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

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

The EZH2 inhibitor tazemetostat upregulates the expression of CCL17/TARC in B-cell lymphoma and enhances T-cell recruitment / EZH2阻害剤tazemetostatは、B細胞リンパ腫におけるCCL17/TARCの発現を上昇させ、T細胞の遊走を促進する

Yuan, Hepei

23 March 2023

京都大学 / 新制・課程博士 / 博士(医学) / 甲第24496号 / 医博第4938号 / 新制||医||1064(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 滝田 順子, 教授 上野 英樹, 教授 河本 宏 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

B-cell lymphoma

CCL17

EZH2 inhibitor

Hodgkin lymphoma

tumor microenvironment

490

Genetische Variabilität in der phagozytären NAD(P)H-Oxidase: Funktionelle Charakterisierung und Bedeutung für die Zytostatika-Therapie / Genetic variability of phagocytic NAD(P)H oxidase: functional characterisation and impact on chemotherapy

Hoffmann, Marion

23 April 2008

No description available.

570 Biowissenschaften, Biologie

Mathematics and Computer Science

NAD(P)H-Oxidase

SNP

Doxorubicin

CHO(E)P

Non-Hodgkin-Lymphoma

Kardiotoxizität

CYBA

NAD(P)H oxidase

SNP

doxorubicin

CHO(E)P

Non-Hodgkin lymphoma

cardiotoxicity

CYBA

42.2

WA 000: Biologie

Radiation-related cardiovascular disease following cancer therapy

Cutter, David J.

January 2014

<b><u>Introduction:</b></u> Some cancer survivors are known to have an elevated risk of morbidity and mortality from cardiovascular disease. An important cause of this elevated risk is recognised to be irradiation of normal tissues during radiotherapy received as part of cancer therapy. There are substantial difficulties in studying radiation-related cardiovascular disease (RRCD). The reasons for this include the complexities of measuring radiation normal tissue doses retrospectively and the prolonged latencies of many of the cardiovascular endpoints. A variety of complimentary research methodologies can help provide additional knowledge to guide the appropriate management of patients treated in the past and of new patients in the future. <b><u>Methods:</b></u> 1) A cohort study of mortality from circulatory disease in the nationwide British Childhood Cancer Survivor Study (BCCSS). 2) A case-control study of valvular heart disease (VHD) in Dutch Hodgkin lymphoma (HL) survivors, including retrospective radiation dosimetry to estimate the radiation dose to heart valves. 3) A dosimetric study of cardiovascular radiation doses in patients entered into the UK NCRI Lymphoma Study Group RAPID trial, including predictions of 15-year cardiac mortality using innovative methods. 4) A modelling study to predict mean whole heart dose (MWHD) from involved field radiotherapy (IFRT) for HL using anatomical measures. 5) A prospective study using cardiovascular magnetic resonance (CMR) imaging to characterise the heart in women receiving radiotherapy for breast cancer. <b><u>Results:</b></u> 1) The risks of all types of circulatory mortality are elevated in survivors of childhood cancer. The absolute excess risks continue to increase 40+ years following diagnosis. The risk of death from cardiomyopathy and heart failure increased substantially with the introduction of anthracycline chemotherapy. There is no evidence of a reduction in risk of circulatory mortality in more recent eras of diagnosis. 2) There is a strong relationship between estimated radiation dose to the affected heart valve and the risk of subsequent VHD (p<0.001). This effect was modelled to allow prediction of the risk of VHD. 3) A proportion of patients treated with IFRT received a substantial cardiac radiation dose (MWHD = 8.8 Gy, SD = 5.6) but, on average, the predicted 15-year cardiac mortality following treatment is low (absolute risk 0.2%, range 0.0 to 2.7%). 4) It is possible to estimate the mean whole heart dose from IFRT prior to detailed radiotherapy planning based on pre-treatment diagnostic imaging to an accuracy of 5-6% of the prescribed dose. 5) Although women received low cardiac doses (MWHD = 1.5 Gy, SD = 0.8) and have a low predicted risk of cardiac radiation-related morbidity and mortality, there is some evidence of subclinical effects on strain and strain rate imaging of the anterior portions of the left ventricle that receive the highest radiation dose. <b><u>Conclusions:</b></u> Using a variety of methods these studies have all succeeded in adding to knowledge about the nature, magnitude and timing of RRCD. This knowledge can be used to help the future management of cancer patients. In addition, each of the studies has natural and planned extensions and will continue to contribute further knowledge into the future.

616.99

Implication du contrôle apoptotique exercé par les couples nétrine-1 et ses récepteurs à dépendance (DCC et UNC5B) au cours du développement embryonnaire et de la tumorigenèse : la signalisation apoptotique des récepteurs à dépendance : interface entre physiologie et pathologie / Involvement of netrin-1/Dependence receptors (DCC and UNC5B) apoptotic control during embryonic development and tumorigenesis : apoptosis induced by dependence receptors : interface between physiology and pathology

Broutier, Laura

20 June 2014

Les récepteurs à dépendance présentent la particularité d’induire deux voies de signalisation différentes selon la disponibilité de leur ligand. En présence de leur ligand, ils transduisent une voie de signalisation favorisant notamment la survie cellulaire (signalisation positive), tandis qu’en son absence, ils induisent activement l’apoptose des cellules (signalisation négative). La dualité fonctionnelle de ces récepteurs pourrait leur conférer un rôle central au cours du développement embryonnaire, mais aussi dans le maintien de l’homéostasie cellulaire chez l’adulte. En effet, du fait de leur signalisation pro-apoptotique, les récepteurs à dépendance pourraient limiter le nombre de cellules (en fonction de la disponibilité en ligand), et réguler leur migration (dans des zones dépourvues de ligand), au cours des processus développementaux mais aussi en cas de prolifération tumorale et de dissémination métastatique. Au cours de ma thèse, j’ai donc développé différentes thématiques de recherche visant à préciser le rôle du contrôle apoptotique exercé par les couples nétrine-1/récepteurs à dépendance (DCC et UNC5B) au cours de la tumorigenèse et du développement embryonnaire. Dans ce cadre, nous avons montré que les souris exprimant une forme mutée du récepteur DCC, ayant perdu la capacité d’induire l’apoptose des cellules en absence de son ligand la nétrine-1, étaient prédisposées à la survenue de (1) cancers colorectaux dans un contexte prédisposant, et de (2) lymphomes non hodgkiniens (LNH) dans un modèle de vieillissement. Ces résultats suggèrent que DCC puisse agir comme un suppresseur de tumeur conditionnel, via sa voie de signalisation négative, en absence de son ligand nétrine-1. De plus, nous avons montré qu’il existe un gain de nétrine-1 dans une fraction significative de LNH de type B (LNH-B) chez l’Homme, gain qui leur confère un avantage sélectif en bloquant constitutivement l’apoptose induite par le récepteur DCC. Réciproquement, nous avons montré que l’utilisation d’un anticorps ciblant la nétrine-1 était capable de restaurer l’apoptose induite par le récepteur DCC non lié, dans des lignées tumorales humaines de LNH-B in vitro et ex-vivo dans un modèle de xénogreffe. Ainsi, nos résultats suggèrent que cibler l’interaction nétrine-1/DCC dans les LNH-B pourrait être une stratégie thérapeutique prometteuse. La partie « développement » de mon travail de thèse est encore préliminaire. Elle se focalise sur le rôle du contrôle apoptotique exercé par les couples nétrine-1/récepteurs à dépendance (DCC et UNC5B) au cours de la mise en place des réseaux vasculaire et nerveux chez l’embryon de souris / Dependence receptors share the common property of inducing two types of signaling cascades according to the availability of their ligand. In presence of their ligand, they induce a positive signal allowing cell survival whereas in its absence, they induce cell death by apoptosis. Dependence receptors dual functionality could play a major role both during the embryonic development and in the regulation of tissue homeostasis in adult. Indeed, apoptosis induced by dependence receptors would be a safeguard mechanism which regulates the number of cells and their migration during developmental or tumorigenic process. Thus, during my PhD, I have investigated the involvement of netrin- 1/dependence receptors (DCC and UNC5B) apoptotic control during tumorigenesis and embryonic development. We observed that DCC-mutant mice in which DCC pro-apoptotic signaling is genetically silenced show a higher propensity to develop colorectal cancers in a predisposing context and B-cell type non-Hodgkin lymphoma (B-NHL) with age, suggesting than DCC could act as a conditional tumor suppressor gene through its pro-apoptotic signaling, in absence of netrin-1. Moreover, we show that netrin-1 is overexpressed in a significant fraction of Human B-NHL, which confers tumor cells a selective advantage by blocking DCC-induced apoptosis. Reciprocally, we showed that inhibiting the interaction between netrin-1 and its DCC receptor restore apoptosis in lymphoma cells in vitro and in vivo in xenografts experiments, suggesting that targeting netrin-1 and DCC interaction in lymphoma could represent a promising anti-tumor therapeutic strategy. The "developmental" part of my PhD work is in progress and we obtained only few preliminary data. It focuses on the role of apoptotic control mediated by netrin1-/dependence receptor (DCC/UNC5B) during the development of vascular and neural networks in the mouse embryo

Récepteurs à dépendance

Apoptose

Cancers

Cancers colorectaux

Lymphomes non hodgkiniens

Dependence receptors

Apoptosis

Cancers

Colorectal cancers

Non-Hodgkin lymphoma

616.994

In vivo- und in vitro-Komplementaktivierung durch den monoklonalen CD20-Antikörper Rituximab bei der Behandlung von Non-Hodgkin-Lymphomen

Gerecke, Christian

07 July 2006

Rituximab (IDEC C2B8) ist ein chimärer monoklonaler Antikörper, der gegen das CD20-Antigen auf B-Lymphozyten gerichtet ist. In klinischen Studien konnten Ansprechraten von 50 Prozent bei Patienten mit niedrigmalignen NHL erzielt werden [61, 62]. Bei den hochmalignen NHL waren die Ansprechraten geringer, doch auch hier konnte eine therapeutische Wirksamkeit von Rituximab nachgewiesen werden [108]. Der genaue Wirkungsmechanismus, durch welchen Rituximab seinen therapeutischen Effekt erzielt, ist weiterhin nicht vollständig geklärt. Hauptsächlich werden dabei Apoptose, Komplement-vermittelte zelluläre Zytotoxizität (CDC) und die Antikörper-vermittelte Zytotoxizität (ADCC) diskutiert. In der vorliegenden Arbeit wurde in vitro die Proliferationsinhibition und die Komplement-vermittelte zelluläre Zytotoxizität durch Rituximab an verschiedenen humanen B-Zellinien geprüft. Anschließend wurde die in vivo-Komplementaktivierung während einer Rituximab-Infusion untersucht. Es konnte gezeigt werden, dass Rituximab in vitro eine unterschiedliche Wirksamkeit bei verschiedenen Lymphomzellinien aufweist. Durch Zugabe von humanem Komplement konnte bei zwei Zellinien eine Rituximab-induzierte CDC beobachtet werden. Bei sechs von zehn Patienten mit unterschiedlichen NHL wurde in vivo ein Anstieg der C3a-desArg-Konzentration im Plasma beobachtet. Die Ergebnisse dieser Arbeit zeigen, dass das Komplementsystem ein wichtiger Mechanismus für die Wirkung von Rituximab zu sein scheint. Die klinischen Erfolge sind viel versprechend, zeigen jedoch auch, dass der therapeutische Nutzen von Rituximab als Monotherapie begrenzt ist. Derzeit laufende prospektive Studien untersuchen die Wirksamkeit von Rituximab in Kombination mit verschiedenen Chemotherapeutika [106, 107]. Erste Ergebnisse sind viel versprechend, doch es bleibt abzuwarten, ob sich diese Ergebnisse auch langfristig in einer Verbesserung der Überlebensrate widerspiegeln. / The chimeric anti-CD20 monoclonal antibody rituximab is a new therapeutic tool for treatment of relapsed B-cell lymphomas. Because rituximab mediates complement-dependent cellular cytotoxicity (CDCC) and antibody-dependent cellular cytotoxicity (ADCC) in the lymphoblastoid cell line SB, it is suggested, that these two mechanisms are responsible for the in vivo antilymphoma effect. We tested the antiproliferative effect of rituximab in 6 CD20 positive human B cell lymphoma cell lines. In the follicular lymphoma cell line, DOHH-2, 1 µg/ml rituximab induces an inhibition of proliferation of 75.5 % (n=5), and in the diffuse large cell lymphoma cell line, Daudi, an inhibition of proliferation of 27.3 % (n=5). No effect was seen in the prelymphocytic leukemia cell line, JVM-2, the hairy cell leukemia cell line, Bonna-12, or the two high-grade lymphoma cell lines, Granta-519 and Raji. To test, whether complement increases the effect of rituximab, we studied the combination of rituximab plus complement. Guinea pig complement (dilution 1:10) increases the inhibitory effect of rituximab on the proliferation of Daudi cells. The degradation product C3a(desArg) is produced during complement cascade activation and could be used as a sensitive and specific marker of complement activation in vivo. So, we measured plasma C3a(desArg) concentration in two CLL patients receiving rituximab monotherapy. In one patient, no increase of plasma C3a(desArg) concentration could be measured during infusion of rituximab. In the other patient, in two treatment cycles C3a(desArg) increases drastically after 2 h of rituximab infusion. We conclude differential in vitro and in vivo effects of rituximab on CD20 positive lymphoma cells. Rituximab inhibits in vitro the proliferation of follicular and diffuse large cell lymphoma cells, which could be amplified by complement in Daudi cells. Furthermore, rituximab mediates in vivo complement cascade activation, highly suggestive of in vivo CDCC.

Rituximab

monoklone Antikörper

CD20

Non-Hodgkin-Lymphome

rituximab

monoclonal antibody

CD 20

Non-Hodgkin-lymphoma

610 Medizin

33 Medizin

ddc:610

Estudo de conjugação do anticorpo anti-CD20 para marcação com radionuclídeos metálicos ou lantanídeos / The study of conjugation of anti-CD20 monoclonal antibody for labeling with metalic or lanthanides radionuclides

Akanji, Akinkunmi Ganiyu

25 April 2013

Linfomas são cânceres que se iniciam a partir da transformação maligna de um linfócito no sistema linfático. Os linfomas são divididos em duas categorias principais: os linfomas de Hodgkin e todos os outros linfomas, denominados linfomas não-Hodgkin (LNH). Os pacientes com LNH são comumente tratados com radioterapia apenas ou combinada com quimioterapia utilizando-se de anticorpo monoclonal anti-CD20, principalmente o rituximab (MabThera&reg). O uso de anticorpos monoclonais (Acm) conjugados à quelantes bifuncionais radiomarcados com radionuclídeos metálicos ou lantanídeos é uma realidade de tratamento para portadores de LNH pelo princípio de radioimunoterapia (RIT). Este estudo concentrou-se nas condições de conjugação do anticorpo monoclonal rituximab (MabThera&reg) com grupamentos quelantes bifuncionais DOTA e DTPA. Na marcação dos Acm conjugados com lutécio-177, foram estudadas as condições de pré-purificação do Acm, condições de conjugação, determinação de número de quelantes acoplados à molécula do anticorpo, purificação do anticorpo conjugado, radiomarcação do anticorpo conjugado, com lutécio-177, purificação do anticorpo marcado, a ligação específica in vitro dos compostos marcados às células Raji, e distribuição biológica em camundongos BALB/c sadios. As três metodologias empregadas na pré-purificação do anticorpo (diálise, cromatografia de exclusão molecular com coluna Sephadex G-50 e ultrafiltração) demonstram-se eficientes e proporcionaram recuperação da amostra superior a 90%. A metodologia de ultrafiltração foi considerada a mais simples e prática, podendo ser aplicada a procedimentos rotineiros de produção de radiofármacos. Além disso, proporcionou a recuperação final de amostra de 97% em microlitros. Nas conjugações do anticorpo com os quelantes DOTA e DTPA em razões molares diferentes do Acm:quelante, observou-se número de grupamentos quelantes acoplados à molécula do Acm proporcional à razão molar estudada. Quando foi avaliada a influência de condições diferentes de conjugação no número de quelantes acoplados à molécula do Acm, não foram observadas diferenças significativas, com resultados de pureza radioquímica (PR) inferior a 80% em todas as condições estudadas. Na comparação de métodos de purificação do Acm conjugado, a abordagem inédita apresentada neste estudo, na qual a cromatografia de exclusão molecular foi combinada com a ultrafiltração resultou em maior eficiência na purificação e preservação da estrutura do anticorpo. Nos estudos de radiomarcação do anticorpo conjugado com DOTA e DTPA, os imunoconjugados de DTPA apresentaram, de forma geral, maior eficiência de marcação com resultados reprodutíveis quando comparados com os imunoconjugados de DOTA, considerando-se as diferentes razões molares utilizadas. As metodologias cromatográficas empregadas no controle de pureza radioquímica do composto radiomarcado proporcionaram a discriminação das diferentes espécies radioquímicas no meio de marcação. A metodologia de purificação do composto conjugado e radiomarcado utilizada proporcionou a obtenção de compostos com alta pureza radioquímica, 97,4&plusmn;1,3% (DOTA 1:50) e 98,7&plusmn;0,2% (DTPA 1:50). Nos estudos de ligação específica às células tumorais Raji, o anticorpo conjugado com quelante DTPA nas razões molares de 1:50 e 1:20 apresentaram perfil semelhante de ligação, com aumento da porcentagem de ligação específica proporcional à concentração celular, enquanto que o imunoconjugado na razão molar de 1:10 apresentou alta porcentagem de ligação não específica. Os resultados obtidos nos estudos de biodistribuição in vivo do anticorpo conjugado e radiomarcado nem sempre se mostraram compatíveis com a biodistribuição de anticorpos radiomarcados íntegros. No caso do quelante DOTA, o imunoconjugado obtido a partir da razão molar 1:20, apresentou melhores características de biodistribuição. No caso do quelante DTPA, a razão molar utilizada pareceu refletir diretamente no clareamento sanguíneo do anticorpo e todas as razões molares utilizadas apresentaram instabilidade in vivo. / Lymphomas are malignancies or cancers that start from the malign transformation of a lymphocyte in the lymphatic system. Lymphomas are divided in two major categories: Hodgkin lymphoma and non-Hodgkin lymphoma (NHL). Patient with NHL are generally treated with radiotherapy alone or combined with immunotherapy using monoclonal antibody rituximab (MabThera&reg). Currently, monoclonal antibodies (Mab) conjugated with bifunctional chelate agents and radiolabeled with metallic or lanthanides radionuclides are a treatment reality for patients with NHL by the principle of radioimmunotherapy (RIT). This study focused on the conditions of conjugation of Acm rituximab (MabThera&reg) with bifunctional chelating agents DOTA and DTPA and labeling with 177-luthetium. Various parameters were studied: method of Acm purification, conditions of Acm conjugation and the determination of the number of chelate coupled to the Acm, the purification of the conjugated Mab, labeling conditions with lutetium-177, purification of the radiolabeled immunoconjugate, radiochemical purity (RP), in vitro specific binding determination to Raji cells (Human Burkitt) and biological distribution performed in normal BALB/c mouse. The three methodologies employed in pre-purification of Acm (dialysis, size exclusion chromatograph and ultrafiltration) demonstrated to be efficient; they provided sample recovery exceeding 90%. However, the methodology of ultrafiltration resulted in greater sample recovery and in microliters. The number of chelate attached to the Mab molecule was proportional to the molar ratio studied. When the influence of different conditions of conjugation in the number of chelate bounded to the Mab was studied, no notable differences were observed. The RP < 80% was observed in all the methods applied. Purification of the conjugated antibody by different methods showed that the innovative combination of Sephadex and ultrafiltration methods resulted in higher efficiency of purification. The optimized conditions for purification of the conjugated antibody preserved the protein integrity. Radiolabelling studies of DOTA and DTPA immunoconjugated showed that DTPA derivatives presented, in general, radiochemical yield superior than DOTA conjugated Mab, considering the different molar ratios studied. The chromatographic methods employed in the RP determination were efficient to separate the different radiochemical species presented in the reaction medium. The methodology used in the purification of the labeled Mab resulted in labeled compounds with high radiochemical purity, 97.4&plusmn;1.3% (DOTA 1:50) and 98.7&plusmn;0.2% (DTPA 1:50). Considering specific cell binding assays (Raji cells), the Mab conjugated to DTPA at 1:50 and 1:20 molar ratios presented similar results, and the percent of cell binding were proportional to the cell concentration, whereas the cell binding for 1:10 molar ratio showed high percent of nonspecific cell binding. The results of in vivo biodistribution studies of labeled Mab not always were compatible with the biodistribution of intact radiolabelled antibody. The DOTA immunoconjugated produced at 1:20 molar ratio, showed better performance in biodistribution studies. In the case of DTPA immunoconjugated, the blood clearance seems to be influenced by the molar ratio applied and the immunoconjugated produced with DTPA chelate at different molar ratio resulted in high in vivo instability compounds.

anticorpo monoclonal

DOTA and DTPA

DOTA e DTPA

linfoma não-Hodgkin

monoclonal antibody

non-Hodgkin lymphoma

radioimmunotherapy

radioimunoterapia

ultrafiltração

ultrafiltration

Eosinophil Cationic Protein : Expression Levels and Polymorphisms

Byström, Jonas

January 2002

<p>The eosinophil cationic protein (ECP) is usually associated with the eosinophil granulocyte. In this thesis the presence and production of this protein has been studied in two other cells. The circulating monocyte was found to contain ECP mRNA and small amounts of ECP, one thousand times less than that found in the eosinophil. The production decreased by differentiation of the myelomonoblastic cell line U937 into a macrophage phenotype. Submucosal lung macrophages did not stain for ECP and alveolar macrophages did not contain ECP mRNA. The circulating neutrophil contains ECP at a level hundred fold less than the eosinophil. We found that the protein is located to the primary granules of the neutrophil but could detect no ECP mRNA in the cell. It was shown in vitro that the protein was taken up by the cell and partly transported to the primary granules. The uptake did not seem to be receptor mediated. Upon stimulation of the neutrophils, ECP previously taken up, was re-secreted. </p><p>The ECP protein is heterogeneous both to molecular characteristics and to function. To evaluate if a genetic component is involved, the ECP gene was analysed in 70 individuals. Three single nucleotide polymorphisms (SNP´s) were found, denoted 277(C>T), 434(G>C) and 562(G>C). The two first were located to the mature peptide-coding region and would change the amino acids, arg45cys and arg97thr. The prevalence of the most common SNP, 434, was evaluated in two eosinophil-related diseases, allergy/asthma and Hodgkin Lymphoma (HL). Forty-three HL patients were evaluated and it was found that the 434GG was significantly more prevalent in patients having nodular sclerosis (NS) as compared to other histologies (p=0.03). Erythrocyte sedimentation rate was also related to the 434GG genotype (p=0.009). In 209 medical students 434GG was more common (p=0.002) in those who indicated allergy. The genotype was unrelated to the production of IgE antibodies to allergens. In analysis of 76 subjects with asthma it was found that the 434GG genotype was significantly more common among allergic asthmatics (p=0.04). Asthma and HL-NS are characterized by fibrosis and eosinophils and ECP has been suggested in fibrosis development. </p>

Medical sciences

Eosinophils

Neutrophils

Monocytes

Macrophages

mRNA

eosinophil cationic protein

DNA

polymorphism

Hodgkin Lymphoma

asthma

allergy

MEDICIN OCH VÅRD

MEDICINE

MEDICIN

Molecular Characterization of Diffuse Large B-cell Lymphoma and Aspects of Transformation

Berglund, Mattias

January 2004

<p>Lymphomas are a heterogeneous group of neoplasias originating from B- or T-lymphocytes. In this thesis, we determined the genetic and immunophenotypic characterization of DLBCL and their prognostic impact. Moreover, genomic alterations associated with the transformation to DLBCL from Hodgkin lymphoma (HL) and follicular lymphoma (FL) were elucidated. </p><p>In order to outline the impact of cytogenetic as well as immunophenotypic prognostic markers in DLBCL, we firstly studied a series of 54 DLBCL tumors using comparative genomic hybridization (CGH) and we identified several frequently occurring chromosomal imbalances. Loss of 22q was more often found in the diagnostic tumors with a more advanced clinical stage, while gain of 18q21 was more commonly identified in relapses. Secondly, we correlated the expression patterns of CD10, bcl-6, IRF-4 and bcl-2 with clinical parameters in a series of 173 de novo DLBCL patients. Patients with a germinal center (GC) phenotype displayed a better survival than the non-GC group. Expression of bcl-6 and CD10 was correlated with a better survival while bcl-2 expression was associated with a poor prognosis.</p><p>In approaching the HL transformation, two novel B-cell lines (U-2932 and U-2940), derived from patients with DLBCL following HL, were characterized. Interestingly, a translocation with materials from 2q and 7q as well as loss of material on 6q was found in both cell lines. For FL transformation, we assessed chromosomal alterations in a panel of 28 DLBCL patients with a previous history of FL. The DLBCL tumors displayed more chromosomal imbalances compared to FL tumors. Loss of 6q16-21 and gain of 7pter-q22 were more commonly found in the DLBCL counterparts, suggesting the chromosomal location of putative genes that may be involved in the transformation process.</p>

Oncology

Diffuse large B-cell lymphoma

Hodgkin lymphoma

follicular lymphoma

transformation

comparative genomic hybridization

prognosis

Onkologi

Oncology

Onkologi

Mast cells in Hodgkin lymphoma : or 'What's a nice cell like you doing in a tumour like this?'

Fischer, Marie

January 2004

<p>Mast cell (MC) accumulation around tumours is an old observation gaining new relevance due to the multifaceted nature of MCs and their many roles in immunity, beyond allergy. Knowledge about tumour specific recruitment of, and interactions with, MCs is needed to unravel the function of their presence.</p><p>This study investigates the participation of mast cells in the tumourigenesis of Hodgkin lymphoma (HL), a tumour with many inflammatory features. We report that MC recruitment into HL lymphomatous tissue is possibly due to the production of CCL5/RANTES by malignant Hodgkin and Reed-Sternberg (HRS) cells. In addition, increased levels of IL-9, a cytokine implicated in mast cell heterogeneity and as an autocrine growth factor for HRS cells, were found in HL patient sera and correlate with negative prognostic factors. The ubiquitous expression of CD30 by HRS cells has been implicated in HL tumour development. In HL tissue MCs were found to be the predominant CD30 ligand (CD30L) expressing cells, and through CD30L/CD30 engagement they induced a proliferative response in HRS cells. This interaction proved to be bi-directional as it induced a degranulation-independent <i>de novo</i> synthesis of a specific set of chemokines in MCs, including IL-8. This novel trigger of MC activation is suggested to be of importance also in atopic dermatitis (AD) and psoriasis since increased numbers of CD30L and IL-8 positive MCs were detected along with increased expression of CD30.</p><p>Data presented in this study supports a specific recruitment of MCs into HL tumours and co-operative interactions between HRS cells and MCs. Our identification of reversed signalling via CD30L as a novel MC trigger provides a mechanism behind leukocyte infiltration and chronic development in diseases associated with CD30 and MCs, such as HL, AD and psoriasis.</p>

Pathology

Hodgkin lymphoma

mast cells

CD30

CD30L

IL-9

CCL5

atopic dermatitis

psoriasis

IL-8

Patologi

Pathology

Patologi