Primary Antibody Deficiency

Primary antibody deficiency syndromes include congenital and acquired antibody deficiencies but not those secondary to other diseases (e.g. myeloma, chronic lymphocytic leukaemia or protein-losing enteropathies). There is often a significant delay in reaching a diagnosis of primary antibody deficiency, leading to an increase in morbidity and mortality.¹

• Common variable immune deficiency: low serum IgG and IgA concentrations, including IgG subclasses, with or without low serum IgM levels
• Bruton's X-linked hypogammaglobulinaemia: usually presents before the age of 2 years and most often from 6-12 months.
• Transient hypogammaglobulinaemia of infancy: delayed onset of immunoglobulin synthesis in infants with presentation in second half of the first year and recovery when aged 2-3 years. High incidence of recurrent upper respiratory infections but usually not severe infections and doesn't require immunoglobulin therapy.
• IgG subclass deficiencies: may be an indication for immunoglobulin replacement therapy in patients with recurrent infections who also do not produce specific IgG antibodies after test immunisations.
• Specific antibody deficiency: occurs in patients with a classic history of humoral immune deficiency who fail to respond to test immunisations, despite having normal serum concentrations of total IgG, IgA, IgM, and IgG subclasses.
• Hyper IgM syndrome: immunoglobulin deficiency but with increased IgM
• Selective IgA deficiency: occurs in 1 in 700 of population. Many affected people may be symptom free, particularly if deficiency is discovered by chance. Patients with the deficiency who have recurrent infections may also have an underlying deficiency in a subclass of IgG or specific antibody.
• Combined B cell and T cell deficiency, e.g. severe combined immune deficiency

Primary immune deficiency is associated with recurrent and severe infections such as sinusitis, otitis media, conjunctivitis, pneumonia, meningitis, septic arthritis and a chronic asymmetrical polyarthritis. The possibility of a primary antibody deficiency is suggested by:

• Unexplained failure to thrive
• Excess of infections. Adults often present with recurrent sinusitis
• Recurrent infections requiring frequent prescription of antibiotics
• Particularly severe, unusual or persistent infections, even if serum immunoglobulin concentrations are normal
• Chronic infections such as tonsillitis, otitis media, or recurrent boils
• Need for instigation of second line tests for chronic infection, e.g. sweat tests
• Abnormal lymphoid tissue, such as nodular lymphoid hyperplasia in the gut or congenital absence of tonsils
• Unexplained signs such as hepatosplenomegaly or arthropathy

Other conditions which cause severe recurrent or chronic respiratory infections such as cystic fibrosis.

• Serum immunoglobulin concentrations, including IgG subclasses
• When serum immunoglobulin concentrations are greatly depressed, confirmatory tests are not always necessary
• Functional antibody responses to immunisations, common bacteria and red cell antigens may be required
• Plasma B lymphocyte sub-populations concerned with antibody production

• Prompt antibiotic treatment. Consider constant prophylaxis
• Regular intravenous immunoglobulin
• Subcutaneous immunoglobulin is an alternative to intravenous administration²
• Higher doses may be needed in patients with known lung damage³
• Side effects (which include headache, nausea, chills, and fever) can be reduced by lowering the rate of infusion.³

Complications of primary antibody deficiency include acute infections, which may be due to unusual organisms such as mycoplasmas, and long term complications⁴:

• Chest: bronchiectasis, fungal infections, polyclonal lymphoid aggregates, granulomas, lymphoma
• Sinuses: recurrent sinusitis
• Bowel: infections (giardia, cryptosporidia), malabsorption, autoimmune enteropathy, sclerosing cholangitis, atrophic gastritis, food sensitive enteropathy, colitis, gastric carcinoma
• Liver: hepatitis, associated autoimmune diseases (chronic active hepatitis, primary biliary cirrhosis, sclerosing cholangitis), non-infective granulomas
• Joints: septic arthropathy, chronic sterile arthropathy and/or arthralgia
• Blood: autoimmune haemolytic anaemia, immune thrombocytopenic purpura, iron deficiency anaemia, anaemia of chronic illness, aplastic anaemia
• CNS: acute enteroviral meningoencephalitis, chronic cerebral granulomas
• Spleen: unexplained splenomegaly in 30%
• Eyes: keratoconjunctivitis, uveitis

Depends on nature and severity of the primary antibody deficiency.