Chédiak-Higashi syndrome: Difference between revisions
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There are several manifestations of Chediak-Hegashi syndrome as mentioned above; however, [[neutropenia]] seems to be the most common. The syndrome is also associated with [[Albinism|oculocutaneous albinism]]. Persons are also prone for infections, especially with Staph. Aureus. | There are several manifestations of Chediak-Hegashi syndrome as mentioned above; however, [[neutropenia]] seems to be the most common. The syndrome is also associated with [[Albinism|oculocutaneous albinism]]. Persons are also prone for infections, especially with Staph. Aureus. | ||
Associated features: Abnormalities in melanocytes (albinism), nerve defects, bleeding disorders. | Associated features: Abnormalities in melanocytes (albinism), nerve defects, bleeding disorders. | ||
==Treatment== | |||
There is no specific treatment for Chédiak–Higashi syndrome. Bone marrow transplants appear to have been successful in several patients. Infections are treated with antibiotics and abscesses are surgically drained when appropriate. Antiviral drugs such as acyclovir have been tried during the | |||
terminal phase of the disease. Cyclophosphamide and prednisone have been tried. Vitamin C therapy has improved immune function and clotting in some patients.<ref name="medline" /> | |||
==See also== | ==See also== | ||
Revision as of 19:48, 27 July 2012
| Chédiak-Higashi syndrome | |
| ICD-10 | E70.3 (E70.340 ILDS) |
|---|---|
| ICD-9 | 288.2 |
| OMIM | 214500 |
| DiseasesDB | 2351 |
| eMedicine | derm/704 |
| MeSH | D002609 |
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Overview
Chédiak-Higashi syndrome is a rare childhood autosomal recessive disorder that affects multiple systems of the body, and arises from a mutation in the lysosomal trafficking regulator gene, LYST.
It is a disease with impaired bacteriolysis due to failure of phagolysosome formation. As a result of disordered intracellular trafficking there is impaired lysosome degranulation with phagosomes, so phagocytosed bacteria are not destroyed by the lysosome's enzymes.
In addition, secretion of lytic secretory granules by cytotoxic T cells is also affected.
The disease is characterised by large lysosome vesicles in phagocytes (neutrophils), which thus have poor bactericidal function, leading to susceptibility to infections, abnormalities in nuclear structure of leukocytes, anaemia, and hepatomegaly.
Clinical findings
There are several manifestations of Chediak-Hegashi syndrome as mentioned above; however, neutropenia seems to be the most common. The syndrome is also associated with oculocutaneous albinism. Persons are also prone for infections, especially with Staph. Aureus.
Associated features: Abnormalities in melanocytes (albinism), nerve defects, bleeding disorders.
Treatment
There is no specific treatment for Chédiak–Higashi syndrome. Bone marrow transplants appear to have been successful in several patients. Infections are treated with antibiotics and abscesses are surgically drained when appropriate. Antiviral drugs such as acyclovir have been tried during the terminal phase of the disease. Cyclophosphamide and prednisone have been tried. Vitamin C therapy has improved immune function and clotting in some patients.[1]
See also
- Griscelli syndrome (also known as "Chédiak-Higashi like syndrome")