Seckel Syndrome: Difference between revisions
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== | == Definition == | ||
Seckel Syndrome also known as microcephalic primordial dwarfism is an extremely rare congenital disorder. This condition is a heterogenous, autosomal recessive disorder. It has been linked to harmful changes in genes that are responsible for maintaining genomic stability. The onset is prenatal and continues postnatally causing severe microcephaly, a bird like face, dwarfism and severe intellectual disability.<ref name=":0">National Organization for Rare Disorders (NORD). Seckel Syndrome. Available from: [[/urlofelectronicpublication/|http://URLofelectronicpublication]] (accessed 29/March/2022)</ref><ref name=":1">James Wynbrandt, Mark Ludman. SC Syndrome. In: The Encyclopedia of Genetic Disorders and Birth Defects. Infobase Publishing.FEB 2008. p344</ref> | |||
== | == Prevalence == | ||
Seckel Syndrome is a rare genetic disorder that affects about 1 in 10, 000 individuals. It affects males and females equally. <br> | |||
== | == Etiology == | ||
Seckel Syndrome is a rare genetic condition that is inherited in an autosomal recessive manner. Listed below are multiple variations of Seckel Syndrome caused by gene mutations on multiple chromosomes. | |||
* Seckel syndrome 1: ataxia-telangiectasia and Rad3-related protein (''ATR'') gene | |||
* Seckel syndrome 2: RB binding protein 8 (''RBBP8'') gene | |||
* Seckel syndrome 4: centromere protein J (''CENPJ'') gene | |||
* Seckel syndrome 5: centrosomal protein 152 (''CEP152'') gene | |||
* Seckel syndrome 6: centrosomal protein 63 (''CEP63'') gene | |||
* Seckel syndrome 7: ninein (''NIN'') gene | |||
* Seckel syndrome 8: DNA 2 protein (''DNA2'') gene | |||
* Seckel syndrome 9: ATR interacting protein (''ATRIP'') gene | |||
* Seckel syndrome 10: SMC5-SMC6 complex SUMO ligase (''NSMCE2'') gene | |||
= | <ref name=":0" /> | ||
== Characteristics/Clinical Presentation == | |||
* Low birth weight | |||
* Dwarfism | |||
* Microcephaly | |||
* Large eyes | |||
* Large prominent nose with beak like protrusion | |||
* Narrow face | |||
* Small brain size | |||
* Clubfoot | |||
* Scoliosis | |||
* Cross eyed | |||
* Underdeveloped thumbs | |||
* Dislocation of the heads of the femurs head out of the acetabulum | |||
* Malformation of genitourinary system | |||
* Intellectual disability (IQ below 50) | |||
<ref name=":1" /><ref name=":0" /><br> | |||
== | == Diagnostics == | ||
Seckel Syndrome can be diagnosed prenatally via ultrasound. Seckel syndrome is suspected if a fetus has a small head, slow growth and changes to the head and face associated to the condition. | |||
Genetic testing can also be used to diagnose pre or postnatally. | |||
In some cases a diagnosis may not be confirmed until the child grows older and exhibits delays in development associated with intellectual disability or height. <ref name=":0" /><br> | |||
== Medical Management == | |||
Thee is no cure for Seckel Syndrome. Treatment is supportive. Therapeutic and Medical management mostly focuses on treating associated hematological abnormalities (anemia, pancytipenia, acute myeloid leukaemia) and supporting the family and the child functional impairments. | |||
== References == | == References == | ||
<references /> | <references /> | ||
Revision as of 02:58, 30 March 2022
Top Contributors - Ravi Kumar, Sukhi Dhaliwal, Uchechukwu Chukwuemeka, Kim Jackson and Vidya Acharya
Definition[edit | edit source]
Seckel Syndrome also known as microcephalic primordial dwarfism is an extremely rare congenital disorder. This condition is a heterogenous, autosomal recessive disorder. It has been linked to harmful changes in genes that are responsible for maintaining genomic stability. The onset is prenatal and continues postnatally causing severe microcephaly, a bird like face, dwarfism and severe intellectual disability.[1][2]
Prevalence[edit | edit source]
Seckel Syndrome is a rare genetic disorder that affects about 1 in 10, 000 individuals. It affects males and females equally.
Etiology[edit | edit source]
Seckel Syndrome is a rare genetic condition that is inherited in an autosomal recessive manner. Listed below are multiple variations of Seckel Syndrome caused by gene mutations on multiple chromosomes.
- Seckel syndrome 1: ataxia-telangiectasia and Rad3-related protein (ATR) gene
- Seckel syndrome 2: RB binding protein 8 (RBBP8) gene
- Seckel syndrome 4: centromere protein J (CENPJ) gene
- Seckel syndrome 5: centrosomal protein 152 (CEP152) gene
- Seckel syndrome 6: centrosomal protein 63 (CEP63) gene
- Seckel syndrome 7: ninein (NIN) gene
- Seckel syndrome 8: DNA 2 protein (DNA2) gene
- Seckel syndrome 9: ATR interacting protein (ATRIP) gene
- Seckel syndrome 10: SMC5-SMC6 complex SUMO ligase (NSMCE2) gene
Characteristics/Clinical Presentation[edit | edit source]
- Low birth weight
- Dwarfism
- Microcephaly
- Large eyes
- Large prominent nose with beak like protrusion
- Narrow face
- Small brain size
- Clubfoot
- Scoliosis
- Cross eyed
- Underdeveloped thumbs
- Dislocation of the heads of the femurs head out of the acetabulum
- Malformation of genitourinary system
- Intellectual disability (IQ below 50)
Diagnostics[edit | edit source]
Seckel Syndrome can be diagnosed prenatally via ultrasound. Seckel syndrome is suspected if a fetus has a small head, slow growth and changes to the head and face associated to the condition.
Genetic testing can also be used to diagnose pre or postnatally.
In some cases a diagnosis may not be confirmed until the child grows older and exhibits delays in development associated with intellectual disability or height. [1]
Medical Management[edit | edit source]
Thee is no cure for Seckel Syndrome. Treatment is supportive. Therapeutic and Medical management mostly focuses on treating associated hematological abnormalities (anemia, pancytipenia, acute myeloid leukaemia) and supporting the family and the child functional impairments.
References[edit | edit source]
- ↑ 1.0 1.1 1.2 1.3 National Organization for Rare Disorders (NORD). Seckel Syndrome. Available from: http://URLofelectronicpublication (accessed 29/March/2022)
- ↑ 2.0 2.1 James Wynbrandt, Mark Ludman. SC Syndrome. In: The Encyclopedia of Genetic Disorders and Birth Defects. Infobase Publishing.FEB 2008. p344
