Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2

Detalhes bibliográficos
Autor(a) principal: Corrêa, Thiago
Data de Publicação: 2020
Outros Autores: Poswar, Fabiano de Oliveira, Feltes, Bruno César, Riegel, Mariluce
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UFRGS
Texto Completo: http://hdl.handle.net/10183/212744
Resumo: In this report, we present a patient with brain alterations and dysmorphic features associated with chromosome duplication seen in 4p16.3 region and chromosomal deletion in a critical region responsible for Cri-du-chat syndrome (CdCS). Chromosomal microarray analysis (CMA) revealed a 41.1 Mb duplication encompassing the band region 4p16.3–p13, and a 14.7 Mb deletion located between the bands 5p15.33 and p15.1. The patient’s clinical findings overlap with previously reported cases of chromosome 4p duplication syndrome and CdCS. The patient’s symptoms are notably similar to those of CdCS patients as she presented with a weak, high-pitched voice and showed a similar pathogenicity observed in the brain MRI. These contiguous gene syndromes present with distinct clinical manifestations. However, the phenotypic and cytogenetic variability in affected individuals, such as the low frequency and the large genomic regions that can be altered, make it challenging to identify candidate genes that contribute to the pathogenesis of these syndromes. Therefore, systems biology and CMA techniques were used to investigate the extent of chromosome rearrangement on critical regions in our patient’s phenotype. We identified the candidate genes PPARGC1A, CTBP1, TRIO, TERT, and CCT5 that are associated with the neuropsychomotor delay, microcephaly, and neurological alterations found in our patient. Through investigating pathways that associate with essential nodes in the protein interaction network, we discovered proteins involved in cellular differentiation and proliferation, as well as proteins involved in the formation and disposition of the cytoskeleton. The combination of our cytogenomic and bioinformatic analysis provided these possible explanations for the unique clinical phenotype, which has not yet been described in scientific literature.
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spelling Corrêa, ThiagoPoswar, Fabiano de OliveiraFeltes, Bruno CésarRiegel, Mariluce2020-08-08T03:46:07Z20201664-8021http://hdl.handle.net/10183/212744001116369In this report, we present a patient with brain alterations and dysmorphic features associated with chromosome duplication seen in 4p16.3 region and chromosomal deletion in a critical region responsible for Cri-du-chat syndrome (CdCS). Chromosomal microarray analysis (CMA) revealed a 41.1 Mb duplication encompassing the band region 4p16.3–p13, and a 14.7 Mb deletion located between the bands 5p15.33 and p15.1. The patient’s clinical findings overlap with previously reported cases of chromosome 4p duplication syndrome and CdCS. The patient’s symptoms are notably similar to those of CdCS patients as she presented with a weak, high-pitched voice and showed a similar pathogenicity observed in the brain MRI. These contiguous gene syndromes present with distinct clinical manifestations. However, the phenotypic and cytogenetic variability in affected individuals, such as the low frequency and the large genomic regions that can be altered, make it challenging to identify candidate genes that contribute to the pathogenesis of these syndromes. Therefore, systems biology and CMA techniques were used to investigate the extent of chromosome rearrangement on critical regions in our patient’s phenotype. We identified the candidate genes PPARGC1A, CTBP1, TRIO, TERT, and CCT5 that are associated with the neuropsychomotor delay, microcephaly, and neurological alterations found in our patient. Through investigating pathways that associate with essential nodes in the protein interaction network, we discovered proteins involved in cellular differentiation and proliferation, as well as proteins involved in the formation and disposition of the cytoskeleton. The combination of our cytogenomic and bioinformatic analysis provided these possible explanations for the unique clinical phenotype, which has not yet been described in scientific literature.application/pdfengFrontiers in Genetics. Lausanne. Vol. 11 (Jun. 2020), 561, p. 1-8Duplicação cromossômicaTrissomiaMonossomiaSíndrome do miado do gatoFenótipoInformática médicaCérebroImagem por ressonância magnéticaCri-du-chat4p16.3PPARGC1ACTBP1TRIOTERTCCT5Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2Estrangeiroinfo:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFRGSinstname:Universidade Federal do Rio Grande do Sul (UFRGS)instacron:UFRGSTEXT001116369.pdf.txt001116369.pdf.txtExtracted Texttext/plain39084http://www.lume.ufrgs.br/bitstream/10183/212744/2/001116369.pdf.txt0bfa34200339dfc14eeddb267b5742b7MD52ORIGINAL001116369.pdfTexto completo (inglês)application/pdf2448439http://www.lume.ufrgs.br/bitstream/10183/212744/1/001116369.pdfd8c6d3f2b268abb0cb5d215eef584524MD5110183/2127442023-01-21 06:10:12.424857oai:www.lume.ufrgs.br:10183/212744Repositório de PublicaçõesPUBhttps://lume.ufrgs.br/oai/requestopendoar:2023-01-21T08:10:12Repositório Institucional da UFRGS - Universidade Federal do Rio Grande do Sul (UFRGS)false
dc.title.pt_BR.fl_str_mv Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
title Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
spellingShingle Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
Corrêa, Thiago
Duplicação cromossômica
Trissomia
Monossomia
Síndrome do miado do gato
Fenótipo
Informática médica
Cérebro
Imagem por ressonância magnética
Cri-du-chat
4p16.3
PPARGC1A
CTBP1
TRIO
TERT
CCT5
title_short Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
title_full Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
title_fullStr Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
title_full_unstemmed Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
title_sort Candidate genes associated with neurological findings in a patient with trisomy 4p16.3 and monosomy 5p15.2
author Corrêa, Thiago
author_facet Corrêa, Thiago
Poswar, Fabiano de Oliveira
Feltes, Bruno César
Riegel, Mariluce
author_role author
author2 Poswar, Fabiano de Oliveira
Feltes, Bruno César
Riegel, Mariluce
author2_role author
author
author
dc.contributor.author.fl_str_mv Corrêa, Thiago
Poswar, Fabiano de Oliveira
Feltes, Bruno César
Riegel, Mariluce
dc.subject.por.fl_str_mv Duplicação cromossômica
Trissomia
Monossomia
Síndrome do miado do gato
Fenótipo
Informática médica
Cérebro
Imagem por ressonância magnética
topic Duplicação cromossômica
Trissomia
Monossomia
Síndrome do miado do gato
Fenótipo
Informática médica
Cérebro
Imagem por ressonância magnética
Cri-du-chat
4p16.3
PPARGC1A
CTBP1
TRIO
TERT
CCT5
dc.subject.eng.fl_str_mv Cri-du-chat
4p16.3
PPARGC1A
CTBP1
TRIO
TERT
CCT5
description In this report, we present a patient with brain alterations and dysmorphic features associated with chromosome duplication seen in 4p16.3 region and chromosomal deletion in a critical region responsible for Cri-du-chat syndrome (CdCS). Chromosomal microarray analysis (CMA) revealed a 41.1 Mb duplication encompassing the band region 4p16.3–p13, and a 14.7 Mb deletion located between the bands 5p15.33 and p15.1. The patient’s clinical findings overlap with previously reported cases of chromosome 4p duplication syndrome and CdCS. The patient’s symptoms are notably similar to those of CdCS patients as she presented with a weak, high-pitched voice and showed a similar pathogenicity observed in the brain MRI. These contiguous gene syndromes present with distinct clinical manifestations. However, the phenotypic and cytogenetic variability in affected individuals, such as the low frequency and the large genomic regions that can be altered, make it challenging to identify candidate genes that contribute to the pathogenesis of these syndromes. Therefore, systems biology and CMA techniques were used to investigate the extent of chromosome rearrangement on critical regions in our patient’s phenotype. We identified the candidate genes PPARGC1A, CTBP1, TRIO, TERT, and CCT5 that are associated with the neuropsychomotor delay, microcephaly, and neurological alterations found in our patient. Through investigating pathways that associate with essential nodes in the protein interaction network, we discovered proteins involved in cellular differentiation and proliferation, as well as proteins involved in the formation and disposition of the cytoskeleton. The combination of our cytogenomic and bioinformatic analysis provided these possible explanations for the unique clinical phenotype, which has not yet been described in scientific literature.
publishDate 2020
dc.date.accessioned.fl_str_mv 2020-08-08T03:46:07Z
dc.date.issued.fl_str_mv 2020
dc.type.driver.fl_str_mv Estrangeiro
info:eu-repo/semantics/article
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
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status_str publishedVersion
dc.identifier.uri.fl_str_mv http://hdl.handle.net/10183/212744
dc.identifier.issn.pt_BR.fl_str_mv 1664-8021
dc.identifier.nrb.pt_BR.fl_str_mv 001116369
identifier_str_mv 1664-8021
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url http://hdl.handle.net/10183/212744
dc.language.iso.fl_str_mv eng
language eng
dc.relation.ispartof.pt_BR.fl_str_mv Frontiers in Genetics. Lausanne. Vol. 11 (Jun. 2020), 561, p. 1-8
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
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reponame_str Repositório Institucional da UFRGS
collection Repositório Institucional da UFRGS
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