Immunodeficiencies

Question 1

What is primary and secondary immunodefiency?

Answer 1

• Primary (congenital): defect in immune system

* Secondary (acquired): caused by another disease

Question 2

What are the clinical features of Immunodeficiencies?

Answer 2

• Recurrent infections (normal: <6-8 URI/year for the 1st 10 years; 6 otitis media and 2 gastroenteritis/year for the 1st 2-3 years)
• Severe infections, unusual pathogens (Aspergillus, Pneumocystis), unusual sites (lives abscess, osteomyelitis)

Question 3

What cells does a primary immunodeffiency effect?

Answer 3

• Adaptive immune system: affect T and B cells

* Innate immune system: affect phagocytes, complement

Question 4

Describe the defects in adaptive immunity

Answer 4

Subclassification- primary component affected (B/T cell or combined).
Often T cell defect impair antibody production.
Defects in lymphocyte development or activation.

Question 5

What are the major B lymphocyte disorders?

Answer 5

• X-linked agammaglobulinaemia (Bruton’s disease)
• Common variable immunodeficiency (CVID)
• Selective IgA deficiency
• IgG2 subclass deficiency
• Specific Ig deficiency with normal Igs

Question 6

Describe X-linked agammaglobulinemia (Bruton’s disease):

Answer 6

• Also known as Bruton’s disease
• Defect in BTK gene (X chromosome)
• Encodes Bruton’s tyrosine kinase
• Block in B-cell development (stop at pre-B cells)
• Recurrent severe bacterial infections
• 2nd half of first year (lung, ears, GI)
• Autoimmune diseases (35% of patients)

Question 7

What causes DiGeorge syndrome?

Answer 7

• 22q11 deletion leading to failure to develop 3+4th pharyngeal pouches.
• Complex array of developmental defects.
• Dysmorphic face: cleft palate, low-set ears, fish-shaped mouth.
• Hypocalcaemia, cardiac abnormalities.
• Variable immunodeficiency (absent/reduced thymus => affects T cell development

Question 8

Describe Wiskott-Aldrich syndrome

Answer 8

• X-linked
• Defect in WASP (protein involved in actin polymerisation => defect in signalling)
• Thrombocytopaenia, eczema, infections
• Progressive immunodeficiency (T cell loss)
• Progressive ↓ T cells; ↓ T cell proliferation
• Ab production (↓ IgM, IgG; high IgE, IgA)

Question 9

What is SCID?

Answer 9

Severe Combined Immunodeficiency (SCID).

Question 10

What causes SCID?

Answer 10

• Involves both T and B.
• 50-60% X-linked; rest - autosomal recessive
• Presentation- well at birth; problems > 1st month. diarrhoea; weight loss; persistent candidiasis. Severe bacterial/viral infections, failure to clear vaccines and unusual infections (Pneumocystis, CMV).
• Common cytokine receptor γ-chain defect (signal transducing component of receptors for IL-2, IL-4, IL-7, IL-9, IL-11, IL-15, IL-21); IL-7 needed for survival T cell precursors => defective T cell development => lack in B cell help (low Ab)
• RAG-1/RAG-2 defect => no T and B cells
• ADA (adenosine deaminase deficiency); => accumulation of deoxyadenosine & deoxy-ATP => toxic for rapidly dividing thymocytes
• Investigations- Lymphocyte subsets: T, B, NK (% and numbers) => low total lymphocyte count => SCID sign! Pattern: very low/absent T; normal/absent B, sometimes also absent NK (γ-chain defect affecting IL-15 receptor). Igs low
• T cell function ↓ (proliferation, cytokines).
• Treatment= isolation. No live vaccines, blood products from CMV-negative donors (cytomegalovirus). I.V. Ig replacement, treat infections, bone marrow/haematopoietic stem cell replacement, gene therapy (for ADA and y-chain).
• Outcome- dependent on prompt diagnosis. Survival >80% with early diagnosis, good donor match and no infections pre-transplant.
• <40% survival for late diagnosis, chronic infections and poorly matched donors.
• Regular monitoring post BMT.

Question 11

Describe coimbined immunodeficiencies- Ataxia-Telangiectasia (AT):

Answer 11

• Autosomal recessive.
• Defect in cell cycle checkpoint gene (ATM) => sensor of DNA damage => activates p53 => apoptosis of cells with damaged DNA.
• ATM gene stabilises DNA double strand break complexes during V(D)J recombination => defect in generation of lymphocyte antigen receptors & lymphocyte development. B cell and antibody deficiency.
• Progressive cerebellar ataxia (abnormal gait).
• Typical telangiectasia (ear lobes, conjunctivae)- small dilated-blood vessels near the surface of the skin or mucous membranes.
• Immunodeficiency. Increased incidence of tumours later in life.
• Combined immunodeficiency (B & T).
• Defects in production of switched Abs (IgA/G2).
• T cell defects (less pronounced) <= thymic hypoplasia.
• Upper & lower respiratory tract infections.
• Autoimmune phenomena, cancer.

Question 12

Phagocyte defects- chronic granulomatous disease:

What defects in phagocytes can occur?

Answer 12

• Defective oxidative killing of phagocytosed microbes; mutation in phagocyte oxidase (NADPH) components
• Killing pathogens is oxygen dependent. Resting phagocyte becomes activated through assembly of NADPH oxidase generation of superoxide anion.
• Formation of granulomas.
• Diagnosis- tests measure oxidative burst e.g. NBT test (Nitroblue tetrazolium reduction- blue in normal red otherwise) and flow cytometry dihydrorhodamine (no change even when stimulates with PMA).

Question 13

Describe Phagocyte defects- Chediak-Higashi syndrome

Answer 13

• Rare genetic disease.
• Defect in LYST gene (regulates lysosome traffic).
• Neutrophils have defective phagocytosis.
• Repetitive, severe infections.
• Defect phagosome-lysosome fusion => defective killing of phagocytosed microbes => recurrent infections.
• Decreased number neutrophils
• Neutrophils have giant granules

Question 14

Describe Phagocyte defects- LAD (leucocyte adhesion deficiency):

Answer 14

• Defect in β2-chain integrins (LFA-1, Mac-1).
• Defect in sialyl-Lewis X (selectin ligand).
• Delayed umbilical cord separation => diagnosis defect in β2-chain integrins (LFA-1, Mac-1).
• Presentation- skin infections, intestinal + perianal ulcers
• Investigation- reduced neutrophil chemotaxis and reduced integrins on phagocytes (flow cytometry).

Question 15

Describe complement deficiencies

Answer 15

• Can affect different complement factors severe/fatal pyogenic infections (C3 deficiency).
• Predisposition to infection with different pathogens.
• Symptoms differ depending on C factor affected.
• Recurrent infections (Neisseria) - deficiency terminal complex (MAC): C5, C6, C7, C8 & C9.
• Severe/fatal pyogenic infections (C3 deficiency)
• SLE-like syndrome (C1q, C2, C4 deficiency)
• Hereditary angioneurotic oedema: failure to inactivate complement (deficiency in C1 inhibitor); intermittent acute oedema skin/mucosa => vomiting, diarrhoea, airway obstruction.
• Investigations- complement function: CH50 (haemolysis). Measure individual components.
•

Question 16

What are the aims of treatment

Answer 16

• Minimise/control infection.
• Replace defective/absent component of IS- Immunoglobulin replacement therapy, Bone marrow transplantation and gene therapy.
• Prompt treatment of infection.
• Prevention of infection: isolation, antibiotic prophylaxis, vaccination (not live vaccines!).
• Good nutrition.

Question 17

Describe secondary immunodeficiency

Answer 17

• Infections: viral, bacterial. Viral: HIV, CMV, EBV, measles, influenza. Chronic bacterial: TB, leprosy. Chronic parasitic: malaria, leishmaniasis. Acute bacterial: septicaemia.
• Malignancy- Myeloma, lymphoma (Hodgkin’s, non-Hodgkin’s) and leukaemia (acute or chronic).
• Extremes of age- prematurity. Infants under 6 months have maternal IgG. Premature delivery interrupts placental transfer of IgG so infant Ig deficient. Old age- decline in normal immune function.
• Nutrition (anorexia, iron deficiencies)
• Chronic renal disease
• Splenectomy
• Trauma/surgery, burns, smoking, alcohol
• Immunosuppressive drugs.