Fabry's disease: Difference between revisions

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*Burning pain of the extremities. This pain can become very intense, especially when one has a fever.  
*Burning pain of the extremities. This pain can become very intense, especially when one has a fever.  
*[[Loss of vision]] or blurry vision from corneal opacities.
*[[Loss of vision]] or blurry vision from corneal opacities.
*Difficulty swallowing ([[dysphagia]])
*[[Abdominal pain]]
*[[Abdominal pain]]
*Greasy stools ([[steatorrhea]])
*[[Chest pain]] and [[palpitations]]
*[[Chest pain]] and [[palpitations]]
*[[Delayed puberty]]
*[[Delayed puberty]]
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*[[Loss of sensation]]s in extremities
*[[Loss of sensation]]s in extremities
*[[Telangiectasis]]
*[[Telangiectasis]]
*Lack of coordination of muscle movement ([[ataxia]])
===Physical Examination===
====Appearance====
*Severe [[growth impairment]]
*Extreme mental and motor retardation
====Vital Signs====
*[[Systemic blood pressure]] may be raised
*[[Pyrexia of unknown origin]]
====Skin====
*[[Angiokeratomas]]
*[[Hypohidrosis]]
*[[Rash]]
*[[Telangiectasias]]
====Head====
*Neck retraction
==== Eyes ====
*Decreased [[visual acuity]]: [[Loss of vision]] or [[blurring of vision]]
*[[Corneal opacity]]
*[[Fundoscopy]]:
**Retinal pathology
==== Ear ====
*[[Sensorineural hearing loss]]
==== Heart ====
==== Abdomen ====
*[[Hepatomegaly]]
*[[Splenomegaly]]
==== Extremities ====
*[[Raynauds phenomenon]]
==== Neurologic ====
*[[Mental retardation]]
*[[Growth retardation]]
*Gradual loss of intellect
*[[Motor retardation]]
*[[Ataxia]]
*[[Seizure]]s
*[[Spasticity]]
*[[Peripheral neuropathy]]
==== Other ====
*[[Fractures]] from [[Osteoporosis|osteoporotic bone]]
*[[Delayed puberty]]: lack of development of [[secondary sexual characteristics]]
*Male [[infertility]]
*[[Priapism]]
=== Laboratory Findings ===
*Blood tests
**[[Anemia]]
**[[Serum creatinine]] may be raised from [[chronic renal failure]]
**Serum [[urea]] may be elevated
**[[BUN]] may be raised
*[[Urinalysis]]:
**[[Hematuria]]
**[[Proteinuria]]
====ECG abnormalities====
*[[AV node]] conduction block
*[[PR interval]] shortening
*[[Arrhythmia]]s
==== Ultrasound ====
*[[Hemangiomas]]


==Treatment==
==Treatment==

Revision as of 03:36, 14 August 2012

Template:DiseaseDisorder infobox Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1];Associate Editor(s)-in-Chief: Aarti Narayan, M.B.B.S [2]

Synonyms and keywords: Anderson-Fabry disease; angiokeratoma corporis diffusum universale; alpha-glucosidase A deficiency; ceramide trihexosidase deficiency; hereditary dystopic lipidosis; GLA deficiency; Sweeley-Klionsky disease

Overview

Fabry disease is an X-linked recessive inherited lysosomal storage disease, characterized by abnormal accumulation of ceramide trihexose in cardiovascular and renal systems.

Historical Perspective

It was named after Johannes Fabry.[1]

Classification

  • Non-neuropathic form
  • Neuropathic form
    • Infantile form
    • Juvenile form

Pathophysiology

  • Fabry's disease follows an X-linked recessive inheritance pattern.
  • A deficiency of the enzyme alpha galactosidase A causes a glycolipid known as globotriaosylceramide (also abbreviated as Gb3, GL-3, or ceramide trihexoside) to accumulate within the blood vessels, mononuclear phagocytes, neurons, other tissues, and organs.
  • This accumulation leads to an impairment of their proper function. The condition affects hemizygous males, as well as both heterozygous and homozygous females; males tend to experience the most severe clinical symptoms, while females vary from virtually no symptoms to those as serious as males.
  • This variability is thought to be due to X-inactivation patterns during embryonic development of the female.

Epidemiology and Demographics

The prevalence of Fabry disease is estimated to range from 1:17,000 to 1:117,000 males in Caucasian populations.[2][3]

Diagnosis

Symptoms

Physical Examination

Appearance

Vital Signs

Skin

Head

  • Neck retraction

Eyes

Ear

Heart

Abdomen

Extremities

Neurologic

Other

Laboratory Findings

ECG abnormalities

Ultrasound


Treatment

  • Until recently, treatment of Fabry's disease targeted the symptomatic effects. However, it is currently being treated at the cellular level through enzyme replacement therapy using Agalsidase alpha (Replagal) and Agalsidase beta (Fabrazyme®).
  • The cost of these drugs is problematic (approximately $170,000 US a year/patient) and remains a barrier to many patients in some countries. Enzyme replacement therapy (typically infused every two weeks) may be performed in the patient's home by the patients themselves. Enzyme replacement therapy is not a cure, and must be infused recurrently for maximum benefit.

References

  1. Template:WhoNamedIt
  2. Branton MH, Schiffmann R, Sabnis SG; et al. (2002). "Natural history of Fabry renal disease: influence of alpha-galactosidase A activity and genetic mutations on clinical course". Medicine. 81 (2): 122–38. PMID 11889412. Unknown parameter |month= ignored (help)
  3. Meikle PJ, Hopwood JJ, Clague AE, Carey WF (1999). "Prevalence of lysosomal storage disorders". JAMA : the Journal of the American Medical Association. 281 (3): 249–54. PMID 9918480. Unknown parameter |month= ignored (help)

External links


de:Morbus Fabry fi:Fabryn tauti

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