Einfluss einer Radiatio in der Salvagetherapie aggressiver Lymphome auf das Gesamtüberleben sowie auf das rezidiv- bzw. progressfreie Überleben in Abhängigkeit von einer Erstlinientherapie mit und ohne Rituximab / Regarding Salvage Therapy of Aggressive B-Cell Lymphoma: Impact of Radiotherapy on Overall and Event-Free Survival Dependent on an Initial Treatment Regime with or without the Anti-CD20 Monoclonal Antibody Rituximab

Börger, Lara

12 June 2019

No description available.

610

Strahlentherapie

Hochmaligne B-Zell Lymphome

Diffus großzelliges B-Zell Lymphom

Rezidiv

Progress

Rituximab

Rituximab

progress

relapse

Aggressive B-cell non-Hodgkin lymphoma

radiation therapy

diffuse large b-cell lymphoma

Medizin (PPN619874732)

Onkologie (PPN619875895)

Hämatologie (PPN61987581X)

Pesquisa de células-tronco tumorais em pacientes com linfoma não-Hodgkin / Research on cancer stem cells in patients with non-Hodgkin lymphoma

Silva, André Luiz Siqueira da

06 May 2014

Células-tronco (CT) são células com um alto poder de indiferenciação, plasticidade celular e autorrenovação. Baseado na autorrenovação das CT, pesquisas recentes sugerem que uma falha durante este processo pode levar ao surgimento de um novo tipo de célula, sendo esta responsável pelo aparecimento, propagação e manutenção de diversos tipos de neoplasias. Além disso, apresenta resistência às formas de tratamento convencionais do câncer. Tais células foram denominadas de células-tronco tumorais (CTT). As CTT já foram caracterizadas em leucemias e em diversos tipos de tumores sólidos, porém, até o presente momento, não foram descritas em linfoma não- Hodgkin (LNH). Por esta razão, o presente estudo teve como objetivo investigar a presença de CTT em pacientes com LNH. Biópsias de linfonodos e medulas ósseas (MO) de pacientes com LNH foram as fontes utilizadas para isolar e cultivar as CT mesenquimais. Uma vez caracterizadas as CTT, estas foram inoculadas em camundongos imunodeprimidos para observar uma possível formação de tumor. As células isoladas de biópsias de linfonodo não apresentaram CD133 positivo, marcador de membrana presente nas CTT, bem como não expressaram os genes de indiferenciação (Nanog e Oct-4) e não formaram tumores quando inoculadas nos animais. Por outro lado, as células isoladas de MO apresentaram subpopulações de células positivas para o CD133, expressaram os genes de indiferenciação e, após inoculadas, desenvolveram tumores em camundongos imunodeprimidos. Com isto, concluise que as células isoladas dos linfonodos possam ser fibroblastos, indicando, assim, uma dificuldade de se isolar as CTT deste material. Enquanto que, como já bem descrito e estabelecido na literatura, CT foram facilmente isoladas de MO, entretanto, quando isoladas de pacientes LNH foi ainda possível caracterizar a presença de uma subpopulação de CTT / Stem cells (SC) are undifferentiated cells, with high capacity of cellular plasticity and self-renewal. Based on the self-renewal, recent research suggests that a failure during this process, it can lead to the emergence of a new type of cell, which is responsible for the development, propagation and maintenance of several types of malignancies. Moreover, it is resistant to the conventional treatment of cancer. These cells are denominated as cancer stem cells (CSC). CSC were already characterized in leukemia and in several types of solid tumors. However, until the present moment nothing was described in non- Hodgkin lymphoma (NHL). For this reason, the present study aimed to investigate the presence of CSC in patients with NHL. Biopsies of lymph nodes and bone marrow (BM) from patients with NHL were used for isolate and cultivate MSC. The techniques used to characterize these cells were flow cytometry and PCR. Once CSC were characterized, these cells were inoculated into immunodeficient animals to observe a possible tumor formation. Cells isolated from lymph node biopsies did not show the presence of CD133, a membrane marker present in the CSC, as well as did not express differentiation genes (Nanog and Oct-4) and no ability to form tumors in immunodeficient mice. In another hands, cells isolated from BM showed a subpopulation of CD133 positive, expressed undifferentiated genes and also after the inoculation was possible to observe the tumor formation in immunodeficient mice. In conclusion, isolated cells from lymph nodes could be fibroblasts, indicating a difficulty to isolate CSC from this material. Whereas, as already describe and establish in the literature, SC were easily isolate from MO. However, when isolated from NHL patients was possible to characterize the presence of CSC subpopulation

Camundongos nus

Cell transformation

Cell division

Células-tronco

Células-tronco neoplásicas

Divisão celular

Humanos

Humans

Linfoma não-Hodgkin

Mice nus

Neoplastic stem cells

Non-Hodgkin lymphoma

Stem cells

Transformação celular

Sobreviventes de linfoma não Hodgkin: agrupamento de sintomas e qualidade de vida / Non-Hodgkin Lymphoma Survivors: Grouping of Symptoms and Quality of Life

OLIVEIRA, Mariany Melo

11 April 2017

Submitted by Rosivalda Pereira (mrs.pereira@ufma.br) on 2017-10-04T19:49:22Z No. of bitstreams: 1 MarianyOliveira.pdf: 2011433 bytes, checksum: 0c698b1c9b1cd49abde1a5c6be92d253 (MD5) / Made available in DSpace on 2017-10-04T19:49:22Z (GMT). No. of bitstreams: 1 MarianyOliveira.pdf: 2011433 bytes, checksum: 0c698b1c9b1cd49abde1a5c6be92d253 (MD5) Previous issue date: 2017-04-11 / Introduction: The growing number of non-Hodgkin lymphoma (NHL) survivors and the lower quality of life (QoL) survivors have been accompanied by the clustering of difficult symptoms. Also, the categorization of survivors from similar characteristics, has been presented as a strategy in the care of this population. Objective: To analyze QoL and clustering of symptoms in NHL survivors. Methods: Cross-sectional study with a non-probabilistic, 79 patients / survivors followed up at a specialized oncohematology outpatient clinic. The EORTC-QLQC30 (QoL), the Revised Piper Fatigue Scale-RPFS (fatigue), the Distress Thermometer-DT (distress), the Mini-Sleep Questionnaire-MSQ (sleep disorders) and the Visual Analog ScaleVAS (pain), as well as socioeconomic, demographic and clinical data were used. Results: Survivors averaged 57,24 (SD = 5.10) years of age, 70.88% were 50 years old or older, 53,16% were males, and 65,82% had a good level of Karnofsky Performance Status Scale (KPS). The mean time since diagnosis was 3,29 years (SD = 3,67), 36,70% were in acute survival, followed by extended survival (24,05%) and long-term survival (19,00%). The overall mean QoL was high (73,12, SD=18,93). Few reported fatigue (18,31%). More than half reported some sleep disturbance and presence of pain, 56,05% and 56,96%, respectively. The prevalence of distress was quite high (81,69%). 62,02% of the sample reported some clustering of symptoms, the most prevalent: distress-pain-sleep disorder (20,25%), distress-pain (11,39%) e distress-pains-sleep disorder-fatigue (11,39%). Survival categories with active disease had worse overall QoL (p = 0.0073) and worse role performance (p = 0.0005). There was significant association between QoL and survival categories (p = 0.0397), with higher means among the categories in remission. Overall QoL scores were higher in the groups with distress (p = 0.0129) and pain (p = 0.0331). No significant association was found between the selected clusters of symptoms and global QoL. Conclusion: The means of QoL were high. The most prevalent survival categories were acute, followed by extended and long term. Association significant between QoL and survival categories was observed, and the categories in remission presented better overall QoL levels. Differences were found between the means of QoL in the distress and pain groups. Clusters of symptoms were present in more than half of the survivors. Distress-pain-sleep disorder was the most frequent. There was no association between the main clusters of symptoms and QoL. / Introdução: O aumento progressivo de sobreviventes de Linfoma não Hodgkin (LNH) e os níveis inferiores de qualidade de vida (QV) vêm sendo acompanhados da ocorrência agrupada de sintomas difíceis. Também, a categorização de sobreviventes, a partir de características semelhantes, vem sendo apresentada como estratégia no seu cuidado. Objetivo: Analisar QV e agrupamento de sintomas em sobreviventes de LNH. Materiais e Métodos: Estudo transversal, com amostra não-probabilística, de 79 pacientes/sobreviventes acompanhados em ambulatórios especializados de oncohematologia. Foram utilizados as escalas EORTCQLQC30 (QV), a Escala de Fadiga de Piper Revisada-EFPR (fadiga), o Termômetro de Distress – TD (distress), o Questionário Mini-Sleep-QMS (distúrbio do sono) e a Escala Visual Analógica-EVA (dor), além de dados socioeconômicos, comportamentais e clínicos. Resultados: Os sobreviventes tinham em média 57,24 anos (dp=5,10), 70,88% tinha 50 anos ou mais, 53,16% eram do sexo masculino, e 65,82% tinham bom nível na Escala de Funcionalidade de Karnofsky (KPS). O tempo médio de diagnóstico foi de 3,29 anos (dp=3,67), 36,70% estavam em sobrevivência aguda, seguidos de sobrevivência estendida (24,05%) e de longo prazo (19,00%). A média global de QV foi elevada (73,12±18,93). Poucos relataram fadiga (18,31%). Mais da metade tinha alguma alteração do sono e presença de dor, 56,05% e 56,96%, respectivamente. A prevalência de distress foi bastante elevada (81,69%). 62,02% da amostra apresentava algum agrupamento de sintomas, sendo os mais prevalentes: distress-dordistúrbio do sono (20,25%), distress-dor (11,39%) e distress-dor-distúrbio do sono-fadiga (11,39%). Categorias de sobrevivência com doença ativa tiveram pior medida global de QV (p=0,0073) e pior desempenho de papeis (p=0,0005). Houve associação significante entre QV e categorias de sobrevivência (p=0,0397), com médias maiores entre as categorias em remissão. Os escores globais da QV foram mais elevados nos grupos com distress (p=0,0129) e com dor (p=0,0331), com diferenças significantes. Não foi encontrada associação significante entre grupos de sintomas selcionados e QV global. Conclusão: A média de QV global foi elevada. As categorias de sobrevivência mais prevalentes foram a aguda, seguida da estendida e da de longo prazo. Foi observada associação entre QV e categorias de sobrevivência, tendo as categorias em remissão apresentado melhores níveis de QV global. Foram encontradas diferenças entre as médias de QV nos grupos com distress e com dor. Os agrupamentos de sintomas estiveram presentes em mais da metade dos sobreviventes, sendo distress-dordistúrbio do sono o mais frequente. Não houve associação entre os principais agrupamentos de sintomas e a QV.

Sobrevivência

Linfoma não Hodgkin

Qualidade de Vida

Fadiga

Estresse Psicológico

Dor

Survival

Non-Hodgkin Lymphoma

Quality of Life

Fatigue

Psychological Stress

Pain

Ciências da Saúde

Bystander Cells and Prognosis in Hodgkin Lymphoma

Molin, Daniel

January 2002

<p>Hodgkin lymphoma (HL) is characterised histologically by a minority of malignant Hodgkin and Reed-Sternberg (HRS) cells surrounded by benign cells, and clinically by a relatively good prognosis. The treatment, however, leads to a risk of serious side effects. Knowledge about the biology of the disease, particularly the interaction between the HRS cells and the surrounding cells, is essential in order to improve diagnosis and treatment. </p><p>HL patients with abundant eosinophils in the tumours have a poor prognosis, therefore the eosinophil derived protein eosinophil cationic protein (ECP) was studied. Serum-ECP (S-ECP) was elevated in most HL patients. It correlated to number of tumour eosinophils, nodular sclerosis (NS) histology, and the negative prognostic factors high erythrocyte sedimentation rate (ESR) and blood leukocyte count (WBC). A polymorphism in the ECP gene (434(G>C)) was identified and the 434GG genotype correlated to NS histology and high ESR.</p><p>The poor prognosis in patients with abundant eosinophils in the tumours has been proposed to depend on HRS cell stimulation by the eosinophils via a CD30 ligand (CD30L)-CD30 interaction. However, CD30L mRNA and protein were detected in mast cells and the predominant CD30L expressing cell in HL is the mast cell. Mast cells were shown to stimulate HRS cell lines via CD30L-CD30 interaction. The number of mast cells in HL tumours correlated to worse relapse-free survival, NS histology, high WBC, and low blood haemoglobin. </p><p>Survival in patients with early and intermediate stage HL, diagnosed between 1985 and 1992, was generally favourable and comparatively limited treatment was sufficient to produce acceptable results for most stages. The majority of relapses could be salvaged. Patients treated with a short course of chemotherapy and radiotherapy had an excellent outcome.</p><p>In conclusion prognosis is favourable in early and intermediate stages and there are possibilities for further improvements based on the fact that mast cells and eosinophils affect the biology and prognosis of HL.</p>

Oncology

Hodgkin Lymphoma

Bystander cells

Eosinophilic granulocytes

Eosinophil cationic protein (ECP)

Mast cells

Prognosis

Early and Intermediate stage

Onkologi

Hodgkin lymfom

eosinofila granulocyter

ECP

mast celler

prognos

tidiga och intermediära stadier

Oncology

Onkologi

Bystander Cells and Prognosis in Hodgkin Lymphoma

Molin, Daniel

January 2002

Hodgkin lymphoma (HL) is characterised histologically by a minority of malignant Hodgkin and Reed-Sternberg (HRS) cells surrounded by benign cells, and clinically by a relatively good prognosis. The treatment, however, leads to a risk of serious side effects. Knowledge about the biology of the disease, particularly the interaction between the HRS cells and the surrounding cells, is essential in order to improve diagnosis and treatment. HL patients with abundant eosinophils in the tumours have a poor prognosis, therefore the eosinophil derived protein eosinophil cationic protein (ECP) was studied. Serum-ECP (S-ECP) was elevated in most HL patients. It correlated to number of tumour eosinophils, nodular sclerosis (NS) histology, and the negative prognostic factors high erythrocyte sedimentation rate (ESR) and blood leukocyte count (WBC). A polymorphism in the ECP gene (434(G&gt;C)) was identified and the 434GG genotype correlated to NS histology and high ESR. The poor prognosis in patients with abundant eosinophils in the tumours has been proposed to depend on HRS cell stimulation by the eosinophils via a CD30 ligand (CD30L)-CD30 interaction. However, CD30L mRNA and protein were detected in mast cells and the predominant CD30L expressing cell in HL is the mast cell. Mast cells were shown to stimulate HRS cell lines via CD30L-CD30 interaction. The number of mast cells in HL tumours correlated to worse relapse-free survival, NS histology, high WBC, and low blood haemoglobin. Survival in patients with early and intermediate stage HL, diagnosed between 1985 and 1992, was generally favourable and comparatively limited treatment was sufficient to produce acceptable results for most stages. The majority of relapses could be salvaged. Patients treated with a short course of chemotherapy and radiotherapy had an excellent outcome. In conclusion prognosis is favourable in early and intermediate stages and there are possibilities for further improvements based on the fact that mast cells and eosinophils affect the biology and prognosis of HL.

Oncology

Hodgkin Lymphoma

Bystander cells

Eosinophilic granulocytes

Eosinophil cationic protein (ECP)

Mast cells

Prognosis

Early and Intermediate stage

Onkologi

Hodgkin lymfom

eosinofila granulocyter

ECP

mast celler

prognos

tidiga och intermediära stadier

Oncology

Onkologi

Assoziation von Genpolymorphismen der 5 flankierenden Region des Interleukin-10-Gens auf das Überleben oder die Remissionsrate beim aggressiven Non-Hodgkin-Lymphom / Association of gen polymorphism of the 5

Hua, Thanh Duc

15 September 2009

No description available.

610 Medizin, Gesundheit

Medicine

IL-10

Polymorphismus

aggressives Non-Hodgkin-Lymphom

Zytokine

Interleukin-10

Genvariationen

IL-10

polymorphism

aggressive Non-Hodgkin lymphoma

cytokine

interleukin-10

gene variations

44.81

MED 424: Onkologie

Étude de mortalité de cinq cancers : mélanome cutané, cancer broncho-pulmonaire, leucémie myéloïde chronique, maladie de Hodgkin et cancer de l’endomètre

Kharmachi, Fathi

12 1900

No description available.

Mélanome cutané

Cancer du poumon

Leucémie myéloïde chronique

Lymphome de Hodgkin

Cancer de l'endomètre

Mortalité

Survie

Lung cancer

Chronic Myelocytic leukemia

Hodgkin Lymphoma

Endometrial Cancer

Mortality

Survival

Prognosis

Skin melanoma

Pronostic

Avaliação da expressão do vírus de Epstein-Barr e metaloproteinase 9 nas células de Hodgkin-Reed-Sternberg e correlação com os parâmetros clínicos e evolutivos em pacientes com Linfoma de Hodgkin clássico no Brasil / Matrix Metalloproteinase-9 is consistently expressed in Hodgkin-Reed-Sternberg cells and has no impact on survival in patients with Epstein-Barr virus (EBV) related and non-related Hodgkin lymphoma in Brazil

Souza, Eni Maria de [UNIFESP]

24 February 2010

Made available in DSpace on 2015-07-22T20:49:30Z (GMT). No. of bitstreams: 0 Previous issue date: 2010-02-24. Added 1 bitstream(s) on 2015-08-11T03:26:30Z : No. of bitstreams: 1 Publico-429a.pdf: 1596515 bytes, checksum: 2107c026687c3e2ecc62f0a5fffa1409 (MD5). Added 1 bitstream(s) on 2015-08-11T03:26:30Z : No. of bitstreams: 2 Publico-429a.pdf: 1596515 bytes, checksum: 2107c026687c3e2ecc62f0a5fffa1409 (MD5) Publico-429b.pdf: 1614171 bytes, checksum: d98715f7a666adc5ceb185cce978000e (MD5). Added 1 bitstream(s) on 2015-08-11T03:26:30Z : No. of bitstreams: 3 Publico-429a.pdf: 1596515 bytes, checksum: 2107c026687c3e2ecc62f0a5fffa1409 (MD5) Publico-429b.pdf: 1614171 bytes, checksum: d98715f7a666adc5ceb185cce978000e (MD5) Publico-429c.pdf: 1500700 bytes, checksum: 77791620b06c9404d28496c4f4ca3dc3 (MD5). Added 1 bitstream(s) on 2015-08-11T03:26:30Z : No. of bitstreams: 4 Publico-429a.pdf: 1596515 bytes, checksum: 2107c026687c3e2ecc62f0a5fffa1409 (MD5) Publico-429b.pdf: 1614171 bytes, checksum: d98715f7a666adc5ceb185cce978000e (MD5) Publico-429c.pdf: 1500700 bytes, checksum: 77791620b06c9404d28496c4f4ca3dc3 (MD5) Publico-429d.pdf: 1826591 bytes, checksum: 70c3dc706cb97372e3f26a7452c01208 (MD5) / O Linfoma de Hodgkin clássico (LHC) é caracterizado pela presença de uma pequena população de células grandes mono ou multinucleadas, denominadas células de Hodgkin-Reed-Sternberg (HRS), circundadas por uma grande massa inflamatória de células não neoplásicas. O vírus Epstein-Barr (EBV) está associado ao Linfoma de Hodgkin em cerca de 50% dos casos. O diagnóstico do LH EBV relacionado é possível por meio da identificação de proteínas virais nas células HRS. Os métodos considerados ideais para essa identificação são as reações de imuno-histoquímica utilizando anticorpos antiproteína latente de membrana (LMP1) e hibridação in situ com uma sonda para o RNA viral (EBER). A LMP-1 é considerada um oncogene clássico. Foi demonstrado que a LMP-1 pode controlar a expressão do gene da metaloproteinase 9 (MMP-9), em linhagem de células C33A. A MMP-9 é um membro da família das endopeptidases que facilita a invasão tumoral e metástases pela degradação do estroma extracelular. Objetivos: avaliar se a expressão da MMP-9 está relacionada ao status do EBV no tumor e se houve impacto na sobrevida livre de eventos (SLE) e sobrevida global (SG) em pacientes com LHC. Casuística e Métodos: foram examinados 97 pacientes com LHC. Todos os pacientes foram submetidos a protocolos de tratamentos equivalentes (MOPPABV ou ABVD). O diagnóstico histopatológico foi revisto e o subtipo classificado de acordo com a OMS. Reações de imuno-histoquímica para LMP-1 e MMP-9 e hibridação in situ para EBER foram realizadas. Resultados: A presença do EBV foi identificada em 52,5% dos casos. Houve uma maior prevalência do subtipo histológico celularidade mista em pacientes EBV positivos (P = 0,005). Não houve diferença na positividade do EBV em relação à faixa etária, sexo, estádio da doença ou pela presença de sintomas B. A presença do EBV no LHC não influenciou a SLE (P = 0,38) ou a SG (P = 0,80) com uma mediana de acompanhamento de 71 meses. A expressão da MMP-9 ocorreu em 87,6% dos casos estudados. Não houve diferença de casos positivos e negativos em relação ao status do EBV (P = 0,59). Quando avaliada a intensidade da expressão da MMP-9 nos casos positivos também não observamos correlação com a presença do EBV (P = 0,62). Não houve diferença entre o resultado da MMP-9 e os parâmetros: subtipo histológico, estádio, presença de sintomas B, idade e sexo. Não houve influência da MMP-9 na SLE (P = 0,98) e SG (P = 0,60). Conclusões: Demonstramos que a prevalência do LH relacionado ao EBV na população estudada é de 52,5%, e que a presença do vírus não altera a evolução clínica, SLE e SG de pacientes tratados uniformemente. Concluímos ainda que a MMP-9 é fortemente expressa nas células HRS. Não há correlação entre a expressão de MMP-9 e o status do EBV. Nem a SG nem a SLE foram influenciadas pela expressão dessa enzima. / Clinical and histological features of classical Hodgkin lymphoma (cHL) are primarily due to the effects of cytokines, enzymes and chemokines produced by Hodgkin-Reed-Sternberg (HRS) cells and their surrounding inflammatory cells in response to signals triggered by etiological factors such as Epstein-Barr virus (EBV). Matrix metalloproteinase-9 (MMP-9) has been associated with poorer survival in patients with aggressive non-Hodgkin lymphomas. In EBV-related cancers the expression of viral latent membrane protein 1 (LMP1) correlates with an increased MMP-9 expression. In this study, we evaluated the prognostic relevance of MMP-9 expression and EBV status in HRS cells in patients with cHL in Brazil. Material and Methods: We selected 97 patients with cHL. Patients were included if they had: 1) > 18 years, 2) Undergone similar chemotherapy protocols, 3) Paraffin blocks available for review and for EBV and MMP-9 detection and 4) Clinical, epidemiological and laboratorial parameters available. Results: EBV was detected in 52.5% of all cases. MMP-9 expression positivity was found in 87.6% of all cases. There was no correlation between MMP-9 expression and EBV status. Response to treatment and relapse rate were independent of MMP-9 expression and EBV status. When stratified according to chemotherapy protocol used or disease stage, we still did not find any difference. MMP-9 positivity did not influence overall survival and event free survival. Conclusion: MMP-9 are expressed in the majority of HRS cells and did not correlated with EBV status or survival. The consistent MMP-9 expression in HRS cells makes this enzyme a potential target for therapy. / TEDE / BV UNIFESP: Teses e dissertações

Epstein-Barr virus

Metaloproteinase 9

Prognóstico

Vírus Epstein-Barr

Linfoma de Hodgkin clássico

Doença de Hodgkin

Herpesvirus Humano 4

Metaloproteinase 9 da Matriz

Metalloproteinase-9

Prognostic

Survival

Hodgkin lymphoma

Hodgkin Disease

Herpesvirus 4, Human

Matrix Metalloproteinase 9

Pesquisa de células-tronco tumorais em pacientes com linfoma não-Hodgkin / Research on cancer stem cells in patients with non-Hodgkin lymphoma

André Luiz Siqueira da Silva

06 May 2014

Células-tronco (CT) são células com um alto poder de indiferenciação, plasticidade celular e autorrenovação. Baseado na autorrenovação das CT, pesquisas recentes sugerem que uma falha durante este processo pode levar ao surgimento de um novo tipo de célula, sendo esta responsável pelo aparecimento, propagação e manutenção de diversos tipos de neoplasias. Além disso, apresenta resistência às formas de tratamento convencionais do câncer. Tais células foram denominadas de células-tronco tumorais (CTT). As CTT já foram caracterizadas em leucemias e em diversos tipos de tumores sólidos, porém, até o presente momento, não foram descritas em linfoma não- Hodgkin (LNH). Por esta razão, o presente estudo teve como objetivo investigar a presença de CTT em pacientes com LNH. Biópsias de linfonodos e medulas ósseas (MO) de pacientes com LNH foram as fontes utilizadas para isolar e cultivar as CT mesenquimais. Uma vez caracterizadas as CTT, estas foram inoculadas em camundongos imunodeprimidos para observar uma possível formação de tumor. As células isoladas de biópsias de linfonodo não apresentaram CD133 positivo, marcador de membrana presente nas CTT, bem como não expressaram os genes de indiferenciação (Nanog e Oct-4) e não formaram tumores quando inoculadas nos animais. Por outro lado, as células isoladas de MO apresentaram subpopulações de células positivas para o CD133, expressaram os genes de indiferenciação e, após inoculadas, desenvolveram tumores em camundongos imunodeprimidos. Com isto, concluise que as células isoladas dos linfonodos possam ser fibroblastos, indicando, assim, uma dificuldade de se isolar as CTT deste material. Enquanto que, como já bem descrito e estabelecido na literatura, CT foram facilmente isoladas de MO, entretanto, quando isoladas de pacientes LNH foi ainda possível caracterizar a presença de uma subpopulação de CTT / Stem cells (SC) are undifferentiated cells, with high capacity of cellular plasticity and self-renewal. Based on the self-renewal, recent research suggests that a failure during this process, it can lead to the emergence of a new type of cell, which is responsible for the development, propagation and maintenance of several types of malignancies. Moreover, it is resistant to the conventional treatment of cancer. These cells are denominated as cancer stem cells (CSC). CSC were already characterized in leukemia and in several types of solid tumors. However, until the present moment nothing was described in non- Hodgkin lymphoma (NHL). For this reason, the present study aimed to investigate the presence of CSC in patients with NHL. Biopsies of lymph nodes and bone marrow (BM) from patients with NHL were used for isolate and cultivate MSC. The techniques used to characterize these cells were flow cytometry and PCR. Once CSC were characterized, these cells were inoculated into immunodeficient animals to observe a possible tumor formation. Cells isolated from lymph node biopsies did not show the presence of CD133, a membrane marker present in the CSC, as well as did not express differentiation genes (Nanog and Oct-4) and no ability to form tumors in immunodeficient mice. In another hands, cells isolated from BM showed a subpopulation of CD133 positive, expressed undifferentiated genes and also after the inoculation was possible to observe the tumor formation in immunodeficient mice. In conclusion, isolated cells from lymph nodes could be fibroblasts, indicating a difficulty to isolate CSC from this material. Whereas, as already describe and establish in the literature, SC were easily isolate from MO. However, when isolated from NHL patients was possible to characterize the presence of CSC subpopulation

Camundongos nus

Células-tronco

Células-tronco neoplásicas

Divisão celular

Humanos

Linfoma não-Hodgkin

Transformação celular

Cell transformation

Cell division

Humans

Mice nus

Neoplastic stem cells

Non-Hodgkin lymphoma

Stem cells

[18F] Fludarabine pour l'imagerie TEP des lymphomes / [18F] Fludarabine-PET for lymphoma imaging

Hovhannisyan, Narinée

26 September 2018

Bien que l’utilité de la TEP au [18F]FDG soit confirmée pour le diagnostic et le suivi thérapeutique chez les patients atteints de lymphome, la spécificité de la captation du [18F]FDG a été mise en doute en raison de sa dépendance au métabolisme du glucose, qui peut augmenter dans des conditions bégnines comme les processus inflammatoire ou infectieux. Compte tenu de ces limites, un nucléoside a été développé en tant que nouvel outil pour l'imagerie TEP ([18F]fludarabine). Une radiosynthèse entièrement automatisée a été mise en place et des études précliniques ont été menées sur des modèles murins de xénogreffes (lignées cellulaires folliculaires: RL7 et DOHH-2, myélome multiple (MM) : RPMI8226, lymphome du système nerveux central (LSNC) : MC116), parallèlement au [18F]FDG. Le profil de distribution de la radioactivité de la [18F]fludarabine dans des organes sélectionnés a confirmé le ciblage spécifique de la tumeur. Dans un modèle de lymphome folliculaire, nous avons évalué sa fiabilité pendant le traitement par rituximab et démontré - pas d’interférence entre le traitement et sa captation - une plus forte corrélation entre la fixation de ce radiopharmaceutique et les valeurs quantitatives extraites de l'histologie, comparée au [18F]FDG-TEP. En conséquence, cet outil TEP peut être considéré comme une approche prometteuse pour détecter la maladie résiduelle persistante pendant ou après un traitement par chimiothérapie. En outre, l’évaluation de la [18F]fludarabine lors d’un processus inflammatoire induit par la térébenthine a montré une accumulation significativement plus faible dans le tissu inflammé par comparaison à celle observée avec le [18F]FDG. Dans le MM, le rôle de la [18F]FDG-TEP reste limité en raison de son manque de sensibilité pour détecter une atteinte diffuse de la moelle osseuse et de petites lésions crâniennes dues à la fixation physiologique du [18F]FDG dans le cerveau. Nos données suggèrent que la TEP à la [18F]fludarabine pourrait représenter une modalité alternative et peut-être plus spécifique pour l'imagerie de MM. Dans notre dernière étude, sur les tumeurs cérébrales de xénogreffes, ce nouvel outil TEP a révélé des réponses significativement divergentes entre le LSNC et le glioblastome (GBM), tandis que le [18F]FDG a montré un chevauchement de fixation entre ces deux modèles. Une première étude chez l'homme a été entreprise pour un diagnostic initial, où 10 patients non traités ont été recrutés avec une leucémie lymphoïde chronique à cellules B (LLC) ou un lymphome B diffus à grandes cellules (LBDGC). Les scanners partiels successifs ont été acquis pendant 250 mn après l’injection i.v d’une activité de 4MBq/kg. Les résultats avec les modalités conventionnelles (TDM et/ou [18F]FDG-TEP) ont également été considérés. L'étude a également été conçue pour estimer la dosimétrie pour les principaux organes. Chez les patients atteints d’un LBDGC, une augmentation de la captation a été observée dans les sites considérés anormaux par TDM et [18F]FDG ; chez deux patients, des résultats contradictoires ont été observés avec ces deux radiopharmaceutiques. Chez les patients LLC, la fixation de la [18F]fludarabine a coïncidé avec les sites susceptibles d'être impliqués et a montré une captation significative dans la moelle osseuse hématopoïétique. Aucune fixation n'a été observée, quel que soit le groupe de maladies, dans le muscle cardiaque et le cerveau. De plus, la dose efficace moyenne a été révélée inférieure à la dose efficace rapportée pour le [18F]FDG. En conclusion, ces résultats précliniques et cliniques ont révélé une grande spécificité de ce radiopharmaceutique pour les tissus lymphoprolifératifs. De plus, cela pourrait être un outil robuste pour quantifier plus précisément la maladie, même avec des processus inflammatoires, évitant ainsi les résultats faussement positifs, et une approche innovante pour l'imagerie des maladies lymphoprolifératives caractérisées par une faible activité mitotique. / Although PET using [18F]FDG has proved to be useful for diagnosis and therapy monitoring in patients with lymphoma, the specificity of [18F]FDG uptake has been critically questioned because of its dependence on glucose metabolism, which may indiscriminately increase in benign conditions such as inflammatory or infectious processes. Considering these drawbacks, an adenine nucleoside analogue was developed as a novel PET imaging probe ([18F]fludarabine). An efficient and fully automated radiosynthesis has been implemented and, subsequently preclinical studies in xenograft murine models (follicular cell lines: RL7 and DOHH-2, multiple myeloma (MM): RPMI8226, central nervous system (CNS) lymphoma: MC116) were conducted with this novel 18F-radiopharmaceutical in parallel with [18F]FDG. The pattern of the radioactivity distribution in selected organs confirmed the tumor-specific targeting. In a follicular lymphoma model, we evaluated its robustness during rituximab therapy and demonstrated - the treatment did not interfere with its uptake - a stronger correlation between quantitative values extracted from this 18F-radiopharmaceutical and histology when compared to [18F]FDG-PET. Accordingly, this PET tool may be considered as a promising approach for detecting the persistence of residual disease during or after rituximab-like treatment. Furthermore, its behaviour in turpentine-induced inflammatory process showed significantly weaker uptake in inflammation when compared to [18F]FDG. In MM, the role of [18F]FDG-PET remains limited because of its lack of sensitivity for detecting diffuse bone marrow involvement, small skull lesions due to the physiological [18F]FDG uptake in brain. Our data suggested that [18F]fludarabine-PET might represent an alternative and perhaps more specific modality for MM imaging. In our latest study, on xenograft brain tumors, this novel PET probe revealed significantly divergent responses between CNS lymphoma and glioblastoma (GBM), while [18F]FDG demonstrated overlap between the groups. A first in man study, was undertaken, for an initial diagnosis, where 10 untreated patients were enrolled with either B-cell chronic lymphocytic leukemia (CLL) or diffuse large B-cell lymphoma (DLBCL). Successive partial body scans were acquired for 250 min after i.v. injection with an activity of 4 MBq/kg. The results with conventional modalities (CT and/or [18F]FDG-PET) have also been investigated. The study was also designed to estimate its radiation dose for major organs. In DLBCL patients, increased uptake was observed in sites considered abnormal by CT and [18F]FDG; in two patients discrepancies were observed in comparison with [18F]FDG. In CLL patients, the uptake coincided with sites expected to be involved and displayed a significant uptake in hematopoietic bone marrow. No uptake was observed, whatever the disease group, in the cardiac muscle and brain. Moreover, its mean effective dose was below the effective dose reported for [18F]FDG. In conclusion, these preclinical and clinical findings revealed a great specificity of this 18F-radiopharmaeutical for lymphoma tissues. Furthermore, it might well be a robust tool for correctly quantifying the disease, even with inflammatory processes, thus avoiding the false-positive results, and an innovative approach for imaging lymphoid neoplasms with low mitotic activity.

Radiopharmaceutique

Fluor-18

TEP

Imagerie

Leucémie lymphoïde chronique

Multiple myélome

Lymphome cérébral

Lymphome non-hodgkinien

Radiopharmaceutical

Lymphoma

Fluorine-18

Imaging

PET

Non-hodgkin lymphoma

Chronic lymphocytic leukemia

Multiple myeloma

Brain lymphoma