title: "Week 3: Immunology & Infectious Disease"

Week 3: Immunology & Infectious Disease

Food Allergy Overview

TypeTimingSymptomsTesting
IgE-mediatedMinutes to 2 hoursUrticaria, angioedema, anaphylaxisSkin prick, specific IgE
Non-IgE-mediatedHours to daysGI (Gastrointestinal) symptoms (diarrhoea, vomiting)Clinical diagnosis only

Prevalence of food allergy: 1 in 10 children. Overall rising, but may have plateaued.


IgE-Mediated Food Allergy

Mechanism

IgE Allergy Mechanism
  1. Sensitisation: Macrophage → Th2 → B cell → IgE production
  2. Re-exposure: Allergen + IgE on mast cells → cross-linking → degranulation → histamine release

Severity

Mild-ModerateAnaphylaxis
Lip/face/eye swellingDifficult/noisy breathing
Hives, weltsTongue/throat swelling
Tingling mouthWheeze, persistent cough
Abdominal pain, vomitingHoarse voice, collapse

Adrenaline autoinjector (AU/NZ) dosing (by weight): 0.15 mg for 7.5–20 kg; 0.3 mg for >20 kg. (Also remember IM adrenaline is 0.01 mg/kg to a max of 0.5 mg.)

Source: ASCIA anaphylaxis guidelines.

Risk Factors for Severe Reaction

Severe Allergy Risk Factors
  • Older child
  • Higher allergen dose
  • Poorly controlled asthma
  • Nuts, shellfish, fish allergens
  • Cofactors: exercise, NSAIDs, alcohol, sleep deprivation, ACE-I, beta-blockers

Investigations

Skin prick testing alone does NOT diagnose allergy. Sensitisation (positive SPT) can occur without clinical allergy; interpret results in clinical context. Wheal size indicates likelihood, not severity.

Source: ASCIA allergy testing guidance.

Warning

Do NOT test: allergen mixes, IgG to foods, random pseudoscience tests. Only test children with history of allergic reaction.

Natural History

High chance of outgrowingLow chance of outgrowing
Milk, egg, soy, wheatPeanut, tree nut, fish, shellfish

LEAP Study (2015): Early oral introduction of peanuts PREVENTS peanut allergy in high-risk infants. Window of opportunity under age 4.


Non-IgE-Mediated Food Allergy

Cow's Milk Protein Intolerance Spectrum

ConditionAgeKey FeaturesTreatment
FPIAP (Proctocolitis)First monthsBlood/mucus in stool, well babyElimination
FPE (Enteropathy)Early infancyMucus ± blood, may affect growthElimination
FPIES (Enterocolitis)6-12 monthsProfuse vomiting 2-4h post-ingestion, lethargy, pallorOndansetron, fluids

FPIES presents with profuse vomiting 2-4 hours after ingestion. Common triggers: rice, cow's milk, soy, oats. Usually outgrown by 2-4 years.

Clinical Pearl

No allergy testing for non-IgE-mediated allergies - diagnosis is clinical!


Eosinophilic Oesophagitis (EoE)

EoE diagnosis: Symptoms of oesophageal dysfunction + ≥15 eosinophils/hpf on biopsy. Endoscopy shows rings, furrows, white exudates.

Presentations:

  • Infants: feeding difficulty, FTT, vomiting
  • Older children: dysphagia, food impaction
  • Adolescents: chest pain when eating

Immunodeficiency

Suspect immunodeficiency with infections that are unusual, opportunistic, disseminated, or recurrent. Also: FTT, chronic diarrhoea, persistent oral Candida.

Types of Immunodeficiency

TypeInfectionsExamples
Humoral (antibody)Encapsulated bacteria: S. pneumoniae, N. meningitidis, H. influenzaeXLA, IgA deficiency, CVID
T cell/SCIDOpportunistic: PCP, fungal, CMV, EBVX-linked SCID, ADA deficiency
Phagocytic (neutrophil)Skin/soft tissue, fungalCGD, leukocyte adhesion deficiency
ComplementNeisseria (terminal), bacterial (C2)C5-C9 deficiency, C2 deficiency
Infection Type → Immune Defect
  • Recurrent bacterial → Humoral or complement
  • Recurrent Neisseria → Complement (terminal)
  • Opportunistic/fungal → T cell/SCID
  • Staph, Pseudomonas, Nocardia → Neutrophil (CGD)

SCID

SCID = Severe Combined Immunodeficiency. Lymphopenia (mainly T cells), absent thymus on CXR (Chest X-Ray). Presents with opportunistic infections and FTT.

SCID screening: Newborn bloodspot tests for TRECs (T-cell receptor excision circles). Absent TRECs = absent thymic T-cell production.

Chronic Granulomatous Disease (CGD)

CGD: Neutrophils fail to undergo oxidative burst. Recurrent bacterial and fungal infections of skin, soft tissue, lungs, liver. Granuloma formation.

Clinical Pearl

Leukocyte adhesion deficiency presents with high neutrophil count but inability to form pus. Classic sign: delayed separation of umbilical cord.


Neonatal Sepsis

Early-Onset (< 7 days)Late-Onset (> 7 days)
Vertical transmission (birth canal)Horizontal (environment, lines)
GBS, E. coli, ListeriaCoag-negative staph, S. aureus, GNB

Group B Strep (GBS) and E. coli are the most common causes of early-onset neonatal sepsis.


Immunisation

Vaccines are either live attenuated (MMR, varicella, rotavirus, BCG) or inactivated (whole, subunit, toxoid, conjugate).

Warning

Contraindications to vaccination: Anaphylaxis to previous dose or vaccine component. Immunocompromised patients should not receive live vaccines.

Clinical Pearl

Vaccines are given at chronological age, not corrected age for premature infants.


Practice Questions

SBAeasyfood allergyinvestigation
2y
OedemaRash

What is the first-line investigation?

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SBAmediumFPIESnon-IgE allergy
9mo
Nausea/vomitingPallorLethargy

What is the most likely diagnosis?

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SBAmediumimmunodeficiencycomplement
A child has recurrent Neisseria meningitidis infections. Which immune deficiency should be suspected?
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SBAmediumSCIDscreening
An infant with SCID is identified on newborn screening. What was tested?
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SBAeasyfood allergyprognosis
Which of the following allergies is MOST likely to be outgrown?
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SBAmediumfood allergyprevention
What is the window of opportunity for oral immunotherapy to prevent peanut allergy in high-risk infants?
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