Chronic granulomatous disease: Difference between revisions
From IDWiki
(Created page with "== Background == * Primary immunodeficiency of neutrophils leading to recurrent infections with catalase-positive organisms === Pathophysiology === * Defect in NADP...") |
(added DDx) |
||
Line 1: | Line 1: | ||
== |
==Background== |
||
* |
*[[Primary immunodeficiency]] of neutrophils leading to recurrent infections with [[catalase-positive]] organisms |
||
=== |
===Pathophysiology=== |
||
* |
*Defect in NADPH oxidase |
||
* |
*Therefore unable to generate superoxide radicals required by phagocytes to kill pathogens |
||
== |
==Clinical Manifestations== |
||
* |
*Recurrent infections with catalase-positive organisms, including [[Staphylococcus aureus]] |
||
* |
*Highest-risk group for [[invasive aspergillosis]] |
||
== |
== Differential Diagnosis == |
||
* Other [[Primary immunodeficiency|primary immunodeficiencies]] |
|||
⚫ | |||
** [[MPO deficiency]], which will have an abnormal DHR test but largely asymptomatic unless concurrent [[diabetes mellitus]] |
|||
⚫ | |||
** [[Hyper-IgE syndrome]], though ''Aspergillus'' will be more typically pulmonary |
|||
⚫ | |||
** IRAK4/MyD88 deficiency, which won't have fungal infections and improves with age |
|||
⚫ | |||
** Humoral immunodeficiencies, such as [[CVID]] or [[Bruton tyrosine kinase deficiency]], though they tend to have more infections with encapsulated organisms and will have abnormal quantitative immunoglobulins |
|||
⚫ | |||
* [[Inflammatory bowel disease]] |
|||
* [[Cystic fibrosis]] |
|||
* [[Sarcoidosis]] |
|||
== Diagnosis == |
|||
* The diagnosis is confirmed with the dihyohodamine-123 (DHR-123) test |
|||
==Management== |
|||
⚫ | |||
⚫ | |||
⚫ | |||
⚫ | |||
⚫ | |||
== Further Reading == |
|||
* Considerations in the Diagnosis of Chronic Granulomatous Disease. ''J Pediatric Infect Dis Soc''. 2018;7(S1):S6-S11. doi: [https://doi.org/10.1093/jpids/piy007 10.1093/jpids/piy007] |
|||
[[Category:Pediatrics]] |
[[Category:Pediatrics]] |
Revision as of 19:39, 15 August 2020
Background
- Primary immunodeficiency of neutrophils leading to recurrent infections with catalase-positive organisms
Pathophysiology
- Defect in NADPH oxidase
- Therefore unable to generate superoxide radicals required by phagocytes to kill pathogens
Clinical Manifestations
- Recurrent infections with catalase-positive organisms, including Staphylococcus aureus
- Highest-risk group for invasive aspergillosis
Differential Diagnosis
- Other primary immunodeficiencies
- MPO deficiency, which will have an abnormal DHR test but largely asymptomatic unless concurrent diabetes mellitus
- Hyper-IgE syndrome, though Aspergillus will be more typically pulmonary
- IRAK4/MyD88 deficiency, which won't have fungal infections and improves with age
- Humoral immunodeficiencies, such as CVID or Bruton tyrosine kinase deficiency, though they tend to have more infections with encapsulated organisms and will have abnormal quantitative immunoglobulins
- Inflammatory bowel disease
- Cystic fibrosis
- Sarcoidosis
Diagnosis
- The diagnosis is confirmed with the dihyohodamine-123 (DHR-123) test
Management
- Treat intercurrent infections
- Prophylaxis with:
- TMP-SMX
- Itraconazole
- Possibly also interferon-γ
Further Reading
- Considerations in the Diagnosis of Chronic Granulomatous Disease. J Pediatric Infect Dis Soc. 2018;7(S1):S6-S11. doi: 10.1093/jpids/piy007