CGD has an estimated prevalence of 1 in 200,000 to 500,000 live births. It predominantly affects males due to the X-linked inheritance pattern of the most common genetic mutation (see RareShare Guide on Genetic Inheritance).

CGD is caused by mutations in genes responsible for producing NADPH oxidase, an enzyme crucial for the production of hydrogen peroxide in white blood cells. This enzyme is necessary for killing certain bacteria and fungi and regulating white blood cell responses to inflammation. About 70% of cases are X-linked mutations in the CYBB gene, while the remaining cases are autosomal recessive mutations in the CYBA, NCF1, NCF2 or NCF4 genes.

Symptoms

• Recurrent, frequent and severe bacterial and fungal infections

• Formation of granulomas in various tissues

• Recurrent pneumonia

• Abscesses in the liver, lungs, spleen, and skin

• Lymphadenitis (inflammation of the lymph nodes)

• Gastrointestinal issues such as colitis and inflammatory bowel disease-like symptoms

• Osteomyelitis (bone infections)

• Delayed growth and development in children

• Delayed wound healing

Diagnosis of CGD is based on clinical presentation and a history of recurrent infections that do not respond to standard treatments. The disease is typically diagnosed in childhood, but some cases are not identified until adulthood. Specific tests may include:  

• Dihydrorhodamine (DHR) Flow Cytometry Test: Measures the respiratory burst in phagocytes by detecting the production of reactive oxygen species.

• Nitroblue Tetrazolium (NBT) Test: Assesses the ability of phagocytes to produce reactive oxygen species.

• Genetic Testing: Identifies mutations in the genes associated with CGD.

• Blood Tests: May show elevated white blood cell counts during infections.

• Immunological tests to evaluate overall immune function.

• Prophylactic antibiotics (e.g., trimethoprim-sulfamethoxazole) and antifungal medications (e.g., itraxonazole) to prevent infections.

• Interferon-gamma therapy to boost the immune system’s ability to fight infections.

• Bone Marrow or Stem Cell Transplantation: Can be curative by providing a source of healthy phagocytes.

• Gene Therapy: Experimental and aimed at correcting the defective gene in phagocytes.

• Supportive Care: Includes regular monitoring and management of symptoms and complications.

The outlook for GCD patients is generally very good as healthcare providers can usually manage symptoms and prevent serious infections. The average patient now survives at least 40 years. Treatment may continue indefinitely to keep infections and inflammation from becoming severe. With ongoing treatment and support, many people with CGD live active and fulfilling lives. Prompt treatment is necessary to treat infections before they become severe or life-threatening. Without treatment, children would often die before age ten.

1. National Organization for Rare Disorders (NORD):  Chronic Granulomatous Disease.

2. MedlinePlus:  Chronic Granulomatous Disease.