Academic literature on the topic 'Maladies rares du développement'
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Journal articles on the topic "Maladies rares du développement"
Isaac, Juliane, Mélodie M. Clerc, François C. Ferré, and Benjamin P. J. Fournier. "Les cellules mésenchymateuses orales, une niche spécifique, du développement à la régénération." médecine/sciences 40, no. 1 (January 2024): 24–29. http://dx.doi.org/10.1051/medsci/2023191.
Full textLévy, Nicolas. "Développement de synergies et partenariats pour les maladies rares : le modèle de la fondation maladies rares." La Presse Médicale 41 (May 2012): S23—S25. http://dx.doi.org/10.1016/j.lpm.2012.02.029.
Full textde La Dure-Molla, Muriel, Céline Gaucher, Nicolas Dupré, Agnès Bloch Zupan, Ariane Berdal, and Catherine Chaussain. "La dent : un marqueur d’anomalies génétiques du développement." médecine/sciences 40, no. 1 (January 2024): 16–23. http://dx.doi.org/10.1051/medsci/2023190.
Full textEl It, Fatima, Laurence Faivre, Christel Thauvin-Robinet, Antonio Vitobello, and Laurence Duplomb. "Des organoïdes cérébraux pour la compréhension et la thérapie des maladies génétiques rares avec troubles neurodéveloppementaux." médecine/sciences 40, no. 8-9 (August 2024): 643–52. http://dx.doi.org/10.1051/medsci/2024100.
Full textNaves, Michel, F. Vallée, and Nicolas Barré. "Observations sur un foyer de dermatophilose sur des bovins Brahman en Guadeloupe. Description, aspects épidémiologiques et économiques." Revue d’élevage et de médecine vétérinaire des pays tropicaux 46, no. 1-2 (January 1, 1993): 297–302. http://dx.doi.org/10.19182/remvt.9382.
Full textTiennot-Herment, Laurence. "Les besoins en recherche et développement pour les maladies rares : le point de vue des malades." médecine/sciences 34 (May 2018): 48–49. http://dx.doi.org/10.1051/medsci/201834s125.
Full textSalamanca, Elisa. "État des lieux du développement de la Banque Nationale de Données Maladies Rares." médecine/sciences 34 (May 2018): 26. http://dx.doi.org/10.1051/medsci/201834s112.
Full textHarambat, Jérôme, and Denis Morin. "Épidémiologie des maladies rénales chroniques en pédiatrie." médecine/sciences 39, no. 3 (March 2023): 209–18. http://dx.doi.org/10.1051/medsci/2023027.
Full textGermain, Lucie, Madeline Voyen, Christine Miro, Philip Böhme, and Phi-Linh Nguyen-Thi. "État des lieux de l’organisation de l’éducation thérapeutique du patient (ETP) à l’hôpital : enquête qualitative auprès d’UTEP de CHU et CHR de France." Education Thérapeutique du Patient - Therapeutic Patient Education 13, no. 2 (2021): 20204. http://dx.doi.org/10.1051/tpe/2021014.
Full textFerry, Antoine. "Quel modèle d’entreprise pour le développement dans les maladies rares ? Intérêt économique versus responsabilité sociétale ?" La Presse Médicale 39, no. 5 (May 2010): 56–58. http://dx.doi.org/10.1016/j.lpm.2010.02.003.
Full textDissertations / Theses on the topic "Maladies rares du développement"
Masson, Aymeric. "Approches multi-omiques des anomalies transcriptionnelles dans les maladies rares du développement." Electronic Thesis or Diss., Bourgogne Franche-Comté, 2024. http://www.theses.fr/2024UBFCI006.
Full textGene expression occurs through the transcription process in the nucleus of eukaryotic cells, which produces RNAs, essential intermediates for protein formation. RNA synthesis and fate are controlled by a complex network of factors, among which are regulatory non-coding DNA sequences that ensure precise spatio-temporal regulation of gene expression and heterogeneous nuclear ribonucleoproteins (hnRNP), able to bind RNA molecules and contributing to their maturation, stability, and localization.The current standard approach for molecular exploration of patients with developmental disorders (DD) and/or intellectual disabilities (ID) uses a combination of chromosomal analysis using DNA microarrays, fragile X testing, exome sequencing, and more recently, genome sequencing to establish a molecular diagnosis. These approaches yield a diagnostic yield of less than 50% for DD/ID. However, the analyses sometimes reveal the presence of variations of uncertain significance in candidate genes not yet implicated in human pathology. Functional tests are then necessary to establish a correct genotype-phenotype correlation. In this way, pathogenic variations have been identified in two candidate genes encoding hnRNPs involved in RNA metabolism: PTBP1 and PTBP2. The aim of this first study is to describe the cellular pathophysiological mechanism related to transcriptional defects causing syndromic (for PTBP1) or non-syndromic (for PTBP2) neurodevelopmental impairment using in vitro and in vivo functional molecular approaches including RNA immunoprecipitation sequencing (RIP-seq) in a cohort of affected individuals.In some cases, genomic analysis identifiy complex structural variations that can disrupt the sequence of a dosage-sensitive gene, alter the activity of an enhancer, or exert position effects on gene expression by altering enhancer/target gene interactions. These molecular communications are facilitated within topological associating domains (TADs), which play an important role in tissue-specific transcriptional regulation. Consequently, any structural variation that reorganizes TADs (fusion, shuffling or even new TAD) can lead to an alteration in gene expression. In this context, the goal of this second research project is to characterize, through high-throughput chromosome conformation capture (Hi-C), the complex rearrangements in patients reorganizing the structure of TADs. Combined with other omic techniques such as long fragment sequencing, transcriptomic or epigenomic analysis, this approach allows the study of the underlying molecular mechanisms on different cellular models derived from affected individuals.These research efforts highlight the physiopathological impact of punctual and structural genetic variations on the transcriptional and post-transcriptional regulatory mechanisms of target genes and pave the way for new biological hypotheses in the context of translational research in human pathology
Garret, Philippine. "Approches bioinformatiques innovantes pour l’analyse de données de séquençage à haut-débit appliquées à l’étude de pathologies génétiques rares avec anomalies du développement." Thesis, Bourgogne Franche-Comté, 2020. http://www.theses.fr/2020UBFCK020.
Full textIn the last years, the advent of exome sequencing (ES) in diagnosis and in research led to the identification of the genetic bases of many Mendelian disorders, allowing many diagnostic wavering cases to be solved. Nevertheless, ES data analysis only leads to the identification of pathogenic or likely pathogenic variants in 30 to 45 % of the undiagnosed cases. Indeed, some limits exist, both at clinical, molecular and bioinformatic levels. The constant evolution of the clinical knowledge, of the number of genes involved in human diseases, and of the clinical-biological correlations, has a significant impact on data analysis, leading to a progressive improvement in diagnostic research. Limits of the current technologies, especially not covered regions, exist, but have been significantly reduced in the recent years. Although genome sequencing will solve some undiagnosed cases, especially in case of non-coding or structural variants, there is still a lot of information to be extracted and analyzed from ES data. Finally, beyond SNV and CNV analyzes, other genetic events can be involved in rare disorders, requiring a bioinformatic development to optimize results.The aim of the project was therefore to improve bioinformatic approaches of ES data analysis in order to identify new molecular mechanisms involved in rare genetic disorders and reduce diagnostic wavering.Several strategies were established. The first one consisted in reanalysing ES data from 80 undiagnosed patients, who were sequenced by the Laboratoire CERBA (CIFRE thesis). It led to the identification of 2 new candidate genes involved in ID, especially OTUD7A gene (article 1). The second strategy was the development of a bioinformatic pipeline in order to extract mitochondrial DNA data from ES data. The mitochondrial genome is not targeted by exome capture kits but can be extracted from off-target data, giving the opportunity to analyze it from preexisting ES data. From the GAD exomes cohort of undiagnosed patients, 2 causal variations were identified in 2 individuals out of 928, affected with neuro-developmental disorder. It thus solved the diagnostic wavering in 0.2 % of patients without diagnosis (article 2). The third strategy consisted in the development of a bioinformatic pipeline to identify mobile elements insertion within ES data, with the expectation that about 0.03 % of the pathogenic variants originate from de novo mobile element insertion. From the GAD exomes cohort of 3322 undiagnosed patients, this step led to the identification of two Alu element insertions in FERMT1 and GRIN2B gene exons (article 3, in process).This PhD permitted to push out some ES limits. Other perspectives exist, and are explored by the GAD team, in connection with the European Solve-RD project
Morkmued, Supawich. "Approches cliniques, précliniques et translationnelles des anomalies bucco-dentaires associées aux maladies rares." Thesis, Strasbourg, 2017. http://www.theses.fr/2017STRAJ040.
Full textThe goal of this thesis is to investigate genetic and environmental factors, both initiating and influencing signaling centers that regulate tooth development and thus producing associated defects. Essentially, my research program utilizes patient-based rare disease phenotypes to create novel mouse models. This study also involved investigating the developmental effects of excess retinoic acid on enamel formation to gain understanding of the mechanisms by which environmental factors can alter enamel development. Other studies investigated enamel and dental anomalies in Ltbp3 and Smoc2 mutant mice. These results advance our understanding of tooth development, and may translate towards optimizing clinical diagnosis, and improving treatment strategies for several human rare diseases. An improved understanding of rare disease models and our testing of clinically relevant approaches using rodent models is a feasible approach to address bone degeneration problems
Hebrard, Maxime. "Conception et développement d’un système d’aide au diagnostic clinique et génétique des rétinopathies pigmentaires." Thesis, Montpellier 1, 2012. http://www.theses.fr/2012MON13519/document.
Full textDiagnosis of retinitis pigmentosa could be difficult regarding both to clinics or molecular issues. Firstly, there are rare diseases, so the prevalence of each pathology in the world population is very low. Secondly, the symptoms of diseases are very similar, so their phenotypic characterization is hard. Moreover, the eye and the visual process are complex and numerous genes' products are implicated. Although retinopathies are mainly monogenic and mendelian inherited diseases, the polymorphisms involved in these diseases are very diverse.These both observations lead us to develop two complementary methodological approaches in a view to better understand the retinopathies.The first approach aims to identify all the genes involved in the diseases using genotyping chips. For this purpose, we studied genetic linkage between single nucleotide variations and pathologies. The second approach leads to the representation of clinical knowledge. An ontological compound was built to make explicit the knowledge involved in the process of diagnosis. The data previously collected by experts were labeled by terms that were organized in a specific thesaurus. The clinic profiles of the patients and diseases were handled as features collections and were compared by similarity calculations. The goal of this work is to build a knowledge-based system for diagnosis
Baala, Lekbir. "Cartographie par autozygotie et identification de gènes de maladies rares dans la population marocaine : application aux génodermatoses et à une anomalie de développement cérébral." Paris 5, 2005. http://www.theses.fr/2005PA05N09S.
Full textRecessive autosomal diseases are a major public health problem in Morocco resulting from a high rate if consanguinity. Autozygosity mapping led to the localization and identification of the genes responsible for 3 rare diseases : anhidrotic ectodermal dysplasia (EDA), and a novel described syndrome with ichthyosis and neonatal sclerosing cholangitis (NISCH), and a syndrome with severe microcephaly, corpus callosum agenesis, craniostenosis and mental retardation. Our study reveals the importance of genetic analysis of rare autosomal recessive diseases in the inbred population
Jabot-Hanin, Fabienne. "Recherche des facteurs génétiques contrôlant la réponse à l’infection par Mycobacterium tuberculosis et le développement d’une tuberculose maladie." Thesis, Sorbonne Paris Cité, 2017. http://www.theses.fr/2017USPCB253/document.
Full textTuberculosis remains a major public health concern, with approximately 10.4 million new cases and 1.8 million deaths due to the disease in 2015 according to WHO. While an estimated one third of the world population is estimated to be infected with Mycobacterium tuberculosis, only about 10% of infected individuals go on to develop a clinical disease. Among them, half will declare the disease in the 2 years following infection, which is generally considered as primary tuberculosis. The other patients will develop the disease more distant in time of primary infection, sometimes several tens of years latter; these are classical pulmonary forms in adults. In humans, the role of genetic factors have been demonstrated in the development of active tuberculosis, in pulmonary forms as in disseminated forms in childhood, et also in the control of M.tuberculosis infection. Nevertheless, most of these genetic factors remain to identify. The first aim of my PhD was to identify genetic factors controlling in vitro interferon-gamma production phenotypes (IGRA) after exposure to M.tuberculosis in a sample of 590 subjects who were in contact with a proven tuberculous patient in Val-de-Marne, Paris suburbs, and in a second time, to try to replicate the findings in a south African familial sample where the tuberculosis is highly endemic. For this purpose, I first performed genome-wide genetic linkage analysis for several quantitative IGRA phenotypes. They led to identify 2 major loci (p<10-4) replicated in South-Africa and linked to the interferon-gamma production induced by live BCG for the first one, and for the second one, by the specific part of the ESAT6 antigen of M.tuberculosis (absent from most of environmental mycobacteria and from BCG), independently of intrinsic ability to respond to mycobacteria. The second step was an association study in the identified linkage regions. A variant associated to the specific ESAT6 phenotype was found (p<10-5), which was significantly contributing to the linkage peak (p<0.001) and previously reported as eQTL of ZXDC gene. The second objective of my PhD was the identification of rare genetic variants underlying the development of pulmonary tuberculosis in infected individuals. To this end, I compared exome data from 120 tuberculous patients and 136 infected individuals without any clinical symptoms. All of them were from Morocco. This study resulted in the lighting of BTNL2 gene, very closed to the HLA region, in which around 10% of patients had a rare loss of function variant whereas the controls didn’t have any
Bouyer, Claire. "Variabilité phénotypique du développement musculaire chez le bovin : analyse fine de la régulation du gène GDF8 codant la myostatine." Thesis, Limoges, 2014. http://www.theses.fr/2014LIMO0054/document.
Full textMyostatin, a member of the TGF- β (Transforming growth factor-beta) superfamily, functions as a negative regulator of skeletal muscle development and growth.Since its discovery in mice in 1997, the myostatin gene has been extensively investigated considering the potential benefits of enhancing muscle growth in clinical and agricultural settings. Loss-of-function mutations which impair myostatin function or those which knockdown myostatin gene expression, result in muscle hypertrophy often referred to as ‘‘double-muscling’’ whereas myostatin overexpression induces profound muscle loss. Here, we identified an unexpected mutation in the myostatin gene that is responsible for increasing muscle mass in Blonde d'Aquitaine cattle breed. In skeletal muscle, the mutant allele was highly expressed leading to an abnormal transcript with a premature termination codon and to residual levels of a correctly spliced transcript. This expression pattern, caused by a leaky intronic mutation with regard to spliceosome, could contribute to the moderate muscle hypertrophy in this cattle breed. This finding is of importance for genetic counseling for meat quantity and quality in livestock production and possibly to manipulate myostatin pre-mRNA in human muscle diseases
Diab, Farah. "Molecular causes and physiopathological consequences of Hallermann-Streiff syndrome." Thesis, Rennes 1, 2019. http://www.theses.fr/2019REN1B042.
Full textHallermann-Streiff syndrome (HSS) is an extremely rare developmental disorder characterized by premature aging, microcephaly, microphtamia, congenital cataracts, beaked nose, and proportionate short stature. Until now, the causative mutations in HSS remain unknown. My PhD work aimed to unravel novel genes in the HSS patients with unknown molecular basis. I revealed four de novo variants in the COL3A1, MYH4, SUCNR1, and UGT2B4 in one HSS patient. In another HSS patient, I detected a de novo mutation in the SCAF1 gene. Except for COL3A1, the identified genes have never been associated any developmental disorder and the variants were predicted as benign by the in silico tools. The null COL3A1 variant however seems most likely to be involved in HSS. Further investigations are required to confirm the pathogenicity of the detected variant in HSS. Recently, trio-based whole exome sequencing (WES) revealed the first candidate variants in the SMC2, SMC4, CHD6, and FAM111A genes in four unrelated HSS patients. My PhD work aimed to investigate the actual involvement of the genes in the etiology of HSS. I demonstrated that the candidate genes co-regulate at the transcriptional and protein levels. Furthermore, I established that most genes dysregulated in HSS are involved in DNA related process including sister chromosome segregation and DNA replication. My findings strongly reinforce the involvement of the genes in the disorder and point to the likelihood of HSS as a chromatin-related disease. Moreover, I revealed that telomere length attrition and impaired cellular proliferation are associated to HSS, consistently with the progeroid features present in the disorder. Altogether, my work revealed the first common features in HSS and shed light onto the pathogenic mechanisms that account for the disease
Grillo, Giacomo. "The ICF syndrome and emergent players in DNA methylation and development : when studying a rare genetic disease sheds new light on an "old" field." Thesis, Sorbonne Paris Cité, 2017. http://www.theses.fr/2017USPCC300/document.
Full textDNA methylation is an essential process for the development of mammals. Its abnormal distribution, particularly at the level of the repeated regions of the genome, is a pathological signature. The discovery of hereditary diseases affecting DNA methylation and the stability of the genome allowed a considerable progress in the identification of their actors and mechanisms. We chose to study the ICF (Immunodeficiency, Centromeric Instability and Facial Abnormalities) syndrome, the first genetic disorder identified with defects in the distribution of DNA methylation, linked to chromosomal instability. When I started my PhD, mutations in two genes had been described to cause the ICF syndrome: DNMT3B and ZBTB24. However, the genetic origin of a subset of ICF patients remained unknown. We identified mutations in CDCA7 and HELLS as causative of the ICF syndrome. I showed that their loss of function in somatic cells results in the loss of DNA methylation at centromeric repeats, strongly suggestive of a role DNA methylation maintenance. Hence, the study of the aetiology of a genetic disease provided new candidate “guardians” of DNA repeats and genome stability, with virtually unknown functions but with exciting potential roles in the DNA methylation machinery and in development. During my PhD, I established methylation maps in ICF patients cells to identify common and distinct targets of these factors, as well as their genomic and epigenomic characteristics. In contrast to DNMT3B mutations, those in ZBTB24, CDCA7 and HELLS affect methylation at CpG-poor regions in intergenic genomic locations and at interspersed DNA repeats, and more generally, at genomic locations with heterochromatic features. Their integrity is required for the methylated status of coding and non-coding clusters of genes, some of which are expressed in a monoallelic manner. To better characterize the role of ZBTB24 in development and DNA methylation pathways, we generated a mouse model carrying mutations in ZBTB24. We showed that ZBTB24 is essential for early development, while it seemed to be dispensable for in vitro differentiation of murine ES cells. We implicated ZBTB24 in the establishment of DNA methylation at DNA repeats, both in tandem or interspersed, in differentiating ES cells. Interestingly, ZBTB24 seems to be also implicated in the establishment of the repressive mark H3K9me3 suggesting that ZBTB24 may indirectly control DNA methylation through an interplay with histone marks. As a whole, our work sheds light on how DNA methylation and heterochromatin marks are established and maintained at unique genes and DNA repeats, and provides new actors and mechanisms to consider in studies of the maintenance of genome stability
Bolze, Alexandre. "La découverte de l’origine génétique de l’asplénie congénitale isolée chez l’homme." Thesis, Paris 5, 2012. http://www.theses.fr/2012PA05T024/document.
Full textIsolated congenital asplenia (ICA) is a rare primary immunodeficiency, first described in 1956, thattypically manifests in childhood with sudden, life-threatening, invasive bacterial disease. Patients withICA do not display any other overt developmental anomalies. The genetic etiology of ICA has remainedelusive. I hypothesized that ICA results from single-gene inborn errors of spleen development. I aimedto decipher the molecular genetic basis of ICA by pursuing a genome-wide approach, based on thesequencing of the whole-exome and the detection of copy number variations in all patients of ourcohort. I found that heterozygous mutations in RPSA, ribosomal protein SA, were present in more thanhalf of ICA patients (19/33). I then showed that haploinsufficiency of RPSA led to ICA in one kindredat least. RPSA is a protein involved in pre-rRNA processing and is an integral part of the ribosome. Thechallenge is, now, to understand the pathogenesis of the disease. How does a mutation in a ubiquitousand highly expressed gene lead to a spleen specific phenotype? This discovery will set the basis for abroader understanding of the development of the spleen in humans and the function of a ribosomalprotein. This discovery will also be beneficial to the families of patients with ICA, guiding geneticcounseling. It will lead to prevention of infections in newborns with mutations in RPSA. Finally themethod we used to analyze the exomes of the ICA cohort will be useful to discover the genetic etiologyof other genetic diseases
Books on the topic "Maladies rares du développement"
Leone, Marc. Maladies rares en réanimation. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0.
Full textClaessens, Yann-Erick, and Luc Mouthon. Maladies rares en médecine d’urgence. Paris: Springer Paris, 2013. http://dx.doi.org/10.1007/978-2-8178-0350-0.
Full textFrancis, Gold, ed. Développement et maladies de l'enfant. Paris: Masson, 1986.
Find full textGuignard, Jean-Pierre. Développement rénal et programmation des maladies cardiovasculaires. Paris: Elsevier, 2005.
Find full textBroca, Alain de. Le développement de l'enfant : aspects neuro-psycho-sensoriels. 3rd ed. Paris: Masson, 2006.
Find full textJaeger, Claude. Le développement au sens de Schumpeter: Une mise en perspective de deux textes rares. Paris: L'Harmattan, 2013.
Find full textHadjouis, Djillali. Les populations médiévales du Val-de-Marne: Dysharmonies cranio-faciales, maladies bucco-dentaires et anomalies du développement dentaire au cours du Moyen Age. Paris: Artcom', 1999.
Find full text1958-, Anderson Vicki, ed. Developmental neuropsychology: A clinical approach. Hove, East Sussex: Psychology, 2001.
Find full textFischer, Gustave-Nicolas. L'expérience du malade: L'épreuve intime. Paris: Dunod, 2008.
Find full textBenkimoun, Paul. Morts sans ordonnance. Paris: Hachette Littératures, 2002.
Find full textBook chapters on the topic "Maladies rares du développement"
Paugam-Burtz, Catherine, and Emmanuel Weiss. "Maladies hépatiques rares." In Maladies rares en réanimation, 289–94. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_26.
Full textTextoris, Julien, and Marc Leone. "Aspects génétiques des maladies rares." In Maladies rares en réanimation, 11–20. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_1.
Full textPotie, Frédéric, Marlène Knezynski, and Olivier Riou. "Dengue en réanimation." In Maladies rares en réanimation, 105–14. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_10.
Full textRiou, Olivier, Marlène Knezynski, and Frédéric Potie. "Chikungunya en réanimation." In Maladies rares en réanimation, 115–19. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_11.
Full textBellefleur, Jean-Pierre, and Jean-Philippe Chippaux. "Envenimations ophidiennes." In Maladies rares en réanimation, 121–31. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_12.
Full textForel, Jean-Marie, Renaud Lepaul-Ercole, Laurent Chiche, and Christophe Guervilly. "Fibroses pulmonaires." In Maladies rares en réanimation, 135–46. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_13.
Full textSantelli, Dominique, Laurent Zieleskiewicz, and Claude Martin. "Myasthénie en réanimation." In Maladies rares en réanimation, 149–66. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_14.
Full textDemory, Didier, Stéphane Donati, and Jean-Michel Arnal. "Sclérose latérale amyotrophique." In Maladies rares en réanimation, 167–76. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_15.
Full textVelly, Lionel, and Nicolas Bruder. "Réanimation et maladie de Parkinson." In Maladies rares en réanimation, 177–90. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_16.
Full textChiche, Laurent, Christophe Guervilly, Bernard Allaouchiche, and Jérôme Allardet-Servent. "Maladies de système en réanimation." In Maladies rares en réanimation, 193–204. Paris: Springer Paris, 2010. http://dx.doi.org/10.1007/978-2-287-99070-0_17.
Full textConference papers on the topic "Maladies rares du développement"
Fricain, M., P. Weidmann, Y. Roche, and J. C. Fricain. "Vitiligo labial associé à une pathomimie." In 66ème Congrès de la SFCO. Les Ulis, France: EDP Sciences, 2020. http://dx.doi.org/10.1051/sfco/20206603003.
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