Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2009 |
| Tipo de documento: | Dissertação |
| Idioma: | por |
| Título da fonte: | Biblioteca Digital de Teses e Dissertações da UERJ |
| Texto Completo: | http://www.bdtd.uerj.br/handle/1/8830 |
Resumo: | Hypocellular primary MDS occurs in a frequency of 10-20% of the adults MDS cases, however it is the most frequent subtype in childhood. Diagnosis of hypocellular primary MDS is very difficult, because the small number of cells in bone marrow and it can be confused with hypocellular AML or AA. The differential diagnosis between these hematologic entities is extremely important because of AML is more aggressive and the possibility of MDS evolve to AML. Besides, MDS and AA are indicated to HSCT, however, conditioning regimens before the transplantation is specific for each disease. The combination between morphologic analysis, carried out through mielogram and bone marrow biopsy, and cytogenetic analysis have been performed a fundamental role on the recognition of hypocellular primary MDS. However, studies have been carried out to try improving the MDS diagnosis considering the biological characteristics as the presence of apoptosis. Thus, the aim of this study was characterize the chromosomal pattern of hypocellular primary MDS and correlate with cellular and clinic aspects. It was analyzed 86 cases of hypocellular primary MDS, 74 RA, 10 RAEB and 2 RAEB-t. Patients with RA presented 50% of abnormal karyotype and all patients with RAEB presented abnormal karyotype as well as RAEB-t patients. The most frequent chromosomal alterations in this study was del(17p) followed by alterations involving chromosome 7. Our results suggest that chromosomal pattern in hypocellular primary MDS is characterized mainly by partial and complete loss of chromosomes (deletion and monosomy). The cytogenetic analysis aided in diagnosis of cases with suspicion of hypocellular primary MDS and it was an important tool for treatment choice. IPSS showed to be a good prognostic scoring system for this group of patients. Alterations involving chromosome 17 were associated with RA subtype and dysplastic characteristics involving granulocytic setor, however, we could see del(17p) in RAEB patients. For apoptosis analysis were used 42 samples of MDS patients, 23 with primary hypocellular MDS, 8 with primary normocelular MDS and 11 with primary hipercelular MDS. The total apoptosis index in cases of hypocellular primary MDS presented a average of 9,5%, whereas patients with primary normocelular MDS and primary hipercelular MDS presented an average of 12% and 14,1%, respectively. For the analysis of specific lineage cells already commited with cellular proliferation program appears to be the main target of apoptosis program. Despite of patients with primary hypocellular MDS presented total apoptosis index more raised than controls they were always lower than primary normocelular MDS and primary hipercelular MDS, except for eritroblasts that were higher in primary hypocellular. The total apoptosis index was higher in initial stage of the disease independently of the bone marrow cellularity. Patients with del(11q) and del(17p) were associated with decreasing of total apoptosis index. Our results suggest that the hypocellularity of bone marrow is not caused by apoptosis process, but probably by probably some defect in cellular proliferation program. |
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Seixas, Teresa de Souza Fernandezhttp://lattes.cnpq.br/9057578752949881Lucena, Stella Beatriz Sampaio Gonçalves dehttp://lattes.cnpq.br/3295965897141052Pimentel, Márcia Mattos Gonçalveshttp://lattes.cnpq.br/9409055728849608Santos, Renata Olicio Jardim doshttp://lattes.cnpq.br/1585409637561480http://lattes.cnpq.br/9961153135038839Souza, Daiane Corrêa de Souza e2021-01-05T19:43:33Z2010-09-272009-05-04SOUZA, Daiane Corrêa de Souza e. Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos. 2009. 118 f. Dissertação (Mestrado em Ciências Médicas) - Universidade do Estado do Rio de Janeiro, Rio de Janeiro, 2009.http://www.bdtd.uerj.br/handle/1/8830Hypocellular primary MDS occurs in a frequency of 10-20% of the adults MDS cases, however it is the most frequent subtype in childhood. Diagnosis of hypocellular primary MDS is very difficult, because the small number of cells in bone marrow and it can be confused with hypocellular AML or AA. The differential diagnosis between these hematologic entities is extremely important because of AML is more aggressive and the possibility of MDS evolve to AML. Besides, MDS and AA are indicated to HSCT, however, conditioning regimens before the transplantation is specific for each disease. The combination between morphologic analysis, carried out through mielogram and bone marrow biopsy, and cytogenetic analysis have been performed a fundamental role on the recognition of hypocellular primary MDS. However, studies have been carried out to try improving the MDS diagnosis considering the biological characteristics as the presence of apoptosis. Thus, the aim of this study was characterize the chromosomal pattern of hypocellular primary MDS and correlate with cellular and clinic aspects. It was analyzed 86 cases of hypocellular primary MDS, 74 RA, 10 RAEB and 2 RAEB-t. Patients with RA presented 50% of abnormal karyotype and all patients with RAEB presented abnormal karyotype as well as RAEB-t patients. The most frequent chromosomal alterations in this study was del(17p) followed by alterations involving chromosome 7. Our results suggest that chromosomal pattern in hypocellular primary MDS is characterized mainly by partial and complete loss of chromosomes (deletion and monosomy). The cytogenetic analysis aided in diagnosis of cases with suspicion of hypocellular primary MDS and it was an important tool for treatment choice. IPSS showed to be a good prognostic scoring system for this group of patients. Alterations involving chromosome 17 were associated with RA subtype and dysplastic characteristics involving granulocytic setor, however, we could see del(17p) in RAEB patients. For apoptosis analysis were used 42 samples of MDS patients, 23 with primary hypocellular MDS, 8 with primary normocelular MDS and 11 with primary hipercelular MDS. The total apoptosis index in cases of hypocellular primary MDS presented a average of 9,5%, whereas patients with primary normocelular MDS and primary hipercelular MDS presented an average of 12% and 14,1%, respectively. For the analysis of specific lineage cells already commited with cellular proliferation program appears to be the main target of apoptosis program. Despite of patients with primary hypocellular MDS presented total apoptosis index more raised than controls they were always lower than primary normocelular MDS and primary hipercelular MDS, except for eritroblasts that were higher in primary hypocellular. The total apoptosis index was higher in initial stage of the disease independently of the bone marrow cellularity. Patients with del(11q) and del(17p) were associated with decreasing of total apoptosis index. Our results suggest that the hypocellularity of bone marrow is not caused by apoptosis process, but probably by probably some defect in cellular proliferation program.A SMD primária hipocelular ocorre com uma frequência de 10-20% dos casos de SMD no adulto, no entanto, é o subtipo mais frequente na infância. O diagnóstico da SMD primária hipocelular é bastante difícil, pois devido à ausência de células na medula óssea esta pode ser confundida com a LMA hipocelular ou AA. O diagnóstico diferencial entre estas entidades hematológicas é de extrema importância devido a maior agressividade da LMA e a possibilidade de evolução da SMD para LMA. Além disso, SMD e AA são indicadas para o TCTH, entretanto, o regime de condicionamento pré-transplante é específico para cada doença. A combinação entre a análise morfológica, realizada através do mielograma e biópsia de medula óssea, e análise citogenética tem desempenhado um papel fundamental no reconhecimento da SMD primária hipocelular. Entretanto, estudos têm sido realizados para tentar melhorar o diagnóstico da doença levando em consideração as características biológicas da SMD como a presença de apoptose. Sendo assim, este estudo teve como objetivo caracterizar o padrão cromossômico da SMD primária hipocelular e correlacionar com aspectos celulares e clínicos. Foram analisados citogeneticamente 86 casos de SMD primária hipocelular, 74 AR, 10 com AREB e 2 com AREB-t. Dentre os pacientes com AR 50% apresentaram cariótipo anormal e todos os pacientes com AREB e AREB-t apresentaram cariótipo anormal. A alteração cromossômica mais frequente foi a del(17p), seguida de alterações envolvendo o cromossomo 7. Nossos resultados sugerem que o padrão cromossômico em SMD primária hipocelular é caracterizado principalmente por perdas parciais e completas de cromossomos (deleções e monossomias). A análise citogenética auxiliou no diagnóstico dos casos com suspeita de SMD primária hipocelular e foi uma importante ferramenta para a escolha do tratamento. O IPSS mostrou ser um bom sistema de escala prognostica para este grupo de pacientes. Alterações envolvendo o cromossomo 17 estiveram associados com o subtipo AR e características displásicas envolvendo o setor granulocítico, no entanto, a del(17p) também pôde ser observada no subtipo AREB. Para análise de apoptose foram utilizadas 42 amostras de pacientes com SMD, 23 com SMD hipocelular, 8 com SMD normocelular e 11 com SMD hipercelular. O índice de apoptose total nos casos de SMD primária hipocelular apresentou uma média de 9,5%, enquanto os pacientes com SMD primária normocelular e hipercelular apresentaram uma média de 12% e 14,1%, respectivamente. Pela análise de linhagens específicas as células já comprometidas com o programa de diferenciação celular parecem ser o principal alvo do programa de apoptose. Apesar dos pacientes com SMD primária hipocelular apresentarem índice de apoptose total mais elevado que os controles eles foram sempre inferiores aos apresentados pela SMD primária normocelular e hipercelular, com exceção dos eritroblastos que foram maiores nos casos de SMD primária hipocelular. O índice de apoptose total foi maior nos estágios iniciais da doença independentemente da celularidade da medula óssea. Os pacientes com del (11q) e del (17p) estiveram associados com a diminuição do índice de apoptose total. Nossos resultados sugerem que a hipocelularidade da medula óssea não é causada pelo processo de apoptose e sim provavelmente por algum defeito no programa de proliferação celular.Submitted by Boris Flegr (boris@uerj.br) on 2021-01-05T19:43:33Z No. of bitstreams: 1 Dissertacao-Daiane Correa de Souza e Souza.pdf: 2574074 bytes, checksum: edfb5ace68a62d94e247d14212f43eb0 (MD5)Made available in DSpace on 2021-01-05T19:43:33Z (GMT). No. of bitstreams: 1 Dissertacao-Daiane Correa de Souza e Souza.pdf: 2574074 bytes, checksum: edfb5ace68a62d94e247d14212f43eb0 (MD5) Previous issue date: 2009-05-04application/pdfporUniversidade do Estado do Rio de JaneiroPrograma de Pós-Graduação em Ciências MédicasUERJBRCentro Biomédico::Faculdade de Ciências MédicasHypocellular Primary Myelodysplastic SyndromeChromosomal abnormalitiesApoptosisDysplasiamedula óssea-doençasanálise citogenéticaSíndrome Mielodisplásica Primária HipocelularAlterações cromossômicasApoptoseDisplasiaCNPQ::CIENCIAS BIOLOGICAS::GENETICA::GENETICA HUMANA E MEDICAEstudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicosChromosomal pattern study in Hypocellular Primary Myelodysplastic Syndrome and its correlation with cellular and clinics aspectsinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisinfo:eu-repo/semantics/openAccessreponame:Biblioteca Digital de Teses e Dissertações da UERJinstname:Universidade do Estado do Rio de Janeiro (UERJ)instacron:UERJORIGINALDissertacao-Daiane Correa de Souza e Souza.pdfapplication/pdf2574074http://www.bdtd.uerj.br/bitstream/1/8830/1/Dissertacao-Daiane+Correa+de+Souza+e+Souza.pdfedfb5ace68a62d94e247d14212f43eb0MD511/88302024-02-26 16:00:07.396oai:www.bdtd.uerj.br:1/8830Biblioteca Digital de Teses e Dissertaçõeshttp://www.bdtd.uerj.br/PUBhttps://www.bdtd.uerj.br:8443/oai/requestbdtd.suporte@uerj.bropendoar:29032024-02-26T19:00:07Biblioteca Digital de Teses e Dissertações da UERJ - Universidade do Estado do Rio de Janeiro (UERJ)false |
| dc.title.por.fl_str_mv |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| dc.title.alternative.eng.fl_str_mv |
Chromosomal pattern study in Hypocellular Primary Myelodysplastic Syndrome and its correlation with cellular and clinics aspects |
| title |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| spellingShingle |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos Souza, Daiane Corrêa de Souza e Hypocellular Primary Myelodysplastic Syndrome Chromosomal abnormalities Apoptosis Dysplasia medula óssea-doenças análise citogenética Síndrome Mielodisplásica Primária Hipocelular Alterações cromossômicas Apoptose Displasia CNPQ::CIENCIAS BIOLOGICAS::GENETICA::GENETICA HUMANA E MEDICA |
| title_short |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| title_full |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| title_fullStr |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| title_full_unstemmed |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| title_sort |
Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos |
| author |
Souza, Daiane Corrêa de Souza e |
| author_facet |
Souza, Daiane Corrêa de Souza e |
| author_role |
author |
| dc.contributor.advisor1.fl_str_mv |
Seixas, Teresa de Souza Fernandez |
| dc.contributor.advisor1Lattes.fl_str_mv |
http://lattes.cnpq.br/9057578752949881 |
| dc.contributor.referee1.fl_str_mv |
Lucena, Stella Beatriz Sampaio Gonçalves de |
| dc.contributor.referee1Lattes.fl_str_mv |
http://lattes.cnpq.br/3295965897141052 |
| dc.contributor.referee2.fl_str_mv |
Pimentel, Márcia Mattos Gonçalves |
| dc.contributor.referee2Lattes.fl_str_mv |
http://lattes.cnpq.br/9409055728849608 |
| dc.contributor.referee3.fl_str_mv |
Santos, Renata Olicio Jardim dos |
| dc.contributor.referee3Lattes.fl_str_mv |
http://lattes.cnpq.br/1585409637561480 |
| dc.contributor.authorLattes.fl_str_mv |
http://lattes.cnpq.br/9961153135038839 |
| dc.contributor.author.fl_str_mv |
Souza, Daiane Corrêa de Souza e |
| contributor_str_mv |
Seixas, Teresa de Souza Fernandez Lucena, Stella Beatriz Sampaio Gonçalves de Pimentel, Márcia Mattos Gonçalves Santos, Renata Olicio Jardim dos |
| dc.subject.eng.fl_str_mv |
Hypocellular Primary Myelodysplastic Syndrome Chromosomal abnormalities Apoptosis Dysplasia |
| topic |
Hypocellular Primary Myelodysplastic Syndrome Chromosomal abnormalities Apoptosis Dysplasia medula óssea-doenças análise citogenética Síndrome Mielodisplásica Primária Hipocelular Alterações cromossômicas Apoptose Displasia CNPQ::CIENCIAS BIOLOGICAS::GENETICA::GENETICA HUMANA E MEDICA |
| dc.subject.por.fl_str_mv |
medula óssea-doenças análise citogenética Síndrome Mielodisplásica Primária Hipocelular Alterações cromossômicas Apoptose Displasia |
| dc.subject.cnpq.fl_str_mv |
CNPQ::CIENCIAS BIOLOGICAS::GENETICA::GENETICA HUMANA E MEDICA |
| description |
Hypocellular primary MDS occurs in a frequency of 10-20% of the adults MDS cases, however it is the most frequent subtype in childhood. Diagnosis of hypocellular primary MDS is very difficult, because the small number of cells in bone marrow and it can be confused with hypocellular AML or AA. The differential diagnosis between these hematologic entities is extremely important because of AML is more aggressive and the possibility of MDS evolve to AML. Besides, MDS and AA are indicated to HSCT, however, conditioning regimens before the transplantation is specific for each disease. The combination between morphologic analysis, carried out through mielogram and bone marrow biopsy, and cytogenetic analysis have been performed a fundamental role on the recognition of hypocellular primary MDS. However, studies have been carried out to try improving the MDS diagnosis considering the biological characteristics as the presence of apoptosis. Thus, the aim of this study was characterize the chromosomal pattern of hypocellular primary MDS and correlate with cellular and clinic aspects. It was analyzed 86 cases of hypocellular primary MDS, 74 RA, 10 RAEB and 2 RAEB-t. Patients with RA presented 50% of abnormal karyotype and all patients with RAEB presented abnormal karyotype as well as RAEB-t patients. The most frequent chromosomal alterations in this study was del(17p) followed by alterations involving chromosome 7. Our results suggest that chromosomal pattern in hypocellular primary MDS is characterized mainly by partial and complete loss of chromosomes (deletion and monosomy). The cytogenetic analysis aided in diagnosis of cases with suspicion of hypocellular primary MDS and it was an important tool for treatment choice. IPSS showed to be a good prognostic scoring system for this group of patients. Alterations involving chromosome 17 were associated with RA subtype and dysplastic characteristics involving granulocytic setor, however, we could see del(17p) in RAEB patients. For apoptosis analysis were used 42 samples of MDS patients, 23 with primary hypocellular MDS, 8 with primary normocelular MDS and 11 with primary hipercelular MDS. The total apoptosis index in cases of hypocellular primary MDS presented a average of 9,5%, whereas patients with primary normocelular MDS and primary hipercelular MDS presented an average of 12% and 14,1%, respectively. For the analysis of specific lineage cells already commited with cellular proliferation program appears to be the main target of apoptosis program. Despite of patients with primary hypocellular MDS presented total apoptosis index more raised than controls they were always lower than primary normocelular MDS and primary hipercelular MDS, except for eritroblasts that were higher in primary hypocellular. The total apoptosis index was higher in initial stage of the disease independently of the bone marrow cellularity. Patients with del(11q) and del(17p) were associated with decreasing of total apoptosis index. Our results suggest that the hypocellularity of bone marrow is not caused by apoptosis process, but probably by probably some defect in cellular proliferation program. |
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2009 |
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2009-05-04 |
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2010-09-27 |
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SOUZA, Daiane Corrêa de Souza e. Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos. 2009. 118 f. Dissertação (Mestrado em Ciências Médicas) - Universidade do Estado do Rio de Janeiro, Rio de Janeiro, 2009. |
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SOUZA, Daiane Corrêa de Souza e. Estudo do padrão cromossômico em síndrome mielodisplásica primária hipocelular e sua correlação com aspectos celulares e clínicos. 2009. 118 f. Dissertação (Mestrado em Ciências Médicas) - Universidade do Estado do Rio de Janeiro, Rio de Janeiro, 2009. |
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