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Wiskott-Aldrich Syndrome

Wiskott-Aldrich Syndrome is a topic covered in the Select 5-Minute Pediatrics Topics.

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Basics

Description

  • An X-linked primary immunodeficiency caused by a mutation in the Wiskott-Aldrich syndrome (WAS) gene
  • Originally described as clinical triad of thrombocytopenia with small platelets, eczema, and recurrent infections with opportunistic and pyogenic organisms
  • Increased bleeding tendency secondary to thrombocytopenia likely results from impaired platelet production, increased turnover, and defective function.
  • Disease variants also resulting from WAS gene mutations include X-linked thrombocytopenia (XLT) and X-linked neutropenia (XLN).
  • Classic WAS is characterized by broad immunodeficiency, decreased number and function of T cells, disturbed marginal B-cell homeostasis, and skewed immunoglobulin isotypes, with defective antibody responses to vaccinations, impaired NK-cell cytotoxicity, and abnormal regulatory T-cell function as well as reduced phagocyte chemotaxis.

Epidemiology

  • Presents in infancy with serious bleeding episodes secondary to thrombocytopenia (such as circumcision with increased bleeding, bloody diarrhea, ecchymoses)
  • Recurrent infections usually start after 6 months of age:
    • Bacterial: otitis media, sinusitis, meningitis, sepsis, and pneumonia
    • Viral infections: herpes simplex virus, varicella with systemic complications
  • Milder phenotypes may lack history of recurrent infections.
  • Decline in T- and B-cell numbers with time
  • Eczema is usually present by 1 year of age (may be resistant to therapy, sometimes requiring systemic antibiotics).

Incidence

  • For WAS/XLT, estimate is 10 in 1 million live births.
  • Prevalence of XLT equal to WAS

Risk Factors

Genetics

  • X-linked recessive disease
  • Defective Wiskott-Aldrich syndrome protein gene located on X p11.22p–11.23
  • ∼60% of cases will have a positive family history for WAS.
  • XLT without the other findings is caused by mutations of the same gene.
  • Genotype/phenotype correlation
    • Lack of Wiskott-Aldrich syndrome protein (WASP) expression: increased infections, severe eczema, intestinal hemorrhage, death from intracranial bleeding, and malignancies
    • Survival rate significantly lower in WASP-negative patients

Etiology

  • Mutations in the gene for the WASP
  • WASP is involved in the reorganization of the actin cytoskeleton in hematopoietic cells:
    • Following activation of WASP, reorganization of actin cytoskeleton results in polarization of cells (e.g., polarized actin mesh in platelets for clotting and in macrophages for phagocytosis, and polarization of T or B cells to form immunologic synapses).
  • WASP is a cytoplasmic protein involved in cell mobility, immune regulation, cell signaling, cell-to-cell interactions, signaling, and cytotoxicity.
  • Defects in WASP can lead to dysfunction in adaptive and innate immunity, immune surveillance, and platelet homeostasis and function as well as neutropenia.
  • “Classic” WAS and XLT result from loss-of-function mutations.
  • XLT can be misdiagnosed as idiopathic thrombocytopenic purpura (ITP) that does not carry increased risk of malignancy, so testing for WASP expression and WAS gene mutation is important in any male with thrombocytopenia and small platelets.
  • XLN results from “activating” mutations in WAS that lead to increased actin polymerization; profound neutropenia, with or without associated lymphopenia; decreased T-cell proliferation in vitro; and increased risk of myelodysplastic changes in bone marrow.
  • WASP is also important for regulatory T-cell function.

Commonly Associated Conditions

Associated with IgA nephropathy, autoimmune disorders, and an increased incidence of B-cell lymphomas

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Citation

Cabana, Michael D., editor. "Wiskott-Aldrich Syndrome." Select 5-Minute Pediatrics Topics, 7th ed., Wolters Kluwer Health, 2015. Medicine Central, im.unboundmedicine.com/medicine/view/Select-5-Minute-Pediatric-Consult/14036/all/Wiskott_Aldrich_Syndrome.
Wiskott-Aldrich Syndrome. In: Cabana MD, ed. Select 5-Minute Pediatrics Topics. 7th ed. Wolters Kluwer Health; 2015. https://im.unboundmedicine.com/medicine/view/Select-5-Minute-Pediatric-Consult/14036/all/Wiskott_Aldrich_Syndrome. Accessed August 21, 2019.
Wiskott-Aldrich Syndrome. (2015). In Cabana, M. D. (Ed.), Select 5-Minute Pediatrics Topics. Available from https://im.unboundmedicine.com/medicine/view/Select-5-Minute-Pediatric-Consult/14036/all/Wiskott_Aldrich_Syndrome
Wiskott-Aldrich Syndrome [Internet]. In: Cabana MD, editors. Select 5-Minute Pediatrics Topics. Wolters Kluwer Health; 2015. [cited 2019 August 21]. Available from: https://im.unboundmedicine.com/medicine/view/Select-5-Minute-Pediatric-Consult/14036/all/Wiskott_Aldrich_Syndrome.
* Article titles in AMA citation format should be in sentence-case
TY - ELEC T1 - Wiskott-Aldrich Syndrome ID - 14036 ED - Cabana,Michael D, BT - Select 5-Minute Pediatrics Topics UR - https://im.unboundmedicine.com/medicine/view/Select-5-Minute-Pediatric-Consult/14036/all/Wiskott_Aldrich_Syndrome PB - Wolters Kluwer Health ET - 7 DB - Medicine Central DP - Unbound Medicine ER -