Sotos Syndrome 1

  1. Home
  2. Sotos Syndrome 1

Alternative Names

  • SOTOS1
  • Sotos Syndrome
  • Cerebral Gigantism
  • Chromosome 5q35 deletion syndrome

Associated Genes

Nuclear Receptor-Binding Set Domain Protein1
Back to search Result
WHO-ICD-10 version:2010

Congenital malformations, deformations and chromosomal abnormalities

Other congenital malformations

OMIM Number

117550

Mode of Inheritance

Autosomal Dominant

Gene Map Locus

5q35.3

Description

Sotos syndrome is a rare autosomal dominant congenital developmental disorder characterized by overgrowth with advanced bone age, craniofacial anomalies, developmental delay, and occasional seizures. The disease occurs at an incidence rate of nearly 1 in 14,000 births. The facial gestalt is very characteristic during childhood with macrocephaly, frontal bossing, prognathism, hypertelorism, and antimongoloid slant of the palpebral fissures. With increasing age, the face gradually lengthens, the jaw becomes more prominent, and macrocephaly is no longer pronounced. The hands and feet are usually large. In infancy growth is rapid, but settles down above the >97th centile in early childhood and tends to follow this during childhood. Height and weight tends to normalize in adulthood. Neurological features are variable and include hypotonia and delay in motor and language development, with a tendency for improvement with age. Sotos sysndrome is also frequently associated with brain, cardiovascular, and urinary anomalies and is occasionally accompanied with various malignancies, including acute lymphoblastic leukemia, lymphomas. Wilms tumor, and hepatocarcinoma.

Sotos syndrome is caused by haploinsufficiency of the NSD1 (nuclear receptor SET domain containing gene 1) gene. NSD1 is expressed in the fetal/adult brain, kidney, skeletal muscle, spleen, and the thymus, and faintly in the lung. The gene encodes 2696 amino acids with SET (su(var)3-9, enhancer-of-zeste, trithorax), PHD (plant homeodomain protein) finger, and PWWP (proline-tryptophan-tryptophan-proline) domains, all of which are possibly related to chromatin regulation, and possibly interact with nuclear receptors (Nrs). Among sporadic Sotos syndrome patients examined by direct sequencing, de novo point mutations predicting truncation of the protein and submicroscopic deletions involving the whole of NSD1 were identified. Two-thirds of Sotos syndrome cases showed NSD1 mutations, so haploinsufficiency of NSD1 is suggested to be the major molecular defect in Sotos syndrome.

Epidemiology in the Arab World

View Map
Subject IDCountrySexFamily HistoryParental ConsanguinityHPO TermsVariantZygosityMode of InheritanceReferenceRemarks
117550.1LebanonUnknownNo Hyperactivity; Short neck; Growth delay;...
Hyperactivity; Short neck; Growth delay; Global developmental delay click to copy
NM_022455.5:c.2339C>THeterozygousAutosomal, DominantJalkh et al. 2019
117550.2United Arab EmiratesMaleNoNo Global developmental delay; Failure to t...
Global developmental delay; Failure to thrive click to copy
NM_022455.4:c.3549dupHeterozygousSaleh et al. 2021 de novo mutation
117550.3Saudi ArabiaFemaleYes Abnormal facial shape; Hypoplasia of the...
Abnormal facial shape; Hypoplasia of the corpus callosum; Periventricular leukomalacia click to copy
NM_022455.5:c.2058T>AHeterozygousAutosomal, DominantMaddirevula et al. 2018 De novo mutation
117550.4Saudi ArabiaMaleNo Global developmental delay; Abnormal fac...
Global developmental delay; Abnormal facial shape; Overgrowth click to copy
NM_022455.5:c.1893delHeterozygousAutosomal, DominantMaddirevula et al. 2018 De novo mutation
Download Table

Other Reports

Egypt

[See: Saudi Arabia > Al Rashed et al., 1999].

Palestine

Nevo et al. (1974) described affected brother and sister and their affected double first cousin in an inbred Arab family. Two of the 3 showed generalized edema and flexion contractures of the feet at birth. It is possible that these features may represent a distinct disorder (i.e., Nevo syndrome).

Saudi Arabia

Al Rashed et al. (1999) described the clinical features of a series of 14 Arab children with Sotos Syndrome diagnosed between 1992 and 1997. The study cohort showed a marginal male predominance with eight boys and six girls. Of the 14 children, eight were Saudis, while there were three Egyptians, two Sudanese, and one Syrian. There was a high rate of consanguinity among the parents (36%), although there was no family history of the condition. More than half the patients had a history of delayed psychomotor development, and a fifth of the patients had had feeding and /or respiratory problems in the neonatal period. All the patients showed the presence of facial gestalt, 93% had microcephaly, 71% showed somatic gigantism, and six of eight psychometrically evaluated children showed mental retardation. More than half the children showed poor coordination, while two had spinal deformities. Six children had seizure disorders, and of these, three showed non-specific abnormal EEGs. Cranial CT scan revealed abnormalities in three children, which included ventricular dilatation in two and corpus callosum dysgenesis in the third.

Al-Mulla et al. (2004) reported a case of acute myeloid leukemia developing in a child with Sotos syndrome. He was treated with standard chemotherapy and achieved sustained remission.

Sudan

[See: Saudi Arabia > Al Rashed et al., 1999].

Syria

[See: Saudi Arabia > Al Rashed et al., 1999].

External Links

https://rarediseases.info.nih.gov/diseases/10091/disease

Contributors

  • Asha Deepthi: 08.02.2022
  • Pratibha Nair: 09.09.2021
  • Pratibha Nair: 10.11.2020
  • Pratibha Nair: 07.09.2014
  • Ghazi O. Tadmouri: 22.03.2007
  • Sarah Al-Haj Ali: 16.05.2005

Edit History

  • Sami Bizzari: 22.11.2022
  • Pratibha Nair: 09.11.2022
  • Asha Deepthi: 08.02.2022
  • Pratibha Nair: 09.09.2021
  • Pratibha Nair: 10.11.2020
  • Asha Deepthi: 02.05.2019
  • Pratibha Nair: 14.09.2014
  • Pratibha Nair: 16.09.2009
  • Sarah Al-Haj Ali: 20.11.2004
  • Sarah Al-Haj Ali: 09.11.2004
  • Ghazi O. Tadmouri: 28.02.2004
Back to search Result
© CAGS 2024. All rights reserved.
© CAGS 2024. All rights reserved.