Diagnosing Primary Immunodeficiencies (PID): The Genetic Revolution

PATHCHAT Edition No. 38
Please contact your local Ampath pathologist for more information.

Introduction

🔹 What Are Primary Immunodeficiencies (PID)?

• PID consists of over 300 known genetic defects affecting the immune system.
• They can present at any age, though severe forms manifest in infancy.
• Due to variable presentation, PID diagnosis is often delayed or missed.

✅ Key Clinical Clues for PID Diagnosis:

• Severe infections requiring hospitalization or intravenous antibiotics.
• Persistent infections (never fully recover).
• Unusual pathogens or infection sites.
• Recurrent infections (multiple episodes of the same infection).
• Family history of immunodeficiency.

📌 A genetic diagnosis confirms PID and aids in family screening, prenatal testing, and selecting targeted therapies.

Ampath’s Next-Generation Sequencing (NGS) PID Panel

✅ Ampath has developed a comprehensive genetic PID panel covering 99 critical genes.
✅ This panel includes genetic testing for:

• Severe Combined Immunodeficiency (SCID).
• Hyper IgM and Hyper IgE syndromes.
• Common Variable Immunodeficiency (CVID).
• Immune dysregulation syndromes.
• Lymphoproliferative syndromes, including autoimmune lymphoproliferative syndrome.
• Chronic Granulomatous Disease (CGD).
• MHC Class I and MHC Class II deficiencies.
• Thymic defects associated with congenital abnormalities.
• Autoimmune and regulatory immune disorders.
• Innate immunity and complement deficiencies.

📌 This test provides a genetic diagnosis that can guide treatment decisions, bone marrow transplantation, and family genetic counselling.

Stepwise Approach to PID Diagnosis

✅ A structured, tiered diagnostic approach ensures cost-effective testing.

Step 1: First-Line Investigations (Basic Screening)

🔹 Rule Out Common Causes Before PID Testing:

• Exclude HIV (HIV ELISA or PCR).
• Assess for atopy (if indicated by history).

🔹 Initial Blood Tests:

• Full Blood Count (FBC) with Differential:
  • Lymphopaenia → Suggests SCID.
  • Small platelets → Seen in Wiskott-Aldrich syndrome.
• Serum Immunoglobulins (IgG, IgM, IgA, IgE):
  • IgE should be tested in suspected hyper-IgE syndrome.
• Cystic Fibrosis (CF) Screening (if clinically indicated).

Step 2: Second-Line Investigations (Functional Immune Tests)

🔹 Assessing Antibody-Mediated Immunity:

• Specific Antibody Responses to Vaccines:
  • Assess responses to polysaccharide antigens (e.g., pneumococcus, H. influenzae).
  • Assess responses to protein antigens (e.g., tetanus, diphtheria).
  • If antibody levels are low, revaccinate and retest after 4 weeks.

🔹 Assessing Lymphocyte Subsets (Flow Cytometry):

• B-Cells (CD19):
  • Absent in X-linked agammaglobulinaemia (XLA).
• T-Cells (CD3, CD4, CD8):
  • Reduced in SCID, combined immunodeficiencies, and some cases of CVID.
• Natural Killer (NK) Cells (CD16, CD56):
  • Low in isolated NK-cell deficiencies (linked to recurrent herpesvirus infections).

🔹 Assessing Neutrophil Function:

• Neutrophil Oxidative Burst Test → Diagnoses Chronic Granulomatous Disease (CGD).
• Neutrophil Adhesion, Chemotaxis, and Phagocytosis Studies → Diagnoses leukocyte adhesion defects.

🔹 Complement Testing:

• Total Haemolytic Complement Assays (Classical & Alternative Pathways):
  • Detect complement deficiencies.

Step 3: Third-Line Investigations (Advanced Functional Testing)

🔹 Lymphocyte Proliferation Studies:

• Tests response to mitogens (PHA, PMA, anti-CD3) and recall antigens (Candida, tetanus, varicella).
• Used to diagnose T-cell defects, including SCID and chronic mucocutaneous candidiasis.

🔹 Neutrophil Antibody Testing:

• Assesses autoimmune neutropaenia.

🔹 Lymphocyte Maturation Markers:

• Naïve vs. memory T-cells → Used for SCID and combined T-cell defects.
• Memory B-cells → Categorizes CVID subtypes.

🔹 TREC/KREC (T-cell and B-cell receptor excision circles):

• Newborn screening for SCID and XLA (performed on dried blood spots).

Step 4: Fourth-Line Investigations (Genetic and Molecular Testing)

✅ Genetic testing is essential for diagnosing severe immunodeficiencies and hereditary immune disorders.

🔹 Available Tests:

• NGS-based genetic PID panel (99 genes).
• Targeted gene sequencing for single-gene disorders.
• Cytokine and enzyme studies.
• T-regulatory cell and Th17 cell analysis.
• Surface marker studies for X-linked SCID.
• BTK mutation analysis (for diagnosing XLA).

📌 Genetic testing must be discussed with an immunology pathologist before ordering.

Genetic Testing for PID at Ampath

🔹 When to Consider Genetic Testing:
✅ For patients with severe or atypical PID requiring bone marrow transplantation.
✅ For screening family members or conducting prenatal testing.
✅ For confirming a suspected single-gene immunodeficiency disorder.

🔹 How to Request Genetic Testing:
✅ Specimen Requirement: One full EDTA tube (test code: PID).
✅ Genetic counselling is mandatory before and after testing.
✅ Estimated cost: R17,600 (subject to medical aid coverage).
✅ Turnaround time: 6 weeks.

📌 Consult Ampath’s immunology pathologists before ordering genetic tests to ensure appropriate selection and interpretation.

Key Takeaways for Clinicians

✅ PID diagnosis requires a structured, stepwise approach.
✅ Initial testing includes full blood count, immunoglobulins, and HIV exclusion.
✅ Functional immune assays guide the next steps in evaluating antibody, T-cell, neutrophil, and complement defects.
✅ Genetic testing is essential for severe PID cases and family screening.
✅ Ampath offers a next-generation sequencing (NGS) panel covering 99 PID-related genes.
✅ Genetic counselling is required before and after genetic testing.

📌 Early diagnosis and intervention in PID improve patient outcomes and reduce infection-related complications.