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Genotype-phenotype associations in Sotos syndrome: an analysis of 266 individuals with NSD1 aberrations

Genotype-phenotype associations in Sotos syndrome: an analysis of 266 individuals with NSD1 aberrations
Genotype-phenotype associations in Sotos syndrome: an analysis of 266 individuals with NSD1 aberrations
We identified 266 individuals with intragenic NSD1 mutations or 5q35 microdeletions encompassing NSD1 (referred to as "NSD1-positive individuals"), through analyses of 530 subjects with diverse phenotypes. Truncating NSD1 mutations occurred throughout the gene, but pathogenic missense mutations occurred only in functional domains (P < 2 x 10(-16)). Sotos syndrome was clinically diagnosed in 99% of NSD1-positive individuals, independent of the molecular analyses, indicating that NSD1 aberrations are essentially specific to this condition. Furthermore, our data suggest that 93% of patients who have been clinically diagnosed with Sotos syndrome have identifiable NSD1 abnormalities, of which 83% are intragenic mutations and 10% are 5q35 microdeletions. We reviewed the clinical phenotypes of 239 NSD1-positive individuals. Facial dysmorphism, learning disability, and childhood overgrowth were present in 90% of the individuals. However, both the height and head circumference of 10% of the individuals were within the normal range, indicating that overgrowth is not obligatory for the diagnosis of Sotos syndrome. A broad spectrum of associated clinical features was also present, the occurrence of which was largely independent of genotype, since individuals with identical mutations had different phenotypes. We compared the phenotypes of patients with intragenic NSD1 mutations with those of patients with 5q35 microdeletions. Patients with microdeletions had less-prominent overgrowth (P = .0003) and more-severe learning disability (P = 3 x 10(-9)) than patients with mutations. However, all features present in patients with microdeletions were also observed in patients with mutations, and there was no correlation between deletion size and the clinical phenotype, suggesting that the deletion of additional genes in patients with 5q35 microdeletions has little specific effect on phenotype. We identified only 13 familial cases. The reasons for the low vertical transmission rate are unclear, although familial cases were more likely than nonfamilial cases (P = .005) to carry missense mutations, suggesting that the underlying NSD1 mutational mechanism in Sotos syndrome may influence reproductive fitness.
frameshift mutation, polymorphism, zinc fingers, gene deletion, cancer, human, mutation, growth disorders, genes, genetics, proteins, amino acid sequence, genetic, height, homozygote, sequence homology, exons, amino acid, syndrome, nuclear proteins, learning disorders, missense, research, male, disability, childhood, female, head, analysis, pair 5, patients, diagnosis, peptides, chromosomes, genotype, molecular sequence data, protein, pathology, prognosis, phenotype, facies, humans, research support, intracellular signaling peptides and proteins, non-U.S.gov't, abnormalities
0002-9297
193-204
Tatton-Brown, K.
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Douglas, J.
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Coleman, K.
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Baujat, G.
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Cole, T.R.
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Das, S.
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Horn, D.
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Hughes, H.E.
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Temple, I.K.
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Faravelli, F.
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Waggoner, D.
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Turkmen, S.
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Cormier-Daire, V.
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Irrthum, A.
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Rahman, N.
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Tatton-Brown, K.
587a8117-77e4-4869-ba22-913c536a77f2
Douglas, J.
060a8293-4c69-46a6-953e-9333d20c61f3
Coleman, K.
dfdbcae1-4ea8-49c1-a523-563d568b0094
Baujat, G.
9be0018b-7cd2-4a64-b8d4-204cc2a78df3
Cole, T.R.
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Das, S.
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Horn, D.
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Hughes, H.E.
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Temple, I.K.
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Faravelli, F.
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Waggoner, D.
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Turkmen, S.
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Cormier-Daire, V.
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Irrthum, A.
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Rahman, N.
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Tatton-Brown, K., Douglas, J., Coleman, K., Baujat, G., Cole, T.R., Das, S., Horn, D., Hughes, H.E., Temple, I.K., Faravelli, F., Waggoner, D., Turkmen, S., Cormier-Daire, V., Irrthum, A. and Rahman, N. (2005) Genotype-phenotype associations in Sotos syndrome: an analysis of 266 individuals with NSD1 aberrations. American Journal of Human Genetics, 77 (2), 193-204. (doi:10.1086/432082).

Record type: Article

Abstract

We identified 266 individuals with intragenic NSD1 mutations or 5q35 microdeletions encompassing NSD1 (referred to as "NSD1-positive individuals"), through analyses of 530 subjects with diverse phenotypes. Truncating NSD1 mutations occurred throughout the gene, but pathogenic missense mutations occurred only in functional domains (P < 2 x 10(-16)). Sotos syndrome was clinically diagnosed in 99% of NSD1-positive individuals, independent of the molecular analyses, indicating that NSD1 aberrations are essentially specific to this condition. Furthermore, our data suggest that 93% of patients who have been clinically diagnosed with Sotos syndrome have identifiable NSD1 abnormalities, of which 83% are intragenic mutations and 10% are 5q35 microdeletions. We reviewed the clinical phenotypes of 239 NSD1-positive individuals. Facial dysmorphism, learning disability, and childhood overgrowth were present in 90% of the individuals. However, both the height and head circumference of 10% of the individuals were within the normal range, indicating that overgrowth is not obligatory for the diagnosis of Sotos syndrome. A broad spectrum of associated clinical features was also present, the occurrence of which was largely independent of genotype, since individuals with identical mutations had different phenotypes. We compared the phenotypes of patients with intragenic NSD1 mutations with those of patients with 5q35 microdeletions. Patients with microdeletions had less-prominent overgrowth (P = .0003) and more-severe learning disability (P = 3 x 10(-9)) than patients with mutations. However, all features present in patients with microdeletions were also observed in patients with mutations, and there was no correlation between deletion size and the clinical phenotype, suggesting that the deletion of additional genes in patients with 5q35 microdeletions has little specific effect on phenotype. We identified only 13 familial cases. The reasons for the low vertical transmission rate are unclear, although familial cases were more likely than nonfamilial cases (P = .005) to carry missense mutations, suggesting that the underlying NSD1 mutational mechanism in Sotos syndrome may influence reproductive fitness.

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Published date: 1 August 2005
Keywords: frameshift mutation, polymorphism, zinc fingers, gene deletion, cancer, human, mutation, growth disorders, genes, genetics, proteins, amino acid sequence, genetic, height, homozygote, sequence homology, exons, amino acid, syndrome, nuclear proteins, learning disorders, missense, research, male, disability, childhood, female, head, analysis, pair 5, patients, diagnosis, peptides, chromosomes, genotype, molecular sequence data, protein, pathology, prognosis, phenotype, facies, humans, research support, intracellular signaling peptides and proteins, non-U.S.gov't, abnormalities
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Identifiers

Local EPrints ID: 60294
URI: http://eprints.soton.ac.uk/id/eprint/60294
DOI: doi:10.1086/432082
ISSN: 0002-9297
PURE UUID: 12fc44d7-996c-44bc-9a2b-72cd7c1f091a
ORCID for I.K. Temple: ORCID iD orcid.org/0000-0002-6045-1781

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Date deposited: 03 Sep 2008
Last modified: 16 Mar 2024 03:03

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Contributors

Author: K. Tatton-Brown
Author: J. Douglas
Author: K. Coleman
Author: G. Baujat
Author: T.R. Cole
Author: S. Das
Author: D. Horn
Author: H.E. Hughes
Author: I.K. Temple ORCID iD
Author: F. Faravelli
Author: D. Waggoner
Author: S. Turkmen
Author: V. Cormier-Daire
Author: A. Irrthum
Author: N. Rahman

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