Course Content
OBSTETRIC AND GYNAECOLOGICAL CONDITIONS
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ANTENATAL CARE
NORMAL LABOUR
Placental Praevia
Placental abruptio
Vasa Praevia
Cervical Lesions
POST-PARTUM HAEMORRHAGE (PPH)
Pre-Eclampsia and Eclampsia
Cerebral Malaria
Meningitis
Shock
Organophosphate Poisoning
Diabetic Coma
DKA/Hyperosmolar/Hypoglycaemia Management
Malaria in Pregnancy
Elimination of Mother-to-Child Transmission of HIV (EMTCT)
Medical Abortion (Termination of Pregnancy)
Threatened Abortion
Inevitable Abortion
Incomplete Abortion
Complete Abortion
Septic Abortion
Missed Abortion
Post-abortion care (PAC)
MOLAR PREGNANCY
COMMON PAEDIATRIC CONDITIONS
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Shock
Diabetic Ketoacidosis (DKA)
Coma
Adrenal Crisis
Anaphylaxis
Aspirin Toxicity
Organophosphate Poisoning
Iron Overdose
Paraquat Poisoning
Drowning and Submersion Injury
Meningitis and Encephalitis
Paediatric Stroke
Raised Intracranial Pressure (ICP)
Paediatric Seizures and Epilepsy
Neurodevelopmental Disorders
Neuromuscular Diseases
Acute Disseminated Encephalomyelitis (ADEM)
Common Cold
Child with Stridor
The Wheezing Child
Pneumonia
Congestive Cardiac Failure (CCF)
Acute Rheumatic Fever (ARF)
Rheumatic Heart Disease
Infective Endocarditis (IE)
Acute Diarrhoea
Persistent Diarrhoea
Severe Acute Malnutrition (SAM)
Acute Upper GI Bleeding
Acute Hepatic Failure
Intussusception
Peptic Ulcer Disease (PUD)
Urinary Tract Infection (UTI)
Nephrotic Syndrome
Acute Glomerulonephritis
Acute Kidney Injury (AKI)
Hypertension in Children
Anaemia
Sickle Cell Disease (SCD)
Glucose 6 Phosphate Dehydrogenase (G6PD) Deficiency
Aplastic Anaemia (Bone Marrow Failure)
Immune Thrombocytopenia (ITP)
Infantile Haemangioma (IH)
Haemophilia
Leukaemia
Lymphomas
Rhabdomyosarcoma (RMS)
Retinoblastoma
Nephroblastoma (Wilms’ Tumour)
Low Grade Gliomas (LGG)
Medulloblastoma
Typhoid (Enteric Fever)
Dysentery
Parasitic Infections
Tuberculosis (TB) in Children
Paediatric Human Immunodeficiency Virus (HIV) And Acquired Immune Deficiency Syndrome (AIDS)
Malaria
Zambian Paediatric & Obstetrics-Gynecology (OB/GYN) Clinical Mastery

Paediatric Infantile Haemangioma (IH) 

Lesson Objectives

By the end of this lesson, learners should be able to:

  1. Define Infantile Haemangioma and understand its natural history.

  2. Recognize clinical features and complications requiring treatment.

  3. List appropriate investigations for evaluation of IH.

  4. Identify indications and contraindications for propranolol therapy.

  5. Describe the stepwise dosing and monitoring of propranolol.

  6. Counsel caregivers regarding treatment, follow-up, and side effects.

Description

Infantile Haemangiomas (IH) are the most common vascular tumours in infants, affecting approximately 4% of newborns. IH appear within the first few weeks of life, proliferate rapidly during the first months, and may continue slow growth for 6–12 months. Most spontaneously involute and do not require treatment, but about 15% develop complications including obstruction, ulceration, or disfigurement, necessitating therapeutic intervention.

Investigations

Investigation Purpose / Notes
FBC Baseline evaluation
Blood glucose Detect hypoglycemia risk before propranolol
Urea & electrolytes Assess renal function
Thyroid function tests (TFTs) Baseline assessment
Liver function tests (LFTs) Baseline assessment
ECG & ECHO Detect cardiac contraindications
Liver ultrasound For infants with >5 cutaneous IH to detect liver involvement
MRI scan For complex or deep lesions requiring detailed imaging

Indications for Treatment with Oral Propranolol

Indication Reason / Clinical Concern
Vision compromise Protect sight
Airway IH Prevent obstruction
Nasal IH Avoid nasal obstruction
Lip IH Prevent functional impairment and/or disfigurement
Auditory canal involvement Prevent recurrent infection
Ulcerated IH When topical therapy is inadequate
Risk of permanent disfigurement Cosmetic/functional concern
Spinal cord compression Prevent neurological sequelae
Liver IH with cutaneous IH Multidisciplinary management in select cases

Contraindications

Type Details
Absolute Recent/ongoing hypoglycemia, 2nd–3rd degree heart block, hypersensitivity to propranolol
Relative Frequent wheezing, abnormal BP or HR for age; require paediatrician supervision

Dosing Protocol (Oral Propranolol, 1 mg/ml solution preferred)

Week Dose Notes
Week 1 1 mg/kg/day in 3 divided doses Start low to monitor tolerance
Week 2 2 mg/kg/day in 3 divided doses Monitor for side effects
Dose escalation 3 mg/kg/day in 3 divided doses if inadequate response Only after 4 weeks and no adverse effects

Administration: Give with or shortly after food. Hold medication if significant vomiting occurs to reduce hypoglycemia risk.

Potential Side Effects

Side Effect Clinical Concern
Bradycardia Monitor HR
Hypoglycemia Especially if reduced oral intake
Heart failure Monitor cardiac status
Hypotension Monitor BP
Cardiac conduction disorders ECG monitoring
Bronchospasms Caution in asthmatic children
Peripheral vasoconstriction Monitor extremities
Weakness, fatigue Supportive care
Sleep disturbances Inform caregivers

Follow-Up and Stopping Therapy

  • Reassess 4 weeks after treatment initiation.

  • Duration should extend beyond proliferative phase to prevent rebound growth.

  • European studies suggest risk of rebound decreases significantly after 17 months of age.

  • Temporarily discontinue propranolol if:

    • Significant reduced oral intake

    • Wheezing requiring treatment

Parental Education: Explain administration, side effects, and monitoring. Provide written information leaflet.

Summary

  • IH are common vascular tumours of infancy; most involute spontaneously.

  • About 15% require treatment due to complications.

  • Propranolol is first-line therapy for complicated IH.

  • Indications include airway, vision, nasal, lip involvement, ulceration, risk of disfigurement, spinal cord or liver involvement.

  • Monitor for cardiac, respiratory, and metabolic side effects.

  • Therapy should continue through proliferative phase; rebound risk decreases after 17 months.

 

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