Alterações bucais em pacientes submetidos ao transplante de células tronco hematopoiéticas: estudo longitudinal / Oral complications in patients undergoing hematopoietic stem cell transplantation: a longitudinal study

Luiz, Ana Cláudia

03 May 2012

A boca é local de frequentes complicações relacionadas ao transplante de células tronco hematopoiéticas (TCTH) tais como xerostomia, disgeusia, disfagia, mucosite, infecções oportunistas e doença do enxerto contra hospedeiro (DECH). Sabe-se que estas complicações podem comprometer a qualidade de vida do paciente e interferir na morbidade pós-TCTH. O dentista é o profissional da saúde que deverá intervir no momento correto para tratar e minimizar esses efeitos secundários do TCTH. Para tanto é importante conhecermos o momento em que cada complicação ocorre para que a intervenção seja pronta e eficiente. O objetivo principal deste estudo foi identificar e quantificar as alterações bucais em indivíduos submetidos ao TCTH em cinco momentos consecutivos desde antes do início do condicionamento pré-TCTH até o dia 100 pós-TCTH. Como objetivos secundários buscamos investigar possíveis relações entre a severidade da mucosite oral e a manifestação da DECH com dados demograficos (sexo, idade), com o status de saude bucal (por meio dos índices IHO-S, CPOD, número de dentes cariados) e com a realização de adequação bucal pré-TCTH, e ainda, somente para a DECH, também foi investigada a possível relação entre esta doença com infecção sistêmica por citomegalovírus e com a manifestação de mucosite oral severa. Foram incluídos no estudo 27 indivíduos com doenças hematológicas do Serviço de Transplante de Medula Óssea do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo (HC-FMUSP), com idade 12 anos que receberam TCTH alogênico. Os indivíduos foram examinados em cinco momentos consecutivos. No primeiro momento, pré-TCTH, foi realizada a coleta de índices de saúde bucal e aplicação de questionário sobre o histórico de tratamentos odontológico prévios. Nos momentos de 10, 20, 60 e 100 dias pós-TCTH foram avaliadas as manifestações bucais presentes. A incidência de mucosite oral foi de 82,6% considerando todos os momentos avaliados. Mucosite oral severa, ou seja, graus 3 e 4 (OMS) foi observada em 57,9% dos pacientes avaliados nos momentos 2 e 3. Dez (37%) pacientes apresentaram GVHD em algum órgão, e destes, 8 (80%) apresentaram GVHD de boca. Infecção sistêmica por CMV foi diagnosticada em 6 (22,2%) pacientes. Concluímos que entre as queixas levantadas, dor bucal e disfagia foram as mais referidas. O período de maior incidência das complicações bucais foi nos segundo e terceiro momentos, ou seja, D+10 e D+20, representando deste forma, o período de maior morbidade do tratamento. Não houve associação entre a severidade de mucosite oral e idade, sexo, fonte de células, regime de condicionamento, número de dentes cariados, IHO-S, CPOD e preparo bucal pré-TCTH. Para a DECH a única relação encontrada foi para fonte de células, tendo sido observada menor chance de ocorrer DECH quando a fonte de células foi o sangue periférico. / The mouth is a well-known site of complications of the hematopoietic stem cell transplantation (HSCT) such as dry mouth, dysgeusia, dysphagia, mucositis, opportunistic infections and graft versus host disease (GVDH). It is known that these complications can compromise the patients quality of life and morbidity post-HSCT. The dentist is the health professional who should interfere at the right time to treat and minimize these side effects of HSCT. Thus, it is important to know the time at which each complication occurs to be dynamic and efficient. The main objective of this study was to identify and quantify the oral complications in patients treated with HSCT in five consecutive moments starting before conditioning chemotherapy until day 100 post-HSTC. As secondary objectives we seek to investigate possible relationships between the severity of oral mucositis and the manifestation of GVHD with demographic data (gender, age), with the oral health status (IHO-S, CPOD, number of decayed teeth) and dental treatment previously HSCT, and, only for GVHD, was also investigated the possible relationship between this disease with systemic cytomegalovirus infection and the manifestation of severe oral mucositis. It was included in the study 27 patients with hematologic diseases who were admitted in the Unit of Bone Marrow Transplantation, Hospital of Clinics, Faculty of Medicine, University of Sao Paulo (HC-FMUSP), 12 years old whom received allogeneic HSCT. The subjects were examined in five consecutive moments. At the first moment, before HSCT, the oral health índex evaluation and a questionnaire about history of previous dental treatments were performed. Besides that, 10, 20, 60 and 100 days after HSCT they were evaluated for oral manifestations. Oral mucositis incidence was 82,6% and 57,9% of these patients presented severe mucositis. Ten (37%) patients had GVHD in any organ, and of these, 8 (80%) had oral GVHD. Infection by CMV was diagnosed in 6 (22.2%) patients. We conclude that among the complaints raised, mouth pain and dysphagia were the most mentioned. The period of increased incidence of oral complications was the second and third times (D +10 and +20), representing the increased morbidity period. There was no association between the severity of oral mucositis and age, sex, cell source, conditioning regimen, number of decayed teeth, IHO-S, CPOD and dental treatment pre-HSCT. For GVHD the only relation found was with source of cells, in which, GVHD was less likely to occur when the source of cells was peripheral blood.

Allogeneic transplantation

Disfagia

Disgeusia

Doença do enxerto contra hospedeiro

Dysgeusia

Dysphagia

Graft versus host disease

Hematopoietic stem cell transplantation

Mucosite oral

Oral mucositis

Transplante alogênico

Xerostomia

Xerostomia

IInfluência do Pegivirus humano (HPgV) na medula óssea: impacto clínico e tropismo viral / Human Pegivirus (HPgV) influence on bone marrow: clinical impact and viral tropism

Dias, Juliana Zanatta de Carvalho

01 February 2019

O HPgV (Pegivirus Humano), conhecido anteriormente por GBV-C, causa infecção assintomática, persistente e com alta carga viral. Sendo o vírus de RNA sem patologia associada mais prevalente no mundo até os dias de hoje, os estudos in vitro ainda não foram capazes de mimetizar a replicação in vivo, permanecendo pouco esclarecidos vários aspectos de sua biologia. Estudos em macacos mostraram que os órgãos responsáveis pela maior replicação viral são o baço e a medula óssea, no entanto as células específicas permissíveis à infecção ainda não foram determinadas. Na década de 90, o HPgV ganhou notoriedade por diminuir os efeitos patológicos do HIV e aumentar a sobrevida de pacientes coinfectados HIV/HPgV, através da diminuição da ativação do sistema imune. Devido a essa característica, diversos estudos tentaram associar a presença de viremia a doenças hematológicas e um deles mostrou que a viremia de HPgV parece estar associada com o desenvolvimento de linfoma não- Hodgkin, porém muitas variáveis de confusão parecem influenciar esse resultado. Em conjunto, os dados mostram que o HPgV pode ter influência sobre a maturação e liberação de células progenitoras da medula óssea e, portanto, tornou-se primordial avaliar o impacto da viremia em pacientes com doenças hematológicas e definir o tropismo viral. Para tanto, o presente trabalho analisou a dinâmica de exposição à viremia de HPgV em pacientes submetidos ao transplante de células-tronco hematopoiéticas (HSCT), em cadáveres autopsiados pelo Sistema de Verificação de Óbitos da Capital de São Paulo (SVOC-SP) e em pacientes submetidos à cirurgia de artroplastia pelo Instituto de Ortopedia e Traumatologia (IOT) do HCSP. A carga viral de HPgV foi mensurada por qRT-PCR em Tempo Real levando em consideração valores adquiridos com um curva padrão desenvolvida para este trabalho. Para os pacientes HSCT, o efeito da presença de viremia antes e após o procedimento foi avaliada quanto aos principais desfechos do transplante: doença enxerto-hospedeiro aguda (aGVHD), recaída da doença hematológica primária e mortalidade. Para amostras SVOC e IOT, células específicas dos tecidos (cérebro, fígado, baço, linfonodo, medula óssea e sangue) foram avaliadas quanto à quantidade de RNA viral de polaridade positiva e negativa, a fim de quantificar a replicação e definir o tropismo do vírus. Os resultados mostraram que a prevalência de HPgV encontrada nos pacientes HSCT foi maior do que em estudos similares: 42% para as amostra pré- HSCT e 31% para as amostras pós-HSCT; porém, para as amostras SVOC, a prevalência foi menor do que o esperado: 1,2%. A presença de alta carga viral de HPgV em pacientes HSCT foi associada com aumento da taxa de incidência de aGVHD (95% CI 1,05-5,37, p=0,038). Dada a alta prevalência de HPgV na população brasileira, é essencial confirmar esse achado em outras coortes, de modo a determinar se o monitoramento do HPgV pode beneficiar o cuidado a esses pacientes. Nas amostras SVOC e IOT, a medula óssea apresentou maior número de populações celulares com replicação viral, com destaque para as células B progenitoras e para as células dendríticas. Porém, devido às condições da coleta e do processamento das amostras, o tipo celular permissível à infecção não pôde ser identificado com clareza, portanto fazendo-se necessária a coleta de um número maior de amostras SVOC / HPgV (Human Pegivirus), previously known as GBV-C, causes asymptomatic, persistent and high viral load infection. To date, it is the most prevalent RNA virus without associated pathologies in the world, yet in vitro studies have not yet been able to mimic the in vivo replication, consequently many aspects of its biology remaining unclear. Studies in non-humam primatas have shown that the organs responsible for the greatest viral replication are spleen and bone marrow, however the specific cells permissible for infection have not yet been determined. In the 1990s, HPgV gained notoriety by decreasing the pathological effects of HIV and increasing the survival of coinfected HIV/HPgV patients, by decreasing the activation of the immune system. Because of this characteristic, several studies have attempted to associate the presence of viremia with haematological diseases, and one has shown that HPgV appears to be associated with the development of non-Hodgkin\'s lymphoma, but many confounding variables still seems to influence this outcome. Together, the data show that HPgV may influence the maturation and release of bone marrow progenitor cells and therefore it has become crucial to evaluate the impact of HPgV viremia in patients with haematological diseases and to define viral tropism. Therefore, the present study analyzed the dynamics of HPgV viremia exposure in patients submitted to hematopoietic stem cell transplantation (HSCT), in cadavers autopsied by the São Paulo City Death Verification System (SVOC-SP) and in patients submitted to arthroplasty surgery by the Orthopedics and Traumatology Institute (IOT) of the Clinics Hospital of Sao Paulo. The HPgV was identified by real-time qRT-PCR and the viral load quantification was estimated by a standard curve developed for this work. For HSCT patients, the effect of viremia before and after the procedure was evaluated for the main transplant outcomes: acute graft vs host disease (aGVHD), relapse of primary haematological disease and mortality. For SVOC and IOT samples, tissue-specific cells (brain, liver, spleen, lymph node, bone marrow and blood) were evaluated for the amount of viral positive and negative RNA strains, in order to quantify replication and define virus tropism. The results showed that the prevalence of HPgV found in HSCT patients was higher than in similar studies: 42% for pre-HSCT samples and 31% for post-HSCT samples; however, for SVOC samples, the prevalence was lower than expected: 1.2%. The presence of high viral load of HPgV in HSCT patients was associated with an increase in the incidence rate of aGVHD (95% CI 1.05-5.37, p = 0.038). Given the high prevalence of HPgV in the Brazilian population, it is essential to confirm this finding in other cohorts, in order to determine if HPgV monitoring can improve the care of these patients. In the SVOC and IOT samples, the bone marrow presented a higher number of cell populations with viral replication, especially the progenitor B cells and the dendritic cells. However, due to the conditions of specimen collection and processing, the major permissible cell could not be clearly identified, thus making it necessary to collect a larger number of SVOC samples

Bone marrow

Doença enxerto-hospedeiro

GB virus C

Graft vs host disease

Hematopoietic stem cell transplantation

Human Pegivirus

Medula óssea

Pegivirus humano

Tropismo viral

Viral tropism

Vírus GB C

Reconstitution immunitaire et immunothérapie adoptive anti-virales après allogreffe de cellules souches hématopoiétiques / Anti-viral immune reconstitution and adoptive immunotherapy after hematopoietic stem cell transplantation

Rothé, Lamia

23 July 2010

L’allogreffe de cellules souches hématopoïétiques (CSH) est un traitement efficace des Hémopathies malignes. Cependant, les complications des allogreffes parmi lesquelles les infections virales sont associées parfois à une morbidité et une mortalité importantes. Ces infections surviennent en l’absence de reconstitution immunitaire. Un monitoring régulier de la charge virale des principaux agents infectieux impliqués est réalisé mais amène parfois à la mise en oeuvre abusive de traitements anti-viraux qui ne sont pas dénués de toxicité.Dans ce travail, nous proposons d’associer à ce monitoring un suivi régulier de la reconstitution immunitaire spécifique afin de cibler parmi les patients présentant une réactivation ceux qui nécessitent un traitement curatif de ceux qui pourront maîtriser l’infection par leur système immunitaire. Nous illustrons ce propos avec le virus d’Epstein Barr (EBV) et avons en cours une étude sur l’Adénovirus (ADV).Dans certains cas parfaitement ciblés, les traitements anti-viraux s’avèrent inefficaces. C’est pourquoi dans ce travail, nous présentons la mise au point d’une technique de grade clinique de production de lymphocytes T cytotoxiques anti-ADV (CTL anti-ADV) en condition GMP (Good Manufacturing Practice), grâce au système CliniMACS et au Cytokine Capture System de Miltenyi, afin de proposer une immunothérapie adoptive.Nous décrivons par la suite trois expériences cliniques de traitement compassionnel d’une infection ADV post-allogreffe de CSH. Enfin, nous présentons les résultats préliminaires de la production de CTL bispécifique anti-ADV et CMV / Hematopoietic stem cells Transplantation (HSCT) is a well recognized strategy for treatment of haematological malignancies. However, HSCT complications among which the viral infections a reassociated with high morbidity and mortality. These infections arise in the absence of immune reconstitution. Monitoring of viral reactivations after allogeneic HSCT is necessary, to identify patients at risk of viral infections, but not sufficient, as patients may be abusively treated. In this work we propose to combine viral DNA load assessment with specific immune monitoring to target patients who need to be treated. We report a retrospective study investigating EBV infection and EBV-specific immune recovery using the functional IFN Elispot assay in 40 allogeneic HSCT patients. We initiated a similar study with ADV which is pending. However, although patients are correctly targeted, anti-viral treatment is sometimes not effective. We present a study on the development of a complete clinical grade generation of Human anti-Adenovirus cytotoxic T cells in GMP (Good Manufacturing Practice) conditions, thanks to the system CliniMACS and the Cytokine Capture System, to propose an adoptive immunotherapy to the recipient.We describe afterwards three clinical experiments of treatment of an ADV infection after HSCT.Finally, we present the preliminary results of the anti-ADV and -CMV bi-specific CTL production.

Infections virales

Reconstitution immunitaire

Immunothérapie adoptive

Hematopoietic stem cell transplantation

Viral infections

Immune reconstitution

Adoptive immunotherapy

Immunothérapie adoptive pour le traitement des infections à Adénovirus réfractaires après allogreffes de Cellules Souches Hématopoïétiques : de la recherche fondamentale à la recherche clinique / Adoptive Cellular Immunotherapy for the treatment of refractory Adenovirus infections after Hematopoietic Stem Cell Transplantation : From bench to bedside

Qian, Chongsheng

14 June 2017

L’allogreffe de cellules souches hématopoïétiques (CSH) est un des seuls traitements curatifs des hémopathies bénignes ou malignes et des déficits immunitaires primitifs. Cependant, les infections notamment virales ainsi que la réaction du greffon contre l’hôte comptent parmi les complications les plus fréquentes des allogreffes associées à une morbidité et une mortalité élevées. Les infections virales surviennent souvent en l’absence de reconstitution immunitaire spécifique dans un contexte d’immunosuppression liée à la GVHD elle-même ou à la prophylaxie ou au traitement de la GVHD. Les traitements médicamenteux anti-viraux préconisés présentent une efficacité inconstante dans ce contexte d’immunodéficience et ne sont pas dénués de toxicité. L’alternative thérapeutique prometteuse est l’immunothérapie adoptive cellulaire notamment celle qui consiste en l’injection de lymphocytes T spécifiques anti-viraux isolés par technique immunomagnétique (VSTs). Cependant, ces lymphocytes T peuvent être la cible des traitements immunosuppresseurs administrés pour la GVHD mais également par eux-mêmes être potentiellement la cause de la survenue ou de la réactivation d’une GVHD. Nous avons montré dans ce travail que l’efficacité des VSTs, qui repose sur leur expansion in vivo lors de la rencontre avec le virus circulant, est principalement permise par les sous-populations lymphocytaires les plus immatures, même si elles ne sont présentes qu’en faible proportion. Nous défendons dans ce travail le fait que l’efficacité des VST ainsi que leur persistance repose prioritairement sur la présence des sous-populations lymphocytaires T les plus immatures et ce quel que soit le degré de compatibilité HLA entre les VSTs et le receveur. De plus, leur sensibilité modérée aux corticoïdes, que nous avons étudiée in vitro, ne justifie pas la modulation de l’immunosuppression lors de l’injection des ADV-VSTs, comme observé in vivo dans le protocole clinique multicentrique de phase I/II que nous avons mené entre 2012 et 2015. En effet, ce protocole clinique ne rapporte aucune GVHD de novo après injection d’ADV-VSTs ; en revanche, la modulation de l’immunosuppression peut potentiellement être incriminée dans la réactivation de GVHD dans les semaines suivant l’injection des ADV-VSTs. La réalisation d’un essai comparatif de phase II permettra de prouver très clairement le rôle des VSTs dans la réactivation de GVHD. / Hematopoietic stem cell transplantation (HSCT) is one of the only curative treatments for benign or malignant hematological diseases and primary immune deficiencies. However, viral infections and graft-versus-host disease (GVHD) are among the most frequent complications after HSCT associated with high morbidity and mortality. Viral infections often occur in the absence of specific immune reconstitution in the context of immunosuppression related to GVHD itself or to the prophylaxis or treatment of GVHD. The recommended anti-viral drug treatments have an inconsistent efficacy in this context of immunodeficiency and are not devoid of toxicity. The promising therapeutic alternative is adoptive immunotherapy, in particular the infusion of specific anti-viral T lymphocytes isolated by immunomagnetic technique (VSTs). However, these T lymphocytes may be targeted by immunosuppressive treatments administered for GVHD, but also may be the cause of the onset or reactivation of GVHD. We have shown in this work that the efficacy of VSTs, which is based on their in vivo expansion when they encounter the circulating virus, is mainly allowed by the most immature lymphocyte subpopulations, even in a small proportion. We argue in this work that the efficacy of VSTs and their persistence is mainly based on the presence of the most immature T lymphocyte subpopulations and this regardless of the degree of HLA compatibility between the VSTs and the recipient. Moreover, their moderate sensitivity to corticosteroids, which we have studied in vitro, does not justify the modulation of immunosuppression at the time of infusion of ADV-VSTs, as observed in vivo in the multicenter phase I / II clinical trial we conducted between 2012 and 2015. Indeed, this clinical trial does not report any de novo GVHD after ADV-VSTs infusion. On the other hand, modulation of immunosuppression may potentially be incriminated in the reactivation of GVHD within weeks of ADV-VST infusion. A Phase II comparative trial will bring the evidence of efficacy and will clearly determine the role of VSTs in the reactivation of GVHD

Immunothérapie adoptive cellulaire

Adenovirus infection

Sous-population de lymphocyte T

Corticoïdes

Hematopoietic stem cell transplantation

Adoptive cellular immunotherapy

Adenovirus infection

Anti-virus specific T-cell (VST)

T cell subpopulation

Corticosteroids

617.95

Periphere Blutstammzellen

Schwella, Nimrod

02 May 2000

Bei Patienten mit Keimzelltumoren werden Mobilisation und Separation peripherer Blut-stammzellen durch das Alter, die zytostatische Vorbehandlung und Art der Mobilisations-chemotherapie statistisch signifikant beeinfluát. Der beste pr diktive Parameter f r die gesammelten Stamm- und Vorl uferzellen ist die Anzahl der peripheren CD34+ Zellen, die am Tag der Leukapherese im Blutkreislauf zirkulieren. F r die Rekonstitution der Granulo- und Thrombozytopoese nach Hochdosischemotherapie ist die Dosis der trans-fundierten CD34+ Zellen von signifikantem Wert. Bei der Transplantation von mehr als 2,5 x 10 hoch 6 CD34+ Zellen/kg kann mit einer schnellen und sicheren Regeneration der H matopoese, einem niedrigeren Bedarf an Antibiotika, Erythrozyten- und Thrombozy-tenkonzentraten sowie einem k rzeren Krankenhausaufenthalt gerechnet werden. / In patients with germ cell cancer the mobilization and collection of peripheral blood progenitor cells are significantly influenced by patient's age, cytotoxic pretreatment and the mobilization chemotherapy used. The best predictive factor for harvested progenitor cells is the number of CD34+ cells circulating in the peripheral blood on the day of leukapheresis. The dose of transfused CD34+ cells has a significant impact on the reconstitution of granulocytes and platelets after high-dose chemotherapy. Transplantation of more than 2,5 x 10 to the power of 6 CD34+ cells/kg results in a rapid and safe regeneration of hematopoiesis, less antibiotics and transfusion requirements (red blood cell and platelet concentrates) and a shorter hospital stay.

Mobilisation und Separation

Hochdosischemotherapie

Autologe Transplantation

hematopoietic stem and progenitor cells

mobilization and collection

high-dose chemotherapy

autologous transplantation

610 Medizin

33 Medizin

XH 8050

ddc:610

Caracterização molecular das cepas do Vírus Sincicial Respiratório identificadas nos anos de 2001 e 2002 em unidade de transplante de células tronco hematopoéticas / Molecular characterization of strains of Respiratory Syncytial Virus in Hematopoietic Stem Cell Transplant Unit identified in 2001 and 2002

Machado, Adriana Freire

12 November 2007

O Vírus Sincicial Respiratório (RSV) é reconhecido como agente causador de infecção nosocomial entre receptores de pacientes de células-tronco hematopoéticas causando morbidade e mortalidade consideráveis nesses pacientes. O objetivo desse estudo foi caracterizar as cepas do RSV isoladas de receptores de transplante de células-tronco hematopoéticas (TCTH) do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo durante sua estação. As cepas do RSV foram tipadas (em grupo A ou B) e genotipadas. Das sete cepas analisadas dos receptores de TCTH durante o ano de 2001, somente duas pertenciam ao grupo B, as outras cinco eram pertencentes ao grupo A. Dessas sete cepas, três eram altamente relacionadas e haviam infectados pacientes que freqüentavam o ambulatório. Em 2002, das doze cepas analisadas, três pertenciam ao grupo A e as outras nove pertenciam ao grupo B. Sete cepas eram altamente relacionadas entre elas e eram também de pacientes de ambulatório sugerindo que a transmissão em hospital-dia era mais provável. Enfim, múltiplços genótipos do RSV co-circularam nas unidades de TCTH (ambulatório e enfermaria) do Hospital das Clínicas entre 2001 e 2002. A transmissão nosocomial foi mais provável ocorrer no ambulatório da unidade de TCTH quando comparada à enfermaria. Políticas de controle de infecção devem ser também implementadas em ambulatórios para evitar transmissão nosocomial do RSV e outros vírus respiratórios em pacientes de ambulatório. / Respiratory Syncytial Virus is recognized as the leading cause of nosocomial respiratory infection among recipients of hematopoietic stem cell transplant (HSCT) causing considerable morbity and mortality among theses patients. The aim this study was characterize the strains of Respiratory Syncytial Virus in recipients Hematopoietic Stem Cell Transplant Unit (HSCT) at Hospital das Clínicas, University of São Paulo Medical School during RSV season in symptomatic HSCT recipients at Hospital das Clínicas. The strains of RSV was typed (in group A or B) and genotyped. Of the seven strains analyzed from HSCT recipients during 2001, only two belonged to group B, the other five belonged to group A. Of these seven strains, three were closely related and were from outpatients. In 2002 , of the twelve strains analyzed, three belonged to group A and the other nine belonged to group B. Seven strains were closely related and were also from outpatients suggesting that nosocomial transmission in hospital-day was more likely. In conclusion, multiples genotypes of RSV co-circulated in the Hematopoietic Stem Cell Transplant units (ward and dayhospital) of Hospital das Clínicas between 2001 and 2002. Nosocomial transmission was more likely to occur at the HSCT Day-hospital as compared to the HSCT ward. Infection control practices should be also implemented at Day-hospital Units to avoid nosocomial transmission of RSV and other respiratory viruses in outpatient units.

BBone marrow transplantation

Células-tronco hematopoéticas

Cross infection

Epidemiologia molecular

Hematopoietic stem cells

Hospedeiro imunocomprometido

Immunocompromissed host

Infecção hospitalar

Molecular epidemiology

Respiratory syncytial virus/transmission

Transplante de medula óssea

Mise au point d’une stratégie de marquage cellulaire par des codes-barres moléculaires en vue d’optimiser l’utilisation des cellules souches hématopoïétiques en thérapies génique et cellulaire / Development of a cellular barcoding strategy in order to optimize hematopoietic stem cell use in gene- and cell- based therapy

Grosselin, Jeanne

04 October 2012

De par leurs propriétés d’autorenouvellement et de multipotentialité, les cellules souches hématopoïétiques (CSH) présentent un intérêt médical majeur et sont au cœur de nombreuses thérapies génique et cellulaire. Cependant, leur utilisation en clinique est encore limitée par leur rareté, leur hétérogénéité fonctionnelle, et leur perte durant l’étape de manipulation in vitro qui précède la transplantation.Dans ce contexte, nous avons mis au point une stratégie de marquage cellulaire par des codes-barres moléculaires afin d’évaluer simultanément et quantitativement les capacités de repopulation des CSH in vivo. Cette stratégie nous a permis de cribler 1200 composés chimiques afin d’identifier des molécules capables (1) d’améliorer l’efficacité de transduction des CSH par un vecteur lentiviral, (2) de maintenir voire d’expandre, lors de l’étape de culture in vitro, les CSH capables de repopulation à long terme. Plusieurs molécules candidates sont en cours de validation.Par ailleurs, grâce au marquage par des codes-barres, nous avons révélé l’hétérogénéité des CSH en comparant leur capacité d’autorenouvellement, la taille de la descendance qu’elles génèrent et leur capacité de différenciation. Notre technique nous a permis non seulement de confirmer l’existence de CSH biaisées vers le lignage myéloïde ou vers le lignage lymphoïde, mais aussi de quantifier leur fréquence.L’application de cette stratégie à un autre système cellulaire nous a permis d’étudier l’influence de facteurs environnementaux et génétiques sur la croissance cellulaire de populations exprimant différentiellement l’-synucléine, une protéine impliquée dans la maladie de Parkinson et certains cancers. / Considerable hope is placed on the use of hematopoietic stem cells (HSC) in engineered gene- and cell- based therapy protocols. Their clinical utilization is, however to some extent, limited by their scarce representation, their heterogeneity and their loss during the ex vivo manipulation procedure. Within this context, we developed a barcode tagging strategy to simultaneously evaluate in vivo the repopulating capacity of HSC cultured in vitro. Barcode deconvolution demonstrated that our strategy constitute a powerful tool for tracking HSC quantitatively even using several dozens of different conditions. Using this strategy, we screened 1200 chemical compounds in order to identify molecules acting (1) on HSC transduction efficiency using a lentiviral vector, (2) on maintenance or even amplification during the in vitro culture step of long-term repopulating HSC. Several candidate molecules are currently under validation. In addition, using this barcoding strategy, we reveal heterogeneous behaviour of HSC examining their proliferation capacity, self-renewal ability and their differentiation lineage option. Our technique allowed us not only to confirm the occurrence of myeloid- and lymphoid-biased HSC, but also to quantify their frequency.We apply this strategy to another cell system to address the effect of different genetic and environmental factors on proliferation of cells expressing -synuclein, a protein involved in Parkinson disease and some cancers.

Cellules souches hématopoïétiques

Codes-barres

Thérapie génique

Thérapie cellulaire

Expansion

Transduction

Cellules souches biaisées

-synucléine

Hematopoietic stem cell

Barcodes

Gene therapy

Cell therapy

Expansion,

Transduction

Biased stem cells

-synuclein

Medidas utilizadas na prevenção de infecções em transplante de células-tronco hematopoéticas: evidências para a prática / Infection prevention measures used in hematopoietic stem cell transplantation: evidences for practice

Garbin, Livia Maria

30 June 2010

O transplante de células-tronco hematopoéticas (TCTH) consiste em um procedimento complexo e relacionado à ocorrência de diversas complicações, dentre elas os processos infecciosos decorrentes do longo período de imunossupressão vivenciado após a instituição do regime de condicionamento. Inúmeras medidas têm sido empregadas visando à prevenção e controle de infecções, porém, observam-se divergências em relação à utilização das mesmas; sendo que o emprego da prática baseada em evidências possibilita ao profissional tomar decisões em relação à sua prática fundamentadas em resultados de pesquisas científicas atuais. Esta revisão integrativa da literatura teve como objetivo identificar e avaliar as evidências disponíveis na literatura e publicadas nos últimos 20 anos em relação ao uso de três medidas de prevenção de infecção em pacientes submetidos ao TCTH durante o período de internação: uso de filtros de ar de alta eficiência, isolamento protetor e máscaras. Para a seleção dos artigos foram utilizadas as bases de dados LILACS, PUBMED, CINAHL, EMBASE e a Biblioteca Cochrane. A amostra foi composta por 15 estudos, sendo que apenas um apresentou nível de evidência forte (nível I), dois apresentaram nível de evidência moderado (nível IV e V) e doze consistiram em estudos com evidências fracas (nível VI e VII). Dez estudos abordaram a utilização dos filtros HEPA, sendo recomendado seu emprego para pacientes submetidos ao transplante alogênico durante o período de neutropenia. A necessidade de seu uso para pacientes submetidos ao transplante autólogo ainda é controversa. Nove trabalhos abordaram o uso do isolamento protetor e, embora alguns autores relatem que o emprego do mesmo parece apresentar benefícios quando não se dispõe de filtros HEPA, a utilização desta medida já não é mais indicada tanto pelos Centers for Disease Control and Prevention (CDC) quanto pela maioria dos estudos analisados. Em relação à utilização de máscaras por pacientes, profissionais de saúde ou visitantes dentro das unidades de internação para TCTH, não foram encontrados estudos com evidências fortes que justifiquem o seu uso. No entanto, recomenda-se que sejam seguidas as diretrizes dos CDC quanto ao uso de respiradores especiais (como as máscaras N95) pelos pacientes imunocomprometidos submetidos ao TCTH ao deixar a unidade de transplante provida de filtro HEPA quando próximo a ela houver áreas de construção/reforma ou atividades geradoras de poeira. Embora os dados evidenciados auxiliem na tomada de decisão para a implementação da assistência de enfermagem a estes pacientes, verificou-se a necessidade de realização de estudos com nível de evidência forte que comprovem ou refutem a efetividade destas medidas. / Hematopoietic stem cell transplantation (HSCT) is a complex procedure related to the occurrence of different complications, including infectious processes deriving from the long period of immunosuppression experienced after the establishment of the conditioning regimen. Countless measures have been used for infection prevention and control, but divergences are observed with regard to their use; evidence-based practice allows professionals to make decisions for practice based on current scientific research results. This integrative literature review aimed to identify and assess evidence available in literature and published in the last 20 years about the use of three infection prevention measures in patients submitted to HSCT during hospitalization: use of high-efficiency air filters, protective isolation and masks. LILACS, PUBMED, CINAHL, EMBASE and the Cochrane Library were used to select the articles. The sample comprised 15 studies, only one of which presented strong evidence (level I), while two presented moderate evidence (levels IV and V) and twelve were studies with weak evidence (levels VI and VII). Ten studies discussed the use of HEPA filters, recommended for patients submitted to allogeneic transplantation during the neutropenia period. It remains controversial whether these filters need to be used for patients submitted to autologous transplant. Nine studies addressed the use of protective isolation and, although some authors report that using this measure can be beneficial when HEPA filters are unavailable, neither the Centers for Disease Control and Prevention (CDC) nor by most of the studies under analysis indicate it any longer. With regard to the use of masks by patients, health professionals or visitors inside HSCT hospitalization units, no studies with strong evidence were found that justify its use. However, it is recommended that CDC recommendations be followed regarding the use of special respirators (like N95 masks) by immunocompromised patients submitted to HSCT when they leave the transplantation unit with a HEPA filter in case of nearby construction/reform areas or activities that generate dust. Although the evidenced data support decision making with a view to nursing care delivery to these patients, research with strong evidence is needed to prove or reject the efficacy of these measures.

Air filtration

Bone marrow transplantation

Dispositivos de proteção respiratória

Filtração do ar

Hematopoietic stem cell transplantation

Infecção

Infection

Isolamento de pacientes

Máscaras

Masks

Patient isolation

Respiratory protective devices

Transplante de medula óssea

Construção e análise funcional de vetores lentivirais de interesse biotecnológico / Construction and functional analysis of lentiviral vectors for biotechnological purposes

Naiara Cristina Pulzi Saito Vedoveli

16 May 2016

Vetores lentivirais são ferramentas fundamentais para modificação celular. Sua utilização ganhou destaque devido à capacidade desses em integrar ao genoma de células que estão ou não em divisão. Grande parte dos vetores desenvolvidos são derivados do genoma do Vírus da Imunodeficiência Humana (HIV-1), portanto, modificações foram necessárias a fim de evitar a formação de Partículas Competentes em Replicação (RCLs) e garantir uma utilização segura. Com as modificações, foram produzidos os vetores lentivirais de terceira geração utilizados atualmente. Esses vetores podem ser usados para expressão constitutiva de genes, produção de proteínas recombinantes, produção de animais transgênicos e terapia gênica. Com isso, torna-se necessário o desenvolvimento de vetores lentivirais para aplicação em pesquisa básica e ensaios clínicos. Dessa forma, o presente estudo teve por objetivo a construção de vetores de expressão lentivirais aplicáveis à: 1- expressão constitutiva de genes de interesse e 2-vetores com promotores específicos para expressão de proteínas em megacariócitos. Esse trabalho descreve a construção desses vetores, sua importância e discute suas possíveis aplicações. As sequências selecionadas para produção dos vetores foram: os genes Runx1C e VkorC1 e os promotores proPF4 e proITGA2b. Todas as sequências encontram-se clonadas em vetor de clonagem e estoques de bactérias com esses vetores congeladas em glicerol foram confeccionados. Para a confecção dos vetores lentivirais, o gene Runx1C foi subclonado no vetor lentiviral base p1054-CIGWS sob controle do promotor forte CMV, enquanto o promotor proITGA2b foi subclonado no vetor base p1054-FVIII, em substituição ao promotor CMV, de forma a controlar a expressão de FVIII. Os dois vetores produzidos apresentam ainda o gene para proteína verde GFP precedida do sítio de ligação do ribossomo IRES, com expressão controlada pelo mesmo promotor interno do vetor. O trabalho possibilitou, portanto, a produção de dois vetores lentivirais bi-cistrônicos: p1054-Runx1C e pL-proITGA2b-FVIII. A construção p1054-Runx1C ainda não foi sequenciada, mas foi confirmada por restrição enzimática e apresenta potencial para aplicação em estudos de diferenciação hematopoética. Já a construção pL-proITGA2b-FVIII foi sequenciada, porém sem confirmação da região de ligação do proITGA2b ao vetor. Reações de PCR e de restrição enzimática confirmaram a ligação e sequenciamento mostrou 67% de similaridade entre a região sequenciada e o promotor ITGA2b depositado no banco de dados. Análise funcional foi realizada através da transfecção desse vetor em células HEK-293T. As células transfectadas apresentaram expressão positiva para GFP e secreção de FVIII no sobrenadante celular, evidenciando que o promotor proITGA2b clonado no vetor encontra-se ativo. Esse vetor apresenta potencial para aplicação em terapia gênica para hemofilias, pois apresenta expressão do fator de coagulação direcionado a megacariócitos e plaquetas, células que estão diretamente relacionadas ao processo de coagulação, representando grandes veículos para secreção desses fatores. Ainda, os dois vetores lentivirais gerados apresentam segurança e eficiência elevadas, pois são vetores de terceira geração auto-inativantes (SIN) e apresentam elementos regulatórios que melhoram o transporte e integração do DNA ao genoma hospedeiro. / Lentiviral vectors are fundamental tools for cell modification that gained prominence due to their ability to integrate the genome of non-dividing cells. Most of developed lentiviral vectors are derived from the genome of Human Immunodeficiency Virus (HIV-1), so modifications were necessary in order to avoid the formation of Competent Replication Particles (RCLs) and ensure safer operations. The modifications led to development of third generation lentiviral vectors currently used. These vectors can be used for constitutive gene expression, production of recombinant protein, production of transgenic animals and gene therapy. It\'s evident the need to develop lentiviral vectors for application in basic research and clinical trials. Thus this study aimed to construct lentiviral expression vectors applicable to: 1- constitutive expression of genes of interest and 2-vectors with specific promoters for expression of proteins in megakaryocytes and platelets. This paper describes the construction of these vectors, their importance and discuss their possible applications. Sequences were selected for production of the vectors: genes Runx1C and VkorC1 and proPF4 and proITGA2b promoters. All four sequences are cloned into cloning vectors and stocks of bacteria with these vectors frozen in glycerol were prepared. Lentiviral vectors were engineered from subcloning the sequence Runx1C into the basic lentiviral vector p1054- CIGWS under control of the strong CMV promoter, and from subcloning proITGA2b promoter into p1054-FVIII basic vector, replacing the CMV promoter in order to control the expression of FVIII. Both vectors exhibit the green fluorescence protein GFP gene preceded by a ribosome binding site IRES under control of vector\'s internal promoter. Therefore, this work resulted in the production of two bi-cistronic lentiviral vectors: p1054-Runx1C and pLproITGA2b-FVIII. The p1054-Runx1C construction has not yet been sequenced, but it was confirmed by digestion and has potential for use in hematopoietic differentiation studies. Though, pL-proITGA2b-FVIII construct was sequenced, but the technique didn\'t allow to confirm the binding region between proITGA2b and the vector. Although PCR reaction and digestion confirmed the construction. Sequence analysis showed 67% similarity between the sequenced region and ITGA2b promoter deposited in the database. Functional analysis was performed by transfection of this vector in HEK-293T cells. The transfected cells showed positive expression of GFP and FVIII secretion in cell supernatant, indicating that the proITGA2b promoter cloned into the vector is active. This vector has potential usage in gene therapy for hemophilia, since it can be used to express coagulation factors in megakaryocytes and platelets and these cells are directly related to the clotting process, representing great vehicles for secretion of these factors. Even more, the two lentiviral vectors generated have higher safety and efficiency, as they are self-inactivating (SIN) third-generation vectors and have regulatory elements that enhance transport and integration of DNA into the host genome.

clonagem molecular

diferenciação hematopoética

HIV-1

ITGA2b

lentivírus

megacariócitos

plaquetas

promotores específicos

Runx1

tecnologia do DNA recombinante

vetores lentivirais

vetores SIN

hematopoietic differentiation

HIV-1

lentiviral vectors

lentivirus

megakaryocytes

platelets

Runx1

SIN vectors

specific promoters, ITGA2b

Alterações bucais em pacientes submetidos ao transplante de células tronco hematopoiéticas: estudo longitudinal / Oral complications in patients undergoing hematopoietic stem cell transplantation: a longitudinal study

Ana Cláudia Luiz

03 May 2012

A boca é local de frequentes complicações relacionadas ao transplante de células tronco hematopoiéticas (TCTH) tais como xerostomia, disgeusia, disfagia, mucosite, infecções oportunistas e doença do enxerto contra hospedeiro (DECH). Sabe-se que estas complicações podem comprometer a qualidade de vida do paciente e interferir na morbidade pós-TCTH. O dentista é o profissional da saúde que deverá intervir no momento correto para tratar e minimizar esses efeitos secundários do TCTH. Para tanto é importante conhecermos o momento em que cada complicação ocorre para que a intervenção seja pronta e eficiente. O objetivo principal deste estudo foi identificar e quantificar as alterações bucais em indivíduos submetidos ao TCTH em cinco momentos consecutivos desde antes do início do condicionamento pré-TCTH até o dia 100 pós-TCTH. Como objetivos secundários buscamos investigar possíveis relações entre a severidade da mucosite oral e a manifestação da DECH com dados demograficos (sexo, idade), com o status de saude bucal (por meio dos índices IHO-S, CPOD, número de dentes cariados) e com a realização de adequação bucal pré-TCTH, e ainda, somente para a DECH, também foi investigada a possível relação entre esta doença com infecção sistêmica por citomegalovírus e com a manifestação de mucosite oral severa. Foram incluídos no estudo 27 indivíduos com doenças hematológicas do Serviço de Transplante de Medula Óssea do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo (HC-FMUSP), com idade 12 anos que receberam TCTH alogênico. Os indivíduos foram examinados em cinco momentos consecutivos. No primeiro momento, pré-TCTH, foi realizada a coleta de índices de saúde bucal e aplicação de questionário sobre o histórico de tratamentos odontológico prévios. Nos momentos de 10, 20, 60 e 100 dias pós-TCTH foram avaliadas as manifestações bucais presentes. A incidência de mucosite oral foi de 82,6% considerando todos os momentos avaliados. Mucosite oral severa, ou seja, graus 3 e 4 (OMS) foi observada em 57,9% dos pacientes avaliados nos momentos 2 e 3. Dez (37%) pacientes apresentaram GVHD em algum órgão, e destes, 8 (80%) apresentaram GVHD de boca. Infecção sistêmica por CMV foi diagnosticada em 6 (22,2%) pacientes. Concluímos que entre as queixas levantadas, dor bucal e disfagia foram as mais referidas. O período de maior incidência das complicações bucais foi nos segundo e terceiro momentos, ou seja, D+10 e D+20, representando deste forma, o período de maior morbidade do tratamento. Não houve associação entre a severidade de mucosite oral e idade, sexo, fonte de células, regime de condicionamento, número de dentes cariados, IHO-S, CPOD e preparo bucal pré-TCTH. Para a DECH a única relação encontrada foi para fonte de células, tendo sido observada menor chance de ocorrer DECH quando a fonte de células foi o sangue periférico. / The mouth is a well-known site of complications of the hematopoietic stem cell transplantation (HSCT) such as dry mouth, dysgeusia, dysphagia, mucositis, opportunistic infections and graft versus host disease (GVDH). It is known that these complications can compromise the patients quality of life and morbidity post-HSCT. The dentist is the health professional who should interfere at the right time to treat and minimize these side effects of HSCT. Thus, it is important to know the time at which each complication occurs to be dynamic and efficient. The main objective of this study was to identify and quantify the oral complications in patients treated with HSCT in five consecutive moments starting before conditioning chemotherapy until day 100 post-HSTC. As secondary objectives we seek to investigate possible relationships between the severity of oral mucositis and the manifestation of GVHD with demographic data (gender, age), with the oral health status (IHO-S, CPOD, number of decayed teeth) and dental treatment previously HSCT, and, only for GVHD, was also investigated the possible relationship between this disease with systemic cytomegalovirus infection and the manifestation of severe oral mucositis. It was included in the study 27 patients with hematologic diseases who were admitted in the Unit of Bone Marrow Transplantation, Hospital of Clinics, Faculty of Medicine, University of Sao Paulo (HC-FMUSP), 12 years old whom received allogeneic HSCT. The subjects were examined in five consecutive moments. At the first moment, before HSCT, the oral health índex evaluation and a questionnaire about history of previous dental treatments were performed. Besides that, 10, 20, 60 and 100 days after HSCT they were evaluated for oral manifestations. Oral mucositis incidence was 82,6% and 57,9% of these patients presented severe mucositis. Ten (37%) patients had GVHD in any organ, and of these, 8 (80%) had oral GVHD. Infection by CMV was diagnosed in 6 (22.2%) patients. We conclude that among the complaints raised, mouth pain and dysphagia were the most mentioned. The period of increased incidence of oral complications was the second and third times (D +10 and +20), representing the increased morbidity period. There was no association between the severity of oral mucositis and age, sex, cell source, conditioning regimen, number of decayed teeth, IHO-S, CPOD and dental treatment pre-HSCT. For GVHD the only relation found was with source of cells, in which, GVHD was less likely to occur when the source of cells was peripheral blood.

Disfagia

Disgeusia

Doença do enxerto contra hospedeiro

Mucosite oral

Transplante alogênico

Xerostomia

Allogeneic transplantation

Dysgeusia

Dysphagia

Graft versus host disease

Hematopoietic stem cell transplantation

Oral mucositis

Xerostomia