(medicine) A hereditary metabolic disorder, transmitted as an autosomal recessive, characterized by excessive amounts of heparitin sulfate in the urine, and manifested by minor skeletal changes and slight hepatomegaly.
Sanfilippo syndrome
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(san·fə′lip·ōz ′sin′drōm)
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| Medical Dictionary: San·fi·lip·po's syndrome |
(săn'fə-lĭp'ōz)
n.
n.
An inherited disorder of mucopolysaccharide metabolism, characterized by the presence of heparitin sulfate in the urine, enlargement of the liver, severe mental retardation, and, sometimes, skeletal abnormalities. Also called type III mucopolysaccharidosis.
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| Sanfilippo Syndrome | |
|---|---|
| Classification and external resources | |
| ICD-10 | E76.2 |
| ICD-9 | 277.5 |
| OMIM | 252900 252920 252940 252930 |
| DiseasesDB | 29177 |
| MedlinePlus | 001210 |
| eMedicine | ped/2040 |
| MeSH | D009084 |
Sanfilippo syndrome, or Mucopolysaccharidosis III (MPS-III) is a rare autosomal recessive lysosomal storage disease caused by a deficiency in one of the enzymes needed to break down the glycosaminoglycan heparan sulfate (which is found in the extra-cellular matrix and on cell surface glycoproteins).
Although undegraded heparan sulfate is the primary stored substrate, glycolipids such as gangliosides are also stored despite no genetic defect in the enzymes associated with their breakdown.
The condition is named for Sylvester Sanfilippo.[1][2]
Contents |
Genetic prevalence
MPS-III has an incidence of approximately 1.89 per 100 000 live births.[citation needed] Higher rates are found in certain populations such as the Ashkenazi Jews.[citation needed]
The four types of MPS-III are due to specific enzyme deficiencies affecting the breakdown of heparan sulfate, which then builds up in various organs. All four types have autosomal recessive inheritance.
| MPS-III type | enzyme | gene location |
|---|---|---|
| MPS-III A | heparan N-sulfatase | 17q25.3 |
| MPS-III B | N-acetyl-alpha-D-glucosaminidase | 17q21 |
| MPS-III C | acetyl-CoA:alpha-glucosaminide acetyltransferase | 8p11-q13 |
| MPS-III D | N-acetylglucosamine-G-sulfate sulfatase | 12q14 |
Diagnosis and Natural History
It should be noted that MPS-III A, B, C and D are considered to be clinically indistinguishable, although mutations in different genes are responsible for each disease. The following discussion is therefore applicable to all four conditions.
The disease manifests in young children. Affected infants are apparently normal, although some mild facial dysmorphism may be noticeable. The stiff joints, hirsuteness and coarse hair typical of other mucopolysaccharidoses are usually not present until late in the disease. The child often develops normally initially. Acquisition of speech is often slow and incomplete. The disease then progresses to increasing behavioural disturbance including temper tantrums, hyperactivity, destructiveness, aggressive behaviour, pica and sleep disturbance. As affected children have normal muscle strength and mobility, the behavioural disturbances are very difficult to manage. The disordered sleep in particular presents a significant problem to care providers. In the final phase of the illness, children become increasingly immobile and unresponsive, often require wheelchairs, and develop swallowing difficulties and seizures. Death eventually results from inanition. The life-span of an affected child does not usually extend beyond late teens to early twenties.
Although the clinical features of the disease are mainly neurological, patients may also develop diarrhea, carious teeth, and an enlarged liver and spleen. There is a broad range of clinical severity. The disease may very rarely present later in life as a psychotic episode.
The diagnosis may be confirmed by assay of enzyme levels in tissue samples and gene sequencing. Prenatal diagnosis is possible.
Treatment
Treatment remains largely supportive. The behavioral disturbances of MPS-III respond poorly to medication. If an early diagnosis is made, bone marrow replacement may be beneficial. Although the missing enzyme can be manufactured and given intravenously, it cannot penetrate the blood-brain barrier and therefore cannot treat the neurological manifestations of the disease.
Along with many other lysosomal storage diseases, MPS-III exists as a model of a monogenetic disease involving the central nervous system. Several promising therapies are in development. Gene therapy is under investigation for MPS-III in animal models. Other potential therapies include chemical modification of deficient enzymes to allow them to penetrate the brain blood-brain barrier, stabilisation of abnormal but active enzyme to prevent its degradation, and implantation of stem cells strongly expressing the missing enzyme. For any future treatment to be successful, it must be administered as early as possible. Currently MPS-III is mainly diagnosed clinically, by which stage it is probably too late for any treatment to be very effective. Neonatal screening programs would provide the earliest possible diagnosis.
See also
References
- ^ "eMedicine - Mucopolysaccharidosis Type III : Article by Germaine L Defendi". http://www.emedicine.com/ped/topic2040.htm.
- ^ Sanfilippo, S. J.; Podosin, R.; Langer, L. O., Jr.; Good, R. A. : Mental retardation associated with acid mucopolysacchariduria (heparitin sulfate type). J. Pediat. 63: 837-838, 1963.
External links
- The National MPS Society page on MPS-III
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Mentioned in
- Alpha-N-acetylglucosaminidase
- Lysosomal storage disease
- N-acetylglucosamine-6-sulfatase
- Heparan-alpha-glucosaminide N-acetyltransferase
- Mucopolysaccharidosis
- List of incurable diseases
- HGSNAT
- List of diseases (S)
- Hematopoietic stem cell transplantation
- ICD-10 Chapter IV: Endocrine, nutritional and metabolic diseases
