Birth Asphyxia

Birth asphyxia (also called perinatal asphyxia) occurs when a baby doesn't receive enough oxygen before, during, or just after birth, leading to hypoxia and hypercapnia. It is a major cause of neonatal morbidity and mortality worldwide.

Overview

Birth asphyxia results in hypoxic-ischaemic injury to multiple organs, with the brain being particularly vulnerable. The severity depends on:
  • Duration and severity of hypoxia
  • Gestational age of the infant
  • Timing of the insult (antepartum, intrapartum, or postnatal)
Incidence:
  • Affects 1-6 per 1,000 live births in developed countries
  • Higher rates (5-26 per 1,000) in developing countries
  • Major contributor to neonatal mortality (23% of neonatal deaths globally)

Aetiology

Birth asphyxia can result from factors affecting oxygen delivery at any point from mother to fetus.
Antepartum causes:
  • Maternal hypoxemia (severe anaemia, respiratory disease, carbon monoxide poisoning)
  • Placental insufficiency (pre-eclampsia, placental abruption, chronic hypertension)
  • Maternal drug use (opioids, anaesthetics)
  • Intrauterine growth restriction (IUGR)
  • Post-term pregnancy
  • Multiple gestation
Intrapartum causes:
  • Prolapsed cord causing compression during birth
  • Nuchal cord (cord wrapped around neck)
  • Cord compression (short cord, true knot)
  • Placental abruption
  • Uterine rupture
  • Prolonged or obstructed labour
  • Shoulder dystocia
  • Maternal shock or intrapartum haemorrhage
  • Uterine hyperstimulation
  • Maternal hypotension (from epidural, haemorrhage)
Postnatal causes:
  • Severe respiratory distress
  • Congenital heart disease with inadequate pulmonary blood flow
  • Persistent pulmonary hypertension of the newborn (PPHN)
  • Severe anaemia or shock
Fetal factors:
  • Prematurity
  • Congenital anomalies
  • Infection (sepsis, pneumonia)
  • Hydrops fetalis

Pathophysiology

Acute phase (minutes to hours):
  1. Initial hypoxia → Redistribution of blood flow to vital organs (brain, heart, adrenals)
  1. Persistent hypoxia → Cellular energy failure (depletion of ATP)
  1. Anaerobic metabolism → Lactic acidosis
  1. Cellular dysfunction → Loss of membrane integrity, cytotoxic oedema
  1. Multi-organ dysfunction
Reperfusion injury (hours to days):
  • Restoration of blood flow paradoxically worsens injury
  • Free radical formation
  • Inflammatory cascade activation
  • Excitotoxicity (excess glutamate)
  • Apoptosis and necrosis
  • Secondary energy failure peaks at 6-15 hours after insult
Chronic phase (days to months):
  • Ongoing cell death
  • Glial scarring
  • Permanent neurological damage

Clinical Features

Immediate signs (delivery room):
  • Failure to initiate or maintain regular breathing
  • Poor muscle tone (floppy, hypotonic)
  • Bradycardia (heart rate <100 bpm)
  • Absent or weak reflexes
  • Pallor or cyanosis
  • Poor Apgar scores:
    • 0-3 at 1 minute
    • <7 at 5 minutes
    • Persistent low scores at 10, 15, 20 minutes
  • Need for active resuscitation (PPV, chest compressions, drugs)
Metabolic abnormalities:
  • Metabolic acidosis: pH <7.0, base deficit ≥12 mmol/L (in umbilical cord blood or early neonatal sample)
  • Hypoglycaemia or hyperglycaemia
  • Hypocalcaemia
  • Hyponatraemia (SIADH)
 
Multi-organ involvement:
Central nervous system (most important):
  • Altered consciousness (lethargy, coma)
  • Hypotonia or hypertonia
  • Seizures (often within first 24 hours)
  • Poor feeding, weak suck
  • Abnormal reflexes
  • Hypoxic-Ischaemic Encephalopathy (HIE) - see below
Cardiovascular:
  • Hypotension
  • Poor perfusion
  • Myocardial dysfunction
  • Tricuspid regurgitation
  • Arrhythmias
Respiratory:
  • Persistent pulmonary hypertension (PPHN)
  • Respiratory distress
  • Pulmonary haemorrhage
Renal:
  • Acute kidney injury
  • Oliguria or anuria
  • Haematuria
Gastrointestinal:
  • Feeding intolerance
  • Necrotising enterocolitis (NEC)
  • Hepatic dysfunction (elevated transaminases, coagulopathy)
Haematological:
  • Thrombocytopenia
  • Disseminated intravascular coagulation (DIC)

Hypoxic-Ischaemic Encephalopathy (HIE)

HIE is the clinical syndrome of abnormal neurological function in the first days of life in term or near-term infants, resulting from birth asphyxia.
Diagnostic criteria for HIE (all must be present):
  1. Evidence of metabolic acidosis (pH <7.0, base deficit ≥12) in cord or early sample
  1. Apgar score 0-3 for >5 minutes OR need for resuscitation at 10 minutes
  1. Clinical evidence of encephalopathy (altered consciousness, abnormal tone, seizures)
  1. Multi-organ dysfunction consistent with asphyxia

Sarnat Staging of HIE

Feature
Stage 1 (Mild)
Stage 2 (Moderate)
Stage 3 (Severe)
Level of consciousness
Hyperalert, irritable
Lethargic
Stuporous, coma
Muscle tone
Normal or increased
Mild hypotonia
Flaccid
Posture
Normal
Flexion
Decerebrate
Tendon reflexes
Hyperactive
Hyperactive
Decreased or absent
Moro reflex
Strong
Weak or incomplete
Absent
Pupils
Dilated, reactive
Constricted, reactive
Variable, poor light reflex
Seizures
Absent
Common (often focal)
Uncommon or decerebrate
EEG
Normal
Low voltage, periodic discharges
Burst suppression, isoelectric
Duration
<24 hours
2-14 days
Days to weeks
Outcome
100% normal
80% normal or mild disability
20% severe disability or death
50% die
Survivors have severe disability

Investigations

Blood tests:
  • Cord blood gases (or arterial blood gas within 1 hour):
    • pH <7.0, base deficit ≥12 mmol/L supports diagnosis
  • Full blood count (thrombocytopenia, anaemia)
  • Renal function (elevated creatinine, urea)
  • Liver function tests (elevated ALT, AST)
  • Coagulation profile (DIC screen)
  • Blood glucose
  • Electrolytes (Na⁺, Ca²⁺, Mg²⁺)
  • Lactate
  • Blood culture (if sepsis suspected)
Neurological investigations:
  • EEG (Electroencephalography):
    • Continuous amplitude-integrated EEG (aEEG) for seizure detection
    • Background pattern correlates with severity and prognosis
    • Abnormal: low voltage, burst suppression, isoelectric
  • Cranial ultrasound:
    • Bedside screening
    • May show increased echogenicity, oedema, haemorrhage
    • Limited sensitivity for HIE
  • MRI brain (preferred neuroimaging):
    • Most sensitive for detecting hypoxic-ischaemic injury
    • Timing: Optimal at 2-8 days of age (after reperfusion injury develops)
    • Patterns:
      • Watershed injury (parasagittal cortex)
      • Basal ganglia and thalamus injury
      • Diffuse cortical injury
    • Diffusion-weighted imaging (DWI): Shows restricted diffusion in acute injury
    • Prognostic value: Helps predict long-term outcome
Other investigations:
  • Chest X-ray (if respiratory distress)
  • Echocardiography (if cardiac dysfunction or PPHN)
  • Urine output monitoring

Management

Immediate resuscitation (delivery room):
  • Follow neonatal resuscitation protocol
  • Ensure effective ventilation (most critical)
  • Chest compressions if HR <60 despite ventilation
  • Medications as needed (adrenaline, volume)
  • Umbilical cord blood gas sampling
Supportive care (NICU):
Respiratory:
  • Oxygen therapy targeting SpO₂ 90-95%
  • Avoid hyperoxia (may worsen injury) and hypoxia
  • Mechanical ventilation if needed (target normal PCO₂ 35-45 mmHg)
  • Avoid hypocapnia (causes vasoconstriction) and hypercapnia
Cardiovascular:
  • Maintain adequate blood pressure (MAP >35-40 mmHg in term)
  • Inotropic support if needed (dopamine, dobutamine)
  • Fluid management (restrict to 40-60 mL/kg/day initially to reduce cerebral oedema)
Metabolic:
  • Maintain normoglycaemia (2.6-6 mmol/L)
  • Correct electrolyte abnormalities
  • Treat metabolic acidosis (optimize ventilation and perfusion)
Neurological:
  • Seizure management:
    • Phenobarbital (first-line): Loading 20 mg/kg IV, may repeat 10 mg/kg doses
    • Phenytoin/fosphenytoin (second-line): 20 mg/kg IV
    • Midazolam, levetiracetam (third-line)
    • Continuous EEG monitoring recommended
Renal:
  • Monitor urine output, fluid balance
  • Adjust fluid and medication doses for renal impairment
Haematological:
  • Correct coagulopathy (vitamin K, FFP, platelets if needed)
Nutritional:
  • Enteral feeding cautious due to NEC risk
  • May need parenteral nutrition initially

Therapeutic Hypothermia (Neuroprotection)

The most important specific intervention for moderate-severe HIE.
Mechanism:
  • Reduces cerebral metabolic rate
  • Decreases secondary energy failure
  • Reduces inflammation, apoptosis, and excitotoxicity
  • Reduces risk of death or major disability by 25%
Inclusion criteria:
  1. Gestational age ≥36 weeks
  1. Evidence of perinatal hypoxia-ischaemia:
      • pH ≤7.0 or base deficit ≥16 in cord or first hour blood gas, OR
      • pH 7.01-7.15 or base deficit 10-15.9 AND prolonged resuscitation or sentinel event
  1. Moderate to severe encephalopathy (Sarnat 2 or 3) OR abnormal aEEG
  1. Age <6 hours at initiation
Exclusion criteria:
  • Major congenital anomalies
  • Severe chromosomal abnormalities incompatible with life
  • Moribund infant (imminent death expected)
  • Severe coagulopathy with active bleeding
  • Birth weight <1800 g
Method:
  • Whole body cooling (most common) or selective head cooling
  • Target temperature: 33-34°C (rectal or oesophageal)
  • Duration: 72 hours
  • Rewarming: Slow (0.5°C per hour) to 36.5°C
  • Monitoring: Continuous temperature, vital signs, aEEG/EEG
Complications of cooling:
  • Bradycardia, arrhythmias
  • Hypotension
  • Coagulopathy
  • Thrombocytopenia
  • Increased risk of sepsis
  • Subcutaneous fat necrosis
  • Metabolic acidosis
Post-cooling care:
  • Continue supportive care
  • MRI at 2-8 days
  • Long-term neurodevelopmental follow-up

Prognosis

Predictive factors (poor prognosis):
  • Severe metabolic acidosis (pH <7.0, base deficit >16)
  • Persistently low Apgar scores (0-3 at 10, 15, 20 minutes)
  • Sarnat stage 3 HIE
  • Early onset refractory seizures
  • Severe abnormality on aEEG (burst suppression, isoelectric)
  • Severe abnormality on MRI (extensive watershed injury, basal ganglia/thalamus injury)
  • Need for prolonged resuscitation (>10 minutes)
Long-term outcomes:
Stage 1 HIE (Mild):
  • 100% survival
  • Normal neurodevelopmental outcome
Stage 2 HIE (Moderate) with therapeutic hypothermia:
  • ~5-10% mortality
  • 70-80% normal or mild disability
  • 20-30% moderate-severe disability
Stage 3 HIE (Severe) with therapeutic hypothermia:
  • 40-50% mortality in first year
  • Survivors: High risk of severe neurodevelopmental impairment
Neurodevelopmental sequelae:
  • Cerebral palsy (most common, especially spastic quadriplegia)
  • Developmental delay
  • Intellectual disability
  • Epilepsy
  • Visual impairment (cortical visual impairment)
  • Hearing loss
  • Learning difficulties
  • Behavioural problems
Follow-up:
  • Regular neurodevelopmental assessment at 3, 6, 12, 18, 24 months
  • Audiology and ophthalmology screening
  • Physical, occupational, and speech therapy as needed
  • Educational support

Prevention

Antenatal:
  • Good antenatal care and risk assessment
  • Management of maternal medical conditions
  • Fetal monitoring in high-risk pregnancies
  • Planned delivery for at-risk pregnancies
Intrapartum:
  • Electronic fetal monitoring (CTG) during labour
  • Fetal scalp blood sampling if CTG abnormalities
  • Prompt response to fetal distress
  • Appropriate use of assisted delivery or caesarean section
  • Avoid prolonged second stage of labour
  • Active management of shoulder dystocia, cord prolapse
Delivery room:
  • Skilled birth attendant at every delivery
  • Neonatal resuscitation team available for high-risk deliveries
  • Equipment prepared and functional
  • Immediate and effective resuscitation when needed
  • Delayed cord clamping (30-60 seconds) if baby stable
Postnatal:
  • Early identification of at-risk infants
  • Prompt initiation of therapeutic hypothermia
  • Multidisciplinary NICU care
Key Points: Birth asphyxia is a major cause of neonatal morbidity and mortality. HIE is graded using Sarnat staging. Therapeutic hypothermia within 6 hours is the cornerstone of treatment for moderate-severe HIE and significantly improves outcomes. Long-term neurodevelopmental follow-up is essential.