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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.

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Showing 11 to 20 of 37 (0.059 seconds)

Spelling suggestions: "subject:"mantle cell"" "subject:"hantle cell""

11

Genetic studies of follicular and mantle cell lymphoma /

Björck, Erik, January 2005 (has links)
Diss. (sammanfattning) Stockholm : Karolinska institutet, 2005. / Härtill 4 uppsatser.
12

Genetic characterization of hematological malignancies with focul on mantle cell lymphoma /

Flordal Thelander, Emma, January 2007 (has links)
Diss. (sammanfattning) Stockholm : Karolinska institutet, 2007. / Härtill 4 uppsatser.
13

Lymphoma at First Sight: A Rare Case of Mantle Cell Lymphoma Presenting as Isolated Periorbital Swelling

Fatima, Zainab, Rahman, Haroon, Oad, Sonia Kumari, Spradling, Elnora, Jaishankar, Devapiran 30 April 2020 (has links)
Mantle cell lymphoma (MCL) represents a heterogenous subtype of non-Hodgkin lymphoma (NHL), which can present in three distinct clinicopathologic variants: indolent type MCL, classic type MCL and blastoid type MCL. Despite the different variations, MCL, in general, is almost always associated with advanced-stage disease at diagnosis, with a strong predilection for significant extranodal involvement, usually to the bone marrow, CNS, peripheral blood and the gastrointestinal tract. However, the literature review reveals ocular involvement is a more rarely described extranodal site of involvement by MCL. Among the reported cases, the orbit was most commonly involved, followed by the eyelid and the lacrimal gland. We report a 63-year-old male who presented with a nine-month history of progressive symptoms of periorbital swelling and eyelid apraxia, causing bilateral visual disturbances. The patient was initially treated for presumed blepharospasm by his ophthalmologist with botulinum toxin injections; however, his periorbital edema continued to worsen, and he developed a discrete nodule in his right lower eyelid. Biopsy of the right eyelid nodule revealed classic type MCL with immunohistochemical testing positive for CD20, CD5, cyclin D1, SOX11 and Ki67 proliferative index of 40%. Fluorescence in situ hybridization (FISH) analysis detected (11;14) translocation. Mantle Cell Lymphoma International Prognostic Index Combined Biologic Index (MIPIb) score was calculated to be 6.5 points based on his age, ECOG performance status of 0-1, normal serum LDH, normal white blood cell count and elevated Ki67 proliferative index, stratifying patient into the high-risk group, with an estimated median overall survival of 37 months. Due to the bulky MCL involvement in the palpebral conjunctiva affecting his vision and eyelid function, he was immediately treated with radiation therapy to the bilateral orbits. PET-CT revealed adenopathy above and below the diaphragm. Bone marrow biopsy revealed focal involvement (5-10%) by MCL. Brain MRI revealed MCL infiltration in the bilateral orbits and lacrimal glands. Upper and lower endoscopy revealed multiple polyps positive for MCL. Given the advanced stage of the disease and his high-risk stratification, he was started on intensive induction chemotherapy with rituximab, dexamethasone, cytarabine, and carboplatin and received prophylactic intrathecal methotrexate. Systemic imaging after completion of four cycles of treatment revealed near resolution of the majority of the lymphadenopathy and all of the lymph nodes no longer demonstrated any significant metabolic activity. He completed two additional cycles of systemic chemotherapy and is currently being evaluated for autologous hematopoietic stem cell transplantation in complete remission-1 given his excellent response to treatment, his young age, high-risk disease at diagnosis, and good performance status. Despite the diffuse and extensive systemic disease, interestingly, our patient did not exhibit any constitutional or metastasis-associated symptoms and only presented with isolated periorbital swelling. Our case emphasizes the rare extranodal site of involvement by MCL and encourages all medical providers to remain cognizant of the varying ways in which MCL can present clinically.
Mantle Cell Lymphoma
Orbital swelling
Non-Hodgkin Lymphoma
Oncology
Lymphatic System
Tumors
14

Molekulární základy klonální heterogenity hematologických onemocnění / Molecular basis of clonal heterogeneity of hematological diseases

Babošová, Oľga January 2019 (has links)
Tumor heterogeneity has been recognized for decades. The molecular mechanisms impacting clonal heterogeneity in hematological diseases, specifically myeloproliferative neoplasms (MPN) and mantle cell lymphoma, with the focus on several inherited genetic factors, inflammation, the protective mechanisms of DNA damage response (DDR) in the leukemic transformation and the treatment strategies are the focus of this thesis. Firstly, I focus on studying germline JAK2 variants and how these may influence the initiation and progression of MPN diseases, and even contribute to further genomic alterations in the mutated clone. A study performed by our cooperating lab in Utah, USA,1 analyzing the mutational landscape of 31 JAK2 V617F-positive polycythemia vera (PV) patients identified two novel germline mutations in JAK2 gene, JAK2 T108A and JAK2 L393V. Another study2 , performed by our cooperating lab in Olomouc, Czech Republic, characterized two germline JAK2 mutations, E846D and R1063H, in a case of hereditary erythrocytosis accompanied by megakaryocytic atypia. The JAK2 R1063H variant was initially described in 3 out of 93 PV patients that were JAK2 V617F-positive.3 Our aim was to identify the role of selected inherited mutations in JAK2 gene in the initiation and progression of myeloproliferative...
15

Role of HSWI/SNF associated PRMT5 and MSIN3A/HDAC in the control of gene expression and cancer

Pal, Sharmistha 27 March 2007 (has links)
No description available.
Biology, Molecular
hSWI/SNF complexes
PRMT5
ST7
Mantle Cell Lymphoma (MCL)
H3R8 and H4R3 methylation
16

Immunoglobulin gene analysis in different B cell lymphomas : with focus on cellular origin and antigen selection /

Thorsélius, Mia, January 2004 (has links)
Diss. (sammanfattning) Uppsala : Univ., 2004. / Härtill 5 uppsatser.
17

Nodální a extranodální lymfomy: klinickopatologická, imunohistochemická, molekulárně-biologická charakteristika / Nodal and Extranodal Lymphomas: Clinicopathological, Immunohistochemical, Molecular-Biological Charactersistics

Veselá, Pavla January 2016 (has links)
3 Abstract The doctor thesis is composed of two major studies, both of them focused on the mantle cell lymphoma (MCL). The first part deals with the verification of the prognostic influence of Mantle Cell Lymphoma International Prognostic Index (MIPI) and of the proliferative activity in 235 patients with MCL diagnosed in 1996-2008 in the Czech Republic. This population study was performed in the collaboration with the Czech Lymphoma Study Group. The clinical data of patients were completed in April 2012. The diagnosis of MCL was confirmed by our central histopathologic examination of pretherapeutic histological samples. The median overall survival (OS) was 47 months, median progression free survival (PFS) was 22 months. We demonstrated the influence of proliferative activity, MIPI and of the therapy type (intensive/non-intensive) on OS and PFS in univariate and multivariate analysis. Using univariate analysis we showed the prognostic influence of aggressive/other cytomorphological variants of MCL, nodal/extranodal localization of primary sample and also of the variants of MIPI - s-MIPI, MIPIb and a completely new variant of MIPI - combined MIPI. The prognostic influence of growth pattern and of the results of immunohistochemical reaction with CD23, CD5 and cyclin D1 antibodies were not confirmed. The other...
18

Nodální a extranodální lymfomy: klinickopatologická, imunohistochemická, molekulárně-biologická charakteristika / Nodal and Extranodal Lymphomas: Clinicopathological, Immunohistochemical, Molecular-Biological Charactersistics

Veselá, Pavla January 2016 (has links)
3 Abstract The doctor thesis is composed of two major studies, both of them focused on the mantle cell lymphoma (MCL). The first part deals with the verification of the prognostic influence of Mantle Cell Lymphoma International Prognostic Index (MIPI) and of the proliferative activity in 235 patients with MCL diagnosed in 1996-2008 in the Czech Republic. This population study was performed in the collaboration with the Czech Lymphoma Study Group. The clinical data of patients were completed in April 2012. The diagnosis of MCL was confirmed by our central histopathologic examination of pretherapeutic histological samples. The median overall survival (OS) was 47 months, median progression free survival (PFS) was 22 months. We demonstrated the influence of proliferative activity, MIPI and of the therapy type (intensive/non-intensive) on OS and PFS in univariate and multivariate analysis. Using univariate analysis we showed the prognostic influence of aggressive/other cytomorphological variants of MCL, nodal/extranodal localization of primary sample and also of the variants of MIPI - s-MIPI, MIPIb and a completely new variant of MIPI - combined MIPI. The prognostic influence of growth pattern and of the results of immunohistochemical reaction with CD23, CD5 and cyclin D1 antibodies were not confirmed. The other...
19

"Análise do perfil de expressão gênica do linfoma de células do manto em fase leucêmica com microarrays de oligonucleotídeos" / "Gene expression profiling of mantle cell lymhoma in leukemic phase with oligonucleotide microarrays"

Rizzatti, Edgar Gil 31 January 2005 (has links)
O linfoma de células do manto é associado à translocação t(11;14)(q13;q32) e à hiperexpressão da ciclina D1. Os pacientes com linfoma de células do manto apresentam-se com doença avançada ao diagnóstico e a fase leucêmica da doença é observada em cerca de um terço dos casos. Os linfócitos B virgens pré-centro germinativo, que ocupam a zona do manto dos folículos linfóides secundários, constituem a origem celular do linfoma de células do manto. A hiperexpressão da ciclina D1, por si só, não é suficiente para a patogênese da neoplasia, e a elucidação das alterações moleculares adicionais poderá fundamentar novas estratégias terapêuticas. Nesse contexto, os métodos de estudo do perfil de expressão gênica em larga escala têm potencial para auxiliar na descoberta dessas alterações moleculares adicionais. Todavia, nos estudos que empregaram esses métodos até o momento, o material genético foi obtido de amostras de gânglios acometidos pelo tumor, que contêm uma proporção variável de células normais do estroma do tecido linfóide. Por isso, ainda não se sabe quais dos genes identificados como alterados no linfoma de células do manto são específicos das células linfomatosas, e quais são dependentes das células normais que perfazem o estroma do gânglio. Com o objetivo de elucidar as alterações moleculares do linfoma de células do manto em nível celular, realizamos um estudo comparativo entre o perfil de expressão gênica de células linfomatosas purificadas e de linfócitos B virgens, utilizando microarrays de oligonucleotídeos. Células linfomatosas e linfócitos B virgens (IgD+CD38±CD27-) foram purificados em colunas magnéticas a partir do sangue periférico de pacientes com linfoma de células do manto em fase leucêmica e de amígdalas de indivíduos normais, respectivamente (pureza > 95%). Três indivíduos foram selecionados em cada grupo e os experimentos foram realizados em duplicatas usando microarrays comerciais modelo CodeLink Human UniSet I, com 10.000 genes. Foram identificados 106 genes com variação de expressão maior do que três vezes, 63 deles induzidos e 43 reprimidos no linfoma de células do manto em relação aos linfócitos B virgens. Dez genes (seis induzidos e quatro reprimidos) foram selecionados para quantificação, por RT-PCR em tempo real, em amostras de sangue periférico de 21 pacientes com linfoma de células do manto em fase leucêmica, além de 14 pacientes com outras doenças linfoproliferativas crônicas e de sete indivíduos sem doenças neoplásicas. Os resultados dos experimentos com microarrays foram confirmados pela quantificação por RT-PCR em tempo real em todos os 10 genes selecionados e os valores de expressão do gene TLR1 obtidos por esse método demonstraram correlação significativa com a sobrevida dos pacientes com linfoma de células do manto. Além de identificar vários genes modulados no linfoma de células do manto em nível celular, este estudo também revelou a expressão aberrante de diversos genes relacionados à apoptose e às vias de sinalização PI3K/AKT, WNT e TGFβ. Esses resultados adicionam informações originais à patogênese molecular do linfoma de células do manto e apontam para vias específicas de sinalização molecular como potenciais alvos para novas abordagens terapêuticas. / Mantle cell lymphoma is associated with the translocation t(11;14)(q13;32) and overexpression of cyclin D1. Mantle cell lymphoma is predominantly disseminated at diagnosis and a frank leukemic phase is detected in one third of patients. The pre-germinal-center naive B-cells, which populate the mantle zone of the secondary lymphoid follicles, are the cells of origin of mantle cell lymphoma. Overexpression of cyclin D1 is not sufficient by itself to cause lymphoma, and a better understanding of the additional molecular lesions may provide insights toward new therapeutic approaches. In this context, large scale gene expression studies may be useful in the investigation of such additional molecular lesions. However, the great majority of mantle cell lymphoma cases studied by these methods to date had the genetic material harvested from lymph nodes, which have a variable proportion of normal cells from the lymphoid stroma. It is therefore not known how many genes identified as differentially expressed in mantle cell lymphoma by tumor versus normal experiments are cell-autonomous rather than dependent on the tumor microenvironment. To address this issue, we compared the gene expression profile of mantle cell lymphoma cells and normal naive B-cells using oligonucleotide microarrays. Lymphoma cells and naive B-cells (IgD+CD38±CD27-) were highly purified, by magnetic activated cell sorting, from the peripheral blood of patients with mantle cell lymphoma in the leukemic phase and from tonsils of normal individuals, respectively (purity > 95% in all samples). Three individuals were selected for each group and experiments were performed in replicates using the Amersham CodeLink Human UniSet I Bioarrays, with 10,000 genes. We identified 106 genes differentially expressed with a fold change of at least three-fold, 63 induced and 43 repressed in mantle cell lymphoma in comparison with naive B-cells. Ten genes were selected (six induced and four repressed in lymphoma cells) for quantification by real-time RT-PCR in non-purified peripheral blood samples from 21 patients with mantle cell lymphoma in the leukemic phase, as well as in 14 patients with other chronic lymphoproliferative diseases and seven normal individuals. Microarray results were confirmed by real-time RT-PCR for all selected genes and expression values of the TLR1 gene as quantified by this method showed significant correlation with patient survival in mantle cell lymphoma. In addition to the identification of several modulated genes in mantle cell lymphoma at cellular level, this study revealed that some genes functionally connected through apoptosis or the PI3K/AKT, WNT and TGFβ signaling pathways are aberrantly expressed in mantle cell lymphoma. These results add original data to the molecular pathogenesis of mantle cell lymphoma and point to specific molecular signaling pathways related to inhibition of apoptosis as potential targets for new therapeutic approaches.
expressão gênica
gene expression profiling
linfoma de células do manto
linfoma não-Hodgkin
mantle cell lymphoma
microarrays
microarrays
non-Hodgkin’s lymphoma
20

"Análise do perfil de expressão gênica do linfoma de células do manto em fase leucêmica com microarrays de oligonucleotídeos" / "Gene expression profiling of mantle cell lymhoma in leukemic phase with oligonucleotide microarrays"

Edgar Gil Rizzatti 31 January 2005 (has links)
O linfoma de células do manto é associado à translocação t(11;14)(q13;q32) e à hiperexpressão da ciclina D1. Os pacientes com linfoma de células do manto apresentam-se com doença avançada ao diagnóstico e a fase leucêmica da doença é observada em cerca de um terço dos casos. Os linfócitos B virgens pré-centro germinativo, que ocupam a zona do manto dos folículos linfóides secundários, constituem a origem celular do linfoma de células do manto. A hiperexpressão da ciclina D1, por si só, não é suficiente para a patogênese da neoplasia, e a elucidação das alterações moleculares adicionais poderá fundamentar novas estratégias terapêuticas. Nesse contexto, os métodos de estudo do perfil de expressão gênica em larga escala têm potencial para auxiliar na descoberta dessas alterações moleculares adicionais. Todavia, nos estudos que empregaram esses métodos até o momento, o material genético foi obtido de amostras de gânglios acometidos pelo tumor, que contêm uma proporção variável de células normais do estroma do tecido linfóide. Por isso, ainda não se sabe quais dos genes identificados como alterados no linfoma de células do manto são específicos das células linfomatosas, e quais são dependentes das células normais que perfazem o estroma do gânglio. Com o objetivo de elucidar as alterações moleculares do linfoma de células do manto em nível celular, realizamos um estudo comparativo entre o perfil de expressão gênica de células linfomatosas purificadas e de linfócitos B virgens, utilizando microarrays de oligonucleotídeos. Células linfomatosas e linfócitos B virgens (IgD+CD38±CD27-) foram purificados em colunas magnéticas a partir do sangue periférico de pacientes com linfoma de células do manto em fase leucêmica e de amígdalas de indivíduos normais, respectivamente (pureza > 95%). Três indivíduos foram selecionados em cada grupo e os experimentos foram realizados em duplicatas usando microarrays comerciais modelo CodeLink Human UniSet I, com 10.000 genes. Foram identificados 106 genes com variação de expressão maior do que três vezes, 63 deles induzidos e 43 reprimidos no linfoma de células do manto em relação aos linfócitos B virgens. Dez genes (seis induzidos e quatro reprimidos) foram selecionados para quantificação, por RT-PCR em tempo real, em amostras de sangue periférico de 21 pacientes com linfoma de células do manto em fase leucêmica, além de 14 pacientes com outras doenças linfoproliferativas crônicas e de sete indivíduos sem doenças neoplásicas. Os resultados dos experimentos com microarrays foram confirmados pela quantificação por RT-PCR em tempo real em todos os 10 genes selecionados e os valores de expressão do gene TLR1 obtidos por esse método demonstraram correlação significativa com a sobrevida dos pacientes com linfoma de células do manto. Além de identificar vários genes modulados no linfoma de células do manto em nível celular, este estudo também revelou a expressão aberrante de diversos genes relacionados à apoptose e às vias de sinalização PI3K/AKT, WNT e TGFβ. Esses resultados adicionam informações originais à patogênese molecular do linfoma de células do manto e apontam para vias específicas de sinalização molecular como potenciais alvos para novas abordagens terapêuticas. / Mantle cell lymphoma is associated with the translocation t(11;14)(q13;32) and overexpression of cyclin D1. Mantle cell lymphoma is predominantly disseminated at diagnosis and a frank leukemic phase is detected in one third of patients. The pre-germinal-center naive B-cells, which populate the mantle zone of the secondary lymphoid follicles, are the cells of origin of mantle cell lymphoma. Overexpression of cyclin D1 is not sufficient by itself to cause lymphoma, and a better understanding of the additional molecular lesions may provide insights toward new therapeutic approaches. In this context, large scale gene expression studies may be useful in the investigation of such additional molecular lesions. However, the great majority of mantle cell lymphoma cases studied by these methods to date had the genetic material harvested from lymph nodes, which have a variable proportion of normal cells from the lymphoid stroma. It is therefore not known how many genes identified as differentially expressed in mantle cell lymphoma by tumor versus normal experiments are cell-autonomous rather than dependent on the tumor microenvironment. To address this issue, we compared the gene expression profile of mantle cell lymphoma cells and normal naive B-cells using oligonucleotide microarrays. Lymphoma cells and naive B-cells (IgD+CD38±CD27-) were highly purified, by magnetic activated cell sorting, from the peripheral blood of patients with mantle cell lymphoma in the leukemic phase and from tonsils of normal individuals, respectively (purity > 95% in all samples). Three individuals were selected for each group and experiments were performed in replicates using the Amersham CodeLink Human UniSet I Bioarrays, with 10,000 genes. We identified 106 genes differentially expressed with a fold change of at least three-fold, 63 induced and 43 repressed in mantle cell lymphoma in comparison with naive B-cells. Ten genes were selected (six induced and four repressed in lymphoma cells) for quantification by real-time RT-PCR in non-purified peripheral blood samples from 21 patients with mantle cell lymphoma in the leukemic phase, as well as in 14 patients with other chronic lymphoproliferative diseases and seven normal individuals. Microarray results were confirmed by real-time RT-PCR for all selected genes and expression values of the TLR1 gene as quantified by this method showed significant correlation with patient survival in mantle cell lymphoma. In addition to the identification of several modulated genes in mantle cell lymphoma at cellular level, this study revealed that some genes functionally connected through apoptosis or the PI3K/AKT, WNT and TGFβ signaling pathways are aberrantly expressed in mantle cell lymphoma. These results add original data to the molecular pathogenesis of mantle cell lymphoma and point to specific molecular signaling pathways related to inhibition of apoptosis as potential targets for new therapeutic approaches.
expressão gênica
linfoma de células do manto
linfoma não-Hodgkin
microarrays
gene expression profiling
mantle cell lymphoma
microarrays
non-Hodgkin’s lymphoma

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