Aspartylglucosaminuria: Difference between revisions
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[[File:Autosomal_recessive_-_en.svg| | {{SI}} | ||
{{Infobox medical condition | |||
| name = Aspartylglucosaminuria | |||
| image = [[File:Autosomal_recessive_-_en.svg|200px]] | |||
| caption = Aspartylglucosaminuria is inherited in an [[autosomal recessive]] pattern. | |||
| synonyms = AGU | |||
| pronounce = | |||
| specialty = [[Medical genetics]] | |||
| symptoms = Developmental delay, [[intellectual disability]], [[coarse facial features]], [[joint laxity]] | |||
| onset = Infancy | |||
| duration = Lifelong | |||
| causes = Mutations in the [[AGA (gene)|AGA gene]] | |||
| risks = | |||
| diagnosis = [[Genetic testing]], [[urine analysis]] | |||
| differential = Other [[lysosomal storage disorders]] | |||
| treatment = Supportive care, [[physical therapy]], [[speech therapy]] | |||
| medication = | |||
| prognosis = Progressive, variable | |||
| frequency = Rare | |||
| deaths = | |||
}} | |||
'''Aspartylglucosaminuria''' (AGU) is a rare [[autosomal recessive]] [[lysosomal storage disorder]] that affects the [[glycoprotein]] degradation pathway. It is characterized by the accumulation of [[aspartylglucosamine]] in the [[lysosomes]] of various tissues due to a deficiency in the enzyme [[aspartylglucosaminidase]]. | |||
== Genetics == | == Genetics == | ||
Aspartylglucosaminuria is caused by mutations in the [[AGA (gene)|AGA gene]], which encodes the enzyme aspartylglucosaminidase. This enzyme is responsible for breaking down glycoproteins in the lysosomes. The disorder follows an autosomal recessive inheritance pattern, meaning that an individual must inherit two defective copies of the gene, one from each parent, to manifest the disease. | Aspartylglucosaminuria is caused by mutations in the [[AGA (gene)|AGA gene]], which encodes the enzyme aspartylglucosaminidase. This enzyme is responsible for breaking down glycoproteins in the lysosomes. The disorder follows an autosomal recessive inheritance pattern, meaning that an individual must inherit two defective copies of the gene, one from each parent, to manifest the disease. | ||
== Pathophysiology == | == Pathophysiology == | ||
The deficiency of aspartylglucosaminidase leads to the accumulation of glycoasparagine in the lysosomes. This accumulation disrupts normal cellular function and leads to the progressive symptoms observed in individuals with AGU. The buildup of these substances primarily affects the [[central nervous system]], but other organs can also be involved. | The deficiency of aspartylglucosaminidase leads to the accumulation of glycoasparagine in the lysosomes. This accumulation disrupts normal cellular function and leads to the progressive symptoms observed in individuals with AGU. The buildup of these substances primarily affects the [[central nervous system]], but other organs can also be involved. | ||
== Clinical Features == | == Clinical Features == | ||
Symptoms of aspartylglucosaminuria typically appear in early childhood and progressively worsen over time. Common clinical features include: | Symptoms of aspartylglucosaminuria typically appear in early childhood and progressively worsen over time. Common clinical features include: | ||
| Line 15: | Line 33: | ||
* Joint stiffness | * Joint stiffness | ||
* Motor dysfunction | * Motor dysfunction | ||
== Diagnosis == | == Diagnosis == | ||
Diagnosis of AGU is based on clinical evaluation, biochemical testing, and genetic testing. Elevated levels of glycoasparagine in the urine can be indicative of the disorder. Genetic testing can confirm the diagnosis by identifying mutations in the AGA gene. | Diagnosis of AGU is based on clinical evaluation, biochemical testing, and genetic testing. Elevated levels of glycoasparagine in the urine can be indicative of the disorder. Genetic testing can confirm the diagnosis by identifying mutations in the AGA gene. | ||
== Treatment == | == Treatment == | ||
Currently, there is no cure for aspartylglucosaminuria. Treatment is primarily supportive and focuses on managing symptoms and improving the quality of life for affected individuals. This may include physical therapy, occupational therapy, and educational support. | Currently, there is no cure for aspartylglucosaminuria. Treatment is primarily supportive and focuses on managing symptoms and improving the quality of life for affected individuals. This may include physical therapy, occupational therapy, and educational support. | ||
== Epidemiology == | == Epidemiology == | ||
Aspartylglucosaminuria is a rare disorder, with a higher prevalence in certain populations, such as the [[Finnish population]]. The incidence in Finland is estimated to be approximately 1 in 18,500 births. | Aspartylglucosaminuria is a rare disorder, with a higher prevalence in certain populations, such as the [[Finnish population]]. The incidence in Finland is estimated to be approximately 1 in 18,500 births. | ||
== Research == | == Research == | ||
Ongoing research aims to better understand the molecular mechanisms of AGU and to develop potential therapies. Gene therapy and enzyme replacement therapy are areas of active investigation. | Ongoing research aims to better understand the molecular mechanisms of AGU and to develop potential therapies. Gene therapy and enzyme replacement therapy are areas of active investigation. | ||
== See also == | == See also == | ||
* [[Lysosomal storage disease]] | * [[Lysosomal storage disease]] | ||
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* [[Glycoprotein]] | * [[Glycoprotein]] | ||
* [[Enzyme replacement therapy]] | * [[Enzyme replacement therapy]] | ||
== References == | == References == | ||
{{Reflist}} | {{Reflist}} | ||
== External links == | == External links == | ||
{{No external links}} | {{No external links}} | ||
[[Category:Genetic disorders]] | [[Category:Genetic disorders]] | ||
[[Category:Lysosomal storage diseases]] | [[Category:Lysosomal storage diseases]] | ||
| Line 45: | Line 55: | ||
[[Category:Neurological disorders]] | [[Category:Neurological disorders]] | ||
[[Category:Rare diseases]] | [[Category:Rare diseases]] | ||
{{medicine-stub}} | {{medicine-stub}} | ||
Latest revision as of 17:09, 4 April 2025
Editor-In-Chief: Prab R Tumpati, MD
Obesity, Sleep & Internal medicine
Founder, WikiMD Wellnesspedia &
W8MD medical weight loss NYC and sleep center NYC
| Aspartylglucosaminuria | |
|---|---|
| |
| Synonyms | AGU |
| Pronounce | |
| Specialty | Medical genetics |
| Symptoms | Developmental delay, intellectual disability, coarse facial features, joint laxity |
| Complications | N/A |
| Onset | Infancy |
| Duration | Lifelong |
| Types | N/A |
| Causes | Mutations in the AGA gene |
| Risks | |
| Diagnosis | Genetic testing, urine analysis |
| Differential diagnosis | Other lysosomal storage disorders |
| Prevention | N/A |
| Treatment | Supportive care, physical therapy, speech therapy |
| Medication | |
| Prognosis | Progressive, variable |
| Frequency | Rare |
| Deaths | |
Aspartylglucosaminuria (AGU) is a rare autosomal recessive lysosomal storage disorder that affects the glycoprotein degradation pathway. It is characterized by the accumulation of aspartylglucosamine in the lysosomes of various tissues due to a deficiency in the enzyme aspartylglucosaminidase.
Genetics[edit]
Aspartylglucosaminuria is caused by mutations in the AGA gene, which encodes the enzyme aspartylglucosaminidase. This enzyme is responsible for breaking down glycoproteins in the lysosomes. The disorder follows an autosomal recessive inheritance pattern, meaning that an individual must inherit two defective copies of the gene, one from each parent, to manifest the disease.
Pathophysiology[edit]
The deficiency of aspartylglucosaminidase leads to the accumulation of glycoasparagine in the lysosomes. This accumulation disrupts normal cellular function and leads to the progressive symptoms observed in individuals with AGU. The buildup of these substances primarily affects the central nervous system, but other organs can also be involved.
Clinical Features[edit]
Symptoms of aspartylglucosaminuria typically appear in early childhood and progressively worsen over time. Common clinical features include:
- Developmental delay
- Intellectual disability
- Coarse facial features
- Skeletal abnormalities
- Joint stiffness
- Motor dysfunction
Diagnosis[edit]
Diagnosis of AGU is based on clinical evaluation, biochemical testing, and genetic testing. Elevated levels of glycoasparagine in the urine can be indicative of the disorder. Genetic testing can confirm the diagnosis by identifying mutations in the AGA gene.
Treatment[edit]
Currently, there is no cure for aspartylglucosaminuria. Treatment is primarily supportive and focuses on managing symptoms and improving the quality of life for affected individuals. This may include physical therapy, occupational therapy, and educational support.
Epidemiology[edit]
Aspartylglucosaminuria is a rare disorder, with a higher prevalence in certain populations, such as the Finnish population. The incidence in Finland is estimated to be approximately 1 in 18,500 births.
Research[edit]
Ongoing research aims to better understand the molecular mechanisms of AGU and to develop potential therapies. Gene therapy and enzyme replacement therapy are areas of active investigation.
See also[edit]
References[edit]
<references group="" responsive="1"></references>
External links[edit]
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