consistently, did not adequately guide triage decisions, and failed to identify patients at risk of deterioration before they became severely ill. The new system classifies dengue into three pragmatic categories – dengue, dengue with warning signs, and severe dengue – based on clinical and laboratory findings that are assessable at the bedside and that directly guide management decisions, particularly the critical question of whether a patient requires hospitalisation.

What are the seven dengue warning signs and why are they important?

The seven WHO dengue warning signs are: abdominal pain or tenderness; persistent vomiting; clinical fluid accumulation (ascites, pleural effusion, or pericardial effusion); mucosal bleeding (bleeding from the gums, nose, or in the eyes); lethargy or restlessness; liver enlargement greater than 2 cm; and a rising haematocrit with a rapid decline in platelet count. These signs are important because they identify patients at high risk of progressing to severe dengue. They typically appear around the time of defervescence, the period when plasma leakage is most active. Any patient with one or more warning signs requires hospital admission and close monitoring, as they may deteriorate rapidly without appropriate fluid management and supportive care.

How is dengue shock syndrome diagnosed and what makes it different from other types of shock?

Dengue shock syndrome (DSS) is diagnosed when a patient with dengue develops signs of circulatory failure due to plasma leakage. The key haemodynamic markers are a narrowed pulse pressure below 20 mmHg (calculated as systolic minus diastolic blood pressure) or frank hypotension (blood pressure below age-appropriate normal values). Unlike septic shock, which is primarily distributive with vasodilation, DSS involves loss of intravascular fluid into body cavities due to increased vascular permeability. This is reflected in rising haematocrit (haemoconcentration) even as blood pressure falls. The fluid lost is plasma, not red cells, so the haematocrit rises proportionally. Identifying a narrowing pulse pressure before frank hypotension develops is critical, as it indicates compensated shock that can still be reversed with appropriate fluid therapy.

What does a positive tourniquet test mean in dengue?

The tourniquet test (Rumpel-Leede test) assesses capillary fragility. A blood pressure cuff is inflated to a point midway between the systolic and diastolic pressure and maintained for five minutes. A positive result is defined as 10 or more petechiae (tiny red dots caused by small haemorrhages) per square inch on the forearm. In dengue, the test is positive because the virus causes capillary fragility. A positive tourniquet test supports the clinical diagnosis of dengue and is one of the diagnostic criteria in the WHO 2009 classification. However, the test has variable sensitivity (40 to 90% across studies) and is not diagnostic alone. It should be interpreted alongside the full clinical picture, and dengue laboratory tests should still be performed for confirmation.

Why should NSAIDs and aspirin be avoided in dengue?

Non-steroidal anti-inflammatory drugs (NSAIDs) such as ibuprofen, naproxen, and diclofenac, and aspirin (acetylsalicylic acid), should be strictly avoided in dengue for two main reasons. First, these medications inhibit platelet function through cyclooxygenase enzyme inhibition, further impairing a platelet-clotting system already compromised by dengue-associated thrombocytopenia. This substantially increases the risk of clinically significant bleeding. Second, NSAIDs irritate the gastric mucosa and increase the risk of gastrointestinal bleeding, which can be life-threatening in dengue. Paracetamol (acetaminophen) at appropriate doses is the recommended analgesic and antipyretic for dengue. Even paracetamol should not be taken in high doses, given that dengue can cause hepatitis, and paracetamol is hepatotoxic in overdose or in the context of liver disease.

How is haematocrit used to monitor dengue severity?

Haematocrit (also called packed cell volume or PCV) is the percentage of blood volume occupied by red blood cells. In dengue, plasma leakage causes the liquid component of blood to escape into body cavities, concentrating the red cells and causing the haematocrit to rise. A rise of 20% or more above the patient’s baseline haematocrit indicates significant plasma leakage and is a warning sign for severe dengue. Serial haematocrit measurements every four to six hours during the critical phase allow clinicians to track plasma leakage in real time and adjust intravenous fluid rates accordingly. Conversely, a falling haematocrit in the context of haemodynamic deterioration may indicate significant internal bleeding rather than plasma leakage, which changes the management approach.

At what platelet count does a dengue patient need a platelet transfusion?

Platelet transfusion in dengue is generally not recommended based on platelet count alone. The decision to transfuse platelets should be based on the presence of active clinically significant bleeding, not on a specific platelet number. Many dengue patients recover without any transfusion even with platelet counts below 10,000 per microlitre. Prophylactic platelet transfusion (given to prevent bleeding in the absence of current active bleeding) has not been shown to improve outcomes in dengue and may actually be harmful in some studies. The WHO guidelines recommend considering platelet transfusion only when platelet counts fall below 10,000 to 20,000 with severe or uncontrolled bleeding, and stress that clinical assessment of bleeding must guide this decision. Unnecessary transfusion risks volume overload and other transfusion-related complications.

Which dengue diagnostic test should be ordered and when?

The choice of dengue diagnostic test depends on the duration of illness. During the first one to five days of fever (early febrile phase), the dengue NS1 antigen test and reverse transcription polymerase chain reaction (RT-PCR) have the highest sensitivity because viral load is highest at this stage. After day five, viral load falls and the immune response matures, making dengue IgM serology the more sensitive test – IgM typically becomes detectable from day four to five and peaks at around two weeks. In secondary dengue infections, IgG may rise rapidly and be detectable earlier. A negative NS1 or RT-PCR result early in illness does not exclude dengue – repeat testing or IgM serology after day five should be performed if clinical suspicion remains high. Full blood count (for leukopenia, thrombocytopenia, and haematocrit) is essential at every clinical visit regardless of which serological test is ordered.

What are the discharge criteria for dengue patients admitted to hospital?

The WHO 2009 guidelines define specific criteria that should all be met before a dengue patient is discharged from hospital. These are: absence of fever for at least 48 hours without the use of antipyretics; improvement in clinical status with good appetite and general wellbeing; adequate urine output (approximately 0.5 ml/kg per hour); stable or improving platelet count above 50,000 per microlitre; stable haematocrit without ongoing intravenous fluid support; and no respiratory distress, no overt bleeding, and no other concerning clinical features. The 48-hour fever-free period is important because it generally indicates that the patient has passed through the critical phase of plasma leakage and is now in the recovery phase. Premature discharge during the critical phase, even in patients who appear well, risks missing rapid deterioration.

Can dengue be managed at home and what home care instructions should patients receive?

Dengue patients classified as dengue without warning signs, who are clinically stable, able to tolerate oral fluids, and have access to prompt follow-up, may be managed at home with appropriate instructions. Home management involves oral rehydration with water, oral rehydration salts, coconut water, or diluted fruit juices; paracetamol (not NSAIDs or aspirin) for fever and pain; adequate rest; and daily clinical review at a healthcare facility to monitor vital signs, blood counts, and the appearance of warning signs. Patients and caregivers must be clearly educated about the seven warning signs and instructed to seek immediate emergency care if any warning sign develops, without waiting for the next scheduled appointment. Written instructions in a language the patient understands are recommended.

How does secondary dengue infection increase the risk of severe disease?

There are four dengue serotypes (DENV-1 through DENV-4), and infection with one serotype provides long-term immunity against that serotype but only short-term cross-protective immunity against the others. During a secondary infection with a different serotype, pre-existing cross-reactive antibodies from the first infection bind to the new serotype but are unable to neutralise it effectively. Instead, these antibodies facilitate viral entry into immune cells (monocytes and macrophages) through Fc receptors, a process called antibody-dependent enhancement (ADE). This dramatically amplifies viral replication and the subsequent immune response, including the release of cytokines that increase vascular permeability – the mechanism underlying plasma leakage and dengue shock syndrome. ADE is the leading hypothesis for why severe dengue is more common in secondary infections, though it is not the only factor involved.

What is the risk of dengue during pregnancy?

Dengue during pregnancy poses risks to both the mother and the foetus. Maternal risks include increased bleeding risk (dengue-associated thrombocytopenia combined with the haemostatic challenges of obstetric haemorrhage), dengue shock syndrome, and premature labour. Foetal and neonatal risks include intrauterine foetal demise, low birth weight, and vertical transmission of dengue from mother to newborn around the time of delivery, causing neonatal dengue. The physiological anaemia and expanded plasma volume of pregnancy complicate haematocrit interpretation, and normal pregnancy haematocrit values (which are lower than non-pregnant values) must be used as the baseline for calculating percentage rise. Pregnant women with dengue require close monitoring and should be managed in a facility with obstetric and neonatal support.

What is the difference between dengue encephalopathy and dengue encephalitis?

Dengue encephalopathy refers to neurological dysfunction (impaired consciousness, confusion, seizures) occurring in the context of dengue, caused by indirect mechanisms rather than direct viral invasion of the brain. These indirect mechanisms include metabolic derangements (hyponatraemia, hypoglycaemia, hepatic encephalopathy from dengue hepatitis), cerebral oedema from profound hyponatraemia, or ischaemic brain injury from prolonged dengue shock syndrome. Dengue encephalitis refers to direct viral invasion and inflammation of the brain parenchyma, which is less common but has been documented by isolating dengue virus from cerebrospinal fluid (CSF) and brain tissue. Distinguishing between the two has therapeutic implications, as encephalopathy management focuses on correcting the underlying metabolic derangement, while encephalitis management is primarily supportive. Both are classified as severe dengue under the WHO 2009 system.

How should fluid management differ between dengue with warning signs and dengue shock syndrome?

The approach to fluid management differs significantly between dengue with warning signs and dengue shock syndrome (DSS). In dengue with warning signs without shock, isotonic crystalloid fluid (normal saline or Ringer’s lactate) is given at maintenance to mildly supra-maintenance rates, guided by clinical response and haematocrit trends, aiming to prevent the development of shock while avoiding fluid overload. In dengue shock syndrome, urgent fluid resuscitation is required: an isotonic crystalloid bolus of 10 ml/kg is given over 15 to 30 minutes with immediate reassessment of vital signs and haematocrit. Boluses are repeated or rate increased based on response. This approach is more conservative than the fluid resuscitation used in septic shock (where 20 to 30 ml/kg boluses are standard), reflecting the risk of fluid overload during the subsequent recovery phase when leaked plasma is reabsorbed.

What are the signs that a dengue patient is entering the recovery phase?

Several clinical and laboratory signs indicate that a dengue patient is transitioning from the critical phase to the recovery phase. These include: return of appetite and improved general wellbeing; resolution of fever (usually on its own without antipyretics in recovery); passing of the convalescent rash, which is characteristically a generalised erythematous rash with scattered islands of white skin; normalising or rising platelet count; and a falling haematocrit as reabsorbed plasma dilutes the blood. An important warning: if intravenous fluids are continued at the same rate during recovery, the combination of ongoing IV infusion and plasma reabsorption can cause fluid overload, pulmonary oedema, and respiratory distress. IV fluids should be reduced or discontinued once the patient is eating and drinking adequately and clinical parameters confirm entry into the recovery phase.

Is dengue a notifiable disease and what are the reporting obligations?

Dengue is a notifiable disease in most endemic countries, meaning healthcare providers are legally required to report confirmed and suspected cases to the relevant public health authority within a specified timeframe. Reporting requirements vary by country: some require reporting within 24 hours, others within a week, and reporting categories (suspected versus confirmed cases) also vary. Public health reporting enables national health authorities to track outbreak patterns, identify clusters for vector control response, and monitor dengue trends over time. Clinicians working in dengue-endemic regions or managing returned travellers should be familiar with the reporting requirements of their jurisdiction. Internationally, dengue reporting contributes to global surveillance data compiled by the WHO and regional organisations.

Can a person get dengue more than once?

Yes, a person can be infected with dengue up to four times during their lifetime, once with each of the four dengue serotypes (DENV-1, DENV-2, DENV-3, and DENV-4). Infection with one serotype provides lasting protective immunity against that same serotype but only temporary cross-protective immunity against the other three. After the short period of cross-protection passes (typically two to three months), the individual remains susceptible to the remaining serotypes. Secondary infection with a different serotype carries a higher risk of severe dengue due to antibody-dependent enhancement. Tertiary and quaternary infections are possible and have been documented, though they are less commonly associated with severe disease. In highly endemic regions, it is not unusual for adults to have experienced multiple dengue infections across their lifetime.

What does abdominal tenderness or pain indicate in dengue?

Abdominal pain or tenderness is one of the seven WHO dengue warning signs and may reflect several pathological processes occurring in severe dengue. Hepatic pain (right upper quadrant tenderness or epigastric discomfort) commonly results from dengue-associated hepatomegaly and hepatitis, as the liver is frequently affected in dengue. Ascites (fluid accumulation in the abdominal cavity due to plasma leakage) can cause abdominal distension and discomfort. In some patients, severe plasma leakage into the retroperitoneal space or early haemorrhage can present as abdominal pain before other warning signs are apparent. Any patient with dengue who develops new or worsening abdominal pain should be assessed promptly – the combination of abdominal pain with rising haematocrit and falling platelets in a febrile patient is a high-risk clinical pattern requiring hospitalisation.

How is the dengue severity calculator different from a clinical scoring system?

This dengue severity calculator is a structured assessment tool rather than a numerical scoring system. Unlike clinical scoring systems that assign points to individual features and sum them to produce a total score, this calculator guides clinicians through the systematic assessment of each WHO 2009 diagnostic criterion and synthesises the findings into the appropriate severity classification: dengue without warning signs, dengue with warning signs, or severe dengue. Each classification carries specific management implications (home care, hospital admission with monitoring, or emergency treatment). The calculator does not replace clinical judgement – it structures the assessment process to reduce the risk of overlooking critical warning signs or severe features, particularly in high-volume clinical settings where time pressure may otherwise lead to incomplete assessment. All findings must be interpreted by a qualified healthcare professional in the context of the complete clinical picture.

What is the typical duration of dengue illness and when does the risk of severe disease pass?

The total duration of dengue illness from onset of fever to full recovery is typically seven to ten days, though individual variation exists. The febrile phase lasts two to seven days. The critical phase of plasma leakage typically spans 24 to 48 hours around the time of defervescence, usually between days three and seven. Once the patient has remained afebrile for 48 hours and clinical and laboratory parameters confirm entry into the recovery phase, the risk of severe dengue complications related to plasma leakage has largely passed. The recovery phase lasts two to five days, during which appetite returns, platelet count rises, and haematocrit normalises. Total weakness and fatigue may persist for several weeks after the acute illness. Post-dengue fatigue syndrome, characterised by prolonged tiredness, difficulty concentrating, and mood disturbances, is recognised in a proportion of patients after recovery from dengue.

What monitoring should be performed in a patient with dengue being observed at home?

Dengue patients managed at home require structured daily monitoring at a healthcare facility to check for the development of warning signs. At each review, the clinician should assess: temperature and general clinical status; signs of dehydration and adequacy of oral intake; presence of any of the seven WHO warning signs (abdominal pain, persistent vomiting, mucosal bleeding, lethargy or restlessness, fluid accumulation, liver enlargement); and a full blood count (haematocrit and platelet count). Home monitoring by the patient or caregiver should include temperature twice daily, fluid intake and urine output, and immediate recognition of warning signs requiring emergency attendance. Patients should be given clear written instructions about the warning signs and how to access emergency care, with a specific instruction not to wait for the next scheduled appointment if warning signs develop.

Are there any specific dietary recommendations during dengue recovery?

There are no specific evidence-based dietary restrictions in dengue, but general nutritional principles apply. Adequate hydration is the most important nutritional consideration – patients should drink plenty of fluids including water, oral rehydration salts, coconut water, and diluted juices. Meals should be light and easily digestible, particularly during the febrile and critical phases when nausea and vomiting are common. Papaya leaf extract has been widely promoted in some regions as a remedy for dengue-associated thrombocytopenia and to accelerate platelet recovery. While some small studies have shown a modest effect on platelet count, evidence is insufficient to support recommending papaya leaf extract as a standard treatment, and it should not delay conventional medical evaluation and treatment. Foods high in iron and folate may support haematopoietic recovery after the acute illness. Return to a normal diet as appetite improves during the recovery phase is appropriate.

How is dengue distinguished from malaria in clinical practice?

Dengue and malaria can present with similar features: high fever, headache, myalgia, thrombocytopenia, and hepatomegaly. However, several clinical features help distinguish them. Dengue more commonly presents with retro-orbital pain, a characteristic skin rash, and a positive tourniquet test. Malaria more commonly presents with cyclical fever patterns (though this is inconsistent in practice), is associated with splenomegaly (which is less prominent in acute dengue), and carries a higher risk of anaemia due to haemolysis of red blood cells. Both can cause severe disease. In clinical practice, when a patient from or returning to a malaria-endemic area presents with febrile illness and thrombocytopenia, both dengue serology and malaria rapid diagnostic test (RDT) or thick and thin blood film should be performed simultaneously, as co-infection with both dengue and malaria has been documented and each condition requires its own specific management approach.

What role does the Aedes mosquito play in dengue transmission and how can exposure be reduced?

Dengue is transmitted to humans through the bite of an infected female Aedes mosquito, primarily Aedes aegypti and secondarily Aedes albopictus. These mosquitoes become infected when they bite a person with dengue during the viremic period (when the virus is circulating in the blood, typically the first five days of fever). The mosquito requires an incubation period of eight to twelve days before becoming infectious and can then transmit dengue to other humans through subsequent bites. Dengue is not transmitted directly from person to person. Aedes mosquitoes are day-biting mosquitoes, most active in the early morning and late afternoon. They breed in small accumulations of clear, stagnant water: flower pots, tyres, gutters, animal drinking containers, and construction materials. Reducing exposure involves eliminating standing water around the home, using DEET-based repellents during peak mosquito activity hours, wearing long-sleeved protective clothing, and using mosquito nets and screens.

What are the dengue vaccines currently available and who should receive them?

Two dengue vaccines have received regulatory approval as of 2025. Dengvaxia (CYD-TDV, Sanofi Pasteur) is a live attenuated tetravalent vaccine approved in several countries for individuals aged nine years and older who have laboratory-confirmed prior dengue infection. It is contraindicated in dengue-naive individuals because it may act as a first dengue infection and increase the risk of severe dengue upon subsequent natural infection. Pre-vaccination screening (serotesting to confirm prior dengue infection) is therefore recommended. Qdenga (TAK-003, Takeda) is a live attenuated tetravalent vaccine that has received regulatory approval in the European Union, Indonesia, Brazil, Argentina, and several other countries. Clinical trials show it reduces dengue hospitalisation by approximately 84% and is effective regardless of prior serostatus in the age groups studied (four years and above), though post-licensure safety data continues to be collected. Vaccination recommendations vary by country and are subject to ongoing review by national immunisation advisory committees.

Conclusion

Dengue fever remains a significant global public health challenge, with its clinical management depending critically on accurate and timely severity assessment. The WHO 2009 classification system provides a clear, clinically actionable framework – categorising patients as dengue without warning signs, dengue with warning signs, or severe dengue – that directly guides treatment decisions from home management to emergency hospital care.

The key principles of dengue management are recognising the warning signs that predict progression to severe disease, understanding the pathophysiology of plasma leakage and its haemodynamic consequences, providing appropriate fluid therapy guided by clinical response and haematocrit trends, and avoiding medications that increase bleeding risk. This dengue severity calculator supports clinicians in applying these principles systematically, reducing the risk of missed or delayed diagnosis in a time-critical illness.

Dengue is a preventable disease, and personal protective measures against Aedes mosquito exposure remain the primary prevention strategy in the absence of universal vaccine availability. For any patient with suspected dengue, early clinical assessment, appropriate laboratory investigation, and clear education about warning signs – with immediate access to emergency care if they develop – are the cornerstones of safe management.

Important Medical Disclaimer

This calculator is provided for informational and educational purposes only. It is not intended to replace professional medical advice, diagnosis, or treatment. Always consult with a qualified healthcare professional before making any medical decisions. The results from this calculator should be used as a reference guide only and not as the sole basis for clinical decisions. Dengue is a dynamic illness – severity can change rapidly, and continuous clinical monitoring by trained healthcare professionals is essential.