Literatura académica sobre el tema "Survivants à un cancer de l’enfant"
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Artículos de revistas sobre el tema "Survivants à un cancer de l’enfant"
Racine, Shanelle, Otto Sanchez, Manon Lemonde, Michael Taccone y Fiona Schulte. "Regards sur les séquelles psychosociales des cancers pédiatriques sur le parcours de réintégration des jeunes survivants devenus adultes : étude qualitative exploratoire". Canadian Oncology Nursing Journal 34, n.º 2 (30 de abril de 2024): 187–95. http://dx.doi.org/10.5737/23688076342187.
Texto completoBoulet-Craig, Aubrée, Philippe Robaey, Maja Krajinovic, Caroline Laverdière, Daniel Sinnett, Serge Sultan y Sarah Lippé. "DÉVELOPPEMENT NEUROCOGNITIF ET CÉRÉBRAL DES SURVIVANTS À LONG TERME DE LA LEUCÉMIE LYMPHOBLASTIQUE AIGUË". Revue québécoise de psychologie 37, n.º 2 (7 de junio de 2017): 43–63. http://dx.doi.org/10.7202/1040037ar.
Texto completoAltounian, Janine. "Lors d’une transmission traumatique, l’amour se vit sans tendresse". Le Coq-héron N° 257, n.º 2 (25 de junio de 2024): 129–33. http://dx.doi.org/10.3917/cohe.257.0129.
Texto completoCalvo-Schimmel, Alejandra, S. Newman, K. Sterba, M. Mueller, C. Miaskowski y S. Qanungo. "Besoins non satisfaits en soins de soutien chez les survivants du cancer de la prostate à un stade avancé : exploration par méthodes mixtes". Canadian Oncology Nursing Journal 32, n.º 4 (24 de octubre de 2022): 526–41. http://dx.doi.org/10.5737/23688076324526.
Texto completoChan, Lucy y Georgia Dewart. "Appel à la création de cliniques pour survivants du cancer dirigées par des infirmières praticiennes : un nouveau modèle doit être développé et généralisé en Ontario". Canadian Oncology Nursing Journal 33, n.º 2 (28 de abril de 2023): 269–78. http://dx.doi.org/10.5737/23688076332269.
Texto completoMutsaers, Brittany, Carrie MacDonald-Liska, Gail Larocque, Robin Morash, Lauren Stenason, Cheryl Harris y Sophie Lebel. "Soins de suivi pour les survivants du cancer : évaluation d’une séance d’information". Canadian Oncology Nursing Journal 31, n.º 1 (3 de febrero de 2021): 57–63. http://dx.doi.org/10.5737/236880763115763.
Texto completoAkharzouz, Caroline, Sarah Chauty y Anne-Gaëlle Bodard. "Enfants ayant reçu une irradiation de la région cranio-cervico-faciale : évaluation du besoin de traitement orthodontique". L'Orthodontie Française 84, n.º 2 (30 de mayo de 2013): 157–68. http://dx.doi.org/10.1051/orthodfr/2013047.
Texto completoGalica, Jacqueline, Stephanie Saunders, Kristen Haase y Christine Maheu. "Écrire entre les lignes : analyse secondaire des commentaires non sollicités de survivants du cancer sur la peur d’une récidive". Canadian Oncology Nursing Journal 31, n.º 1 (3 de febrero de 2021): 92–101. http://dx.doi.org/10.5737/2368807631192101.
Texto completoGuibout, C., O. Oberlin, J. Michon, T. D. N’guyen, C. Béhar, M. Sauvage, P. Y. Bondiau, I. Diallo y F. de Vathaire. "P1-9 - Schéma d’actualisation et caractéristiques d’une cohorte française de survivants d’un cancer de l’enfant". Revue d'Épidémiologie et de Santé Publique 54 (agosto de 2006): 62–63. http://dx.doi.org/10.1016/s0398-7620(06)76883-3.
Texto completoHoude, Pascale, Philippe Bergeron y Sébastien Simard. "Les biais attentionnels associés à la peur de la récidive du cancer : Une recension des écrits". Psycause : revue scientifique étudiante de l'École de psychologie de l'Université Laval 14, n.º 1 (31 de octubre de 2024): 6–15. http://dx.doi.org/10.51656/hsa00s21.
Texto completoTesis sobre el tema "Survivants à un cancer de l’enfant"
Ducos, Claire. "Cancers secondaires chez les patients ayant survécu à un cancer durant l’enfance et Identification de variants rares associés". Electronic Thesis or Diss., université Paris-Saclay, 2024. http://www.theses.fr/2024UPASR013.
Texto completoOne in 440 children in France is expected to develop cancer before reaching the age of majority. In recent decades, thanks to improvements in treatment and patient care, the 5- year survival rate for children diagnosed with cancer has reached over 80 %. However, the frequency and diversity of late iatrogenic events have also increased. Second cancers are one of the most significant adverse effects on mortality and morbidity in this growing population. Although the treatment received for pediatric cancer is a well-known risk factor, it is not sufficient to fully explain the risk of secondary cancers, suggesting the existence of a genetic component modulating this risk. Initially, we aimed to better understand the risk factors for one of the most frequent second cancers, thyroid cancer, by investigating the impact of radiation received by lymphoid organs. We have identified an association between this risk and irradiation of the spleen and thymus, two key immune system organs. Then, to better understand the genetic impact on the risk of second cancers, we conducted a systematic review of the literature, compiling all the variants, genes and biological pathways already associated with the risk of various types of second cancers. Finally, a case-control study nested in the French Childhood Cancer Survivors Study (FCCSS) cohort showed that various genes carrying rare variants, such as APOBEC3F and RNASEL, were associated with the risk of second cancers. We also demonstrated an association between the risk of second breast cancer with the FANCM gene, and second thyroid cancer with, notably, the IFI16 and HINFP genes. The results obtained in this thesis provide promising directions that could contribute to the identification of patients at the highest risk of second cancers. Once validated, our results could be applied to adapt the long-term follow-up of survivors and the treatment of pediatric cancer patients to minimize the risk of second cancers in adulthood
Aba, Naïla. "Étude de la survenue de maladies cardiaques à long terme après le traitement du cancer dans l'enfance : Identification de marqueurs biologiques associés". Electronic Thesis or Diss., université Paris-Saclay, 2024. http://www.theses.fr/2024UPASR012.
Texto completoAdvances in pediatric oncology have improved the prognosis of patients treated for childhood or adolescent cancer, with a 5-year survival rate of over 80%. However, these patients are at increased risk of late following cancer treatment. Cardiac diseases are a major concern in this population of survivors who have been exposed to cardiotoxic treatments such as anthracyclines and/or radiation to the heart. The ability of models to predict cardiac diseases from clinical and treatment factors is still insufficient. In similarly treated survivors, interindividual variability in cardiotoxicity susceptibility has been observed, suggesting the existence of genetic factors modulating this susceptibility. In a first part, we studied the risks associated with cardiotoxic treatments on the. occurrence of late cardiac diseases in children treated for cancer within the French Childhood Cancer Study cohort. We highlighted the role of low-volume cardiac irradiation and the interaction between cardiac irradiation and anthracycline administration. In the second part, we report on a systematic of the literature on genetic factors associated with cardiac diseases in survivors of childhood cancer. In the third part, a matched case-control study nested in the FCCSS cohort was conducted to identify transcriptome biomarkers associated with cardiac diseases and heart failure in particular. The NFE2L2 gene was identified, with high expression associated with a reduced risk of these events. In conclusion, the work of this thesis contributes to a better understanding of the factors impacting the risk of late cardiac complications in children treated for cancer. Once validated, our findings could be incorporated into current clinical practice to adapt the therapeutic management of children with cancer, as well as recommendations for their long-term follow-up
Fresneau, Brice. "Analyses pronostiques en oncologie pédiatrique : Identification de facteurs de susceptibilité tumorale ou individuelle à l’efficacité et/ou à la toxicité des traitements anticancéreux utilisés chez l’enfant Investigating the Heterogeneity of Alkylating Agents' Efficacy and Toxicity Between Sexes: A Systematic Review and Meta-Analysis of Randomized Trials Comparing Cyclophosphamide and Ifosfamide (MAIAGE Study) Is Alpha-Fetoprotein Decline a Prognostic Factor of Childhood Non-Seminomatous Germ Cell Tumours? Results of the French TGM95 Study New Insight into Severe Ototoxicity after Childhood Cancer. Is there an Impact of Melphalan and Busulfan? A French Childhood Cancer Survivor Study A Pharmacokinetic and Pharmacogenetic Analysis of Osteosarcoma Patients Treated with High-Dose Methotrexate: Data from the OS2006/Sarcoma-09 Trial". Thesis, université Paris-Saclay, 2020. http://www.theses.fr/2020UPASS034.
Texto completoTherapeutic advances in pediatric oncology have improved survival rates reaching over 80%. In order to increase cure rates and decrease complications and treatment sequelae, international collaborative efforts led to the development of therapeutic trials stratified on major prognostic factors including biological factors. However, treatment adaptation to individual patient characteristics remains marginal.In this thesis, our objective was to better understand how somatic (tumor-related) and constitutional (patient-related) characteristics could modify efficacy and toxicity of anticancer therapies used in pediatric oncology. Several works were performed: 1- Prognostic analysis of tumor markers: assessment of the alpha-foetoprotéine (AFP) decline prognostic value in childhood malignant germ cell tumors; 2- Prognostic analysis of constitutional factors: (i) assessment of the interaction between gender and type of alkylating agents on efficacy and acute toxicity; (ii) assessment of the efficacy and toxicity impact of genetic polymorphisms in patients with osteosarcoma treated with high-dose methotrexate; 3- Risk factors analysis of long-term toxicities: analysis of severe ototoxicity in the French Childhood Cancer Survivors Study (FCCSS)
Malouf, Camille. "Identification et caractérisation des cibles transcriptionnelles de ETV6, un facteur de transcription impliqué dans la leucémie de l’enfant". Thèse, 2012. http://hdl.handle.net/1866/7046.
Texto completoAcute lymphoblastic leukemia (ALL) accounts for approximately 25% of all paediatric cancers. Approximately 85% of ALL cases happen in immature B precursors lymphocytes (pre-B ALL). Pre-B ALL is a sporadic cancer that leads to the massive proliferation of leukemia pre-B lymphocytes in the bone marrow. During the past 30 years, the scientific community has developed efficient therapeutic treatments against paediatric ALL, reaching more than 80% cure rate. However, these treatments lack specificity because of the lack of knowledge regarding the molecular mechanisms involved in the initiation and progression of paediatric pre-B ALL. In other words, we know little about the aetiology of this disease. Approximately 25% of children affected with pre-B ALL carry the chromosomal translocation t(12;21)(p13;q22) involving the ETV6 and AML1 genes. This translocation originates in utero and leads to the expression of the transcriptional chimera ETV6-AML1, which alone is insufficient to trigger the development of pre-B ALL. Therefore, other genetic events would be required to initiate paediatric leukemogenesis. The deletion of the residual allele of ETV6 is frequently observed at the diagnosis of pre-B ALL t(12;21)+. This leads to the complete inactivation of ETV6 in leukemia pre-B lymphocytes. ETV6 is a transcriptional repressor of the Ets family. My research hypothesis is that ETV6 acts as a tumour suppressor gene in paediatric pre-B ALL. The inactivation of ETV6 would lead to the deregulated expression of its transcriptional targets and, consequently, would favour the initiation and progression of paediatric leukemogenesis. Given the fact that only very few ETV6 transcriptional targets are known, I initially performed chromatin immunoprecipitation experiments and luciferase assays that enabled the identification of six novel transcriptional targets: TP53 (p53 and Δ133p53), SPHK1, IL-18, PTGER4 and LUM. The ETV6-mediated transcriptional regulation involves both functional domains: PNT (protein interactions) and ETS (DNA-binding domain). These functional domains facilitate the recognition of consensus EBS sites located in a region close to the basal promoter, a molecular mechanism used according to the target promoter and cellular context. Functional studies using leukemia pre-B lymphocytes were useful to understand the role of the ETV6 transcriptional targets during cell proliferation, induction of apoptosis and cell migration through the CXC12/CXCR4 signalling pathway. These functional studies showed the implication of SPHK1, IL-18 and PTGER4 genes during paediatric leukemogenesis. This study is one of the first to support the role of ETV6 as a tumour suppressor gene in paediatric pre-B ALL. Once ETV6 is inactivated, the increased expression of its transcriptional targets favours the proliferation and survival of leukemia pre-B lymphocytes in the bone marrow. The identification of new genes involved in the development of paediatric pre-B ALL opens new doors to the development of therapeutic treatments with a better specificity toward the aetiology of the disease.
Capítulos de libros sobre el tema "Survivants à un cancer de l’enfant"
Vander Haegen, Marie, Céline Stassart, Caroline Tilkin, Charlotte Grégoire y Cécile Flahault. "Ajustement psychoclinique de l’adulte et de l’enfant dans le champ de l’oncologie". En Pratiques et interventions en psychologie de la santé, 153–64. Editions des archives contemporaines, 2020. http://dx.doi.org/10.17184/eac.3193.
Texto completoLABRELL, Florence, Hugo CÂMARA-COSTA y Marine ERBA. "Stress maternel en cas de tumeurs cérébrales pédiatriques". En Le patient et son entourage, 103–14. Editions des archives contemporaines, 2023. http://dx.doi.org/10.17184/eac.7255.
Texto completoActas de conferencias sobre el tema "Survivants à un cancer de l’enfant"
Akerzoul, N. y S. Chbicheb. "Cartographie des cancers de la cavité orale chez l’enfant". En 66ème Congrès de la SFCO. Les Ulis, France: EDP Sciences, 2020. http://dx.doi.org/10.1051/sfco/20206603005.
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