Etude structurale et fonctionnelle d'un domaine intrinsèquement désordonné de l'oncoprotéine BCR-ABL responsable de la leucémie myéloïde chronique / Structural and functional study of an intrinsically disordered domain of the BCR-ABL oncoprotein responsible for chronic myeloid leukemia

Maneville, Stephanie

09 October 2013

L'oncoprotéine BCR-ABL est responsable de la physiopathologie de la Leucémie Myéloïde Chronique (LMC). La fusion d'une partie de la protéine ABL et de BCR entraîne une dérégulation de l'activité kinase portée par ABL. Plusieurs domaines contenus dans ces deux protéines jouent un rôle important dans l'activation du pouvoir oncogène. L'un d'entre eux est une région de BCR, située en N-terminal, contenant un domaine de liaison au domaine SH2. Durant ce travail de thèse, j'ai caractérisé, pour la première fois, les propriétés structurales de cette région, à l'aide de plusieurs méthodes biophysiques: le domaine de BCR est intrinsèquement désordonné. En parallèle, j'ai étudié les interactions entre le domaine de liaison de BCR et les domaines SH d'ABL. J'ai identifié de nouveaux sites d'interactions avec ABL sur BCR. Enfin, j'ai évalué l'impact fonctionnel des nouveaux sites d’interactions au sein de l'oncoprotéines BCR-ABL, dans un modèle cellulaire. Les résultats préliminaires montrent que deux nouveaux sites auraient un rôle dans le pouvoir oncogénique de BCR-ABL. Ces résultats offrent la possibilité de développer de nouveaux médicaments complémentaires aux existants, qui cibleraient une nouvelle région de BCR-ABL, ainsi pourraient lutter contre les résistances apparues chez les patients vis-à-vis des traitements actuels. / The BCR-ABL oncoprotein is responsible for the pathogenesis of chronic myelogenous leukemia (CML). The fusion of a part of ABL and BCR leads to deregulation of kinase activity of ABL. Several domains in these two proteins play an important role in the activation of oncogenic properties. One of them is a BCR region, located at the N- terminal part, containing a SH2 domain binding. In this thesis , I have characterized for the first time , the structural properties of this region, using several biophysical methods : the domain of BCR is intrinsically disordered. In parallel, I have studied the interactions between the binding domain of BCR and theSH domains of ABL. I identified new sites of interaction with ABL into BCR. Finally, I evaluated the functional impact of new sites of interaction within the BCR- ABL oncoprotein in a cellular model. Preliminary results show that two new sites have a role in the oncogenic properties of BCR- ABL. These results offer the possibility to develop new drugs complementary to existing , that target a new region of BCR- ABL and could fight against the resistance occurred in patients vis-a-vis current treatments.

BCR-ABL

Domaine intrinsèquement désordonné

Interaction

Inhibition

LMC

Pouvoir oncogène

BCR-ABL

Intrinsically disordered domain

Interaction

Inhibition

CML

Oncogenic propertie

572

Controle da expressão de TRAIL, OSM, FAIM e NIPA pelo oncogene bcr-abl. / bcr-abl regulation of TRAIL, OSM, FAIM and NIPA expression.

Leroy, Janine Marie Gisele

03 July 2008

A leucemia mielóide crônica (LMC) é uma doença mieloproliferativa e sua patogênese está associada à expressão de um neogene, bcr-abl, que codifica uma proteína tirosina quinase Bcr-Abl. Esse trabalho tem como objetivos o estudo dos mecanismos envolvidos na resistência à morte das células Bcr-Abl positivas e a identificação de alterações gênicas nessas células. Dados de expressão gênica global obtidos por \"microarray\" mostraram uma superexpressão nas células HL-60.Bcr-Abl com relação a HL-60 dos genes faim e nipa, que foi confirmada por qRT-PCR em diferentes linhagens celulares Bcr-Abl positivas. Já os genes de trail e osm, apresentaram uma diminuição significativa em HL-60.Bcr-Abl, que foi confirmada para trail, porém osm não teve seu resultado validado. A avaliação da expressão dos genes em células de pacientes portadores de LMC, em diferentes fases da doença também foi estudada. Com esses resultados, o presente estudo visa a melhor compreensão de como alterações na expressão desses genes contribuem na fisiopatologia da LMC. / Chronic myelogenous leukemia (CML) is a stem cell disease characterized by the presence of the Bcr-Abl oncoprotein, which is the cause of the malignant transformation and the extreme resistance to apoptosis displayed by CML patients. Our aim was to analyze the alteration in global gene expression in Bcr-Abl expressing cells. Data obtained from microarray analysis showed significant up-regulation of nipa and faim in HL60.Bcr-Abl and down-regulation of osm and trail. These results were further confirmed by Real-Time PCR to nipa, faim and trail, but not for osm expression in HL-60.Bcr-Abl cells. To evaluate the potential of some of the modified genes as therapeutic targets or prognostic markers for CML, we also analyzed the expression of these genes in samples from CML patients.

Apoptose

Apoptosis

Bcr-Abl

Bcr-Abl

Chronic myelogenous leukemia

Death receptors

Expressão gênica

Gene expression

Leucemia mielóide crônica

Receptores de morte

Trail

Trail

Aspectos moleculares da transformação celular induzida por Bcr-Abl. / Molecular aspects of Bcr-Abl-induced cell transformation.

Silva, Ana Elisa Barreiros Bueno da

11 April 2008

As leucemias cromossomo Ph-positivas estão intimamente associadas à expressão da tirosina-quinase Bcr-Abl. Esta oncoproteína promove independência de fatores de crescimento, alterações na adesão e inibição da apoptose por mecanismos ainda não totalmente elucidados. O objetivo desse estudo foi avaliar a contribuição da atividade quinase de Bcr-Abl para seu potencial anti-apoptótico e identificar alterações moleculares envolvidas na transformação celular induzida por essa proteína. Nossos resultados sugerem que a resistência à apoptose não depende da manutenção constante da atividade tirosina-quinase de Bcr-Abl, tampouco da presença de proteínas fosforiladas em tirosina. A comparação do proteoma de células HL-60.vetor e HL-60.Bcr-Abl revelou que a presença de Bcr-Abl causa alterações profundas no padrão de expressão protéica. As proteínas afetadas estão associadas a diversos processos celulares, como adesão, transdução de sinais, proliferação e morte celular. Esses achados devem contribuir para a identificação de novos marcadores de prognóstico e alvos terapêuticos. / Ph chromosome-positive leukemias are closely associated with the expression of Bcr-Abl tyrosine kinase. This oncoprotein promotes growth factor independence, alters cell adhesion and confers resistance to apoptosis by mechanisms that are not fully understood. The aim of this study was to evaluate the contribution of Bcr-Abl kinase activity for its antiapoptotic potential and identify molecular alterations involved in Bcr-Abl-induced cell malignant transformation. Our results suggest that Bcr-Abl is not required to be constantly active to maintain the resistance to apoptosis and pY-containing proteins may not be responsible for the antiapoptotic effect of Bcr-Abl. The comparison between the proteome of HL-60.vector and HL-60.Bcr-Abl cells revealed that the presence of Bcr-Abl alters the expression of a great variety of proteins. The affected molecules are associated with several cellular processes, including cell adhesion, signal transduction, proliferation and cell death. Our findings might help the identification of new prognostic markers and therapeutic targets.

Apoptose

Apoptosis

Bcr-Abl

Bcr-Abl

Cell transformation

Chronic myeloid leukemia

Leucemia mielóide crônica

Proteoma

Proteome

Tirosina-quinase

Transformação celular

Tyrosine kinase

Expressão de galectina-1 e -3 na leucemia mielóide crônica e sua contribuição para a progressão da doença. / Expression of galectin-1 and -3 in chronic myeloid leukemia and its contribution to disease progression.

Castro, Monica Alexandra Yon

09 June 2009

A galectina-1 (LGALS1) participa em diferentes etapas da neoplasia, mas sua função na leucemia mielóide crônica (LMC) é desconhecida. Neste trabalho, a expressão etópica de BCR-ABL selvagem, mas não de BCR-ABL quinase deficiente, em linhagens celulares hematopoéticas, resultou em aumento de LGALS1. O efeito foi revertido com a inibição da tirosina quinase pelo mesilato de imatinibe. Este resultado indicou que a galectina-1 é modulada pela atividade tirosina-quinase de BCR-ABL. Em pacientes com LMC, a maior expressão de LGALS1 foi correlacionada a altos níveis de BCR-ABL, progressão da doença e a um tempo de sobrevida menor. Adicionalmente, as células K562 com LGALS1 inibida por RNA de interferência exibiram crescimento mais lento do que as células K562 com LGALS1 intacta, em camundongos nude. Portanto, o pior prognóstico de pacientes com altos níveis de galectina-1 sugere um efeito cooperativo de galectina-1 na tumorigênese de BCR-ABL reforçando o conceito de que a galectina-1 é um forte candidato para intervenção terapêutica na LMC. / Galectin-1 (LGALS1) participates in different steps of neoplasia but its role in chronic myeloid leukemia (CML) is unknown. In this work, ectopic expression of wild-type but not kinase-deficient BCR-ABL in different hematopoietic cells resulted in LGALS1 upregulation. Tyrosine-kinase inhibition by imatinib mesylate reversed this effect. This result indicate that galectin-1 is modulated by tyrosine kinase activity. In CML patients, the elevated expression of LGALS1 was correlated with high BCR-ABL levels, disease progression and shorter survival time. Additionally, in nude mice, LGALS1-deficient K562 cells obtained by RNA interference were less efficient in tumor formation than control K562 cells. Therefore, the worst prognosis in patients bearing high LGALS1 levels suggests a cooperative role for galectin-1 in BCR-ABL-positive leukemia and support the concept that galectin-1 is a strong candidate for CML therapeutic intervention.

BCR-ABL

BCR-ABL

Chronic myeloid leukemia

Galectin-1

Galectin-3

Galectina-1

Galectina-3

Immunology

Imunologia

Leucemia mielóide crônica

Tirosina quinase

Tumorigênese

Tumorigenesis

Tyrosine kinase

Efeito do veneno bruto e da L-aminoácido oxidase de Bothrops pirajai em células BCR-ABL positivas / Effect of Bothrops pirajai crude venom and L-amino acid oxidase in BCR-ABL positive cells.

Burin, Sandra Mara

01 July 2011

A leucemia mielóide crônica (LMC) é uma doença mieloproliferativa caracterizada citogeneticamente pela presença do cromossomo Philadelfia (Ph) e molecularmente pelo neogene bcr-abl1 que codifica a oncoproteína BCR-ABL com alta atividade de tirosina-quinase. A célula leucêmica BCR-ABL+ apresenta baixa adesão ao estroma medular, resistência à apoptose e potencial mitogênico exacerbado. A LMC possui curso evolutivo trifásico (fase crônica, acelerada e blástica) e seu tratamento pode ser realizado por meio de diferentes modalidades terapêuticas, destacando-se o mesilato de imatinibe (MI) que inibe a TK BCR-ABL induzindo altas taxas de remissão citogenética dos pacientes na fase crônica da doença. Apesar do MI ser eficiente, os pacientes na fase acelerada e blástica da doença são comumente refratários a essa terapia e na fase crônica há casos de resistência ao MI descritos. Nesse contexto, potenciais novos fármacos são investigados para melhorar a eficiência da terapia da LMC. Nesse estudo, investigamos o efeito do veneno bruto (VB) e da enzima L-amino-ácido-oxidase (LAAO) da Bothrops pirajai em desencadear apoptose em células BCR-ABL+. A apoptose das células HL-60 e HL-60.BCR-ABL foi quantificada pela detecção da percentagem de células com núcleos hipodiplóides pela da citometria de fluxo e confirmada pela observação da ativação das caspases 3, 8 e 9 por western-blot. Os resultados obtidos indicam que a LAAO é capaz de induzir apoptose em células HL-60 e HL-60.BCR-ABL por ativação das vias extrínseca e intrínseca. Além disso, foi verificado que a LAAO diminui a fosforilação de BCR-ABL em células HL-60.BCR-ABL e quando associada ao MI potencializou a inibição da atividade quinase de BCR-ABL. Os dados da presente investigação indicaram ainda que a LAAO é capaz de modular a expressão de bad, bak, bax, bid, bimel, fas,fasl, a1, bcl-2, bcl-xl, bcl-w e c-flip, genes reguladores da apoptose celular. Apesar do pouco conhecimento acerca do mecanismo de ação dessa toxina, os dados obtidos sugerem que a LAAO possui o potencial de estimular a apoptose nas linhagens HL-60 e HL-60.BCR-ABL e aumentar o efeito do inibidor da atividade quinase, MI, dados relevantes para estudos futuros associados a descrição de novos fármacos contra leucemia mielóide crônica. / Chronic myeloid leukemia (CML) is a myeloproliferative disorder cytogenetically characterized by the presence of Philadelphia chromosome (Ph) and molecularly by bcr-abl1 neogene that encodes the BCR-ABL oncoprotein with high tyrosine kinase (TK) activity. The leukemic cell BCR-ABL+ presents poor adhesion to bone marrow stroma, resistance to apoptosis and exacerbated mitogenic potential. The CML has a three-phase course (chronic, accelerated and blastic phase) and its treatment can be performed by different therapeutic modalities, especially the imatinib mesylate (IM) that inhibits the TK BCR-ABL inducing high rates of cytogenetic remission in chronic phase. Although MI is effective, patients in accelerated and blastic phases of the disease are often refractory to this therapy and there are also cases of resistance to MI described in chronic phase. In this context, potential new drugs are investigated to improve the efficiency of the therapy of CML. In this study, we investigated the effect of crude venom (CV) and of the enzyme L-amino acid oxidase (LAAO) from Bothrops pirajai in triggering apoptosis in BCR-ABL+. The apoptosis of HL-60 cells and HL-60. BCR-ABL was quantified by detecting the percentage of cells with hypodiploid nuclei by flow cytometry and confirmed by observation of the activation of caspases 3, 8 and 9 by Western blot. The results indicate that LAAO is able to induce apoptosis in HL-60 cells and HL-60. BCR-ABL by activation of the extrinsic and intrinsic pathways. Furthermore, it was found that LAAO decreases phosphorylation of BCR-ABL in HL-60 cells. BCR-ABL when associated with MI potencialized the inhibition of kinase activity of BCR-ABL. The data from this study also indicated that the LAAO is able to modulate the expression of bad, bak, bax, bid, bimel, fas, FasL, A1, bcl-2, bcl-xl, bcl-w and c-flip, regulatory genes of apoptosis. Even though there is little knowledge about the mechanism of action of this toxin, the data obtained suggests that LAAO has the potential to stimulate apoptosis in HL-60 lines and HL-60. BCR-ABL and increase the effect of the inhibitor of protein kinase activity, MI, relevant data for future studies associated with the description of new drugs against chronic myeloid leukemia.

Apoptose

apoptosis

BCR-ABL

BCR-ABL

chronic myeloid leukemia

Leucemia Mielóide Crônica

L’hypothèse d’un contrôle extrinsèque de la leucémie myéloïde chronique : place des lymphocytes iNKT et de la cytokine/alarmine IL-3 / The hypothesis of an extrinsic control of Chronic Myeloid Leukemia : role of iNKT cells and the cytokine/alarmin IL-33

Levescot, AnaÏs

25 October 2013

Les traitements actuels de la leucémie myéloïde chronique (LMC) ne permettent pas d’éliminer la totalité des cellules leucémiques. Dans le but de développer un traitement curatif, il est donc nécessaire de parvenir à une meilleure compréhension des mécanismes sous-jacents des réponses partielles aux traitements, Dans ce travail, nous avons postulé qu’il existe des mécanismes de contrôle extrinsèques de la LMC pouvant influencer l’efficacité des différents traitements. Nous avons choisi d’étudier le rôle potentiel dans la LMC des lymphocytes iNKT, cellules T de type « inné » auxquelles la littérature attribue de nombreuses fonctions antitumorales et des facteurs moléculaires, la cytokine/alarmine IL-33, produite dans la niche hématopoïétique, et son récepteur ST2 à la surface des cellules hématopoïétiques comme cibles de l’IL-33.La première partie de notre travail a ainsi permis de mettre en évidence de profondes altérations fonctionnelles des lymphocytes iNKT chez les patients atteints de LMC ainsi qu’une correction partielle de ces défauts après traitement par l’Imatinib (IM) ou l’IFN-. L’ensemble de ces résultats permet de proposer que l’altération des fonctions des cellules iNKT au cours du développement de la LMC pourrait participer aux mécanismes d’échappement de la tumeur au contrôle par le système immunitaire. La deuxième partie de notre travail a permis de mettre en évidence une expression de la molécule ST2, chaîne spécifique du récepteur à l’IL-33, à la surface des cellules CD34+ de patients atteints de LMC, expression non décelée chez les sujets sains et les patients en rémission après traitement par l’IM. De plus, contrairement aux cellules CD34+ de sujets sains, les cellules progénititrices de patients en phase chronique prolifèrent en réponse à l’IL-33. Enfin, nous avons montré que l’IL-33 est capable de contrecarrer in vitro les effets antiprolifératifs de l’IM. Ainsi nous pouvons émettre l’hypothèse selon laquelle l’IL-33, une cytokine/alarmine, puisse participer aux phénomènes conduisant à la persistance de progéniteurs hématopoïétiques leucémiques chez les patients sous traitement par IM. / To date, treatment of Chronic Myeloid Leukaemia (CML) is not sufficient to completely eradicate leukaemia cells. Hence, in order to develop a curative treatment, it is necessary to have a better understanding of the underlying mechanisms explaining why response to treatment is only partial..We therefore addressed the question whether the extrinsic mechanisms of CML control can affect the effectiveness of different treatments. We first provided evidence of profound functional impairments of iNKT cells in patients with CML. Interestingly these impairments were partially corrected after treatment with Imatinib (IM) or IFN-. Consequently our results suggest that altered functions of iNKT cells during the development of CML could facilitate tumour escape from immune destruction. . The second part of our work revealed that CD34+ progenitors from CML patients upregulate their cell surface expression of the IL-33-specific receptor chain ST2, proliferate and produce cytokines in response to IL-33, conversely to CD34+ cells from healthy individuals. Moreover, ST2 overexpression is normalized following IM therapy, while IL-33 counteracts in vitro IM-induced growth arrest in CML CD34+ progenitors. From these findings, it can be surmised that IL-33, a cytokine/alarmin likely expressed in the hematopoietic niche, facilitates the development of CML and IM resistance.

CML

BCR-ABL

IFN-α

Imatinib

INKT

Cellules progénitrices CD34+

IL-33

ST2

CML

BCR-ABL

IFN-α

Imatinib

INKT

CD34+ progenitors

IL-33

ST2

Zur Resistenzentwicklung von Zellen der chronischen myeloischen Leukämie gegenüber Tyrosinkinase-Inhibitoren: Regulation und Funktion des ABC-Transporters A3 / Resistance mechanism of chronic myeloid lekuemia cells against tyrosine kinase inhibitors: regulation and function of the ABC transporter A3

Hupfeld, Timo

30 October 2012

No description available.

570 Biowissenschaften, Biologie

Medicine

42.13 Molekularbiologie

CXCR4 : nouvelle cible thérapeutique de la cellule leucémique ? : rôle du couple SDF-1 / CXCR4 dans la leucémie aiguë / CXCR4 : a new therapeutic target of the leukaemic cell ? : role of the SDF-1/CXCR4 axis in acute leukaemia

Tavernier-Tardy, Emmanuelle

16 December 2011

CXCR4, récepteur de la chimiokine SDF-1 (stromal cell-derived factor 1) joue un rôle capital dans l’hématopoïèse normale mais aussi dans la biologie de la cellule leucémique. Ce récepteur est exprimé à la surface des blastes et participe à « l’ancrage » de la cellule souche leucémique (CSL) au sein de la niche médullaire. Les interactions de la CSL avec le micro-environnement sont source de signaux de survie et de résistance à l’apoptose. La première partie de ce travail correspond à deux analyses en cytométrie en flux de l’expression de CXCR4 et de molécules d’adhérence sur des échantillons diagnostiques de LAM (leucémie aiguë myéloïde). Ce travail confirme la valeur pronostique péjorative de l’expression de CXCR4 et propose un modèle de stratification pronostique des patients, en fonction de leur phénotype d’adhérence. La deuxième partie s’intéresse à l’identification de potentielles cibles thérapeutiques dans un modèle de LAL à chromosome Philadelphie, pathologie au pronostic sombre malgré les progrès thérapeutiques liés aux ITK (inhibiteurs de tyrosine kinase). L’inhibition de CXCR4 par l’AMD3100 permet de potentialiser l’efficacité de l’aracytine et du dasatinib dans un modèle de co-culture stromale avec la lignée SUPB15. Une deuxième piste de ciblage thérapeutique de la LAL Phi+ est l’inhibition de la protéine chaperone HSP90. Une expression forte de HSP90 (dans les LAL Phi+ par rapport aux LAL Phi-) s’associe à une plus grande cytotoxicité du 17-AAG. En conclusion, CXCR4 est un récepteur clé de la cellule leucémique. L’étude de son niveau d’expression permet des stratifications pronostiques des patients et son blocage en fait une cible thérapeutique prometteuse / CXCR4, receptor of the chemokine SDF-1 (stromal cell-derived factor 1) plays a major role in the normal hematopoiesis but also in the biology of the leukaemic cell. This receptor is expressed on the surface of blasts and is a key molecule in "the anchoring" of the leukaemic stem cell (LSC) within the bone marrow niche. The interactions of the LSC with the bone marrow microenvironment promote survival signals and drug resistance. The first part of this work consists of two flow cytometry analyses of CXCR4 and adhesion molecules expression in patients with AML (acute myeloid leukaemia) at diagnosis. The results confirm that CXCR4 expression is associated with poor prognosis and this work proposes to stratify patients, according to their adhesive phenotype, in order to establish risk-adapted strategies. The second part deals with the identification of potential therapeutic targets in a model of ALL with chromosome Philadelphia. Despite therapeutic improvements with the ITK (tyrosine kinase inhibitors) era, long term survival remains poor. The inhibition of CXCR4 by the AMD3100 enhances the sensitivity of SUPB15 cell line to cytarabine and dasatinib therapy in a model of stromal co-culture. A second way of therapeutic targeting of the ALL Phi + is the inhibition of the heat-shock protein HSP90. High percentage of HSP90-positive cells (in Ph+ ALL samples) is associated with high sensitivity to 17-AAG. In conclusion, CXCR4 appears as a key receptor of the leukaemic cell. The analysis of its level of expression allows prognostic stratifications and its blockade represents a promising therapeutic target

CXCR4

Molécules d’adhérence

Leucémie aiguë

Chromosome Philadelphie (Bcr- Abl)

Facteurs pronostiques

Cible thérapeutique

CXCR4

Adhesion molecules

Acute leukaemia

Philadelphia chromosome (Bcr-Abl)

Prognostic factors

Therapeutic target

615.5

Efeito do veneno bruto e da L-aminoácido oxidase de Bothrops pirajai em células BCR-ABL positivas / Effect of Bothrops pirajai crude venom and L-amino acid oxidase in BCR-ABL positive cells.

Sandra Mara Burin

01 July 2011

A leucemia mielóide crônica (LMC) é uma doença mieloproliferativa caracterizada citogeneticamente pela presença do cromossomo Philadelfia (Ph) e molecularmente pelo neogene bcr-abl1 que codifica a oncoproteína BCR-ABL com alta atividade de tirosina-quinase. A célula leucêmica BCR-ABL+ apresenta baixa adesão ao estroma medular, resistência à apoptose e potencial mitogênico exacerbado. A LMC possui curso evolutivo trifásico (fase crônica, acelerada e blástica) e seu tratamento pode ser realizado por meio de diferentes modalidades terapêuticas, destacando-se o mesilato de imatinibe (MI) que inibe a TK BCR-ABL induzindo altas taxas de remissão citogenética dos pacientes na fase crônica da doença. Apesar do MI ser eficiente, os pacientes na fase acelerada e blástica da doença são comumente refratários a essa terapia e na fase crônica há casos de resistência ao MI descritos. Nesse contexto, potenciais novos fármacos são investigados para melhorar a eficiência da terapia da LMC. Nesse estudo, investigamos o efeito do veneno bruto (VB) e da enzima L-amino-ácido-oxidase (LAAO) da Bothrops pirajai em desencadear apoptose em células BCR-ABL+. A apoptose das células HL-60 e HL-60.BCR-ABL foi quantificada pela detecção da percentagem de células com núcleos hipodiplóides pela da citometria de fluxo e confirmada pela observação da ativação das caspases 3, 8 e 9 por western-blot. Os resultados obtidos indicam que a LAAO é capaz de induzir apoptose em células HL-60 e HL-60.BCR-ABL por ativação das vias extrínseca e intrínseca. Além disso, foi verificado que a LAAO diminui a fosforilação de BCR-ABL em células HL-60.BCR-ABL e quando associada ao MI potencializou a inibição da atividade quinase de BCR-ABL. Os dados da presente investigação indicaram ainda que a LAAO é capaz de modular a expressão de bad, bak, bax, bid, bimel, fas,fasl, a1, bcl-2, bcl-xl, bcl-w e c-flip, genes reguladores da apoptose celular. Apesar do pouco conhecimento acerca do mecanismo de ação dessa toxina, os dados obtidos sugerem que a LAAO possui o potencial de estimular a apoptose nas linhagens HL-60 e HL-60.BCR-ABL e aumentar o efeito do inibidor da atividade quinase, MI, dados relevantes para estudos futuros associados a descrição de novos fármacos contra leucemia mielóide crônica. / Chronic myeloid leukemia (CML) is a myeloproliferative disorder cytogenetically characterized by the presence of Philadelphia chromosome (Ph) and molecularly by bcr-abl1 neogene that encodes the BCR-ABL oncoprotein with high tyrosine kinase (TK) activity. The leukemic cell BCR-ABL+ presents poor adhesion to bone marrow stroma, resistance to apoptosis and exacerbated mitogenic potential. The CML has a three-phase course (chronic, accelerated and blastic phase) and its treatment can be performed by different therapeutic modalities, especially the imatinib mesylate (IM) that inhibits the TK BCR-ABL inducing high rates of cytogenetic remission in chronic phase. Although MI is effective, patients in accelerated and blastic phases of the disease are often refractory to this therapy and there are also cases of resistance to MI described in chronic phase. In this context, potential new drugs are investigated to improve the efficiency of the therapy of CML. In this study, we investigated the effect of crude venom (CV) and of the enzyme L-amino acid oxidase (LAAO) from Bothrops pirajai in triggering apoptosis in BCR-ABL+. The apoptosis of HL-60 cells and HL-60. BCR-ABL was quantified by detecting the percentage of cells with hypodiploid nuclei by flow cytometry and confirmed by observation of the activation of caspases 3, 8 and 9 by Western blot. The results indicate that LAAO is able to induce apoptosis in HL-60 cells and HL-60. BCR-ABL by activation of the extrinsic and intrinsic pathways. Furthermore, it was found that LAAO decreases phosphorylation of BCR-ABL in HL-60 cells. BCR-ABL when associated with MI potencialized the inhibition of kinase activity of BCR-ABL. The data from this study also indicated that the LAAO is able to modulate the expression of bad, bak, bax, bid, bimel, fas, FasL, A1, bcl-2, bcl-xl, bcl-w and c-flip, regulatory genes of apoptosis. Even though there is little knowledge about the mechanism of action of this toxin, the data obtained suggests that LAAO has the potential to stimulate apoptosis in HL-60 lines and HL-60. BCR-ABL and increase the effect of the inhibitor of protein kinase activity, MI, relevant data for future studies associated with the description of new drugs against chronic myeloid leukemia.

Apoptose

BCR-ABL

Leucemia Mielóide Crônica

apoptosis

BCR-ABL

chronic myeloid leukemia

Controle da expressão de TRAIL, OSM, FAIM e NIPA pelo oncogene bcr-abl. / bcr-abl regulation of TRAIL, OSM, FAIM and NIPA expression.

Janine Marie Gisele Leroy

03 July 2008

A leucemia mielóide crônica (LMC) é uma doença mieloproliferativa e sua patogênese está associada à expressão de um neogene, bcr-abl, que codifica uma proteína tirosina quinase Bcr-Abl. Esse trabalho tem como objetivos o estudo dos mecanismos envolvidos na resistência à morte das células Bcr-Abl positivas e a identificação de alterações gênicas nessas células. Dados de expressão gênica global obtidos por \"microarray\" mostraram uma superexpressão nas células HL-60.Bcr-Abl com relação a HL-60 dos genes faim e nipa, que foi confirmada por qRT-PCR em diferentes linhagens celulares Bcr-Abl positivas. Já os genes de trail e osm, apresentaram uma diminuição significativa em HL-60.Bcr-Abl, que foi confirmada para trail, porém osm não teve seu resultado validado. A avaliação da expressão dos genes em células de pacientes portadores de LMC, em diferentes fases da doença também foi estudada. Com esses resultados, o presente estudo visa a melhor compreensão de como alterações na expressão desses genes contribuem na fisiopatologia da LMC. / Chronic myelogenous leukemia (CML) is a stem cell disease characterized by the presence of the Bcr-Abl oncoprotein, which is the cause of the malignant transformation and the extreme resistance to apoptosis displayed by CML patients. Our aim was to analyze the alteration in global gene expression in Bcr-Abl expressing cells. Data obtained from microarray analysis showed significant up-regulation of nipa and faim in HL60.Bcr-Abl and down-regulation of osm and trail. These results were further confirmed by Real-Time PCR to nipa, faim and trail, but not for osm expression in HL-60.Bcr-Abl cells. To evaluate the potential of some of the modified genes as therapeutic targets or prognostic markers for CML, we also analyzed the expression of these genes in samples from CML patients.

Apoptose

Bcr-Abl

Expressão gênica

Leucemia mielóide crônica

Receptores de morte

Trail

Apoptosis

Bcr-Abl

Chronic myelogenous leukemia

Death receptors

Gene expression

Trail