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Common variable immunodeficiency

From Wikipedia, the free encyclopedia

Common variable immunodeficiency
Classification & external resources
ICD-10 D83
ICD-9 279.06

Common variable immunodeficiency (CVID) is a group of 20-30 primary immunodeficiencies (PIDs) which have a common set of symptoms but with different underlying causes.

Contents

[edit] Causes and types

CVID is believed to be a genetically determined primary immune defect; however, the underlying causes are different. The result of these defects is that the patient doesn't produce sufficient antibodies in response to exposure to pathogens. As a result, the patient's immune system fails to protect them against common bacterial and viral (and occasionally parasitic and protozoan) infections. The net result is that the patient is prone to illness. Both parts of the immune system (the cellular and humoral system) are affected, hence its classification as a combined immunodeficiency.

CVID appears to include a number of defects, some of which have been identified. For the majority, the genetic causes are still unknown. It is possible that environmental agents provoke the immune defect, due to genetic predisposition, but this has not been clarified.

See also X-linked agammaglobulinemia, a similar disorder, better characterised than CVID. hypogammaglobulinemia (CVID) and X-linked agammaglobulinemia (XLA) are often intermixed by physicians, as their clinical conditions and treatment are almost identical.

[edit] Symptomology

Symptoms of CVID are:

  • hypogammaglobulinemia, or low levels of immunoglobulin G (IgG), IgA and/or IgM.
  • lack of normal levels of antibody in the serum is part of the diagnosis
  • polyarthritis, or joint pain, spread across most joints, but specifically fingers, wrists, elbows, toes, ankles and knees
  • chronic infections. (most common symptom) Specifically: [[upper respiratory tract infection - e.g. bronchitis, sinusitis which respond to antibiotics but return or reoccur.
  • Viral infections that usually respond to antivirals, (URTIs), sinusitis, tonsilitis, epiglottitis, dermatological abscesses/boils (often, but not exclusively, facial and axillary), pneumonia, bronchitis, pleurisy, stomach/intestinal infections, colds, influenza, shingles, conjunctivitis
  • Tiredness
  • Chronic swelling of the lymph glands
  • Enlarged speen
  • atrophic gastritis with pernicious anemia
  • nodular lymphoid hyperplasia of the intestine. This finding can be mistaken for intestinal lymphoma
  • bacterial overgrowth of the intestine.
  • villous atrophy in the small intestine, which can resemble coeliac disease and cause diarrhoea and malabsorption
  • chronic diarrhoea (often arises as a result of "minor" intestinal infections, including protozoan and parasitic infections)
  • increased incidence of inflammatory bowel disease
  • bronchiectasis (lung tissue damage as a result of repeated chest infections) leading to shortness of breath
  • poor titer levels in response to vaccination. Responsiveness may be tested after administration of polysaccharide and non-polysaccharide coated pathogens (e.g. streptococci and tetanus respectively)
  • children may show a "failure to thrive" - they may be underweight and underdeveloped compared with "normal" peers
  • patients may lose weight

Diagnosis is often delayed; and diagnosis is often made in the second or third decade of life after referral to an immunologist.

As with several other immune cell disorders, CVID may predispose to [lymphoma] or possibly stomach cancer. There also appears to be a predilection for autoimmune diseases, with a risk of up to 25%. Autoimmune destruction of platelets or red cells are the commonest of these.

[edit] Treatment

Treatment usually consists of immunoglobulin therapy, which is an injection of human antibodies harvested from blood donations: intravenous immunoglobulin (IVIG, most common treatment), subcutaneous immunoglobulin G (SCIG, relatively new therapy) or intramuscular immunglobulin (IMIG, less effective, painful). This is not a cure, but it strenghtens immunity by ensuring that the patient has "normal" levels of antibodies, which helps to prevent recurrent infections. IG therapy can't be used if the patient has anti-IgA antibodies but in this case, products low in IgA can be used; subcutaneous delivery also is a means of permitting such patients to have adequate antibody replacement.

Some CVID patients may experience reactions to IG therapies; reactions may include:

  • anaphylactic shock (very rare)
  • hives (rare)
  • difficulty breathing
  • headache (relatively common, may be relieved by an antihistamine, paracetamol/acetaminophen, or an anti-inflammatory (naproxen, advil, aspirin)
  • nausea (common)
  • fever (common)
  • aseptic meningitis (rare)
  • severe fatigue
  • muscle aches and pain, or joint pain
  • thrombotic events (rare)

Patients should not receive therapy if they are fighting an active infection as this increases the risk of reaction. Also, patients changing from one brand of product to another may be at higher risk of reaction for the first couple of treatments on the new brand.

Reactions can be minimised by taking an antihistamine and/or hydrocortisone and some paracetamol/acetaminophen/anti-inflammatory (naproxen, advil, aspirin) prior to treatment; patients should also be thoroughly hydrated and continue to drink water before, after and during treatment (if possible).

[edit] Research

Research is currently focussing on genetic analysis, and in differentiating between the various different disorders in order to allow a cure to be developed. Cures are likely to be genetic in nature, repairing faulty genes and allowing the individual to start producing antibodies. Funding for research in the US is provided by the National Institutes of Health. Key research in the UK is funded by the Primary Immunodeficiency Association (PiA), and funding is raised through the annual Jeans for Genes campaign.

[edit] Epidemiology

CVID has an estimated prevalence is about 1:25,000 to 1:50,000. The typical patient is between 20 and 40, and males and females are equally affected. About 20% of patients are diagnosed in childhood.

[edit] History

Janeway et al (1953) is generally credited with the description of the first case of CVID.

[edit] Reference

  • Janeway CA, Apt L, Gitlin D. Agammaglobulinemia. Trans Assoc Am Physicians 1953;66:200-2. PMID 13136263.

[edit] External links

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