A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease

Detalhes bibliográficos
Autor(a) principal: Ferreira, Elisa Napolitano
Data de Publicação: 2016
Outros Autores: Barros, Bruna Durães Figueiredo, Souza, Jorge Estefano de, Almeida, Renan Valieris, Torrezan, Giovana Tardin, Garcia, Sheila, Krepischi, Ana Cristina Victorino, Mello, Celso Abdon Lopes de, Cunha, Isabela Werneck da, Pinto, Clóvis Antonio Lopes, Soares, Fernando Augusto, Dias-Neto, Emmanuel, Lopes, Ademar, Souza, Sandro José de, Carraro, Dirce Maria
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UFRN
Texto Completo: https://repositorio.ufrn.br/jspui/handle/123456789/23051
Resumo: Background: Genome-wide profiling of rare tumors is crucial for improvement of diagnosis, treatment, and, consequently, achieving better outcomes. Desmoplastic small round cell tumor (DSRCT) is a rare type of sarcoma arising from mesenchymal cells of abdominal peritoneum that usually develops in male adolescents and young adults. A specific translocation, t(11;22)(p13;q12), resulting in EWS and WT1 gene fusion is the only recurrent molecular hallmark and no other genetic factor has been associated to this aggressive tumor. Here, we present a comprehensive genomic profiling of one DSRCT affecting a 26-year-old male, who achieved an excellent outcome. Methods: We investigated somatic and germline variants through whole-exome sequencing using a family based approach and, by array CGH, we explored the occurrence of genomic imbalances. Additionally, we performed mate-paired whole-genome sequencing for defining the specific breakpoint of the EWS-WT1 translocation, allowing us to develop a personalized tumor marker for monitoring the patient by liquid biopsy. Results: We identified genetic variants leading to protein alterations including 12 somatic and 14 germline events (11 germline compound heterozygous mutations and 3 rare homozygous polymorphisms) affecting genes predominantly involved in mesenchymal cell differentiation pathways. Regarding copy number alterations (CNA) few events were detected, mainly restricted to gains in chromosomes 5 and 18 and losses at 11p, 13q, and 22q. The deletions at 11p and 22q indicated the presence of the classic translocation, t(11;22)(p13;q12). In addition, the mapping of the specific genomic breakpoint of the EWS-WT1 gene fusion allowed the design of a personalized biomarker for assessing circulating tumor DNA (ctDNA) in plasma during patient follow-up. This biomarker has been used in four post-treatment blood samples, 3 years after surgery, and no trace of EWS-WT1 gene fusion was detected, in accordance with imaging tests showing no evidence of disease and with the good general health status of the patient. Conclusions: Overall, our findings revealed genes with potential to be associated with risk assessment and tumorigenesis of this rare type of sarcoma. Additionally, we established a liquid biopsy approach for monitoring patient follow-up based on genomic information that can be similarly adopted for patients diagnosed with a rare tumor.
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spelling Ferreira, Elisa NapolitanoBarros, Bruna Durães FigueiredoSouza, Jorge Estefano deAlmeida, Renan ValierisTorrezan, Giovana TardinGarcia, SheilaKrepischi, Ana Cristina VictorinoMello, Celso Abdon Lopes deCunha, Isabela Werneck daPinto, Clóvis Antonio LopesSoares, Fernando AugustoDias-Neto, EmmanuelLopes, AdemarSouza, Sandro José deCarraro, Dirce Maria2017-05-23T13:53:35Z2017-05-23T13:53:35Z2016https://repositorio.ufrn.br/jspui/handle/123456789/2305110.1186/s40246-016-0092-0engDesmoplastic small round cell tumorGenomic profilingWhole-exome sequencingEWS-WT1 gene fusionPersonalized biomarkerLiquid biopsyA genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive diseaseinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/articleBackground: Genome-wide profiling of rare tumors is crucial for improvement of diagnosis, treatment, and, consequently, achieving better outcomes. Desmoplastic small round cell tumor (DSRCT) is a rare type of sarcoma arising from mesenchymal cells of abdominal peritoneum that usually develops in male adolescents and young adults. A specific translocation, t(11;22)(p13;q12), resulting in EWS and WT1 gene fusion is the only recurrent molecular hallmark and no other genetic factor has been associated to this aggressive tumor. Here, we present a comprehensive genomic profiling of one DSRCT affecting a 26-year-old male, who achieved an excellent outcome. Methods: We investigated somatic and germline variants through whole-exome sequencing using a family based approach and, by array CGH, we explored the occurrence of genomic imbalances. Additionally, we performed mate-paired whole-genome sequencing for defining the specific breakpoint of the EWS-WT1 translocation, allowing us to develop a personalized tumor marker for monitoring the patient by liquid biopsy. Results: We identified genetic variants leading to protein alterations including 12 somatic and 14 germline events (11 germline compound heterozygous mutations and 3 rare homozygous polymorphisms) affecting genes predominantly involved in mesenchymal cell differentiation pathways. Regarding copy number alterations (CNA) few events were detected, mainly restricted to gains in chromosomes 5 and 18 and losses at 11p, 13q, and 22q. The deletions at 11p and 22q indicated the presence of the classic translocation, t(11;22)(p13;q12). In addition, the mapping of the specific genomic breakpoint of the EWS-WT1 gene fusion allowed the design of a personalized biomarker for assessing circulating tumor DNA (ctDNA) in plasma during patient follow-up. This biomarker has been used in four post-treatment blood samples, 3 years after surgery, and no trace of EWS-WT1 gene fusion was detected, in accordance with imaging tests showing no evidence of disease and with the good general health status of the patient. Conclusions: Overall, our findings revealed genes with potential to be associated with risk assessment and tumorigenesis of this rare type of sarcoma. 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dc.title.pt_BR.fl_str_mv A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
title A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
spellingShingle A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
Ferreira, Elisa Napolitano
Desmoplastic small round cell tumor
Genomic profiling
Whole-exome sequencing
EWS-WT1 gene fusion
Personalized biomarker
Liquid biopsy
title_short A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
title_full A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
title_fullStr A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
title_full_unstemmed A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
title_sort A genomic case study of desmoplastic small round cell tumor: comprehensive analysis reveals insights into potential therapeutic targets and development of a monitoring tool for a rare and aggressive disease
author Ferreira, Elisa Napolitano
author_facet Ferreira, Elisa Napolitano
Barros, Bruna Durães Figueiredo
Souza, Jorge Estefano de
Almeida, Renan Valieris
Torrezan, Giovana Tardin
Garcia, Sheila
Krepischi, Ana Cristina Victorino
Mello, Celso Abdon Lopes de
Cunha, Isabela Werneck da
Pinto, Clóvis Antonio Lopes
Soares, Fernando Augusto
Dias-Neto, Emmanuel
Lopes, Ademar
Souza, Sandro José de
Carraro, Dirce Maria
author_role author
author2 Barros, Bruna Durães Figueiredo
Souza, Jorge Estefano de
Almeida, Renan Valieris
Torrezan, Giovana Tardin
Garcia, Sheila
Krepischi, Ana Cristina Victorino
Mello, Celso Abdon Lopes de
Cunha, Isabela Werneck da
Pinto, Clóvis Antonio Lopes
Soares, Fernando Augusto
Dias-Neto, Emmanuel
Lopes, Ademar
Souza, Sandro José de
Carraro, Dirce Maria
author2_role author
author
author
author
author
author
author
author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Ferreira, Elisa Napolitano
Barros, Bruna Durães Figueiredo
Souza, Jorge Estefano de
Almeida, Renan Valieris
Torrezan, Giovana Tardin
Garcia, Sheila
Krepischi, Ana Cristina Victorino
Mello, Celso Abdon Lopes de
Cunha, Isabela Werneck da
Pinto, Clóvis Antonio Lopes
Soares, Fernando Augusto
Dias-Neto, Emmanuel
Lopes, Ademar
Souza, Sandro José de
Carraro, Dirce Maria
dc.subject.por.fl_str_mv Desmoplastic small round cell tumor
Genomic profiling
Whole-exome sequencing
EWS-WT1 gene fusion
Personalized biomarker
Liquid biopsy
topic Desmoplastic small round cell tumor
Genomic profiling
Whole-exome sequencing
EWS-WT1 gene fusion
Personalized biomarker
Liquid biopsy
description Background: Genome-wide profiling of rare tumors is crucial for improvement of diagnosis, treatment, and, consequently, achieving better outcomes. Desmoplastic small round cell tumor (DSRCT) is a rare type of sarcoma arising from mesenchymal cells of abdominal peritoneum that usually develops in male adolescents and young adults. A specific translocation, t(11;22)(p13;q12), resulting in EWS and WT1 gene fusion is the only recurrent molecular hallmark and no other genetic factor has been associated to this aggressive tumor. Here, we present a comprehensive genomic profiling of one DSRCT affecting a 26-year-old male, who achieved an excellent outcome. Methods: We investigated somatic and germline variants through whole-exome sequencing using a family based approach and, by array CGH, we explored the occurrence of genomic imbalances. Additionally, we performed mate-paired whole-genome sequencing for defining the specific breakpoint of the EWS-WT1 translocation, allowing us to develop a personalized tumor marker for monitoring the patient by liquid biopsy. Results: We identified genetic variants leading to protein alterations including 12 somatic and 14 germline events (11 germline compound heterozygous mutations and 3 rare homozygous polymorphisms) affecting genes predominantly involved in mesenchymal cell differentiation pathways. Regarding copy number alterations (CNA) few events were detected, mainly restricted to gains in chromosomes 5 and 18 and losses at 11p, 13q, and 22q. The deletions at 11p and 22q indicated the presence of the classic translocation, t(11;22)(p13;q12). In addition, the mapping of the specific genomic breakpoint of the EWS-WT1 gene fusion allowed the design of a personalized biomarker for assessing circulating tumor DNA (ctDNA) in plasma during patient follow-up. This biomarker has been used in four post-treatment blood samples, 3 years after surgery, and no trace of EWS-WT1 gene fusion was detected, in accordance with imaging tests showing no evidence of disease and with the good general health status of the patient. Conclusions: Overall, our findings revealed genes with potential to be associated with risk assessment and tumorigenesis of this rare type of sarcoma. Additionally, we established a liquid biopsy approach for monitoring patient follow-up based on genomic information that can be similarly adopted for patients diagnosed with a rare tumor.
publishDate 2016
dc.date.issued.fl_str_mv 2016
dc.date.accessioned.fl_str_mv 2017-05-23T13:53:35Z
dc.date.available.fl_str_mv 2017-05-23T13:53:35Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
format article
status_str publishedVersion
dc.identifier.uri.fl_str_mv https://repositorio.ufrn.br/jspui/handle/123456789/23051
dc.identifier.doi.none.fl_str_mv 10.1186/s40246-016-0092-0
url https://repositorio.ufrn.br/jspui/handle/123456789/23051
identifier_str_mv 10.1186/s40246-016-0092-0
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