Complicações pulmonares relacionadas ao transplante de medula óssea / Pulmonary complications related to bone marrow transplantation

Flavia Cristina Almeida Leite Figueiredo

24 September 2008

Transplante de medula óssea (TMO) é um procedimento terapêutico que tem como o objetivo a substituição da medula óssea doente por outra saudável. É utilizado em pacientes oncológicos e pode representar a cura da malignidade hematológica ou o resgate da medula óssea para a continuidade do tratamento antineoplásico. No TMO são empregadas drogas com alta toxicidade que agem ao nível sistêmico e que podem causar severos danos ao organismo. Esses danos resultam em complicações diversas que irão influenciar o prognóstico e sobrevida do paciente. As complicações pulmonares são associadas a altas taxas de mortalidade, sobretudo quando a ventilação mecânica (VM) é necessária. Ainda não há consenso na literatura quanto às causas, os fatores de risco e o tratamento adequado. Este estudo teve como objetivo identificar os fatores preditivos para insuficiência respiratória (IRP) em paciente oncológicos após o TMO autólogo e investigar o impacto da ventilação não-invasiva (VNI) na evolução clínica destes pacientes. Foi realizado o levantamento retrospectivo de 161 pacientes submetidos ao TMO autólogo no Hospital A.C. Camargo entre 1995 e 2005. Houve forte associação de IRP e óbito (p< 0,001) e também observamos associação com mucosite (p=0,016) e etilismo (p=0,036), essa associação permaneceu significante na análise multivariada [mucosite (p=0,004) e etilismo (p=0,02)]. De acordo com a análise de sobrevida encontramos associação com o maior número de regimes de quimioterapia no passado (p= 0.005), mucosite (p= 0.029), etilismo (p= 0.044) e redução da capacidade de difusão de monóxido de carbono (p=0.048). Em nosso estudo a taxa de mortalidade permanece alta para aqueles pacientes que desenvolvem IRP e necessitam de VM. A VNI não demonstrou efeito protetor na sobrevida dos pacientes que evoluíram com IRP. A mucosite mostrou-se um fator de piora no prognóstico destes pacientes devendo ser agressivamente evitada e tratada. O impacto do etilismo na incidência de insuficiência respiratória (IRP) e mortalidade destes pacientes merece destaque especial com necessidade de mais pesquisas. O stress oxidativo parece ter um importante efeito causal para as complicações pulmonares após o TMO podendo ser potencializado pelo etilismo. O maior número de esquemas de quimioterapia no passado aumentou a mortalidade, isso poderia representar pacientes com neoplasias mais resistentes ao tratamento ou pacientes que foram expostos ao efeito cumulativo das drogas. A capacidade de difusão de monóxido de carbono é um teste bastante útil para prever risco de óbito / Bone marrow transplantation (BMT) is a therapeutic procedure to replace unable marrow for another healthy one. Its used in cancer patients to cure or refresh marrow to keep the cancer treatment. Respiratory failure (RF) after BMT is associated with high mortality specially when mechanical ventilation (MV) is needed, it may be due to treatment-related toxicity, infection, or immunologic insufficiency. Many studies have trying to identify causes, predicting factors and response for the usual treatment, but until now there is no agreement in literature. The aim of this study is to identify which factors evaluated in routine anamnesis and exams pretransplant can affect the prognosis of those patients. We retrospectively collected variables in 161 consecutive cancer patients who had undergone autologous BMT. The variables obtained from the in-hospital period were submitted to univariated and multivariated stepwise logistic regression analyses. Survival analysis also was computed in 100 days follow up. There were highest association for respiratory failure (RF) with death (p<0.001) and we also found a significant association with alcohol abuse (p =0.036) and mucositis (p=0.016), and those variables remained statically significant in multivariated analysis [mucositis (p=0.004) and alcohol abuse (p=0.02)]. According to survival analysis we found significance for the major number of chemotherapy regimens received in the past (p= 0.005), mucositis (p= 0.029), alcohol abuse (p= 0.044) and decreased monoxide carbon diffusion (p=0.048). In our study the mortality rate remains high for those patients who develop RF and need MV. It seems not to have impact what kind of ventilatory support is used (invasive or non-invasive ventilation). Mucositis needs special attention because treating it we can be preventing RF and decrease mortality rates. The effect of alcohol abuse in mortality rate and RF deserve a special attention because its socially accepted and his deleterious action its not explained. The oxidative stress seems to have an important main effect over post-transplant complications and it can be increased by alcohol abuse history. The major number of chemotherapy regimens received in the past increase mortality, it could represent patients who had baseline disease more difficult to treat, more resistant, or patients who were exposed to a cumulative side effect of drugs. Monoxide carbon diffusion is a useful test to identify the risk for death

Alcoolismo

Insuficiência respiratória

Mucosite

Neoplasias

Quimioterapia

Transplante de medula óssea

Alcoholism

Bone marrow transplantation

Continuous positive airway pressure

Drug therapy

Mucositis

Neoplasms

Respiratory insufficiency

Controle tardio da inflamação em esclerose múltipla em pacientes tratados com transplante autólogo de células tronco hematopoiéticas / Late control of inflammation in multiple sclerosis in patients treated with autologous hematopoietic stem cell transplantation

Lara Zupelli Lauar

05 June 2017

A esclerose múltipla (EM) é uma doença desmielinizante inflamatória crônica recorrente, restrita ao sistema nervoso central (SNC), cuja característica histológica é a ocorrência de desmielinização relacionada com infiltrado inflamatório perivenular com relativa preservação axonal. A forma clássica da doença se caracteriza pela recorrência de ataques (surtos), seguidos de remissão dos sintomas (RRMS), com a presença de múltiplas lesões focais dispersas pelo SNC (dissociação espacial) com processo inflamatório exuberante na fase aguda, coexistindo com lesões crônicas (dissociação temporal) sem atividade inflamatória evidenciavel pela quebra de barreira hematoencefálica e realce na fase contrastada na imagem de ressonância magnética (MRI). Alguns pacientes tem uma evolução benigna, permanecendo livre de sequelas significativas por mais de 20 anos da doença. Outros pacientes têm uma forma agressiva da doença, ficando restritos à cadeira de rodas em 8 a 10 anos de evolução. Um desafio é modificar o curso desta forma agressiva, o que pode ser feito com o uso de imunomoduladores, quimioterápicos e, eventualmente, transplante autólogo de células tronco hematopoiéticas (aHSCT). O objetivo da utilização do aHSCT é a restauração da atividade imunológica livre dos ataques à mielina (\"autoimune reset\"). Uma das maneiras de se monitorar a eficácia do tratamento é a identificação da ocorrência de novas lesões e de lesões com reforço visíveis em exames de RM seriados. Objetivo: Testar a hipótese de que o tratamento de pacientes com EM, utilizando AHSCT, foi eficaz em evitar a recorrência de inflamação e o aparecimento de novas lesões visíveis na SB ao exame de MRI, a longo prazo. Resultados: Na nossa Instituição, cerca de 66 pacientes portadores de EM foram tratados com aHSCT no período de 2004 a 2011, sendo seguidos desde então pelas disciplinas de hematologia, neurologia/neuroimunologia e pela seção de RM do CCIFM-HCRP. Método: Foram revisados os exames de RM de encéfalo adquiridos de maneira prospectiva e protocolada, de 76 pacientes submetidos ao aHSCT, com seguimento por MRI há mais de cinco anos. As imagens de RM foram arquivadas nos servidores do CCIFM, foram recuperadas, anonimizadas e revistas por pelo menos dois radiologistas experientes, de maneira independente e por confrontação. Foi considerada falha terapêutica a identificação de lesões novas e/ou lesões com reativação inflamatória. Resultados: Dez pacientes foram excluídos. Doze pacientes (18,18%) apresentaram novas lesões ou recorrência do processo inflamatório, com reforço. Conclusão: Na nossa amostra o aHSCT foi capaz de controlar a recorrência de lesões e da atividade inflamatória perceptível na RM em mais de 87% dos casos, caracterizando uma importante opção terapêutica de segunda linha nos casos de maior agressividade da doença / Multiple sclerosis (MS) is a recurrent chronic inflammatory demyelinating disease, restricted to the central nervous system (CNS), whose histological feature is the occurrence of perivenular inflammatory infiltrate, leading to demyelination with relative axonal preservation. The classic form of the disease is characterized by the recurrence of attacks (outbreaks), followed by remission of symptoms (RRMS), with the presence of multiple focal lesions dispersed by the CNS (spatial dissociation) with exuberant inflammatory process in the acute phase, coexisting with chronic lesions (Temporal dissociation) without inflammatory activity evidenced by the breakdown of blood-brain barrier and contrast-enhanced contrast-enhanced magnetic resonance imaging (MRI). Some patients have a benign course, remaining free of significant sequelae for more than 20 years of the disease. Other patients have an aggressive form of the disease, being restricted to the wheelchair in 8 to 10 years of evolution. One challenge is to modify the course in this aggressive way, which can be done with the use of immunomodulators, chemotherapeutics and, eventually, autologous hematopoietic stem cell transplantation (aHSCT). The goal of using aHSCT is to restore immune activity free of myelin attacks (\"autoimmune reset\"). One of the ways to monitor treatment efficacy is to identify the occurrence of new lesions and visible reinforcing lesions on serial MRI scans. Objective: To test the hypothesis that the treatment of patients with MS using AHSCT was effective in avoiding the recurrence of inflammation and the appearance of new visible lesions in SB at the long-term examination of MRI. Results: At our institution, approximately 66 patients with MS were treated with aHSCT from 2004 to 2011, followed by the hematology, neurology / neuroimmunology and MRI sections of the CCIFM-HCRP. Methods: Brain and MRI scans acquired in a prospective and protocolized way from 76 patients who underwent aHSCT were followed up with MRI for more than five years. The MR images were archived on the CCIFM servers, retrieved, anonymised and reviewed by at least two experienced radiologists, independently and by confrontation. The identification of new lesions and / or lesions with inflammatory reactivation was considered therapeutic failure. Results: Ten patients were excluded. Twelve patients (18.18%) presented new lesions or recurrence of the inflammatory process, with reinforcement. Conclusion: In our sample, aHSCT was able to control the recurrence of lesions and the inflammatory activity detected in MRI in more than 87% of the cases, characterizing an important second line therapeutic option in the cases of greater aggressiveness of the disease.

Esclerose múltipla

Imagem de ressonância magnética

Transplante autólogo de medula óssea

Bone marrow transplante (BMT)

Magnetic ressonance imaging

Multiple sclerosis

Estudo da interação das células-tronco mesenquimais e linfócitos no modelo da doença do enxerto contra hospedeiro / Study of mesenchymal stem cells and lymphocytes interaction in graft versus host disease model

Marília Normanton

10 July 2014

Uma das principais complicações inerentes ao transplante de células-tronco hematopoiéticas é a doença do enxerto contra hospedeiro (DECH), que se trata da resposta imunológica contra os tecidos do receptor pelas células T do doador contidas no transplante. Este quadro é responsável por 15-30% das mortes que ocorrem após o transplante de células-tronco hematopoiéticas alogênicas. Apesar dos recentes avanços para reduzir a incidência de DECH através de alternância de regimes profiláticos reduzindo a intensidade do condicionamento, são poucos os tratamentos efetivos. Recentemente, o potencial imunomodulador das células-tronco mesenquimais tornou-se o foco de vários estudos. Alguns autores descreveram a atuação destas células na redução da resposta imunológica através da inibição da proliferação de células T, representando um novo potencial terapêutico para DECH. Mediante esse conhecimento, investigamos o papel das células-tronco mesenquimais na proliferação, apoptose e na produção de citocinas por linfócitos T. Nossos resultados mostraram que a presença de células-tronco mesenquimais nas culturas regulam negativamente a proliferação de linfócitos T estimulados de forma independente de contato e a apoptose de forma parcialmente dependente de contato. Observamos também que linfócitos T virgens em diferenciação para Th17 na presença de células-tronco mesenquimais apresentam redução na capacidade de produzir duas importantes citocinas efetoras implicadas na DECH, o interferon gama (IFN-y) e a interleucina 17A (IL-17A). Investigamos se a prostaglandina E2 (PGE2), por depletar triptofano, estava envolvida com a diminuição de proliferação de linfócitos T quando em cultivo com células-tronco mesenquimais. Utilizamos nas culturas a indometacina (IDT), um anti-inflamatório bloqueador de cicloxigenase (COX 1 e 2) e portanto da via da PGE2. Entretanto, observamos que o bloqueio da via da PGE2 inibia ainda mais a proliferação de linfócitos T e isto ocorria de acordo com a dose de IDT. Com o resultado deste experimento concluímos que, se a proliferação de linfócitos é inibida pela depleção de triptofano do meio, ela não ocorre via PGE2. Entretanto ainda não conseguimos esclarecer se esta via é ativada por outras moléculas, ou se é esta a via realmente responsável pela inibição da proliferação de linfócitos. No que concerne a via de inibição de apoptose, mostramos que a cadeia alpha do receptor de IL-7 (CD127) está aumentada na superfície de linfócitos T quando em presença de células-tronco mesenquimais. Verificamos que o bloqueio de IL-7 nas culturas aumenta a apoptose em linfócitos, bem como sua adição causa diminuição de apoptose. Identificamos a produção intracelular de IL-7 nas células-tronco mesenquimais, relacionando estas células e IL-7 com a inibição de apoptose em linfócitos T nestas condições. Este trabalho gerou dados que permitiram a compreensão de alguns possíveis mecanismos pelos quais as MSCs podem atuar sobre linfócitos T ativados e/ou alorreativos; mecanismos estes que podem ser utilizados como base para futuras investigações na elucidação e prevenção da DECH / A major complication after hematopoietic stem cell transplantation is the graft versus host disease (GVHD), which is an immunological response of transplanted donor T cells against the recipient tissues; this outline is responsible for 15-30% of deaths that can occur after allogeneic hematopoietic stem cells transplant. Despite recent advances in reducing GVHD incidence by alternating prophylactic regimens, thus reducing the intensity of conditioning, there are few effective treatments. Recently, the immune modulatory potential of mesenchymal stem cells has become the focus of several studies. Some authors described the role of these cells in reducing immune response by inhibiting T cell proliferation, representing a potential new therapy for GVHD. Through this knowledge, we investigated the mesenchymal stem cells role into T lymphocytes proliferation, apoptosis and cytokine production. Our results showed that the presence of mesenchymal stem cells into the cultures downregulates the proliferation of stimulated lymphocytes independent of contact and apoptosis of stimulated lymphocytes in partially contact-dependent manner. We also observed during naive T lymphocytes differentiation into Th17 cells, that the mesenchymal stem cell presence reduces the lymphocyte ability in producing the GVHD major effectors cytokines, interferon gamma (IFN-y) and interleukin-17A (IL-17A). We investigated whether prostaglandin E2 (PGE2) was involved in the reduction of T lymphocytes proliferation, when cultured with mesenchymal stem cells, by tryptophan depletion. Indomethacin (IDT), an anti-inflammatory drug blocker of cyclooxygenase (COX 1 and 2) and therefore PGE2 pathway, was used. However, we observed that, according to IDT dose, blocking this pathway further inhibited lymphocyte proliferation. With this result we conclude that if lymphocyte proliferation is inhibited by tryptophan depletion, it does not occur via PGE2. However, we still cannot say whether this pathway is activated by other molecules, or if this pathway is actually responsible for T lymphocytes proliferation inhibition. Regarding the apoptosis inhibition in T lymphocytes, we show that the IL-7 receptor alpha chain (CD127) is increased on the surface of T lymphocytes when in the presence of mesenchymal stem cells. We found that IL-7 blockage in the cultures increases apoptosis in T lymphocytes, as well as their addition causes apoptosis decrease. We also identified the intracellular production of IL-7 on mesenchymal stem cells, linking these cells and IL-7 directly with apoptosis inhibition in T lymphocytes under these conditions This work has generated data that allowed the understanding of some possible mechanisms by which MSCs can act on activated and/or alloreactive T lymphocytes; mechanisms that can be used as a basis for future research in the elucidation and prevention of GVHD

Apoptose

Células-tronco adultas

Doença enxerto-hospedeiro

Interleucina-7

Linfócitos T

Proliferação de células

Transplante de medula óssea

Adult stem cells

Apoptosis

Bone marrow transplantation

Cellular prolipheration

Graft vs host desease

Interleukin-7

T-lymphocytes

O atendimento odontológico no transplante de medula óssea: impacto clínico e econômico / Dental attendance in bone marrow transplants: clinical and economic impact

Letícia Mello Bezinelli

22 June 2010

A Mucosite Oral é uma das principais e mais debilitantes complicações do Transplante de Medula Óssea. (Schubert et al., 1986; Borowski et al., 1994; Sonis, 1998; Peterson, 2004; Sonis, 2004; Scully, 2006; Sonis, 2009). Nessa terapia sua incidência varia entre 75-100%. (Wardley et al., 2000; Barasch; Peterson, 2003; Schubert et al., 2007; Blijlevens, 2008; Vokurka et al., 2009 ). A extensão e a severidade da Mucosite Oral estão significativamente correlacionadas com dias de narcótico injetável, alimentação parenteral, febre, risco de infecção importante, dias de hospitalização, custos hospitalares e mortalidade. (Sonis et al., 2001; Vera-Llonch et al., 2007). Nosso trabalho trata-se de um estudo de avaliação clínica e econômica, retrospectivo, de pacientes submetidos ao transplante de medula óssea no Hospital Israelita Albert Einstein, entre os anos de 2000 e 2008. Foram avaliados 167 pacientes, que foram divididos em dois grupos: Grupo I, composto por 91 pacientes que receberam atendimento odontológico e Laserterapia durante o TMO e Grupo II, composto por 76 pacientes que não receberam atendimento odontológico nem Laserterapia. Dados como idade, sexo, diagnóstico da doença de base, protocolo quimioterápico, tipo de transplante, uso de medicação para dor, dias de febre, utilização de alimentação parenteral, dias de internação, presença de infecção e grau de mucosite oral, com e sem atendimento odontológico, foram coletados e analisados. Uma análise descritiva, com base em tabelas de frequências e testes Qui-quadrado (ou exato de Fisher, quando este se mostrou mais apropriado), foi feita com o objetivo de verificar a associação estatística entre as variáveis de interesse. Estimativas dos riscos relativos, com intervalos de confiança de 95%, foram calculadas para avaliar a associação entre o desfecho (grau máximo) e as variáveis explicativas de interesse e o tempo médio de internação (em dias) nos diferentes grupos e tipos de transplantes foi comparado por meio de um modelo de análise de variância. Valores de p menores que 0,05 foram considerados como estatisticamente significantes. Pudemos concluir com esse trabalho que a extensão e a severidade da Mucosite Oral foram maiores no grupo sem atendimento Odontológico, sendo que o risco do paciente desse grupo apresentar grau III ou IV foi de 13 vezes maior que o grupo com Cirurgião-Dentista. Além disso, observamos que atendimento odontológico durante o TMO, quando praticado da forma descrita nesse estudo, é custo-efetivo, sendo capaz de reduzir as morbidades clínicas do TMO e que os benefícios do atendimento odontológico excederam os custos e, portanto, devem ser adotados. Foi constatado também que os pacientes que tiveram o acompanhamento do Cirurgião-Dentista apresentaram melhor qualidade de vida durante TMO e que o atendimento odontológico durante o TMO gerou economia para o hospital. / Oral mucositis is one of the main and most debilitating complications of Bone Marrow Transplants. In this therapy its incidence ranges between 75-100%. The extent and severity of Oral Mucositis are significantly correlated with the days of receiving injectable narcotics, parenteral feeding, fever, and risk of important infection, number of days of hospitalization, hospital costs and mortality. This study is a retrospective clinical and economic evaluation of patients submitted to bone marrow transplant at the \"Hospital Israelita Albert Einstein\", between the years 2000 and 2008. A total of 167 patients were evaluated, and were divided into two groups: Group I, composed of 91 patients who received dental treatment and Laser therapy during the BMT and Group II, composed of 76 patients who did not receive dental attendance or laser therapy. Data such as age, sex, diagnosis of the underlying disease, chemotherapy protocol, type of transplant, use of pain relief medication, days of fever, use of parenteral feeding, days of hospitalization, presence of infection and degree of oral mucositis, with and without dental attendance were collected and analyzed. A descriptive analysis, based on Frequency tables and Chi-square tests (or Fishers exact test, when this was shown to be more appropriate), was performed with the aim of verifying the statistical association among the variables of interest. Estimates of relative risks, with confidence intervals of 95% were calculated to evaluate the association between the outcome (maximum degree) and the explicative variables of interest and the mean time of hospitalization (in days) in the different groups and types of transplants was compared by means of an analysis of variance model. p- Values lower than 0.05 were considered statistically significant. By means of this study, it could be concluded that the extent and severity of Oral Mucositis were greater in the group without Dental attendance, as the risk of the patient in this group presenting Grade III or IV was 13 times higher than it was in the group attended by a Dentist. Moreover, it was observed that dental attendance during BMT, when performed in the manner described in this study, is cost-effective, as it is capable of reducing the clinical morbidities of BMT. Furthermore the benefits of dental attendance outweighed the costs, and therefore, must be adopted. It was also found that patients that were followed-up by the Dentist presented a better quality of life during BMT and that dental attendance during BMT resulted in savings for the hospital.

Atendimento Odontológico

Custo- Minimização

Custo-Benefício

Custo-Efetividade

Custo-Utilidade

Mucosite Oral

Transplante de Medula Óssea

Bone Marrow Transplant

Cost- Effectiveness

Cost-Benefit

Cost-Minimization

Cost-Utility

Dental Attendance

Oral Mucositis

Expressão de genes de repressão gênica em tumor primário em relação à presença ou ausência de células metastáticas ocultas na medula óssea em pacientes com câncer de mama / Expression of genes involved in transcriptional repression in the primary tumor of breast cancer patients in the presence or absence of occult metastatic cells in the bone marrow

Ana Paula Santana de Abreu

25 August 2006

Estudos sugerem que a presença de células metastáticas ocultas em medula óssea pode ser fator prognóstico em câncer de mama. Além disso, é possível que um perfil gênico tumoral específico, caracterizado por repressão da expressão gênica, esteja associado à detecção de células tumorais na medula óssea. O silenciamento de genes é controlado pela desacetilação de histonas e metilação de DNA, esta última catalisada por enzimas DNA metil transferases. Outro alvo de metil-transferases são as histonas, e histona H3 quando sofre metilação em lisina 9, gera sítio de ligação a proteínas HP1 (Heterocromatin protein-1 ou cromobox). Membros da família HP1 (HP1Hsalfa, HP1Hsbeta e HP1HsY) participam da formação da heterocromatina e da regulação da expressão de genes. Logo, nosso objetivo foi determinar no tumor primário de mama, a expressão de HP1Hsalfa, HP1Hsbeta e HP1Hsy , que participam da repressão gênica, em relação à presença ou ausência de células metastáticas ocultas na medula óssea. Neste estudo foram incluídas 37 pacientes de forma prospectiva, atendidas no Instituto Brasileiro de Controle do Câncer (IBCC) no período de junho de 2004 a julho de 2005, com diagnóstico histopatológico de carcinoma invasivo de mama, estádio clínico (EC) I (16,2%), II (51,4%) ou III (32,4%), segundo a classificação patológica. A idade mediana das pacientes foi 63 anos (41 a 90) e 62.2% delas encontravam-se na pós-menopausa, sendo que 24.3% relatava história familiar para câncer de mama. O tipo histológico predominante foi carcinoma ductal invasivo (89.2% dos casos), sendo, o restante, representado por carcinoma lobular invasivo (10.8%). Foram coletadas amostras de tumor primário de mama e de aspirado de medula óssea de cada paciente. A presença de células metastáticas ocultas (CMO) na medula óssea (MO) foi detectada através da expressão de citoqueratina 19 (CK19) pelo método de nested RT-PCR. A expressão relativa dos genes HP1Hsalfa, HP1Hsbeta e HP1Hsy foi determinada no tumor primário, usando-se a técnica de RT-PCR em tempo real. Presença de CMO foi detectada na MO de 20 pacientes (54.1%). Não observamos diferença na expressão de HP1Hs? (1,93 ± 2,25 MO- vs 3,84 ± 5,53 MO+), HP1Hs? (6,74 ± 6,31 MO- vs 6,49 ± 5,86 MO+) e HP1Hs? (24,58 ± 11,14 MO- vs 24,91 ± 15,88 MO+) entre as amostras tumorais de pacientes com presença (MO+) ou ausência (MO-) de micrometástase medular. Também não observamos variação da expressão de genes HP1 em relação ao comprometimento linfonodal, dimensão e grau histológico do tumor, expressão tumoral de receptores de estrógeno e estado menopausal da paciente. A expressão de HP1Hsalfa em tumores de pacientes com câncer de mama ERBB2 negativos, entretanto, foi maior do que em tumores ERBB2 positivos. Nossos dados indicam que em tumores de mama, a expressão de HP1Hsalfa, HP1Hsbeta e HP1Hsy não parece se associar à presença de células ocultas em medula óssea / Studies suggest that the presence of occult metastatic cells (OMC) in the bone marrow (BM) may be a prognostic factor in breast cancer. Besides, it is possible that a specific tumor gene profile, characterized by repression of gene expression, may be associated to the presence of tumoral cells in the bone marrow. Gene silencing is controlled by histone deacetylation and DNA methylation, the last one catalized by enzymes DNA methyltransferases (DNMTs). Histones are another target of methyltransferases, and methylation of histone H3 on lysine-9 generate a binding site for HP1 proteins (Heterocromatin protein-1 or chromobox). Members of the HP1 family (HP1Hsalfa, HP1Hsbeta e HP1Hsy) take part in heterochromatin formation and gene expression regulation. Hence, our aim was to determine in the primary tumor of the breast, the expression of HP1Hsalfa, HP1Hsbeta e HP1Hsy, which participate in gene repression, in the presence or absence of occult metastatic cells in the bone marrow. In this study, 37 patients treated at Instituto Brasileiro de Controle do Câncer, from June 2004 to July 2005, with invasive breast cancer histopathologically confirmed, pathological clinical stages I (16,2%), II (51,4%) or III (32,4), were included. The median age of the patients was 63 years (41 to 90), 62.2% were post-menopausal and 24.3% reported family history of breast cancer. Invasive ductal carcinoma was diagnosed in most patients (89.2%), and invasive lobular carcinoma was detected in the other patients (10.8%). Tumor samples and bone marrow aspirates were obtained from each patient. The presence of CMO in BM was detected by keratin-19 (CK19) expression by nested RT-PCR. The relative expression of the genes HP1Hsalfa, HP1Hsbeta e HP1Hsy was determined by real-time RT-PCR. Occult metastatic cells (OMC) in BM were detected in 20 patients (54.1%). No differences were observed in the expression of HP1Hs? (1,93 ± 2,25 BM- vs 3,84 ± 5,53 BM+), HP1Hsalfa (6,74 ± 6,31 BM- vs 6,49 ± 5,86 BM+) and HP1Hsbeta (24,58 ± 11,14 BM- vs 24,91 ± 15,88 BM+) between tumor samples of BM+ patients and BM- patients. Variations of HP1 gene expression were neither observed according to lymph node involvement, tumor size, histological grade, estrogen receptor status and menopausal status. However, HP1Hsbeta expression in ERBB2-negative tumors was higher than in ERBB2-positive tumors. Our data indicate that in breast cancer tumors, expression of HP1Hsalfa, HP1Hsbeta e HP1Hsy does not seem to be associated with the presence of occult metastatic cells in the bone marrow

Heterocromatina/genética

Inativação gênica

Medula óssea/patologia

Neoplasias mamárias/genética

Queratina/análise

Bone marrow/pathology

Breast neoplasms/genetics

Gene silencing

Heterochromatin/genetics

Keratin/analysis

Expressão gênica diferencial das células estromais obtidas de medula óssea na presença ou ausência de célula tumoral oculta em pacientes com câncer de mama / Differential gene expression of bone marrow stromal cells from breast cancer patients in the presence or abscence of occult tumor cells

Cintia Milani

21 September 2006

A célula estromal pode influenciar o desenvolvimento do tumor no sítio primário e secundário, mas pouco é conhecido sobre as características moleculares das células estromais presentes na medula óssea de pacientes com câncer de mama. Nosso objetivo foi avaliar a expressão gênica diferencial entre as células estromais oriundas de medula óssea na presença ou ausência de célula tumoral oculta. Coletamos dez aspirados de medula óssea das pacientes com câncer de mama. A classificação do comprometimento da medula por células tumorais ocultas foi realizada pela detecção da expressão de CK19 por Nested-RT-PCR e quatro entre dez pacientes apresentaram presença de célula tumoral na medula óssea. Estabelecemos culturas primárias de células estromais de todas as amostras e, selecionamos amostras originárias de duas pacientes contendo linfonodos comprometidos e presença de célula tumoral oculta em medula e também de duas pacientes que não apresentavam linfonodos comprometidos e nem célula tumoral oculta na medula. As pacientes selecionadas eram pós-menopausadas com diagnóstico de carcinoma ductal invasor e expressão imunohistoquímica positiva para receptor de estrógeno e progesterona. Realizamos avaliação do perfil de expressão gênica entre estes dois grupos, o que nos revelou 21 genes diferencialmente expressos dentre os 4.608 genes imobilizados em lâmina de cDNA microarray; nove genes hiperexpressos em célula estromal de medula comprometida (PTHLH, TLOC1, NCOA6, C17orf57, ANAPC11, MAST4, POLR3E, CPNE1 e B4GALT5) e doze genes hipoexpressos em célula estromal de medula comprometida (MRPL2, NAT10, DAP, RNF2, FLOT2, FKBP10, SLIT3, EBNA1BP2, SLC35B2, MICAL2, GPR3, TSPAN17). Nossos dados sugerem que apesar da expressão gênica de células estromais oriundas de medula óssea comprometida ou não por micrometástases ser semelhante, algumas diferenças podem ser identificadas. / Stromal cells may influence tumor development in primary and secundary sites, however, molecular characteristics of bone marrow stromal cells from breast cancer patients are almost unknown. Our aim was to evaluate the differential gene expression of bone marrow stromal cells from breast cancer patients in the presence or abscence of occult tumor cells. Bone marrow (BM) aspirates were obtained from 10 breast cancer patients. The presence of occult bone marrow disseminated tumor cells was detected by CK19 expression quantified by reverse transcriptase polymerase chain reaction (RT-PCR). Presence of tumoral cell was detected in four of ten BM samples. Stromal cells primary cultures were established and samples from two patients with positive lymph nodes and presence of occult tumor cells in bone marrow and samples from two patients with negative lymph nodes and abscence of occult tumor cells in bone marrow were selected. All the included patients were postmenopausal with invasive ductal carcinoma and positive estrogen and progesterone receptors detected by immunohistochemical analysis. Gene profile evaluated in cDNA microarray slides containing 4.608 spotted genes revealed 21 differencially expressed genes, nine upregulated (PTHLH, TLOC1, NCOA6, C17orf57, ANAPC11, MAST4, POLR3E, CPNE1 e B4GALT5) and twelve downregulated (MRPL2, NAT10, DAP, RNF2, FLOT2, FKBP10, SLIT3, EBNA1BP2, SLC35B2, MICAL2, GPR3, TSPAN17) in stromal cell derived from bone marrow in the presence of tumor breast cancer cell. Our data suggest that gene expression from bone marrow derived stromall cells in the presence or abscence of occult tumor cells seems similar, however small differences may be identified.

Células estromais

Expressão gênica

Medula óssea

Neoplasias mamárias

Queratina/análise

Bone marrow

Breast neoplasms

Gene expression

Keratin/analysis

Stromal cells

Perfil transcricional de fibroblastos de tumor primário, linfonodo e medula óssea de pacientes com câncer de mama / Transcriptional profile of fibroblasts obtained from primary tumor, lymph node and bone marrow of breast cancer patients

Paulo Roberto Del Valle

01 March 2013

Introdução: Em câncer de mama, existem evidências de que o microambiente pode influenciar o desenvolvimento do tumor no sítio primário, bem como em metástases regionais e a distância. Neste contexto, fibroblastos são importantes células estromais que podem influenciar a proliferação e a migração de células do câncer e podem prover um nicho apropriado para o desenvolvimento tumoral. Objetivos:O principal objetivo deste trabalho é comparar células estromais obtidas do tumor primário (PT), metástase linfonodal (N+) e medula óssea (BM) de pacientes com câncer de mama, através do perfil de expressão gênica. Pacientes e Métodos: Foi analisada a expressão gênica de fibroblastos (cultura primária) de 11 pacientes com câncer de mama. O perfil de expressão foi determinado em PT (n=4), N+(n=3) e BM (n=4) através de uma plataforma de cDNA microarray customizada (contendo 4.800 sequencias imobilizadas, representando cerca de 4600 genes), e os genes diferencialmente expressos foram identificados pelo teste SAM multiclasse, seguido pelo teste SAM de duas classes (TMEV, FDR 0%). A análise funcional foi realizada pelo software DAVID v6.7. Validação técnica foi realizada em 6 amostras previamente analisadas no microarray e a validação biológica em fibroblastos obtidos de outros 16 pacientes utilizando-se de RT-qPCR. Resultados: O perfil de expressão gênica dos fibroblastos obtidos de diferentes sítios mostraram 267 genes diferencialmente expressos, os quais apropriadamente agruparam os fibroblastos de acordo com suas origens (PT vs. N+ vs. BM). Apesar das diferenças entre PT e N+ serem representadas por 20 genes, as diferenças entre PT vs. BM e N+ vs BM foram mais significantes (235 e 245 genes diferencialmente expressos respectivamente). Análise funcional dos genes diferencialmente expressos mostrou enriquecimento de funções relacionadas ao desenvolvimento e morfogênese.A seguir, a expressão de alguns genes selecionados foi analisada em uma série diferente de amostras (validação biológica). Desse modo observamos que NOTCH2 confirmou uma alta expressão em N+ (vs. PT), e ADCY2, HECTD1, HNMT, LOX, MACF1 e USP16 confirmaram alta expressão em BM (vs PT). Conclusão:Em pacientes com câncer de mama, células estromais obtidas de diferentes origens apresentam um perfil de expressão gênica diferencial, o qual pode influenciar o comportamento do tumor / may influence tumor development in the primary site of breast cancer, as well as in regional and distant metastatic sites. In this context, fibroblasts are important stromal cells which influence proliferation and migration of cancer cells and may also provide an appropriate niche to tumor development. Objectives: The main objective of this work is the comparison of stromal cells from the primary tumor (PT), lymph node metastasis (N+) and bone marrow (BM) obtained from breast cancer patients, through gene expression profile. Patients and Methods: The gene expression profile was analyzed in fibroblasts primary culture from 11 breast cancer patients. The expression profiles of PT cells (n=4), N+ cells (n=3) and BM cells (n=4) were determined through a customized cDNA microarray platform (containing 4800 immobilized sequences which represents 4600 genes approximately). The analysis were performed by SAM multiclass (TMEV; FDR 0%), followed by SAM two classes test (TMEV; FDR 0%). Functional analysis was performed using DAVID v6.7. Technical validation was performed in same 6 samples that were previously analyzed in microarray experiments and biological validation was performed in fibroblasts obtained from other group of 16patients by RT-qPCR Results: The expression profile of fibroblasts obtained from three sites revealed 267 differentially expressed genes, which appropriately clustered fibroblasts in three different branches, in accordance with their origin (PT vs. N+ vs. BM). Although the differences between PT and N+ were represented by 20 genes, differences between PT vs. BM and N+ vs. BM were more significant (235 and 245 differentially expressed genes respectively). Functional analysis revealed enrichment of functions related to development and morphogenesis. Afterwards, the expression of some selected genes were analyzed in a different batch of samples (biological validation).Thereby, NOTCH2 confirmed high expression in N+ (vs. PT), and ADCY2, HECTD1, HNMT, LOX, MACF1 and USP16 confirmed high expression in BM (vs. PT). Conclusion: In breast cancer patients, stromal cells obtained from different origins present a differential gene expression profile, which may influence tumor behavior

Células mesenquimais estromais

Fibroblastos

Linfonodos

Medula óssea

Microambiente tumoral

Neoplasias da mama

Bone marrow

Breast neoplasm

Fibroblasts

Gene expression profiling

Lymph node

Mesenchymal stromal cells

Tumor microenvironment

Défauts de la réparation de l’ADN et développement lymphoïde : Analyse de situations pathologiques chez l’homme et la souris / DNA repair defects and lymphocyte development : Study of pathological contexts in human and mice

Vera, Gabriella

12 November 2012

Au cours de leur développement, les cellules du système hématopoïétique sont très exposées aux dommages à l’ADN qui peuvent avoir une origine exogène ou endogène. Les organismes vivants ont développé de nombreux mécanismes de réparation pour y faire face, et leur dysfonctionnement est responsable de maladies rares mais sévères chez l’Homme. Un des deux mécanismes de réparation des cassures double-brin (CDB) de l’ADN joue un rôle prépondérant dans le développement du système immunitaire (SI) des mammifères. Il s’agit de la voie de réparation des extrémités non-homologues (NHEJ) qui est absolument essentiel au bon déroulement de la recombinaison V(D)J dans les progéniteurs lymphocytaires de la moelle osseuse et du thymus. En effet, la formation de CDB de l’ADN est une étape clé de ce remaniement. De même, bien que dans une moindre mesure, le NHEJ intervient pour réparer les cassures induites par AID lors de la commutation de classe des immunoglobulines (Ig- CSR). Notre équipe a précédemment identifié un nouveau facteur du NHEJ, Cernunnos (ou XLF), responsable chez l’Homme de déficit immunitaire combiné sévère (DCIS) associé à une sensibilité aux rayonnements ionisants (RI) et à une microcéphalie. Afin de mieux comprendre le rôle de Cernunnos dans le système hématopoïétique et dans le développement des lymphocytes en particulier, nous avons créé un modèle murin invalidé pour ce gène. De façon surprenante, le développement lymphocytaire se fait quasi normalement dans ces souris, le seul défaut observé est une diminution du nombre de lymphocytes. Cependant, l’analyse fine du répertoire des cellules T a permis de mettre en évidence un biais dans l’utilisation des segments variables V et J de la chaîne α du récepteur (TCRα). Ce serait là la signature d’un défaut de survie des thymocytes, passant par une activation chronique de la voie de l’apoptose dépendante de p53 en réponse à l’accumulation de dommages de l’ADN. Certaines sous- populations de lymphocytes T, comme les iNKTs et les MAITs, seraient ainsi affectées. Par ailleurs, notre équipe poursuit la caractérisation génétique et fonctionnelle de pathologies chez des patients dont le tableau clinique laisse penser qu’il existe un déficit immunitaire ou hématologique primaire associé à un défaut de réparation de l’ADN. Nous nous sommes intéressés à un patient dont le tableau clinique combinant déficit hématopoïétique et instabilité génomique suggère une origine génétique forte. Grâce aux techniques de séquençage haut- débit et à l’étude de ségrégation au sein de la famille nous avons pu isoler plusieurs mutations dont une nous a interpellé plus particulièrement / Throughout their development, hematopoietic cells are exposed to many DNA damages of either exogenous or endogenous origin. Living organisms evolved a variety of DNA repair mechanisms in order to face those threats, and their impairment leads to rare but severe diseases in human. Of the two mechanisms involved in the repair of DNA double-strand break (DSB) repair, one plays a major role in mammal’s Immune System (IS). The non-homologous end joining (NHEJ) pathway is essential for the correct proceeding of V(D)J recombination in lymphocyte progenitors from bone marrow and thymus. Indeed, the formation of DNA DSB is a key step of the rearrangement. In similar fashion, though to a lesser degree, NHEJ is involved in repair of AID induced breaks during immunoglobulin class switch recombination (Ig-CSR). Our team previously identified a new NHEJ factor, Cernunnos (or XLF), as being responsible for a human syndrome of severe combined immunodeficiency (SCID) associated with ionizing radiation (IR) sensitivity (RS-SCID) and microcephaly. To better understand Cernunnos role in the hematopoietic system and particularly in lymphocyte development, we engineered a knock-out (KO) mouse model for this gene. Surprisingly, lymphocyte development is almost normal in these mice, the only defect observed being a decrease of lymphocyte number. However, a refined analysis of T cell repertoire allowed us to uncover a bias in the use of V and J segments from the receptor’s α chain (TCRα). This is the signature of a survival defect in thymocytes, caused by chronic activation of the p53 dependent apoptosis pathway in response to DNA damage. Some discrete T cell populations, such as iNKTs and MAITS, would be affected. In the meantime, our team pursues the uncovering of genetic diseases and their functional description in patients showing signs of immune or hematopoietic deficiency combined to impaired DNA repair. We focused on a patient harboring clinical signs of genomic instability and hematopoietic defects with strong evidence for genetic cause. Thanks to high-throughput DNA sequencing technology and whole genome association study (WGAS), we identified several mutations, one of them striking us as pertinent

NHEJ

Cernunnos

XLF

Recombinaison V(D)J

Réparation de l’ADN

Déficits immunitaires

Instabilité génomique

Aplasie médullaire

NHEJ

Cernunnos

XLF

V(D)J recombination

DNA repair

Immune deficiency

SCID

Genomic instability

Bone marrow failure

Bone marrow niche-mimetics modulate hematopoietic stem cell function via adhesion signaling in vitro

Kräter, Martin

09 November 2017

As graft source for lymphoma or leukemia treatment, hematopoietic stem and progenitor cells (HSPCs) have been the focus of translational medicine for decades. HSPCs are defined by their self-renewing capacity and their ability to give rise to all mature blood cells. They are found anchored to a specialized microenvironment in the bone marrow (BM) called the hematopoietic niche. HSPCs can be enriched by sorting them based on the presence of the surface antigen CD34 before clinical or tissue engineering use. As these cells represent a minority in most graft sources and the amount of applicable cells is limited, ex vivo expansion-cultures were established using cytokine cocktails or small molecules. However, in vitro culture of HSPCs as suspension-cultures result in heterogeneous cell populations with undefined cellular identities. In the BM niche, HSPCs are not exclusively maintained by cytokines but also by cell-matrix adhesions mediated by integrins (ITGs). Thus, β1 and β2 ITGs were found to promote initial contact of HSPCs with mesenchymal stromal cells (MSCs) and ITGβ3 expression was shown to be a marker for long-term repopulating HSPCs in vivo. Consequently, ex vivo remodeling of the BM niche using co-cultures of HSPCs and niche cells like MSCs came into spotlight and was proven to be a promising tool for stem cell expansion. However, in clinical and research applications, direct contact of two cell populations necessitates HSPC post-culture purification. To address these problems, we established a novel culture method for remodeling the BM extra cellular stroma in vitro wherein we used decellularized extracellular matrix (ECM) scaffolds derived from immortalized mesenchymal stromal cells (SCP-1). Such scaffolds were found to be highly reproducible and served as in vitro niche for HSPCs by being more effective for the expansion of CD34+ cells, compared to classical suspension cultures. ECMs were shown to consist of multiple proteins including fibronectins, collagens, and a major niche chemokine responsible for BM homing and retention of HSPCs in vivo, namely, stromal derived factor 1 (SDF-1). SDF-1 is known to be secreted by MSCs and is anchored to matrix proteins. This reveals that ECM scaffolds produced by SCP-1 cells are a naïve reconstructed microenvironment. When CD34+ cells were seeded, only around 20% of the cells adhered to the provided ECM scaffold. These cells recognized SDF-1 via C-X-C chemokine receptor type 4 (CXCR-4), as shown by laser scanning confocal microscopy. Thus, adhesive sides as they are present in the BM niche are provided. However, CD34+ cells isolated from G-CSF mobilized peripheral blood of healthy donors were found to be heterogenous with respect to adhesion capacity. Nonetheless, it was similar to HSPC co-cultures with SCP-1 cells as feeder layer. Therefore, we separated and analyzed two cell fractions, the adherent (AT-cells) and the non- adherent supernatant (SN-cells) cells. Other signals provided by the BM extracellular stroma to HSPCs are physical cues that control HSPC fate. HSPCs sense these physical features through focal contacts and accordingly remodel their morphological and biomechanical properties. Using real-time deformability cytometry (RT-DC) to uncover biomechanical phenotypes of freshly isolated HSPCs, SN-cells, AT-cells, and classical suspension cultured HSPCs in plastic culture dishes (PCD) were analyzed. We found freshly isolated cells to be less deformable and small. AT-cells displayed actin polymerization to stress fibers, and exhibited a stiffer mechanical phenotype compared to PCD-cultured or SN-cells. This might constitute the first hint of functional adaptation. Integrins are known to establish mechanosensing focal contacts. Thus, we analyzed ITG surface expression and identified ITGαIIb, ITGαV, and ITGβ3 to be enriched on AT-cells compared to freshly isolated cells or SN-cells. Active integrins need to form heterodimers consisting of one α- and one β subunit. Interestingly, the identified ITGs exclusively interact with each other to form RGD peptide receptors. RGD is a tripeptide consisting of the amino acids arginine, glycine, and aspartic acid and was identified as an adhesion sequence within fibronectin and other extracellular proteins. Consequently, we could confirm an important role for ITGαVβ3 in HSPC- ECM interaction with respect to adhesion and migration. However, we also identified ITGβ3 expression on a subset of CD34+ cells either freshly isolated or ECM cultured cells, as a marker for erythrocyte differentiation. These findings demonstrate that, in vitro, the ECM compartment acts as a regulator of HSPC fate and portray mechanical recognition as a potent driver of differentiation. In this context, targeted modulation of ECM scaffolds could enhance cell-ECM interactions and accelerate stem cell expansion or differentiation. These modulations could also provide further insights into HSPC-niche regulation. We demonstrate that ECMs derived from osteogenic differentiated SCP-1 cells increase HSPC expansion but do not lead to increased cell adhesion. As ECM adhesion preliminary alters HSPC function, we aimed at developing ECM scaffolds with increased adhesion capacity. Using lentiviral transduction, we generated a stable knock down of fibulin-1 in SCP-1 cells. Fibulin-1 is an ECM protein known to form anti-adhesion sites with fibronectin. However, we failed to increase adherent cell numbers or enhance HSPC expansion in the fibulin-1 knock down ECMs. Taken together, SCP-1 cell-derived ECM protein scaffolds provide an in vitro niche for HSPCs capable of stem cell expansion. Integrin mediated signaling altered the biomechanical and functional properties of HSPCs and hints at suspension cultures as being inappropriate to study the physiological aspects of HSPCs. Targeted modulation of ECM scaffolds could theoretically generate suitable ex vivo environments with the capacity to gain detailed insight into HSPC regulation within their niche. This will enhance the functionality of new biomaterials and will lead to improved regenerative therapies like BM transplantation.

Knochenmarksnische

Integrin beta 3

extrazelluläre Miatrix

blutbildende Stammzelle

Bone marrow niche-mimetics

Integrin beta 3

extracellular matrix

hematopoietic stem cell

ddc:610

rvk:WE 2400

Blutstammzelle

Extrazelluläre Matrix

Knochenmark

Integrine

Impact d’une prise en charge par la relaxation psychothérapique sur l’ajustement émotionnel, la qualité de vie et l’image du corps de patients atteints d’un cancer hématologique, hospitalisés en secteur stérile pour une greffe de moelle osseuse / Impact of psychotherapeutic relaxation interventions on emotional adjustment, quality of life and body image in hematologic cancer patients hospitalized in a sterile hospital's area for a bone marrow transplantation

Kostopoulou-Grolleau, Panagiota

14 December 2015

Introduction : La prise en charge psychologique de patients pendant le processus de greffe demoelle osseuse pour un cancer hématologique fait partie intégrante du parcoursthérapeutique. Cette étude a deux objectifs : (1) tester l’impact d’une prise en charge par larelaxation psychothérapique, Méthode Sapir à court et à moyen terme, auprès de cettepopulation (2) savoir si des variables dispositionnelles (alexithymie, optimisme) et desvariables transactionnelles (stratégies de coping, soutien social perçu) peuvent influencer cetimpact.Méthode : 39 patients ont été inclus. Le groupé expérimental (N=20) a bénéficié d’une priseen charge par la relaxation psychothérapique tandis que le groupe contrôle (N = 19) a eu unsuivi psychologique traditionnel. Les patients ont été évalués 4 jours avant la greffe (T1),puis 45 jours (T2) et 100 jours (T3) après la greffe. Les variables dispositionnelles(alexithymie, optimisme), les variables transactionnelles (coping, soutien social perçu) et lesissues à prédire (état émotionnel, image du corps et qualité de vie) ont été mesurées.Résultats : A T3, les patients du groupe expérimental sont significativement moins anxieux(p<0,001), éprouvent une meilleure satisfaction corporelle (p<0,01) et ont une meilleureQDV physique (p≤0,001) qu’à T1. Chez les patients du groupe contrôle aucun changementsignificatif n’est observé avec le temps. Par ailleurs, aucune différence significative entre lesdeux groupes n’a été trouvée aux trois temps de l’étude. A T3, les patients alexithymiques dugroupe expérimental sont significativement moins dépressifs (p<0,05), ont une meilleureQDV cognitive (p<0,01) et émotionnelle (p<0,01) qu’à T1.A T3, les patients les plusoptimistes du groupe expérimental rapportent une meilleure QDV physique (p<0,05) etémotionnelle (p<0,05) qu’à T1.Chez les patients du groupe contrôle aucune modération del’alexithymie et de l’optimisme sur l’ajustement au cancer n’est observée. Enfin, l’effet demédiation du coping et du soutien social perçu n’a pas été démontré dans cette étude.Conclusion : La prise en charge par la relaxation psychothérapique a une place auprès decette population. L’illustration de deux cas cliniques vient confirmer ces propos. Cependant,au regard du faible nombre de sujets, il convient de contre-valider ces résultats auprès d’unepopulation plus large. / Introduction: The psychological care of patients during the process of bone marrowtransplantation for a hematological cancer is part of the therapeutic process. This study hastwo objectives: (1) to test at a short and medium term the impact of psychotherapeuticrelaxation, Sapir’s method, on the psychological adjustment of patients with hematologiccancer hospitalized at a sterile hospital’s room for bone marrow transplantation; (2) toexamine weather dispositional variables (alexithymia, optimism) and transactional variables(coping, perceived social support) can influence this impact.Method: 39 patients were included. The experimental group (N=20) received a care ofpsychotherapeutic relaxation while the control group received a traditional psychologicalfollow-up. Patients were evaluated 4 days before transplantation (T1), 45 days aftertransplantation (T2) and 100 days post-transplantation (T3), respectively. Personalityvariables (alexithymia, optimism), adjustment of cancer variables (emotional state, bodyimage, quality of life) and transactional variables (coping, perceived social support) weremeasured.Results: The patients in the experimental group at T3 are significantly less anxious(p<0.001), experienced a better body satisfaction (p<0.01) and a better physical quality oflife (p≤0.001) than at T1. In patients of the group control, no significant positive or negativemovements are observed by the time on studied variables. Moreover, no significantdifferences are found between two groups on three times of study. The alexithymic patientsof the experimental group are significantly less depressed at T3 (p<0.01) and experienced abetter cognitive (0.01) and emotional (p<0.01) quality of life. The most optimistic patients ofthe experimental group have a better physical (p<0.05) and emotional (p<0.05) quality oflife. In patients of the control group, no moderation of alexithymia and optimism is observedon cancer adjustment. Finally, the mediating effect of coping and perceived social support isnot demonstrated in this study.Conclusion: The psychotherapeutic relaxation has an important place to this population. Thisis confirmed by the illustration of two cases. Finally, due to the small number of subjectsincluded, these results require validation on a larger population.

Allogreffe de moelle osseuse

Prise en charge psychologique

Relaxation psychothérapique

Ajustement émotionnel

Image du corps

Qualité de vie

Alexithymie

Optimisme

Coping

Soutien social perçu

Allogeneic bone marrow transplantation

Psychological care

Psychotherapeutic relaxation

Emotional adjustment

Body image

Quality of life

Alexithymia

Optimism

Coping

Perceived social support