Pediatric sepsis

Last updated: April 23, 2026

Summary

Pediatric sepsis is an acute, life-threatening condition in which infection leads to organ dysfunction. Without prompt intervention, affected children frequently progress to septic shock and multiple organ failure. The precipitating infection is most commonly bacterial. Clinical features are often nonspecific and include fever, tachycardia, signs of organ dysfunction (e.g., reduced GCS, jaundice), and signs of shock. Diagnosis occurs alongside management and involves blood cultures, lactate, assessment for markers of infection and end-organ dysfunction, and investigation of the underlying etiology. Initial stabilization focuses on the delivery of the hour-1 bundle for children, which combines definitive treatment (empiric antibiotic therapy) and resuscitation (intravenous fluids, vasoactive medications). Ongoing management includes nutritional support, tailored antibiotic therapy, and regular reassessment. Prevention of sepsis involves infection control measures and early recognition and management of severe infections.

For neonates, see "Neonatal bacterial infections."

Definitions

Sepsis in children: suspected infection and signs of organ dysfunction (e.g., renal impairment, hypoxia, altered mental state) ^[1]^[2]
Septic shock in children: sepsis with evidence of cardiovascular dysfunction (e.g., hypotension, need for vasoactive medications, significantly elevated lactate) ^[1]^[2]

Epidemiology

Worldwide, half of sepsis cases occur in children ≤ 18 years of age. ^[3]
- ∼ 25 million cases (> 80% in children < 5 years of age)
- ∼ 3 million deaths
Estimated prevalence in the US ^[4]
- 2.25 per 1000 in those aged 1–12 months
- 0.23–0.52 per 1000 in those aged between 1 and 19 years of age

Epidemiological data refers to the US, unless otherwise specified.

Etiology

Common sources of sepsis in children ^[5]^[6]

Common pathogens ^[5]

Risk factors for sepsis in children ^[7]

Age < 12 months ^[4]
Immunosuppression
Indwelling devices (e.g., central venous catheter)
Serious comorbidities (e.g., congenital heart disease, neurological disease)

Clinical features

In addition to features of the underlying primary infection (e.g., clinical features of pneumonia in children), the following nonspecific symptoms may be present. ^[1]^[8]

Fever or below normal temperature
Tachycardia
Tachypnea
Clinical features of organ dysfunction, e.g.: ^[1]
- Reduced GCS
- Hypoxia
- Jaundice
Features of septic shock, e.g.: ^[2]^[9]
- Hypotension, low MAP
- Signs of poor peripheral perfusion
- Decreased urine output
Additional features in infants ^[1]^[8]
- Poor tone
- Irritability
- Poor feeding

Management

Approach ^[1]^[10]

Consult urgently with specialists (e.g., infectious disease, critical care); PICU admission may be required.
Start continuous monitoring (e.g., cardiac monitoring, pulse oximetry, urine output).
Provide initial stabilization with:
- The hour-1 bundle for sepsis in children, which includes:
- Respiratory support in children as needed
Perform additional diagnostic studies to:
- Confirm the diagnosis.
- Assess for end-organ dysfunction.
- Determine the underlying cause.
Regularly reassess patients for deterioration and provide further management as needed.

Initial stabilization

Hour-1 bundle for children with sepsis ^[1]^[11]

As part of initial studies for sepsis in children:
- Obtain serum lactate.
- Draw blood cultures (ideally prior to antibiotic administration).
Begin empiric broad-spectrum antibiotics.
Begin fluid resuscitation in children with sepsis.
Septic shock and/or persistent hypotension: Start vasopressors.

Administer antibiotics as soon as possible: within 1 hour in children with septic shock and within 3 hours in children without septic shock. ^[10]

Antibiotics and infection management ^[10]

Unclear source of infection: Give empiric antibiotic therapy; follow local hospital protocols when available.
If a specific source is suspected, tailor antibiotic therapy, e.g.:
- Empiric antibiotics for pediatric UTI
- Empiric antibiotic therapy for pediatric CAP
Antiviral or antifungal therapy may be required (e.g., in patients with immunocompromise or atypical features).
Source control for sepsis (e.g., removal of infected intravascular device) may also be required. ^[10]

Empiric antibiotics for sepsis in children (unknown source) ^[12]^[13]
Patient characteristics	Commonly used regimens
Community-acquired sepsis in previously healthy children	Ceftriaxone (off-label) ^[12]^[13] PLUS vancomycin if in an area of high prevalence (e.g., > 10%) for MRSA or ceftriaxone resistance ^[12]^[13] PLUS aminoglycoside (e.g., gentamicin ) if in an area of high prevalence for ceftriaxone resistance in gram-negative pathogens ^[12]^[13]
Immunocompromised or hospital-acquired sepsis	Multidrug regimes are preferred. ^[10] Consider one of the following: ^[12] Third-generation or higher cephalosporin, e.g., cefepime (off-label) ^[13] OR extended-range penicillin/beta-lactamase inhibitor combination, e.g., piperacillin/tazobactam (off-label) ^[13] PLUS one or both of the following: ^[12] Vancomycin ^[13] AND/OR an aminoglycoside, e.g., gentamicin ^[13]

Fluid resuscitation for children with sepsis ^[10]

Assess for signs of significant dehydration, shock, and organ dysfunction (see "Phoenix sepsis score").
If sepsis-related organ dysfunction or shock is present:
- Give isotonic crystalloid 10–20 mL/kg over 5–20 minutes; if ICU care is unavailable, administer only if hypotensive. ^[1]^[10]^[14]
- Reassess hemodynamic status (repeat after any subsequent fluid boluses). ^[1]^[10]
  - Assess for markers of cardiac output (e.g., heart rate, BP, capillary refill, urine output, serum lactate).
  - Assess for signs of fluid responsiveness (e.g., passive leg raise test).
  - Consider advanced monitoring. ^[10]
- If hypotensive and fluid responsive, repeat boluses as needed. ^[10]
  - ICU available: 40–60 mL/kg total in the first hour
  - No ICU available: 40 mL/kg total in the first hour

Discontinue IV fluids if signs and/or symptoms of fluid overload develop. ^[1]

Management of pediatric septic shock ^[1]^[10]

Vasopressors can be given before or after the initial fluid bolus. ^[10]
First-line: epinephrine or norepinephrine via peripheral or central line
The optimum MAP is unclear. ^[10]
If central venous access is available, aim for central venous oxygen saturation ≥ 70%. ^[10]
Refractory shock ^[10]
- Add adjuvant vasopressin.
- Consider intubation and mechanical ventilation in children. ^[10]
If still unresponsive, consider extracorporeal membrane oxygenation (ECMO). ^[10]

While hydrocortisone is not recommended for routine management of septic shock, it is indicated for suspected adrenal insufficiency. ^[10]

Respiratory support ^[10]

Start respiratory support (e.g., oxygen therapy for children) to maintain saturations between 92 and 98% (88–92% for children who are intubated). ^[1]^[10]
If acute respiratory distress syndrome (ARDS) is suspected, consider in consultation with a specialist: ^[15]
- BiPAP
- Inhaled nitric oxide
Invasive mechanical ventilation in children may be required; for refractory hypoxia, consider ECMO.

Diagnostics for sepsis

Initial studies for sepsis in children ^[1]^[10]

As part of the hour-1 bundle for children, obtain:
- Blood cultures
- Lactate
Assess for markers of infection.
- CBC with differential: may show leukopenia, leukocytosis, thrombocytopenia
- Inflammatory markers (e.g., CRP, procalcitonin): typically raised
Assess for markers of end-organ dysfunction.
- Comprehensive metabolic panel: may show renal or hepatic dysfunction (e.g., raised creatinine, deranged liver studies)
- Coagulation panel: may show increased PT, PTT, and INR ^[9]
- Blood gas analysis: may show metabolic acidosis or hypoxia

Obtain blood cultures before administering antibiotics, unless doing so delays treatment. ^[10]

Further diagnostics to identify the source of infection ^[8]

Obtain additional studies (e.g., microbiology, imaging) based on the suspected source of sepsis in children, e.g.:

Chest x-ray as part of diagnostics for pediatric CAP
Urine dipstick and culture as part of diagnostics for UTI in children
CSF analysis as part of diagnostics for meningitis in children

Bilateral hyperinflation and right lung consolidation Pyuria and bacteriuria on microscopy

Phoenix sepsis score

The Phoenix sepsis score is a pediatric organ dysfunction scoring system developed in 2024 by the Society of Critical Care Medicine. ^[2]
Points are based on dysfunction of the respiratory, cardiovascular, coagulation, and neurological systems. ^[2]

‎Phoenix sepsis score for pediatric sepsis ^[2]
‎Criteria	Points
Respiratory (0–3 points)	0 point: either of the following PaO₂: FiO₂ ratio ≥ 400 SpO₂≥ 98% on room air OR SpO₂: FiO₂ ratio ≥ 292 1 point: either of the following on any respiratory support PaO₂: FiO₂ ratio < 400 SpO₂: FiO₂ < 292 2 points: either of the following on invasive mechanical ventilation (IMV) PaO₂: FiO₂ ratio 100–200 SpO₂: FiO₂ ratio 148–220 3 points: either of the following on IMV PaO₂: FiO₂ ratio < 100 SpO₂: FiO₂ ratio < 148
Cardiovascular (0–6 points)	Vasoactive medications 0 points: no medication 1 point: one medication 2 points: two or more medications Lactate 0 points: < 5 mmol/L 1 point: 5–10.9 mmol/L 2 points: ≥ 11 mmol/L MAP by age-specific thresholds 0: normal 1: decreased 2: significantly decreased
Coagulation (0–2 points)	0 points: Platelets ≥ 100,000/mm³ INR ≤ 1.3 D-dimer ≤ 2 mg/L Fibrinogen ≥ 100 mg/dL 1 point each (max. 2 points): Platelets < 100 × 10³/µL INR > 1.3 D-dimer > 2 mg/L Fibrinogen < 100 mg/dL
Neurological (0–2 points)	0: GCS > 10, pupils reactive 1: GCS ≤ 10 2: Fixed pupils bilaterally
Sepsis: suspected infection and Phoenix sepsis score ≥ 2 points Septic shock: sepsis with ≥ 1 cardiovascular point

The criteria for SIRS and severe sepsis are not used in children. ^[9]

Further management

Regularly reassess patients for signs of deterioration.
Provide electrolyte repletion as needed. ^[10]
Consider in consultation with a specialist: ^[10]
- Blood transfusion for severe anemia
- Renal replacement therapy for children with refractory fluid overload
- Immune stimulants in select cases (e.g., children with concurrent cancer)
Consider supportive care for pediatric fever if the child is uncomfortable. ^[10]
If blood cultures are positive for a pathogen: ^[10]
- Discuss with infectious disease or medical microbiology.
- Tailor antibiotics to sensitivities.
Start an early rehabilitation bundle. ^[10]
Following resolution of sepsis ^[10]
- Educate patients and caregivers on potential long-term complications of pediatric sepsis.
- Assess for complications of pediatric sepsis both before and at regular intervals after discharge.

Nutritional supplements (e.g., thiamine, ascorbic acid, vitamin D) are not recommended in children with sepsis unless treating deficiency. ^[10]

Differential diagnoses

See "Differential diagnoses of sepsis" and "Causes of pediatric fever."
In shock, consider: ^[8]
In multiorgan involvement, consider:
- Macrophage activation syndrome ^[16]
- Hemolytic uremic syndrome ^[16]
- Multisystem inflammatory syndrome in children ^[17]
In neonates, consider: ^[8]
- Congenital heart disease
- Inborn errors of metabolism

The differential diagnoses listed here are not exhaustive.

Complications

Severe complicatiosn of sepsis include: ^[1]^[10]
- Shock
- Pediatric ARDS
- DIC
- Death
Sequelae are seen in up to a third of survivors, including: ^[1]^[10]
- Impaired baseline functional ability (e.g., sustained disability)
- Recurrent severe infections

We list the most important complications. The selection is not exhaustive.

Prevention

Primary prevention

Prevention of infection, e.g.: ^[18]
- Routine immunizations
- Antibiotic prophylaxis (e.g., in patients with asplenia)
- Prevention of health care-associated infections (e.g., via hand hygiene, respiratory hygiene, aseptic technique)
- Population-level interventions (e.g., safe drinking water, access to health care) ^[19]
Once infections develop, early identification and treatment can prevent sepsis. ^[20]

Screening for sepsis in children

The role of screening for sepsis in acutely unwell children is unclear. ^[10]
If performed, no specific screening tool is recommended; follow local protocols. ^[10]^[21]

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