Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma

Detalhes bibliográficos
Autor(a) principal: Pinheiro, Maísa [UNESP]
Data de Publicação: 2016
Tipo de documento: Tese
Idioma: por
Título da fonte: Repositório Institucional da UNESP
Texto Completo: http://hdl.handle.net/11449/137932
Resumo: The identification of predisposing genes and characterization of genetic risk factors for cancer development are essential for the diagnosis, prognosis and genetic counseling of affected patients and their families. A significant number of patients with breast (BC) and papillary thyroid carcinomas (TC) and family history of these tumors suggest the involvement a hereditary cancer predisposition gene. The aim of this study was to evaluate new predisposing genes related to BC and TC by whole exome sequencing, in patients who are affected by at least one of these tumors and have cancer family history. Six patients with CM, 12 with CT and six with both tumors were included in the study, all of them with family history of these tumors. DNA from peripheral blood sample was sequenced by HiSeq 1000 platform (Illumina). After the bioinformatics analysis, variations in high and lowpenetrance genes were identified; most of them were considered common according to 1000 Genomes and 6500 Exomes. Furthermore, rare variations were described in these genes, which were considered pathogenic in at least three databases and observed in up to two patients. Patient 14 presented the p.R233X mutation in PTEN confirming the diagnosis of Cowden Syndrome. Other genes were investigated in order to characterize new variations related to the phenotype studied. This analysis resulted in 911 SNVs (single nucleotide variations), 287 non-synonymous alterations and 50 rare pathogenic variations (detected in at least three databases). From these, 13 alterations were mapped in genes that interact with high and low-penetrance genes previously described in literature. Alterations were also identified in genes recently described as associated with hereditary PTC and BC (HABP2, PARP4 and SRRM2). Enrichment analysis revealed compromised functions in the Thyroid hormone Synthesis and RAP1 Signaling pathways, involving deleterious alterations in 10 and 14 patients, respectively. Specifically, the thyroid hormone synthesis pathway may be potentially deregulated in individuals from Families I and II through PLCB3 and PAX8 alterations, respectively. Promising SNP candidates included the rs35169799 (PLCB3), one of the most frequent alterations, those classified as genome maintenance (rs61997220: ZC3H12D, rs61902276: DDIAS, rs61754785: MUS81, rs62619782: RNASEH2A), and mapped in potentially deregulated pathways (rs3188996: PAX8). Confirmation and validation analysis were performed for two variants rs61754785 (MUS81) and rs7080536 (HABP2) in 7 and 9 index patients, and also in their family members; the last one gives an additional support for literature data as not involved in hereditary PTC and BC. Furthermore, the data generated in this study could be incorporated into the general knowledge of cancer genetics, allowing the development of prevention strategies, screening and genetic counseling in these families.
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spelling Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exomaIdetification of predisposition genes associated with thyroid and breast carcinomas syndrome by exome sequencingCâncer de mamaCâncer de tireoideSíndromes de predisposição ao câncerSequenciamento do exomaThe identification of predisposing genes and characterization of genetic risk factors for cancer development are essential for the diagnosis, prognosis and genetic counseling of affected patients and their families. A significant number of patients with breast (BC) and papillary thyroid carcinomas (TC) and family history of these tumors suggest the involvement a hereditary cancer predisposition gene. The aim of this study was to evaluate new predisposing genes related to BC and TC by whole exome sequencing, in patients who are affected by at least one of these tumors and have cancer family history. Six patients with CM, 12 with CT and six with both tumors were included in the study, all of them with family history of these tumors. DNA from peripheral blood sample was sequenced by HiSeq 1000 platform (Illumina). After the bioinformatics analysis, variations in high and lowpenetrance genes were identified; most of them were considered common according to 1000 Genomes and 6500 Exomes. Furthermore, rare variations were described in these genes, which were considered pathogenic in at least three databases and observed in up to two patients. Patient 14 presented the p.R233X mutation in PTEN confirming the diagnosis of Cowden Syndrome. Other genes were investigated in order to characterize new variations related to the phenotype studied. This analysis resulted in 911 SNVs (single nucleotide variations), 287 non-synonymous alterations and 50 rare pathogenic variations (detected in at least three databases). From these, 13 alterations were mapped in genes that interact with high and low-penetrance genes previously described in literature. Alterations were also identified in genes recently described as associated with hereditary PTC and BC (HABP2, PARP4 and SRRM2). Enrichment analysis revealed compromised functions in the Thyroid hormone Synthesis and RAP1 Signaling pathways, involving deleterious alterations in 10 and 14 patients, respectively. Specifically, the thyroid hormone synthesis pathway may be potentially deregulated in individuals from Families I and II through PLCB3 and PAX8 alterations, respectively. Promising SNP candidates included the rs35169799 (PLCB3), one of the most frequent alterations, those classified as genome maintenance (rs61997220: ZC3H12D, rs61902276: DDIAS, rs61754785: MUS81, rs62619782: RNASEH2A), and mapped in potentially deregulated pathways (rs3188996: PAX8). Confirmation and validation analysis were performed for two variants rs61754785 (MUS81) and rs7080536 (HABP2) in 7 and 9 index patients, and also in their family members; the last one gives an additional support for literature data as not involved in hereditary PTC and BC. Furthermore, the data generated in this study could be incorporated into the general knowledge of cancer genetics, allowing the development of prevention strategies, screening and genetic counseling in these families.A identificação de fatores de predisposição e a caracterização de fatores genéticos de risco para o desenvolvimento do câncer são essenciais para o diagnóstico, prognóstico e aconselhamento genético dos pacientes afetados e seus familiares. Há uma alta incidência de pacientes que possuem carcinomas de mama (CM) e/ou carcinoma de tireoide (CT) e com história familial destes tumores, sugerindo o envolvimento de gene(s) associado(s) com a predisposição hereditária ao câncer. O objetivo deste trabalho foi investigar a presença de genes de predisposição ao desenvolvimento de CM e CT por meio do sequenciamento total do exoma, em pacientes que sejam afetados por pelo menos um destes tumores e possuam história familial de câncer. Foram incluídas seis pacientes que apresentavam CM, 12 com CT e seis com ambos os tumores, todos com história destes tumores em suas famílias. O DNA de sangue periférico foi sequenciado pela plataforma HiSeq 1000 (Illumina). Após análise de bioinformática foram identificadas alterações em genes de alta e baixa penetrância comuns e raras. As alterações raras destes genes foram consideradas como patogênicas quando presentes em pelo menos três bancos de dados e em até dois indivíduos. A paciente 14 teve diagnóstico de síndrome de Cowden confirmado pela presença da mutação p.R233X no gene PTEN. Também foram investigadas outras alterações em novos genes o que resultou em 911 SNVs (single nucleotide variations), sendo 287 não- sinônimas e 50 alterações raras consideradas patogênicas em pelo menos três bancos de dados. Entre as 50 alterações patogênicas, 13 mostraram interação proteica com produtos codificados por genes de alta ou baixa penetrância previamente descritos em síndromes hereditárias clássicas. Também foram identificadas alterações em genes recentemente descritos como associados à CT e ou CM hereditários (HABP2, PARP4 e SRRM2). Foi verificado que as vias de produção de hormônios tireoidianos e de sinalização RAP1 podem ter suas funções comprometidas por alterações deletérias que foram detectadas em 10 e 14 pacientes deste estudo, respectivamente. Especificamente a via de síntese de hormônio tireoidiano revelou estar potencialmente desregulada nas Famílias I e II por meio das alterações em PLCB3 e PAX8, respectivamente. As alterações consideradas mais promissoras incluem a rs35169799 (PLCB3), as classificadas como de manutenção do genoma (rs61997220: ZC3H12D, rs61902276: DDIAS, rs61754785: MUS81 e rs62619782: RNASEH2A) e as potencialmente desreguladas em vias importantes (rs3188996: PAX8). As variantes rs61754785 (MUS81) e rs7080536 (HABP2) foram confirmadas e validadas nos pacientes índice e em seus familiares; a última dando suporte adicional a dados da literatura como não envolvida em casos com CT não papilífero hereditário e CM. Este estudo revelou genes candidatos com potencial para contribuir para o diagnóstico molecular e aconselhamento genético destes pacientes e suas famílias.Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)FAPESP: 2014/03983-8Universidade Estadual Paulista (Unesp)Rogatto, Silvia Regina [UNESP]Universidade Estadual Paulista (Unesp)Pinheiro, Maísa [UNESP]2016-04-13T17:29:23Z2016-04-13T17:29:23Z2016-02-12info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesisapplication/pdfapplication/pdfhttp://hdl.handle.net/11449/13793200087027433004064026P9porinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UNESPinstname:Universidade Estadual Paulista (UNESP)instacron:UNESP2023-12-03T06:14:38Zoai:repositorio.unesp.br:11449/137932Repositório InstitucionalPUBhttp://repositorio.unesp.br/oai/requestopendoar:29462024-08-05T19:23:42.215918Repositório Institucional da UNESP - Universidade Estadual Paulista (UNESP)false
dc.title.none.fl_str_mv Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
Idetification of predisposition genes associated with thyroid and breast carcinomas syndrome by exome sequencing
title Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
spellingShingle Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
Pinheiro, Maísa [UNESP]
Câncer de mama
Câncer de tireoide
Síndromes de predisposição ao câncer
Sequenciamento do exoma
title_short Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
title_full Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
title_fullStr Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
title_full_unstemmed Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
title_sort Identificação de genes de predisposição à síndrome dos carcinomas de mama e tireoide por sequenciamento total do exoma
author Pinheiro, Maísa [UNESP]
author_facet Pinheiro, Maísa [UNESP]
author_role author
dc.contributor.none.fl_str_mv Rogatto, Silvia Regina [UNESP]
Universidade Estadual Paulista (Unesp)
dc.contributor.author.fl_str_mv Pinheiro, Maísa [UNESP]
dc.subject.por.fl_str_mv Câncer de mama
Câncer de tireoide
Síndromes de predisposição ao câncer
Sequenciamento do exoma
topic Câncer de mama
Câncer de tireoide
Síndromes de predisposição ao câncer
Sequenciamento do exoma
description The identification of predisposing genes and characterization of genetic risk factors for cancer development are essential for the diagnosis, prognosis and genetic counseling of affected patients and their families. A significant number of patients with breast (BC) and papillary thyroid carcinomas (TC) and family history of these tumors suggest the involvement a hereditary cancer predisposition gene. The aim of this study was to evaluate new predisposing genes related to BC and TC by whole exome sequencing, in patients who are affected by at least one of these tumors and have cancer family history. Six patients with CM, 12 with CT and six with both tumors were included in the study, all of them with family history of these tumors. DNA from peripheral blood sample was sequenced by HiSeq 1000 platform (Illumina). After the bioinformatics analysis, variations in high and lowpenetrance genes were identified; most of them were considered common according to 1000 Genomes and 6500 Exomes. Furthermore, rare variations were described in these genes, which were considered pathogenic in at least three databases and observed in up to two patients. Patient 14 presented the p.R233X mutation in PTEN confirming the diagnosis of Cowden Syndrome. Other genes were investigated in order to characterize new variations related to the phenotype studied. This analysis resulted in 911 SNVs (single nucleotide variations), 287 non-synonymous alterations and 50 rare pathogenic variations (detected in at least three databases). From these, 13 alterations were mapped in genes that interact with high and low-penetrance genes previously described in literature. Alterations were also identified in genes recently described as associated with hereditary PTC and BC (HABP2, PARP4 and SRRM2). Enrichment analysis revealed compromised functions in the Thyroid hormone Synthesis and RAP1 Signaling pathways, involving deleterious alterations in 10 and 14 patients, respectively. Specifically, the thyroid hormone synthesis pathway may be potentially deregulated in individuals from Families I and II through PLCB3 and PAX8 alterations, respectively. Promising SNP candidates included the rs35169799 (PLCB3), one of the most frequent alterations, those classified as genome maintenance (rs61997220: ZC3H12D, rs61902276: DDIAS, rs61754785: MUS81, rs62619782: RNASEH2A), and mapped in potentially deregulated pathways (rs3188996: PAX8). Confirmation and validation analysis were performed for two variants rs61754785 (MUS81) and rs7080536 (HABP2) in 7 and 9 index patients, and also in their family members; the last one gives an additional support for literature data as not involved in hereditary PTC and BC. Furthermore, the data generated in this study could be incorporated into the general knowledge of cancer genetics, allowing the development of prevention strategies, screening and genetic counseling in these families.
publishDate 2016
dc.date.none.fl_str_mv 2016-04-13T17:29:23Z
2016-04-13T17:29:23Z
2016-02-12
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/11449/137932
000870274
33004064026P9
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dc.language.iso.fl_str_mv por
language por
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
application/pdf
dc.publisher.none.fl_str_mv Universidade Estadual Paulista (Unesp)
publisher.none.fl_str_mv Universidade Estadual Paulista (Unesp)
dc.source.none.fl_str_mv reponame:Repositório Institucional da UNESP
instname:Universidade Estadual Paulista (UNESP)
instacron:UNESP
instname_str Universidade Estadual Paulista (UNESP)
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institution UNESP
reponame_str Repositório Institucional da UNESP
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repository.name.fl_str_mv Repositório Institucional da UNESP - Universidade Estadual Paulista (UNESP)
repository.mail.fl_str_mv
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