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Pathogenic variants in SOX11 mimicking Pitt‐Hopkins syndrome phenotype

Pitt‐Hopkins syndrome (PTHS) is a rare neurodevelopmental disorder characterised by severe intellectual disability (ID), distinctive facial features and autonomic nervous system dysfunction, caused by TCF4 haploinsufficiency. We clinically diagnosed with PTHS a 14 6/12‐year‐old female, who had a nor...

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Published in:	Clinical genetics 2024-01, Vol.105 (1), p.81-86
Main Authors:	Pasquetti, Domizia, L'Erario, Federica Francesca, Marangi, Giuseppe, Panfili, Arianna, Chiurazzi, Pietro, Sonnini, Elena, Orteschi, Daniela, Alfieri, Paolo, Morleo, Manuela, Nigro, Vincenzo, Zollino, Marcella
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Language:	English
Subjects:	Autonomic nervous system Child Congenital defects Facies Female Haploinsufficiency Humans Hypertrichosis Hyperventilation - diagnosis Hyperventilation - genetics Intellectual disabilities Intellectual Disability - diagnosis Intellectual Disability - genetics Intellectual Disability - pathology Microencephaly Neurodevelopmental disorders Phenotype Phenotypes Pitt‐Hopkins syndrome SOX11 SOXC Transcription Factors - genetics Transcription Factor 4 - genetics whole exome sequencing
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creator	Pasquetti, Domizia L'Erario, Federica Francesca Marangi, Giuseppe Panfili, Arianna Chiurazzi, Pietro Sonnini, Elena Orteschi, Daniela Alfieri, Paolo Morleo, Manuela Nigro, Vincenzo Zollino, Marcella
description	Pitt‐Hopkins syndrome (PTHS) is a rare neurodevelopmental disorder characterised by severe intellectual disability (ID), distinctive facial features and autonomic nervous system dysfunction, caused by TCF4 haploinsufficiency. We clinically diagnosed with PTHS a 14 6/12‐year‐old female, who had a normal status of TCF4. The pathogenic c.667del (p.Asp223MetfsTer45) variant in SOX11 was identified through whole exome sequencing (WES). SOX11 variants were initially reported to cause Coffin‐Siris syndrome (CSS), characterised by growth restriction, moderate ID, coarse face, hypertrichosis and hypoplastic nails. However, recent studies have provided evidence that they give rise to a distinct neurodevelopmental disorder. To date, SOX11 variants are associated with a variable phenotype, which has been described to resemble CSS in some cases, but never PTHS. By reviewing both clinically and genetically 32 out of 82 subjects reported in the literature with SOX11 variants, for whom detailed information are provided, we found that 7/32 (22%) had a clinical presentation overlapping PTHS. Furthermore, we made a confirmation that overall SOX11 abnormalities feature a distinctive disorder characterised by severe ID, high incidence of microcephaly and low frequency of congenital malformations. Purpose of the present report is to enhance the role of clinical genetics in assessing the individual diagnosis after WES results. On the top of the graphical percentage of SOX11‐patients and individual clinical manifestations are shown. Comparison of the most distinctive clinical signs of patients with mutations in SOX11, ARID1B and TCF4, respectively, is shown on the bottom, along with a representation of the overlapping phenotypes.
doi_str_mv	10.1111/cge.14414
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We clinically diagnosed with PTHS a 14 6/12‐year‐old female, who had a normal status of TCF4. The pathogenic c.667del (p.Asp223MetfsTer45) variant in SOX11 was identified through whole exome sequencing (WES). SOX11 variants were initially reported to cause Coffin‐Siris syndrome (CSS), characterised by growth restriction, moderate ID, coarse face, hypertrichosis and hypoplastic nails. However, recent studies have provided evidence that they give rise to a distinct neurodevelopmental disorder. To date, SOX11 variants are associated with a variable phenotype, which has been described to resemble CSS in some cases, but never PTHS. By reviewing both clinically and genetically 32 out of 82 subjects reported in the literature with SOX11 variants, for whom detailed information are provided, we found that 7/32 (22%) had a clinical presentation overlapping PTHS. Furthermore, we made a confirmation that overall SOX11 abnormalities feature a distinctive disorder characterised by severe ID, high incidence of microcephaly and low frequency of congenital malformations. Purpose of the present report is to enhance the role of clinical genetics in assessing the individual diagnosis after WES results. On the top of the graphical percentage of SOX11‐patients and individual clinical manifestations are shown. 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Furthermore, we made a confirmation that overall SOX11 abnormalities feature a distinctive disorder characterised by severe ID, high incidence of microcephaly and low frequency of congenital malformations. Purpose of the present report is to enhance the role of clinical genetics in assessing the individual diagnosis after WES results. On the top of the graphical percentage of SOX11‐patients and individual clinical manifestations are shown. Comparison of the most distinctive clinical signs of patients with mutations in SOX11, ARID1B and TCF4, respectively, is shown on the bottom, along with a representation of the overlapping phenotypes.</abstract><cop>Oxford, UK</cop><pub>Blackwell Publishing Ltd</pub><pmid>37558216</pmid><doi>10.1111/cge.14414</doi><tpages>6</tpages><orcidid>https://orcid.org/0000-0003-4871-9519</orcidid><orcidid>https://orcid.org/0000-0003-2197-9417</orcidid><oa>free_for_read</oa></addata></record>
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subjects	Autonomic nervous system Child Congenital defects Facies Female Haploinsufficiency Humans Hypertrichosis Hyperventilation - diagnosis Hyperventilation - genetics Intellectual disabilities Intellectual Disability - diagnosis Intellectual Disability - genetics Intellectual Disability - pathology Microencephaly Neurodevelopmental disorders Phenotype Phenotypes Pitt‐Hopkins syndrome SOX11 SOXC Transcription Factors - genetics Transcription Factor 4 - genetics whole exome sequencing
title	Pathogenic variants in SOX11 mimicking Pitt‐Hopkins syndrome phenotype
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