Global ETD Search

1	Risk of recurrence following ductal carcinoma in situ of the breast / Habel, Laurel A. January 1996 (has links) Thesis (Ph. D.)--University of Washington, 1996. / Vita. Includes bibliographical references.
2	Gene expression profiling of the breast tumour microenvironment : characterization of gene expression heterogeneity in the breast tumour microenvironment and its influence on clinical outcome Finak, Grzegorz. January 2008 (has links) Breast cancer is a very heterogeneous disease. This heterogeneity can be observed at many levels, including gene expression, chromosomal aberrations, and disease pathology. A clear understanding of these differences is important since they impact upon treatment efficacy and clinical outcome. Recent studies have demonstrated that the tumour microenvironment also plays a critical role in cancer initiation and progression. Genomic technologies have been used to gain a better understanding of the impact of gene expression heterogeneity on breast cancer, and have identified gene expression signatures associated with clinical outcome, histopathological breast cancer subtypes, and a variety of cancer-related pathways and processes. However, little work has been done in this context to examine the role of the tumour microenvironment in determining breast cancer outcome, or in defining breast cancer heterogeneity. Additionally, little is known about gene expression in histologically normal tissue adjacent to breast tumour, if this is influenced by the tumour, and how this compares with non-tumour-bearing breast tissue. By applying laser--capture microdissection and gene expression profiling to clinical breast cancer specimens the research presented in this thesis addresses these questions. / We have generated gene expression profiles of morphologically normal epithelial and stromal tissue, isolated using laser capture microdissection, from patients with breast cancer or undergoing breast reduction mammoplasty. We determined that morphologically normal epithelium and stroma exhibited distinct expression profiles, but molecular signatures that distinguished breast reduction tissue from tumour-adjacent normal tissue were absent. Stroma isolated from morphologically normal ducts adjacent to tumour tissue contained two distinct expression profiles that correlated with stromal cellularity, and shared similarities with soft tissue tumors with favourable outcome. Adjacent normal epithelium and stroma from breast cancer patients showed no significant association between expression profiles and standard clinical characteristics, but did cluster ER/PR/HER2-negative breast cancers with basal-like subtype expression profiles with poor prognosis. Our data reveal that morphologically normal tissue adjacent to breast carcinomas has not undergone significant gene expression changes when compared to breast reduction tissue, and provide an important gene expression data set for comparative studies of tumour expression profiles. / We compared gene expression profiles of tumour stroma from primary breast tumors and derived signatures strongly associated with clinical outcome. We present a new stroma-derived prognostic predictor (SDPP) that stratifies disease outcome independently of standard clinical prognostic factors and published expression-based predictors. The SDPP predicts outcome in several published whole tumour--derived expression data sets, identifies poor-outcome individuals from multiple clinical subtypes, including lymph node--negative tumors, and shows increased accuracy with respect to previously published predictors, especially for HER2-positive tumors. Prognostic power increases substantially when the predictor is combined with existing outcome predictors. Genes represented in the SDPP reveal the strong prognostic capacity of differential immune responses as well as angiogenic and hypoxic responses, highlighting the importance of stromal biology in tumour progression. / We show that gene expression in the breast tumour microenvironment is highly heterogeneous, identifying at least six different classes of tumour stroma with distinct expression patterns and distinct biological processes. Two of these classes recapitulate the processes identified in the stroma-derived prognostic predictor, while the others are new classes of stroma associated with distinct clinical outcomes. One of these is associated with matrix remodelling and is strongly associated with the basal molecular subtype of breast cancer. The remainder are independent of the previously published molecular subtypes of breast cancer. Additionally, based on independent data from over 800 tumors, the combinations of stroma classes and breast cancer subtypes identify new subgroups of breast tumors that show better discrimination between good and poor outcome individuals than the molecular breast cancer subtypes or the stroma classes alone, suggesting a novel classification scheme for breast cancer. This research demonstrates an important role for the tumour microenvironment in defining breast cancer heterogeneity, with a consequent impact upon clinical outcome. Novel therapies could be targeted at the processes that define the stroma classes suggesting new avenues for individualized treatment. Breast Neoplasms -- pathology. Carcinoma, Ductal, Breast -- pathology. Stromal Cells -- physiology. Prognosis. Gene Expression Profiling.
3	Análise da relevância clínica da classificação histológica dos carcinomas de mama de tipos lobular e ductal e sua relação com a classificação molecular Moraes Neto, Francisco Alves [UNESP] 27 August 2014 (has links) (PDF) Made available in DSpace on 2015-06-17T19:33:57Z (GMT). No. of bitstreams: 0 Previous issue date: 2014-08-27. Added 1 bitstream(s) on 2015-06-18T12:47:47Z : No. of bitstreams: 1 000830951.pdf: 1671352 bytes, checksum: e150ad97472df641fe9aede1e51165a5 (MD5) / INTRODUÇÃO: O valor prognóstico da classificação molecular do carcinoma de mama recentemente proposta tem sido validado por numerosos estudos. Entretanto, a maioria destes trabalhos estudou o tipo histológico mais comum denominado carcinoma ductal invasivo usual (CDI), uma entidade reconhecidamente heterogênea. Poucos estudos concentraram-se especificamente em outros tipos histológicos como o carcinoma lobular invasivo (CLI) que é o tipo especial mais frequente. O CLI apresenta-se com características clínico-patológicas e história natural bastante distintas do CDI sendo claramente entidades biológicas diferentes. Além disso, é uma doença relativamente frequente com aumento de sua incidência no mundo. OBJETIVO: Estudar comparativamente os subtipos moleculares luminais A e B de dois grupos de pacientes com CLI e CDI da mama, bem como determinar o valor prognóstico independente da classificação molecular nestes tumores correlacionando os subtipos moleculares com a sobrevida específica por carcinoma de mama (BCSS) e a sobrevida global (OS). SUJEITOS E MÉTODOS: Estudo do tipo transversal analítico. Foram selecionados blocos de parafina de mulheres com diagnóstico histopatológico de CLI e CDI no Laboratório de Patologia do Hospital Amaral Carvalho (HAC), Jaú, São Paulo, Brasil. Os respectivos prontuários médicos e o Registro Hospital de Câncer (RHC) do HAC foram consultados para a pesquisa das informações clínicas e de seguimento destas mulheres (média de 121,77 e 131,27 meses para o CLI e CDI, respectivamente), totalizando 186 casos. Dos blocos doadores, foram extraídas duas amostras de 2 mm de diâmetro e depositadas nos blocos de parafina receptores usando Tissue Microarray Builder ab1802 (Abcam®, Cambridge, UK). Nestes cortes foi feita a pesquisa dos seguintes marcadores imunoistoquímicos: receptor de estrógeno α (RE), receptor de progesterona (RP), HER2 e Ki67. Os subtipos moleculares (luminal A, luminal ... / INTRODUCTION: The prognostic value of the molecular classification of breast cancer recently proposed has been validated by many studies. However, the great majority of these studies has focused on invasive ductal carcinoma no special type (IDC), a widely recognized heterogeneous entity. Few papers have studied other special types of breast cancer such as invasive lobular carcinoma (ILC) the most common special type. ILC shows clinico-pathological features and natural history quite distinctive from IDC being clearly separate biologic entities. Moreover, ILC is relatively frequent and has been increasing in incidence over the recent years. OBJECTIVE: to study comparatively the luminal molecular subtypes A e B of two groups of patients with ILC and IDC and to determine the prognostic independent value of the molecular classification in ILC patients by correlating the molecular subtypes with clinical outcomes such as breast cancer specific survival (BCSS) and overall survival (OS). MATERIALS AND METHODS: archival paraffin blocks from women diagnosed with ILC and IDC at the Pathology Laboratory of Hospital Amaral Carvalho, Jau, Sao Paulo, Brazil, were retrieved. Patient's charts and the Hospital Amaral Carvalho Cancer Registry were consulted for obtaining the staging and follow-up information (median 121.77 and 131.27 months for ILC and IDC, respectively) and 186 patients were selected. Two samples from each paraffin block were extracted to mount tissue microarray (TMA) blocks by using a Tissue Microarray Builder ab1802 (Abcam®, Cambridge, UK). The following immunohistochemical markers were performed in the TMA blocks: estrogen receptor α, progesterone receptor, HER2 and Ki67 protein. The intrinsic molecular subtypes (luminal A, luminal B, HER2 and triple negative) were determined based on the immunohistochemical profile of each tumor. Prognostic clinico-pathological features were analysed in absolute (n) and relative frequency (%). The ... Mamas - Cancer Carcinoma ductal de mama Carcinoma lobular Estudos transversais Tumores Carcinoma, Ductal, Breast Carcinoma, Lobular
4	Análise da relevância clínica da classificação histológica dos carcinomas de mama de tipos lobular e ductal e sua relação com a classificação molecular / Moraes Neto, Francisco Alves. January 2014 (has links) Orientador: Rozany Mucha Dufloth / Coorientador: Fernando Carlos de Lander Schmitt / Banca: Mariângela Esther Alencar Marques / Banca: Luis Otávio Zanatta Sarian / Resumo: INTRODUÇÃO: O valor prognóstico da classificação molecular do carcinoma de mama recentemente proposta tem sido validado por numerosos estudos. Entretanto, a maioria destes trabalhos estudou o tipo histológico mais comum denominado carcinoma ductal invasivo usual (CDI), uma entidade reconhecidamente heterogênea. Poucos estudos concentraram-se especificamente em outros tipos histológicos como o carcinoma lobular invasivo (CLI) que é o tipo especial mais frequente. O CLI apresenta-se com características clínico-patológicas e história natural bastante distintas do CDI sendo claramente entidades biológicas diferentes. Além disso, é uma doença relativamente frequente com aumento de sua incidência no mundo. OBJETIVO: Estudar comparativamente os subtipos moleculares luminais A e B de dois grupos de pacientes com CLI e CDI da mama, bem como determinar o valor prognóstico independente da classificação molecular nestes tumores correlacionando os subtipos moleculares com a sobrevida específica por carcinoma de mama (BCSS) e a sobrevida global (OS). SUJEITOS E MÉTODOS: Estudo do tipo transversal analítico. Foram selecionados blocos de parafina de mulheres com diagnóstico histopatológico de CLI e CDI no Laboratório de Patologia do Hospital Amaral Carvalho (HAC), Jaú, São Paulo, Brasil. Os respectivos prontuários médicos e o Registro Hospital de Câncer (RHC) do HAC foram consultados para a pesquisa das informações clínicas e de seguimento destas mulheres (média de 121,77 e 131,27 meses para o CLI e CDI, respectivamente), totalizando 186 casos. Dos blocos doadores, foram extraídas duas amostras de 2 mm de diâmetro e depositadas nos blocos de parafina receptores usando Tissue Microarray Builder ab1802 (Abcam®, Cambridge, UK). Nestes cortes foi feita a pesquisa dos seguintes marcadores imunoistoquímicos: receptor de estrógeno α (RE), receptor de progesterona (RP), HER2 e Ki67. Os subtipos moleculares (luminal A, luminal ... / Abstract: INTRODUCTION: The prognostic value of the molecular classification of breast cancer recently proposed has been validated by many studies. However, the great majority of these studies has focused on invasive ductal carcinoma no special type (IDC), a widely recognized heterogeneous entity. Few papers have studied other special types of breast cancer such as invasive lobular carcinoma (ILC) the most common special type. ILC shows clinico-pathological features and natural history quite distinctive from IDC being clearly separate biologic entities. Moreover, ILC is relatively frequent and has been increasing in incidence over the recent years. OBJECTIVE: to study comparatively the luminal molecular subtypes A e B of two groups of patients with ILC and IDC and to determine the prognostic independent value of the molecular classification in ILC patients by correlating the molecular subtypes with clinical outcomes such as breast cancer specific survival (BCSS) and overall survival (OS). MATERIALS AND METHODS: archival paraffin blocks from women diagnosed with ILC and IDC at the Pathology Laboratory of Hospital Amaral Carvalho, Jau, Sao Paulo, Brazil, were retrieved. Patient's charts and the Hospital Amaral Carvalho Cancer Registry were consulted for obtaining the staging and follow-up information (median 121.77 and 131.27 months for ILC and IDC, respectively) and 186 patients were selected. Two samples from each paraffin block were extracted to mount tissue microarray (TMA) blocks by using a Tissue Microarray Builder ab1802 (Abcam®, Cambridge, UK). The following immunohistochemical markers were performed in the TMA blocks: estrogen receptor α, progesterone receptor, HER2 and Ki67 protein. The intrinsic molecular subtypes (luminal A, luminal B, HER2 and triple negative) were determined based on the immunohistochemical profile of each tumor. Prognostic clinico-pathological features were analysed in absolute (n) and relative frequency (%). The ... / Mestre Mamas - Cancer. Carcinoma ductal de mama Carcinoma lobular Estudos transversais. Neoplasias. Carcinoma, Ductal, Breast. Carcinoma, Lobular.
5	Gene expression profiling of the breast tumour microenvironment : characterization of gene expression heterogeneity in the breast tumour microenvironment and its influence on clinical outcome Finak, Grzegorz January 2008 (has links) No description available. Gene Expression Profiling. Stromal Cells -- physiology. Prognosis. Carcinoma, Ductal, Breast -- pathology. Breast Neoplasms -- pathology.
6	"Análise da expressão de E-caderina, Snail e Hakai em células epiteliais de tumor e tecido peritumoral de mulheres com carcinoma ductal invasivo da mama: correlação com comprometimento linfonodal" / E-cadherin, Snail and Hakai mRNA expression in epithelial cells from tumoral and peritumoral tissue from women with breast invasive ductal carcinoma. Correlation with axillary's lymph node involvement Makdissi, Fabiana Baroni Alves 08 June 2006 (has links) A expressão de E-caderina (Ecad) pode ser regulada pré ou pós transcricionalmente por Snail e Hakai, respectivamente. Nosso objetivo foi determinar a expressão de Ecad, Snail e Hakai, em células epiteliais (CE) de tecido tumoral e peritumoral de pacientes com carcinoma ductal invasivo da mama e correlacionar sua expressão ao comprometimento linfonodal axilar (LN+). As CE de amostras de tecidos de 45 pacientes (52% LN+) foram extraídas por método imunomagnético, o RNA foi extraído por RT-PCR em tempo real e utilizou-se primers específicos para a moléculas. A expressão de Ecad, Snail e Hakai não variou entre o tecido tumoral e peritumoral e não houve correlação com comprometimento linfonodal / E-cadherin (Ecad) expression may be transcriptionally or post-transcriptionally regulated by Snail and Hakai. Our aim was to determine the expression of Ecad, Snail and Hakai, in epithelial cells (EC) obtained from tumor and its adjacent tissue from women with invasive ductal breast carcinoma (IDC) and evaluate their correlation to the axillary's lymph node (LN+) involvement. Tissue from 45 patients (52% LN+) had their EC recovered by immunomagnetic antibody process, RNA was extracted and real-time RT-PCR was performed using specific primers. Ecad, Snail and Hakai mRNA expression did not vary between tumoral and peritumoral samples and their expression was not correlated to LN involvement Breast neoplasms Carcinoma Ductal Breast Carcinoma ductal de mama Células epiteliais Epithelial cells Expressão gênica Gene expression Linfonodos Lymph nodes Mulheres Neoplasias mamárias Women
7	"Análise da expressão de E-caderina, Snail e Hakai em células epiteliais de tumor e tecido peritumoral de mulheres com carcinoma ductal invasivo da mama: correlação com comprometimento linfonodal" / E-cadherin, Snail and Hakai mRNA expression in epithelial cells from tumoral and peritumoral tissue from women with breast invasive ductal carcinoma. Correlation with axillary's lymph node involvement Fabiana Baroni Alves Makdissi 08 June 2006 (has links) A expressão de E-caderina (Ecad) pode ser regulada pré ou pós transcricionalmente por Snail e Hakai, respectivamente. Nosso objetivo foi determinar a expressão de Ecad, Snail e Hakai, em células epiteliais (CE) de tecido tumoral e peritumoral de pacientes com carcinoma ductal invasivo da mama e correlacionar sua expressão ao comprometimento linfonodal axilar (LN+). As CE de amostras de tecidos de 45 pacientes (52% LN+) foram extraídas por método imunomagnético, o RNA foi extraído por RT-PCR em tempo real e utilizou-se primers específicos para a moléculas. A expressão de Ecad, Snail e Hakai não variou entre o tecido tumoral e peritumoral e não houve correlação com comprometimento linfonodal / E-cadherin (Ecad) expression may be transcriptionally or post-transcriptionally regulated by Snail and Hakai. Our aim was to determine the expression of Ecad, Snail and Hakai, in epithelial cells (EC) obtained from tumor and its adjacent tissue from women with invasive ductal breast carcinoma (IDC) and evaluate their correlation to the axillary's lymph node (LN+) involvement. Tissue from 45 patients (52% LN+) had their EC recovered by immunomagnetic antibody process, RNA was extracted and real-time RT-PCR was performed using specific primers. Ecad, Snail and Hakai mRNA expression did not vary between tumoral and peritumoral samples and their expression was not correlated to LN involvement Carcinoma ductal de mama Células epiteliais Expressão gênica Linfonodos Mulheres Neoplasias mamárias Breast neoplasms Carcinoma Ductal Breast Epithelial cells Gene expression Lymph nodes Women
8	Caracterização da expressão de microRNAs em carcinoma de mama receptores hormonais positivos e HER-2 negativo / Caracterização da expressão de microRNAs em carcinoma de mama receptores hormonais positivo e HER-2 negativo Mendes, Daniele Carvalho Calvano 27 January 2015 (has links) Introdução: O câncer de mama é, em sua essência, uma doença genética. O acúmulo de alterações moleculares no genoma das células somáticas é a base para a progressão do câncer. Além de ter biologia natural mais favorável, os tumores com alta expressão de receptores de estrogênio têm terapia-alvo bem estabelecida. Apesar disso, as pacientes podem apresentar resistência medicamentosa, recidiva e óbito. Os microRNAs (miRNAs) são uma classe de pequenas moléculas não codificadoras de proteínas que regulam a expressão gênica durante a etapa de tradução. Esta regulação é feita pelo pareamento de bases com o mRNA-alvo (RNA mensageiro), resultando na supressão da tradução ou na clivagem do mRNA. Se os miRNAs têm como alvo genes supressores de tumor ou oncogenes, podem atuar como supressores tumorais ou oncogenes. OBJETIVO: avaliar a expressão de microRNAs, por PCR em tempo real, no carcinoma mamário ductal invasivo (CDI) com receptores hormonais positivos e HER-2 negativo (luminal A). MÉTODOS: Foram avaliados materiais em parafina de 33 pacientes com tumores luminal A, bem como tecido mamário histologicamente normal. Foram utilizados kit para extração de RNA de amostras fixadas e parafinadas - miRNeasy FFPE; kit para síntese de cDNA - miScript II RT; kit miScript SYBR Green PCR e miScript miRNA PCR Arrays para análise de 84 sequências de miRNA de câncer humano. Analisaram-se dados clínicos, como idade, paridade, amamentação, estado menopausal; variáveis histológicas, como tamanho do tumor, estado linfonodal, invasão linfática; características imunoistoquímicas, como expressão de Ki-67. Para a análise estatística utilizou-se o software miScript miRNA PCR Array Data Analysis, que emprega o método de quantificação relativa ??Ct. RESULTADOS: A análise comparativa dos 33 casos de CDI luminal A com os 15 casos de parênquima mamário normal revelou haver microRNAs hiperexpressos, sendo eles: miR-96-5p (fold-regulation = 9,245, p = 0,000192), miR-182-5p (fold-regulation = 6,4813, p = 0,00024), miR-21-5p (fold-regulation = 6,3129, p = 0,000001), miR- 210-3p (fold-regulation =4,3584, p =0,001002) e. miR-7-5p (fold-regulation = 4,0166, p = 0,036407). Apontou, ainda, microRNAs com hipoexpressão, a saber: miR-204-5p (Fold-regulation = -8,2104, p = 0,000000), miR-125b-5p (Fold-regulation = --6,332, p=0,000000), let-7c-5p (Fold-regulation: -4,5142, p=0,000000) e let-7e-5p (Fold-regulation = -4,059, p = 0,011625): CONCLUSÕES: CDI luminal A apresentou hiperexpressão de miR-96-5p, miR-182-5p, miR-21-5p, miR-210-3p e miR-7-5p. Apontou, ainda, hipoexpressão do miR-204-5p, miR-125b-5p, let-7c-5p e let-7e-5p, permitindo diferenciá-lo do tecido normal / INTRODUCTION: Breast cancer is a genetic disease and the accumulation of molecular alterations in the genome of somatic cells is the basis for cancer progression. Besides having a more favorable natural biology, tumors with high expression of estrogen receptor have a well established targeted therapy. Nevertheless, patients may present with resistance and eventually relapse and death. MicroRNAs (miRNAs) are a class of small non-coding protein molecules that regulate gene expression during the translation stage. This adjustment is made by base pairing with the mRNA (messenger RNA) target resulting in suppression of translation or cleavage of the mRNA. Depending on whether miRNAs target tumor suppressor genes or oncogenes, they can act as tumor suppressors or oncogenes. OBJECTIVE: evaluate the expression of microRNAs by RT-PCR in positive hormonal receptors, negative HER 2 (luminal A) invasive ductal carcinoma (IDC). METHODS: Paraffin embedded tumor material from 33 patients with luminal A IDC, and histologically normal breast tissue. Were used: Kit for RNA extraction from fixed and paraffin embedded samples - miRNeasy FFPE; cDNA synthesis kit - miScript II RT; miScript SYBR Green PCR Kit and miScript miRNA PCR Arrays for analysis of 84 miRNA sequences of human cancer. Clinical data such as age, parity, breastfeeding, menopausal status; histological variables such as tumor size, lymph node status, lymphatic invasion; immunohistochemical characteristics, such as expression of Ki-67, were evaluated. For statistical analysis the miScript miRNA PCR Array Data Analysis software, which uses the method of relative quantification ??Ct, was used. RESULTS: A comparative analysis of 33 cases of luminal A IDC with 15 cases of normal breast parenchyma defined microRNAs overexpressed, as follows: miR-96-5p (fold-regulation = 9,245, p = 0,000192), miR-182-5p (fold-regulation = 6,4813, p = 0,00024), miR-21-5p (fold-regulation = 6,3129, p = 0,000001), miR- 210-3p (fold-regulation =4,3584, p =0,001002) and miR-7-5p (fold-regulation = 4,0166, p = 0,036407). Furthermore, microRNAs with reduced expression, as follows:. miR-204-5p (Fold-regulation = -8,2104, p = 0,000000), miR-125b-5p (Fold-regulation = -6,332, p=0,000000), let-7c-5p (Fold-regulation: -4,5142, p=0,000000) and let-7e-5p (Fold-regulation = -4,059, p = 0,011625): CONCLUSION: Luminal A CDI breast cancer has shown overexpression of miR-96-5p, miR-182-5p, miR-21-5p, miR-210-3p and miR-7-5p. Also has shown,downregulation of miR-204-5p, miR-125b-5p, let-7c-5p e let-7e-5p, allowing differentiating it from normal tissue Breast neoplasms/pathology Carcinoma ductal breast/genetics Carcinoma ductal breast/pathology Carcinoma ductal de mama/genética Carcinoma ductal de mama/patologia Expressão gênica Gene expression Genes supressores de tumor Genes tumor suppressor Immunohistochemistry Imuno-histoquímica Marcadores biológicos de tumor/análise MicroRNAs MicroRNAs Neoplasias da mama/patologia Prognosis Prognóstico Real-time polymerase chain reaction Tumor markers biological/analysis
9	Caracterização da expressão de microRNAs em carcinoma de mama receptores hormonais positivos e HER-2 negativo / Caracterização da expressão de microRNAs em carcinoma de mama receptores hormonais positivo e HER-2 negativo Daniele Carvalho Calvano Mendes 27 January 2015 (has links) Introdução: O câncer de mama é, em sua essência, uma doença genética. O acúmulo de alterações moleculares no genoma das células somáticas é a base para a progressão do câncer. Além de ter biologia natural mais favorável, os tumores com alta expressão de receptores de estrogênio têm terapia-alvo bem estabelecida. Apesar disso, as pacientes podem apresentar resistência medicamentosa, recidiva e óbito. Os microRNAs (miRNAs) são uma classe de pequenas moléculas não codificadoras de proteínas que regulam a expressão gênica durante a etapa de tradução. Esta regulação é feita pelo pareamento de bases com o mRNA-alvo (RNA mensageiro), resultando na supressão da tradução ou na clivagem do mRNA. Se os miRNAs têm como alvo genes supressores de tumor ou oncogenes, podem atuar como supressores tumorais ou oncogenes. OBJETIVO: avaliar a expressão de microRNAs, por PCR em tempo real, no carcinoma mamário ductal invasivo (CDI) com receptores hormonais positivos e HER-2 negativo (luminal A). MÉTODOS: Foram avaliados materiais em parafina de 33 pacientes com tumores luminal A, bem como tecido mamário histologicamente normal. Foram utilizados kit para extração de RNA de amostras fixadas e parafinadas - miRNeasy FFPE; kit para síntese de cDNA - miScript II RT; kit miScript SYBR Green PCR e miScript miRNA PCR Arrays para análise de 84 sequências de miRNA de câncer humano. Analisaram-se dados clínicos, como idade, paridade, amamentação, estado menopausal; variáveis histológicas, como tamanho do tumor, estado linfonodal, invasão linfática; características imunoistoquímicas, como expressão de Ki-67. Para a análise estatística utilizou-se o software miScript miRNA PCR Array Data Analysis, que emprega o método de quantificação relativa ??Ct. RESULTADOS: A análise comparativa dos 33 casos de CDI luminal A com os 15 casos de parênquima mamário normal revelou haver microRNAs hiperexpressos, sendo eles: miR-96-5p (fold-regulation = 9,245, p = 0,000192), miR-182-5p (fold-regulation = 6,4813, p = 0,00024), miR-21-5p (fold-regulation = 6,3129, p = 0,000001), miR- 210-3p (fold-regulation =4,3584, p =0,001002) e. miR-7-5p (fold-regulation = 4,0166, p = 0,036407). Apontou, ainda, microRNAs com hipoexpressão, a saber: miR-204-5p (Fold-regulation = -8,2104, p = 0,000000), miR-125b-5p (Fold-regulation = --6,332, p=0,000000), let-7c-5p (Fold-regulation: -4,5142, p=0,000000) e let-7e-5p (Fold-regulation = -4,059, p = 0,011625): CONCLUSÕES: CDI luminal A apresentou hiperexpressão de miR-96-5p, miR-182-5p, miR-21-5p, miR-210-3p e miR-7-5p. Apontou, ainda, hipoexpressão do miR-204-5p, miR-125b-5p, let-7c-5p e let-7e-5p, permitindo diferenciá-lo do tecido normal / INTRODUCTION: Breast cancer is a genetic disease and the accumulation of molecular alterations in the genome of somatic cells is the basis for cancer progression. Besides having a more favorable natural biology, tumors with high expression of estrogen receptor have a well established targeted therapy. Nevertheless, patients may present with resistance and eventually relapse and death. MicroRNAs (miRNAs) are a class of small non-coding protein molecules that regulate gene expression during the translation stage. This adjustment is made by base pairing with the mRNA (messenger RNA) target resulting in suppression of translation or cleavage of the mRNA. Depending on whether miRNAs target tumor suppressor genes or oncogenes, they can act as tumor suppressors or oncogenes. OBJECTIVE: evaluate the expression of microRNAs by RT-PCR in positive hormonal receptors, negative HER 2 (luminal A) invasive ductal carcinoma (IDC). METHODS: Paraffin embedded tumor material from 33 patients with luminal A IDC, and histologically normal breast tissue. Were used: Kit for RNA extraction from fixed and paraffin embedded samples - miRNeasy FFPE; cDNA synthesis kit - miScript II RT; miScript SYBR Green PCR Kit and miScript miRNA PCR Arrays for analysis of 84 miRNA sequences of human cancer. Clinical data such as age, parity, breastfeeding, menopausal status; histological variables such as tumor size, lymph node status, lymphatic invasion; immunohistochemical characteristics, such as expression of Ki-67, were evaluated. For statistical analysis the miScript miRNA PCR Array Data Analysis software, which uses the method of relative quantification ??Ct, was used. RESULTS: A comparative analysis of 33 cases of luminal A IDC with 15 cases of normal breast parenchyma defined microRNAs overexpressed, as follows: miR-96-5p (fold-regulation = 9,245, p = 0,000192), miR-182-5p (fold-regulation = 6,4813, p = 0,00024), miR-21-5p (fold-regulation = 6,3129, p = 0,000001), miR- 210-3p (fold-regulation =4,3584, p =0,001002) and miR-7-5p (fold-regulation = 4,0166, p = 0,036407). Furthermore, microRNAs with reduced expression, as follows:. miR-204-5p (Fold-regulation = -8,2104, p = 0,000000), miR-125b-5p (Fold-regulation = -6,332, p=0,000000), let-7c-5p (Fold-regulation: -4,5142, p=0,000000) and let-7e-5p (Fold-regulation = -4,059, p = 0,011625): CONCLUSION: Luminal A CDI breast cancer has shown overexpression of miR-96-5p, miR-182-5p, miR-21-5p, miR-210-3p and miR-7-5p. Also has shown,downregulation of miR-204-5p, miR-125b-5p, let-7c-5p e let-7e-5p, allowing differentiating it from normal tissue Carcinoma ductal de mama/genética Carcinoma ductal de mama/patologia Expressão gênica Genes supressores de tumor Imuno-histoquímica Marcadores biológicos de tumor/análise MicroRNAs Neoplasias da mama/patologia Prognóstico Breast neoplasms/pathology Carcinoma ductal breast/genetics Carcinoma ductal breast/pathology Gene expression Genes tumor suppressor Immunohistochemistry MicroRNAs Prognosis Real-time polymerase chain reaction Tumor markers biological/analysis
10	"Evolução oncológica de pacientes com carcinoma avançado de mama submetidas à reconstrução mamária imediata" / Oncologic progression of patients with advanced breast carcinoma undergoing immediate breast reconstruction Trinconi, Angela Francisca 21 July 2006 (has links) Estudo retrospectivo de 119 pacientes com diagnóstico de adenocarcinoma ductal invasivo no estádio clínico III tratadas com quimioterapia neoadjuvante (FEC), mastectomia e adjuvância. Destas, 85 optaram por reconstrução mamária imediata (RMI) com retalho transverso músculo-cutâneo de reto-abdominal e 34, não. Com seguimento médio de 52,7 meses avaliou-se o tempo de hospitalização, a inter-relação com a adjuvância, recidiva local, o tempo livre de doença e o tempo total de sobrevida, concluindo-se que, apesar de aumentar o tempo de hospitalização, a RMI não interfere com os demais ítens, podendo ser indicada para pacientes portadoras de carcinoma mamário em estádio clínico avançado / A retrospective study with 119 patients diagnosed with invasive ductal adenocarcinoma of the breast treated with neoadjuvant chemotherapy (FEC), mastectomy and adjuvant therapy. Eight-five patients chose immediate breast reconstruction (IBR) with transverse rectus abdominis myocutaneous flap and, 34 did not do it. The mean follow-up was 52.7 months. Length of stay, adjuvant therapy interrelation, local recurrence, disease-free survival and overall survival were evaluated. It was concluded that despite a longer stay, IBR did not interfere with any of the other factors analyzed and may be indicated for patients with advanced breast disease Carcinoma ductal breast Carcinoma ductal de mama Disease-free survival Length of stay Mastectomia radical Mastectomy radical Neoadjuvant therapy Retalhos cirúrgicos Sobrevivência Sobrevivência livre de doença Surgical flaps Survival Tempo de internação Terapia neoadjuvante

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