Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2002 |
| Outros Autores: | , , |
| Tipo de documento: | Artigo |
| Idioma: | eng |
| Título da fonte: | Revista Brasileira de Cancerologia (Online) |
| Texto Completo: | https://rbc.inca.gov.br/index.php/revista/article/view/2157 |
Resumo: | The objective of present work is to investigate the occurrence of numerical alterations in lesions and bladder carcinomas that may be helpful in early diagnosis. Fluorescence in situ hybridization (FISH) was applied to identify such alterations in chromosomes 7, 9 and 17, in interphase nuclei of 14 fresh bladder tumor specimens (13 transitional cell carcinomas, TCC, and 1 undifferentiated anaplasic carcinoma, UAC), and 5 specimens derived from the TCC patients (2 chronic cystitis, UCC, and 3 macroscopically normal urothelium biopsies, MNU). The most frequent anomalies in malignant tumors of the bladder were trisomy /tetrasomy 7 (6/14=43%), trisomy/tetrasomy 17 (7/14=50%) and monosomy 9 (4/14=29%). The two chronic cystitis samples showed monosomy 9, whereas one macroscopically normal urothelium sample presented similar findings (polysomy 7, 9, and 17) observed in the matched tumoral tissue. Two carcinomas, an invasive grade IV (TCC13) and an invasive primary (UAC14), presented trisomy/tetrasomy 7, 9 and 17 suggesting that the cells were polyploidy. These results strengthens the involvement of chromosomes 7, 9, and 17 in urothelial carcinogenesis. The alterations of chromosomes 7 and 9 are related to the initiation process; and of chromosome 17, to tumoral progression and recurrence. Moreover, the results also support the hypothesis that chronic cystitis and normal urothelium from patients with bladder carcinoma can carry important chromosome abnormalities which may predict risk for tumor progression and recurrence. Thus, interphase FISH may be a useful tool for early diagnosis in patients at risk of disease and for follow-up in cases of recurrence and metastase. |
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Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridizationAneuploidias cromossômicas em câncer da bexiga, cistite crônica e urotélio normal detectadas por hibridizaçao in situ fluorescenteNeoplasias da BexigaCarcinomaCistiteAneuploidiasFluorescência em Hibridização in SituCromossomosBladder NeoplasmsCarcinomaCystitisAneuploidyFluorescence In Situ HybridizationChromosomesThe objective of present work is to investigate the occurrence of numerical alterations in lesions and bladder carcinomas that may be helpful in early diagnosis. Fluorescence in situ hybridization (FISH) was applied to identify such alterations in chromosomes 7, 9 and 17, in interphase nuclei of 14 fresh bladder tumor specimens (13 transitional cell carcinomas, TCC, and 1 undifferentiated anaplasic carcinoma, UAC), and 5 specimens derived from the TCC patients (2 chronic cystitis, UCC, and 3 macroscopically normal urothelium biopsies, MNU). The most frequent anomalies in malignant tumors of the bladder were trisomy /tetrasomy 7 (6/14=43%), trisomy/tetrasomy 17 (7/14=50%) and monosomy 9 (4/14=29%). The two chronic cystitis samples showed monosomy 9, whereas one macroscopically normal urothelium sample presented similar findings (polysomy 7, 9, and 17) observed in the matched tumoral tissue. Two carcinomas, an invasive grade IV (TCC13) and an invasive primary (UAC14), presented trisomy/tetrasomy 7, 9 and 17 suggesting that the cells were polyploidy. These results strengthens the involvement of chromosomes 7, 9, and 17 in urothelial carcinogenesis. The alterations of chromosomes 7 and 9 are related to the initiation process; and of chromosome 17, to tumoral progression and recurrence. Moreover, the results also support the hypothesis that chronic cystitis and normal urothelium from patients with bladder carcinoma can carry important chromosome abnormalities which may predict risk for tumor progression and recurrence. Thus, interphase FISH may be a useful tool for early diagnosis in patients at risk of disease and for follow-up in cases of recurrence and metastase.O presente trabalho investigou a ocorrência de anomalias cromossômicas numéricas em lesões da bexiga que possam auxiliar no diagnóstico precoce. A técnica de Hibridação in situ Fluorescente (FISH) foi aplicada para identificar tais anomalias nos cromossomos 7, 9 e 17 em núcleos interfásicos de 14 amostras de tumores da bexiga frescos (13 carcinomas de células transicionais, TCC, e 1 carcinoma anaplásico indiferenciado, UAC), e 5 amostras derivadas de pacientes com TCC (2 cistites crônicas e 3 biopsias de urotélio macroscopicamente normais). As anomalias mais freqüentes nos tumores malignos da bexiga foram trissomia/tetrassomia 7 (6/14=43%), trissomia/tetrassomia 17 (7/14=50%) e monossomia 9 (4/14=29%). As duas amostras de cistites crônicas apresentaram monossomia 9, uma das amostras de urotélio macroscopicamente normal exibiu resultado semelhante (polissomia 7, 9 e 17) ao do tecido tumoral correspondente. Dois carcinomas, um grau IV invasivo (TCC13) e um primário invasivo (UAC14), exibiram trissomia e tetrassomia 7, 9 e 17 sugerindo a ocorrência de poliploidia. Tais resultados reforçam o envolvimento dos cromossomos 7, 9 e 17 na carcinogênese urotelial. As alterações dos cromossomos 7 e 9 estão relacionadas com os processo de iniciação e do cromossomo 17 com progressão e recorrência tumoral. Os resultados também suportam a hipótese de que as cistites crônicas e o urotélio normal de pacientes com carcinoma de bexiga podem conter anormalidades cromossômicas importantes, que podem predizer risco para progressão e recorrência tumoral. Assim, a técnica de FISH pode ser uma ferramenta útil para o diagnóstico precoce, em pacientes com risco de desenvolver a doença e acompanhamento em casos de recorrência e metástases.INCA2002-12-30info:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersionArtigos, Avaliado pelos paresapplication/pdfhttps://rbc.inca.gov.br/index.php/revista/article/view/215710.32635/2176-9745.RBC.2002v48n4.2157Revista Brasileira de Cancerologia; Vol. 48 No. 4 (2002): Oct./Nov./Dec.; 517-522Revista Brasileira de Cancerologia; Vol. 48 Núm. 4 (2002): oct./nov./dic.; 517-522Revista Brasileira de Cancerologia; v. 48 n. 4 (2002): out./nov./dez.; 517-5222176-9745reponame:Revista Brasileira de Cancerologia (Online)instname:Instituto Nacional de Câncer José Alencar Gomes da Silva (INCA)instacron:INCAenghttps://rbc.inca.gov.br/index.php/revista/article/view/2157/1330https://creativecommons.org/licenses/by/4.0info:eu-repo/semantics/openAccessDi Cézar, Lucimari Bizari Mesquita, José Carlos Denadai, Eliseu Silva, Ana Elizabete 2023-07-25T15:14:13Zoai:rbc.inca.gov.br:article/2157Revistahttps://rbc.inca.gov.br/index.php/revistaPUBhttps://rbc.inca.gov.br/index.php/revista/oairbc@inca.gov.br0034-71162176-9745opendoar:2023-07-25T15:14:13Revista Brasileira de Cancerologia (Online) - Instituto Nacional de Câncer José Alencar Gomes da Silva (INCA)false |
| dc.title.none.fl_str_mv |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization Aneuploidias cromossômicas em câncer da bexiga, cistite crônica e urotélio normal detectadas por hibridizaçao in situ fluorescente |
| title |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization |
| spellingShingle |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization Di Cézar, Lucimari Bizari Neoplasias da Bexiga Carcinoma Cistite Aneuploidias Fluorescência em Hibridização in Situ Cromossomos Bladder Neoplasms Carcinoma Cystitis Aneuploidy Fluorescence In Situ Hybridization Chromosomes |
| title_short |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization |
| title_full |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization |
| title_fullStr |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization |
| title_full_unstemmed |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization |
| title_sort |
Chromosomal aneuploidies in bladder cancer, chronic cystitis and normal urothelium detected by fluorescence in situ hybridization |
| author |
Di Cézar, Lucimari Bizari |
| author_facet |
Di Cézar, Lucimari Bizari Mesquita, José Carlos Denadai, Eliseu Silva, Ana Elizabete |
| author_role |
author |
| author2 |
Mesquita, José Carlos Denadai, Eliseu Silva, Ana Elizabete |
| author2_role |
author author author |
| dc.contributor.author.fl_str_mv |
Di Cézar, Lucimari Bizari Mesquita, José Carlos Denadai, Eliseu Silva, Ana Elizabete |
| dc.subject.por.fl_str_mv |
Neoplasias da Bexiga Carcinoma Cistite Aneuploidias Fluorescência em Hibridização in Situ Cromossomos Bladder Neoplasms Carcinoma Cystitis Aneuploidy Fluorescence In Situ Hybridization Chromosomes |
| topic |
Neoplasias da Bexiga Carcinoma Cistite Aneuploidias Fluorescência em Hibridização in Situ Cromossomos Bladder Neoplasms Carcinoma Cystitis Aneuploidy Fluorescence In Situ Hybridization Chromosomes |
| description |
The objective of present work is to investigate the occurrence of numerical alterations in lesions and bladder carcinomas that may be helpful in early diagnosis. Fluorescence in situ hybridization (FISH) was applied to identify such alterations in chromosomes 7, 9 and 17, in interphase nuclei of 14 fresh bladder tumor specimens (13 transitional cell carcinomas, TCC, and 1 undifferentiated anaplasic carcinoma, UAC), and 5 specimens derived from the TCC patients (2 chronic cystitis, UCC, and 3 macroscopically normal urothelium biopsies, MNU). The most frequent anomalies in malignant tumors of the bladder were trisomy /tetrasomy 7 (6/14=43%), trisomy/tetrasomy 17 (7/14=50%) and monosomy 9 (4/14=29%). The two chronic cystitis samples showed monosomy 9, whereas one macroscopically normal urothelium sample presented similar findings (polysomy 7, 9, and 17) observed in the matched tumoral tissue. Two carcinomas, an invasive grade IV (TCC13) and an invasive primary (UAC14), presented trisomy/tetrasomy 7, 9 and 17 suggesting that the cells were polyploidy. These results strengthens the involvement of chromosomes 7, 9, and 17 in urothelial carcinogenesis. The alterations of chromosomes 7 and 9 are related to the initiation process; and of chromosome 17, to tumoral progression and recurrence. Moreover, the results also support the hypothesis that chronic cystitis and normal urothelium from patients with bladder carcinoma can carry important chromosome abnormalities which may predict risk for tumor progression and recurrence. Thus, interphase FISH may be a useful tool for early diagnosis in patients at risk of disease and for follow-up in cases of recurrence and metastase. |
| publishDate |
2002 |
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2002-12-30 |
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info:eu-repo/semantics/article info:eu-repo/semantics/publishedVersion Artigos, Avaliado pelos pares |
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article |
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https://rbc.inca.gov.br/index.php/revista/article/view/2157 10.32635/2176-9745.RBC.2002v48n4.2157 |
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https://rbc.inca.gov.br/index.php/revista/article/view/2157 |
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10.32635/2176-9745.RBC.2002v48n4.2157 |
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eng |
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https://rbc.inca.gov.br/index.php/revista/article/view/2157/1330 |
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INCA |
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INCA |
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Revista Brasileira de Cancerologia; Vol. 48 No. 4 (2002): Oct./Nov./Dec.; 517-522 Revista Brasileira de Cancerologia; Vol. 48 Núm. 4 (2002): oct./nov./dic.; 517-522 Revista Brasileira de Cancerologia; v. 48 n. 4 (2002): out./nov./dez.; 517-522 2176-9745 reponame:Revista Brasileira de Cancerologia (Online) instname:Instituto Nacional de Câncer José Alencar Gomes da Silva (INCA) instacron:INCA |
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