Structure Function Analysis of Drug Resistance Driver Mutations in Acute Lymphoblastic Leukemia

Carpenter, Zachary Wayne

January 2017

Acute Lymphoblastic Leukemia (ALL) is an aggressive hematologic tumor and is the most common malignancy in children (Horton and Steuber 2014). This disease is characterized by the infiltration of bone marrow by malignant immature lymphoid progenitor cells and is invariably fatal without treatment. Although multi-agent combination chemotherapy is curative in a significant fraction of ALL patients, treatment currently fails in approximately 20% of children and up to 50% of adults with ALL, making relapse and drug resistance the most substantial challenge in the treatment of this disease(Fielding, Richards et al. 2007, Aster and DeAngelo 2013). Understanding what causes treatment failure is of great medical importance as second line therapies also fail in the majority of relapse T-cell ALL (TALL) patients (Fielding, Richards et al. 2007, Aster and DeAngelo 2013). Using next-generation sequencing to compare the genomes of tumors before and after therapy, mutations in gene cytosolic 5’-nucleotidase II (NT5C2) were discovered in 19% of pediatric samples with relapsed T-ALL(Tzoneva, Carpenter et al. 2013). Preliminary structure function analysis and subsequent in vitro experimental nucleotidase activity assays confirmed that these mutations lead to hyperactive NT5C2 protein. Furthermore, NT5C2 mutant proteins conferred resistance to 6-mercaptopurine and 6-thioguanine chemotherapy drugs when expressed in ALL lymphoblasts, suggesting NT5C2 is responsible for the inactivation of nucleoside-analog chemotherapy drugs. In order to assess the ability of these mutations to lead to novel inhibitor schemes, the functional impact of each mutation was analyzed through robust structure function methods. The result of this in silico analysis, is the identification of a potential allosteric regulatory mechanism of negative feedback inhibition never before described. Most notably, the majority of NT5C2 mutations identified have characteristics that suggest they abrogate the function of this proposed mechanism, yielding a novel viable target for the development of allosteric inhibitors specific for constitutively active NT5C2 mutant proteins. Overall these findings support a prominent role for activating mutations in NT5C2 and chemotherapy resistance in ALL, and highlight new avenues for relapsed ALL therapy development in the future.

Lymphoblastic leukemia in children

Pediatric hematology

Bones--Cancer--Treatment

Bone marrow--Cancer

Drug resistance in cancer cells

Lymphoblastic leukemia

Bioinformatics

Oncology

Pharmacology

Emotional and behavioral late effects in pediatric oncology survivors

Garcia, Michael Isaac

27 January 2011

The most common form of childhood cancer is Acute Lymphoblastic Leukemia (ALL). Patients treated for ALL may experience short- and long-term physiological and cognitive effects due to treatment. However, delayed emotional and behavioral effects in pediatric survivors, as well as risk-factors that may make them more susceptible to developing problems with psychological and behavioral functioning are less understood. Studies investigating pediatric survivors have demonstrated that negative emotional and behavioral late effects can and do occur (Hobbie et al., 2000; Buizer et al. 2006; Novakovic et al., 1996; Mulhern, Wasserman, Friedman, & Fairclough, 1989), and it has been purported that survivors experience higher rates of depression, anxiety and low self-esteem (Koocher, O’Malley, Gogan, & Foster, 1980; Kazak, 1994). Anxiety in particular, has been identified as one of the longest lasting psychological sequelae of cancer (Kazak, 1994). Still, the data on long-term psychological sequelae is mixed, with some studies suggesting healthy, long-term, psychological adjustment (Brown et al., 1992; Fritz, Williams & Amylon, 1988; Greenberg, Kazak, & Meadows, 1989). This pilot study attempted to investigate emotional and behavioral late effects of cancer as reported by survivors and their caregivers on the Behavior Assessment System for Children, Second Edition (BASC-2). This study also investigated potential risk factors that made it more likely to develop emotional and behavioral late-effects. This study hypothesized that females, those undergoing high intensity chemotherapy, and those starting chemotherapy at an earlier age, would report significantly more internalizing and externalizing problems. Analysis revealed significant differences in reporting of anxiety, depression, attention and hyperactivity symptoms combined based on the age when treatment started. No other significant findings were uncovered; however, in an effort to provide directions for future research, patterns in the data were examined by comparing overall means on BASC-2 subscales. For example, females reported more hyperactive symptoms than males. In general, individuals who started treatment at younger ages reported more difficulty with emotional and behavioral functioning. Additionally, males and females adaptive behavior fell within normal limits. Overall, no BASC-2 mean scores were in the at-risk or clinically significant range of impairment suggesting adequate emotional, behavioral and adaptive functioning overall. / text

Late effects

Leukemia in children

Cancer in children

Cancer treatment

Pediatric cancer

Pediatric oncology

Depression in cancer patients

Children survivors of cancer

Children with acute leukemia : a comparison of outcomes and cost-effectiveness from allogeneic blood stem cell and bone marrow transplantation.

Lin, Yu-Feng. Lairson, David R., Brenner, Malcolm K., Chan, Wenyaw, Du, Xianglin L.

Unknown Date

Source: Dissertation Abstracts International, Volume: 70-07, Section: B, page: 4063. Adviser: David R. Lairson. Includes bibliographical references.

As mães cuidadoras de crianças em tratamento de Leucemia Linfocítica Aguda (LLA) em uma instituição de Manaus

Fonseca, Itaciara Malcher

29 August 2014

Submitted by Geyciane Santos (geyciane_thamires@hotmail.com) on 2015-06-26T14:04:35Z No. of bitstreams: 1 Dissertação - Itaciara Malcher Fosnseca.pdf: 1382556 bytes, checksum: 5b6d1e57202aa36a6efc0b6b952c7a3f (MD5) / Approved for entry into archive by Divisão de Documentação/BC Biblioteca Central (ddbc@ufam.edu.br) on 2015-06-26T14:10:17Z (GMT) No. of bitstreams: 1 Dissertação - Itaciara Malcher Fosnseca.pdf: 1382556 bytes, checksum: 5b6d1e57202aa36a6efc0b6b952c7a3f (MD5) / Approved for entry into archive by Divisão de Documentação/BC Biblioteca Central (ddbc@ufam.edu.br) on 2015-06-26T14:43:10Z (GMT) No. of bitstreams: 1 Dissertação - Itaciara Malcher Fosnseca.pdf: 1382556 bytes, checksum: 5b6d1e57202aa36a6efc0b6b952c7a3f (MD5) / Made available in DSpace on 2015-06-26T14:43:12Z (GMT). No. of bitstreams: 1 Dissertação - Itaciara Malcher Fosnseca.pdf: 1382556 bytes, checksum: 5b6d1e57202aa36a6efc0b6b952c7a3f (MD5) Previous issue date: 2014-08-29 / Outras / The aim of this study is to analyze the conditions of life of mothers of child caregivers (a) in the treatment of ALL and the work of the social worker at the Foundation. Hemoam. Seeks to identify the determinants of the condition of life of mothers of children caregivers in ALL treatment process; point representations that these mothersin the health -disease (a) child (a) sick (a); identify the contradiction between the condition of life of mothers and carers quality of life of their children (as) bearer of ALL children; and reflect on the work of the social worker in the service provided to these caring mothers of children (a) in the treatment of ALL in the institution in question. The methodology was critical approach to qualitative and quantitative nature of a universe of 80 mothers caregivers withdrew a sample of five mothers livingin Manaus and five mothers living in the countryside. And in the case of social workers, the sample was the same: three professional social service Social Service Department of Hemoam Patient Foundation. Sampling in accordance with the criteria for inclusion and exclusion of research and consent of the participants in this study voluntarily contribute by signing the Informed Consent Form (ICF). Mothers and interview guide was used social workers form along together. The analysis of data collected after theapplication form along with caring mothers and conducting interviews with the social workers the light of knowledge on Public Health was held regarding the virtue of health care and cancer control in Brazil and on the transformation of the context of health care and its impact on the family caregiver and the caregiver health. The data reported indicate that the the condition of life of caregivers mothers reflect negatively on their practice of interfering with careful treatment of the sick child process aswell as in the quality of life of the carer parent due to the overhead imposed by their living conditions and treatment son (a) sick. As for the work of the social worker with this demand, the study identified that there is no specific work done by the social worker with the mothers of child caregivers (a) with ALL, being pointed intervention of professional, starts from the understanding of reality the patient's family as a whole, pointing right abstraction of professional theoretical knowledge in relation to specific practical condition of life of caregivers of mothers carrying children with ALL. We conclude that the problem addressed by this study is relevant and meaningful to generate theoretical knowledge to practical healthcare professionals, particularly social workers, on the condition of life of caregivers mothers of children suffering from ALL and the direct consequences of this condition of life in the treatment and / or cure the sick and compromised quality of life of the carer parent child process. / O objetivo deste estudo é analisar as condições de vida das mães cuidadoras de filho (a) em tratamento de LLA e o trabalho do assistente social na Fundação. Hemoam. Busca identificar os determinantes da condição de vida das mães cuidadoras de crianças em processo tratamento da LLA; apontar as representações que destas mães no processo saúde -doença do (a) filho (a) enfermo (a); identificar a contradição entre a condição de vida das mães cuidadoras e a qualidade de vida de seus filhos (as) portador de LLA infantil; e refletir sobre o trabalho do assistente social no serviço prestado a essas mães cuidadoras de filho (a) em tratamento de LLA na instituição em análise. A metodologia teve abordagem crítica de natureza qualiquantitativa, de um universo de 80 mães cuidadoras retirou-se uma amostra de cinco mães residentes em Manaus e cinco mães residentes no interior. E no caso das assistentes sociais, a amostra fora o mesmo: três profissionais de serviço social do Serviço Social de Atendimento ao Paciente da Fundação Hemoam. Amostragem em conformidade com os critérios de inclusão e exclusão da pesquisa e consentimento de seus participantes em contribuir voluntariamente com este estudo através da assinatura do Termo de Consentimento Livre Esclarecido (TCLE). Foi utilizado formulário junto as mães e roteiro de entrevista junto as assistentes sociais. A análise dos dados coletados após aplicação de formulário junto às mães cuidadoras e a realização de entrevista junto as Assistentes Sociais foi realizada a luz de conhecimentos sobre Saúde Pública, no que concerne, a inerência do cuidado em saúde e o controle do câncer no Brasil e sobre as transformações do contexto do cuidado em saúde e seus reflexos sobre o cuidador familiar e o cuidador de saúde. Os dados informados apontam que o a condição de vida das mães cuidadoras refletem negativamente sobre sua prática de cuidado interferindo no processo de tratamento da criança enferma, bem como, na qualidade de vida da mãe cuidadora devido à sobrecarga imposta pela sua condição de vida e pelo tratamento do filho (a) doente. Quanto ao trabalho do Assistente Social junto a esta demanda, o estudo identificou que não existeum trabalho específico desenvolvido pelo assistente social junto às mães cuidadoras de filho (a) com LLA, sendo apontada intervenção deste profissional, se dá a partir do entendimento da realidade da família do paciente como um todo, o que aponta certa abstração do profissional em relação ao conhecimento teórico-prático específico da condição de vida das mães cuidadoras de filhos portadores de LLA. Conclui-se que, a problemática abordada por este estudo é relevante e significativa ao gerar conhecimento teórico-prático aos profissionais de saúde, particularmente dos assistentes sociais, sobre a condição de vida das mães cuidadoras de filhos portadores de LLA e os reflexos diretos desta condição de vida no processo de tratamento e/ou cura da criança enferma e comprometimento da qualidade de vida da mãe cuidadora.

Mães Cuidadoras

Leucemia em criança

Assistencia social

Caring mothers

Leukemia in children

Social assistance

Rôles de RUNX1 dan la pathogenèse des leucémies aiguës lymphoblastiques à réarrangement ETV6-RUNX1. / Roles of RUNX1 in the pathogenesis of ETV6-RUNX1 acute lymphoblastic leukaemias.

Jakobczyk, Hélène

19 October 2018

Les leucémies aiguës lymphoblastiques de la lignée B (LAL-B) sont les cancers pédiatriques les plus fréquents. Dans ce type de leucémie, l'une des anomalies génétiques les plus fréquentes est la translocation t(12 ;21) aboutissant à la protéine de fusion ETV6-RUNX1. Cette pathologie est décrite comme un modèle à deux « hits ». Le premier, se produit in utero et génère la protéine de fusion. Le second, correspond à l’acquisition d’anomalies génétiques après la naissance. Ces réarrangements génomiques aberrants ont été décrits comme provenant d’une activité anormale de la recombinasse RAG. Notre travail a consisté dans un premier temps à compléter le modèle de leucémogénèse à plusieurs « hits ». En continuant notre étude des LAL B à translocation ETV6-RUNX1, nous nous sommes concentrés sur le rôle de RUNX1, gène dérégulé dans ce type de leucémie.L’ensemble de nos résultats confirme le rôle prépondérant de RUNX1 dans l’hématopoïèse et la leucémogenèse grâce à sa capacité à s’associer à des protéines aux fonctions différentes et grâce à son implication dans la transcription de gènes clé en hématologie. Nos résultats ouvrent donc de nouvelles perspectives dans la compréhension du contrôle de l’activité transcriptionnelle de RUNX1 et dans son rôle dans les hémopathies malignes. / B-cell precursor acute lymphoblastic leukemia (B-ALL) is the most common pediatric cancer. In this type of leukemia, one of the most common genetic abnormalities is the ETV6-RUNX1 rearrangement. This malignancy is described as a two "hits" model. The first event occurs mainly in utero and generates the fusion gene ETV6-RUNX1. The second event consists in the acquisition of additional genetic abnormalities after birth. These aberrant genomic modifications have been described as resulting from abnormal activity of the RAG recombinase. Our work consisted initially in completing the leukemogenesis model. In continuing our study of ETV6-RUNX1 B-ALL, we focused on the role of RUNX1, an upregulated gene in this type of leukemia. All results confirm the predominant role of RUNX1 in hematopoiesis and leukemogenesis thanks to its ability to associate with proteins with different functions and its involvement in the transcription of key genes in hematology. Our results therefore open new perspectives in understanding the control of transcriptional activity of RUNX1 and its role in malignant hematology.

Runx1

Leucémogenèse

Etv6-Runx1

Hématopoïèse

Runx1

Leukemogenesis

Acute lymphoblastic leukemia in children

Etv6-Runx1

Hematopoiesis

The psychosocial functioning in pediatric cancer survivors: The role of neurocognitive abilities.

Begyn, Elizabeth

08 1900

With the increase in survival for children with cancer, part of the focus of current research is aimed towards evaluating how these children are adapting psychosocially. Neurocognitive deficits have been well established. However, there are multiple facets encompassing quality of life, including general mental health, lifestyles and health behaviors, and academic and cognitive functioning. The relationship between neurocognitive and psychosocial functioning has yet to be thoroughly evaluated. The purpose of this study was to investigate the relationship between neurocognitive and psychosocial functioning in survivors of brain tumors and acute lymphoblastic leukemia. Data was collected from existing archival database comprised of patients of the at Cook Children's Medical Center in Texas. The sample consisted of 177 patients between the ages of 3 and 12 who were at least two years post-diagnosis. Measures used included the NEPSY and the Behavioral Assessment for Children. Statistical analyses included a several one-way analysis of variances, an independent samples t-test, a univariate analysis of variance, a hierarchical multiple regression, and odds ratio analyses. Results indicated survivors treated with neurosurgery alone appear to be less at risk for developing behavior problems than other treatment modalities. Also, brain tumor survivors demonstrate more problematic behaviors than survivors of acute lymphoblastic leukemia. Visuospatial functioning, diagnosis, and type of treatment were found to be predictive variables of behavior problems. Attention, and perhaps language, deficits may predispose children to more problems in their behavior. It is concluded that there are other factors affecting behavior in this population that were not accounted for in this analysis. It is recommended for future studies to research the individual clinical scales of the Behavior Assessment System for Children, obtain information from multiple informants, study this relationship longitudinally, and research additional factors that may be influencing the relationship between neurocognitive and psychosocial functioning. This provides evidence of risk factors that should be monitored as the child returns home and to school.

Pediatric cancer survivor

neurocognitive

psychosocial

Cognitive neuroscience.

Behavior disorders in children.

Brain -- Tumors.

Lymphoblastic leukemia in children.

Effets de l’hypoxie sur la régulation de l’expression et la fonction de la tétraspanine CD9 dans les leucémies aiguës lymphoblastiques de l’enfant / Effects of Hypoxia on the Regulation of the Expression and the Function of the CD9 Tetraspanin in Childhood Acute Lymphoblastic Leukemias

Gaudichon, Jérémie

03 October 2018

Les leucémies aiguës lymphoblastiques (LAL) sont le cancer le plus fréquent chez l’enfant et dérivent le plus souvent de précurseurs lymphoïdes B. D’importants progrès thérapeutiques ont permis d’améliorer considérablement le pronostic. Néanmoins, 15 à 20 % des enfants rechutent encore. Ces rechutes peuvent survenir de façon isolée ou combinée dans la moelle osseuse, le site primitif des lymphoblastes, et/ou dans des organes extramédullaires tels que le testicule ou le système nerveux central. Notre équipe a montré que la protéine transmembranaire CD9 jouait un rôle majeur dans la migration des blastes dans ces sites et notamment le testicule, par l’activation de la voie RAC1 en réponse à la stimulation des cellules par le CXCL12. Ici, nous avons mis en évidence qu’un faible niveau d’oxygène, caractéristique commune aux niches médullaire et extramédullaires, régulait positivement l’expression de CD9 aux niveaux transcriptionnel et protéique, via la voie majeure de réponse à l’hypoxie, dépendante du facteur de transcription Hypoxia Inducible Factor 1a (HIF1a). Nous montrons que HIF1a se fixe directement sur le promoteur de CD9 pour induire sa transcription. Nous montrons aussi que la protéine CD9 est essentielle aux propriétés d’adhérence et de migration des blastes dans des conditions de basse oxygénation, et que son action pourrait s’exercer à travers RAC1 comme en normoxie. Nos résultats dans des expériences de xénogreffe à des souris indiquent que la voie HIF1a favorise la dissémination des blastes, possiblement à travers la régulation qu’elle exerce sur CD9. Ainsi, ce travail contribue à mieux comprendre le rôle de CD9 dans la pathogenèse des LAL de l’enfant. / Acute lymphoblastic leukemia (ALL) are the most frequent cancer in children and derive most often from B-cell precursors. Huge therapeutic improvements have allowed to reach high survival rates near 90% at 10 years from diagnosis. However, 15-20% of children still relapse with a significant risk of death. Relapses can occur in bone marrow and/or extramedullary sites such as testis or central nervous system, usually referred as “sanctuary sites”. Our previous work showed that the transmembrane protein CD9 plays a major role in lymphoblasts migration into these sites, especially in testis, through the activation of RAC1 signaling upon blasts stimulation with C-X-C chemokine ligand 12 (CXCl12). Here, we addressed the question of putative common factors shared by bone marrow and extramedullary niches which could upregulate CD9 expression and function. Consequently, we found that low oxygen levels could actually enhance CD9 expression both at mRNA and protein levels. We further determined that Hypoxia Inducible Factor 1a (HIF1a), the master transcription factor involved in hypoxia response, binds directly CD9 promoter to induce its transcription. We also showed that CD9 protein is crucial for leukemic cell adhesion and migration at low oxygen levels, possibly through its action on RAC1 signaling. Mouse xenograft experiments indicate that HIF1a signaling pathway favors ALL cells dissemination, which may involve CD9 as well. The present work increments our understanding of CD9 implication in ALL pathogenesis.

Teneur en oxygène

Protéine CD9

Tétraspanines

Etv6-Runx1

Lymphoblastic leukemia in children

Oxygen content

CD9 protein

Tetraspanins

Etv6-Runx1

Analyse de l'hypothèse de la perturbation des biorythmes par les champs magnétiques d'extrêmement basse fréquence: mécanismes possibles, impact en santé publique, protocoles de mise a l'épreuve / Analysis of the hypothesis of biorhythms disruption by extremely low frequency magnetic fields: possible mechanisms, public health impact, testing protocols

Vanderstraeten, Jacques

17 June 2013

RESUME GENERAL<p><p>Contexte :une association entre exposition prolongée aux champs magnétiques (CM) d’extrêmement basses fréquences (ELF) et risque sanitaire a été établie pour la leucémie infantile (CM 50/60 Hz de l’électricité, RR = 2,0 pour ≥ 0,4 µT d‘intensité moyennée dans le temps) et est suggérée pour le décès par maladie d’Alzheimer (CM 50/60 Hz, CM 16,7 Hz des voies ferrées pour 21 µT d’intensité moyennée dans le temps) et pour certaines hémopathies chez l’adulte (CM 16,7 Hz). Ces associations restent inexpliquées à ce jour. Sur base d’observations animales (effets des CM ELF sur la sécrétion de mélatonine) d’une part, et de la sensibilité magnétique confirmée des cryptochromes (régulateurs des biorythmes) d’autre part, il a été suggéré que ces associations puissent être dues à une perturbation des biorythmes par les CM ELF. Selon les instances internationales, une intensité > 1 mT est requise pour l’existence d’effets biologiques. <p>Objectifs et méthode :sur base d’une revue exhaustive de la littérature et de modèles théoriques reconnus, le présent travail développe certains mécanismes possibles pour un effet perturbateur des biorythmes par les CM ELF. L’impact en santé publique de cette hypothèse est ensuite évalué. Enfin, des protocoles sont proposés pour sa mise à l’épreuve, tenant compte des mécanismes envisagés. <p>Résultats :la possibilité existe d’une interaction des oscillations ELF de l’intensité et/ou de l’orientation du CM (somme vectorielle du CM ELF et du CM terrestre ou CMT) avec les cryptochromes rétiniens. Chez l’animal magnétosensible (dont le rongeur), une perturbation des biorythmes pourrait être consécutive à un mécanisme non spécifique de perturbation sensorielle. Toute observation animale pourrait donc ne pas être extrapolable à l’Homme. Chez ce dernier, une perturbation des biorythmes pourrait être causée par les oscillations de l’intensité du CM (peut- être dès < 100 µT d’intensité de CM ELF). Une telle perturbation pourrait aussi être causée par les variations spatiales de l’intensité du CMT qui existent dans l’environnement résidentiel (proximité de structures métalliques). Par ailleurs, dans l’éventualité de l’existence, chez l’Homme également, d’une sensibilité directionnelle basée sur les cryptochromes rétiniens, les oscillations de l’orientation du CM pourraient alors aussi interférer avec ces cryptochromes (peut-être dès ≤ 10 µT). Dans l’hypothèse où une telle interférence affecte les biorythmes, seules pourraient alors être concernées les oscillations dont l’amplitude atteint plusieurs degrés d’angle. Un tel mécanisme ne pourrait donc s’appliquer à la relation entre CM ELF et leucémie infantile que dans l’éventualité où les intensités les plus élevées (+ 1 à 2 SD) de CM ELF y jouent un rôle. Au cas où l’hypothèse de la perturbation des biorythmes par les CM ELF se voyait confirmée, d’autres troubles de santé seraient alors concernés et d’autres sources de CM seraient en cause, tels les CM statiques d’intensité variable émis par les lignes de transport électrifié. Les paramètres d’exposition considérés devraient inclure l’orientation relative CM ELF/CMT, mais aussi l’intensité locale du CMT (facteur à la fois déterminant et confondant dans la présente hypothèse). L’expérimentation animale devrait investiguer l’expression des clock genes. L’expérimentation humaine devrait investiguer les biorythmes chez l’enfant. Et l’épidémiologie devrait investiguer l’incidence de troubles liés à une perturbation des biorythmes en relation avec l’exposition aux CM ELF ainsi qu’aux variations locales de l’intensité du CMT. <p>Conclusions :malgré les incertitudes persistantes quant aux fonctions précises des cryptochromes de la rétine humaine et quant à l’exactitude des modèles théoriques qui décrivent les interactions entre CM et cryptochromes, certains mécanismes paraissent possibles pour une interaction entre CM ELF et biorythmes. En l’absence persistante d’alternative valide pour l’explication de l’association entre CM ELF et leucémie infantile, l’hypothèse de la perturbation des biorythmes par ces CM paraît devoir être investiguée plus avant, mais en tenant compte des variations locales d’intensité du CMT. <p>Background: An association between prolonged exposure to extremely low frequency (ELF) magnetic fields (MF) and health risk has been established for childhood leukemia (50/60 Hz MF of electricity, RR = 2.0 for ≥ 0.4 µT of time-averaged intensity) and is suggested for death by Alzheimer's disease (50/60 Hz MF, 16.7 Hz MF of railways at 21 µT of time-averaged intensity) and for some hematologic malignancies in adults (16.7 Hz MF). These associations remain unexplained so far. Based on animal studies (effects of ELF MF on melatonin secretion) on the one hand, and on the confirmed magnetic sensitivity of cryptochromes (regulators of biorhythms) on the other hand, it has been suggested that these associations may be due to a disruption of biorhythms by ELF MF. From current data, however, biological effects seem only possible at > 1 mT of intensity.<p>Objectives and methods: on the basis of an exhaustive literature review and with use of recognized theoretical models, this paper develops some possible mechanisms for disruption of biorhythms by ELF MF. The public health impact of this hypothesis is then evaluated. Finally, protocols are proposed for the testing of it, with taking into account the proposed mechanisms.<p>Results: an interaction seems possible between ELF oscillations of the intensity and/or the orientation of the ambient MF (the vector sum of both the ELF MF and the geomagnetic field or GMF) with retinal cryptochromes. In magnetosensitive animals (including rodents), disruption of biorhythms may then be secondary to a non-specific mechanism of sensory disturbance. All animal observation could therefore not be extrapolated to humans. In the latter, on his turn, a disruption of biorhythms may be caused by the oscillations of the MF intensity (perhaps from <100 µT of ELF MF intensity). Such disruption could also be caused by spatial variations of the intensity of the GMF that exist in residential environment (near steel structures). Moreover, in case of the existence in humans (like in animals) of a directional sensitivity based on retinal cryptochromes, then the oscillations of the MF orientation also could interfere with these cryptochromes (perhaps from ≤ 10 µT). In the event that such interference affects biorhythms, only oscillations of several degrees of amplitude would then be concerned. As a consequence, such a mechanism could apply to the relation between ELF MF and childhood leukemia only in the event that the highest MF intensities (Mean + 1-2 SD) also play a role in that relation. In the event the hypothesis of disruption of biorhythms by ELF MF is confirmed, other health problems would be concerned and other kind of MF would be involved, such as the static MF of variable intensity that are emitted by the lines of electrified transport. The considered exposure parameters should include the relative orientation of ELF MF and GMF, but also the local intensity of GMF (both determining factor and confounder in this case). Animal experiments should investigate the expression of clock genes. Human experimentation should investigate biorhythms in children. And epidemiology should investigate the incidence of disorders related to disruption of biorhythms in relation to exposure to ELF MF as well as to local variations in the intensity of the GMF.<p>Conclusions: Despite the persisting uncertainties about the precise functions of retinal cryptochrome as well as about the accuracy of the theoretical models that describe the interactions between MF and cryptochromes, some mechanisms seem possible for an interaction between ELF MF and biorhythms. In the persisting absence of valid alternative explanation for the association between childhood leukemia and ELF MF, the hypothesis of biorhythm disturbance by ELF MF deserves further investigation, however with taking into account local intensity variations of the GMF.<p> / Doctorat en Sciences de la santé publique / info:eu-repo/semantics/nonPublished

Santé publique

Cryptochrome

Biological rhythms

Magnetic fields -- Physiological effect

Leukemia in children

Cryptochrome

Rythmes biologiques

Leucémie chez l'enfant

cryptochromes

leucémie infantile

électricité

mélatonine / chronobiology

melatonin

electricity

childhood leukemia

chronobiologie

Contribution à l'étude de la physiopathologie de l'anémie et de la thrombocytopénie associées à une affection néoplasique chez l'enfant

Corazza, Francis

10 October 2008

L’objectif de notre travail était de déterminer le rôle joué par l’érythropoïétine et la<p>thrombopoïétine, respectivement, dans l’anémie et la thrombocytopénie observées<p>chez des enfants souffrant d’une hémopathie maligne.<p>Par le dosage simultané de la forme soluble du récepteur de la transferrine et de<p>l’érythropoïétine dans le sérum nous avons montré que l’anémie observée chez ces<p>patients est bien la conséquence d’une réduction du nombre de progéniteurs<p>érythropoïétiques (atteinte médullaire centrale) mais que celle-ci n’est pas la<p>conséquence d’une production insuffisante d’érythropoïétine. Nous avons fait la<p>même observation chez des enfants souffrant d’une tumeur solide non<p>hématologique et chez des patients en cours de traitement par chimiothérapie.<p>Chez ces derniers patients, en appliquant un modèle de culture de moelle à long<p>terme, nous avons pu démontrer l’existence d’une altération du microenvironnement<p>médullaire, probablement induite par la chimiothérapie, se<p>traduisant par une réduction de son aptitude à supporter le développement de la<p>lignée érythroïde. Ceci expliquant au moins partiellement l’inadéquation de la<p>réponse érythropoïétique observée chez ces patients en réponse à l’anémie.<p>Dans la dernière partie du travail, nous avons montré que la thrombocytopénie très<p>fréquemment observée chez les patients leucémiques s’accompagne dans la<p>majorité des cas d’une élévation exponentielle de la concentration de<p>thrombopoïétine, excepté dans les cas de leucémies de la lignée myéloïde. Chez ces<p>derniers la concentration de thrombopoïétine est proche des valeurs observées chez<p>des sujets normaux alors qu’elle devrait être 10 à 100 fois plus élevée compte tenu<p>du nombre de plaquettes extrêmement bas. Nous avons pu montrer que ces taux<p>très bas sont la conséquence de la liaison de la thrombopoïétine à un récepteur<p>spécifique et fonctionnel présent à la surface des cellules leucémiques myéloïdes<p>qui, en l’utilisant comme facteur de croissance, (stimulant leur prolifération et<p>retardant leur mort cellulaire) « consomment » la thrombopoïétine présente dans le<p>sérum. / Doctorat en Sciences médicales / info:eu-repo/semantics/nonPublished

Médecine pathologie humaine

Anemia in children -- Pathophysiology

Leukemia in children

Erythropoietin

Thrombopoietin

Leucémie chez l'enfant

Erythropoïétine

Thrombopoïétine

erythropoietin

leukemia

thrombopoietin

cancer

anemia

PI3K in juvenile myelomonocytic leukemia

Goodwin, Charles B.

20 November 2013

Indiana University-Purdue University Indianapolis (IUPUI) / Juvenile Myelomonocytic Leukemia (JMML) is rare, fatal myeloproliferative disease (MPD) affecting young children, and is characterized by expansion of monocyte lineage cells and hypersensitivity to Granulocyte Macrophage-Colony Stimulating Factor (GM-CSF) stimulation. JMML is frequently associated with gain-of-function mutations in the PTPN11 gene, which encodes the protein tyrosine phosphatase, Shp2. Activating Shp2 mutations are known to promote hyperactivation of the Ras-Erk signaling pathway, but Akt is also observed to have enhanced phosphorylation, suggesting a potential role for Phosphatidylinositol-3-Kinase (PI3K)-Akt signaling in mutant Shp2-induced GM-CSF hypersensitivity and leukemogenesis. Having demonstrated that Class IA PI3K is hyperactivated in the presence of mutant Shp2 and contributes to GM-CSF hypersensitivity, I hypothesized the hematopoietic-specific Class IA PI3K catalytic subunit p110δ is a crucial mediator of mutant Shp2-induced PI3K hyperactivation and GM-CSF hypersensitivity in vitro and MPD development in vivo. I crossed gain-of-function mutant Shp2 D61Y inducible knockin mice, which develop fatal MPD, with mice expressing kinase-dead mutant p110δ D910A to evaluate p110δ’s role in mutant Shp2-induced GM-CSF hypersensitivity in vitro and MPD development in vivo. As a comparison, I also crossed Shp2 D61Y inducible knockin mice with mice bearing inducible knockout of the ubiquitously expressed Class IA PI3K catalytic subunit, p110α. I found that genetic interruption of p110δ, but not p110α, significantly reduced GM-CSF-stimulated hyperactivation of both the Ras-Erk and PI3K-Akt signaling pathways, and as a consequence, resulted in reduced GM-CSF-stimulated hyper-proliferation in vitro. Furthermore, I found that mice bearing genetic disruption of p110δ, but not p110α, in the presence of gain-of-function mutant Shp2 D61Y, had on average, smaller spleen sizes, suggesting that loss of p110δ activity reduced MPD severity in vivo. I also investigated the effects of three PI3K inhibitors with high specificity for p110δ, IC87114, GDC-0941, and GS-9820 (formerly known as CAL-120), on mutant Shp2-induced GM-CSF hypersensitivity. These inhibitors with high specificity for p110δ significantly reduced GM-CSF-stimulated hyperactivation of PI3K-Akt and Ras-Erk signaling and reduced GM-CSF-stimulated hyperproliferation in cells expressing gain-of-function Shp2 mutants. Collectively, these findings show that p110δ-dependent PI3K hyperactivation contributes to mutant Shp2-induced GM-CSF hypersensitivity and MPD development, and that p110δ represents a potential novel therapeutic target for JMML.

JMML

PI3K

PTPN11

Shp2

p110 delta

Leukemia in children -- Research

Chronic diseases in children -- Research

Blood -- Diseases -- Diagnosis

Cell lines -- Research

Hematopoiesis

Leukemia -- Genetic aspects

Leukemia -- Etiology

Monocytes -- Research

Human genome -- Research

Protein-tyrosine phosphatase -- Research