📇 Rhumatologue · SOTTEVILLE LES ROUEN · (76) · Libéral
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2 raisons identifiées
Praticien-chercheur
13 articles scientifiques publiés — formation continue solide
Délais de RDV courts dans la région
119.2 rhumatos / 100 000 hab. — département bien doté
✨ Génération du profil synthétique IA en cours…
CABINET DU DR DAVID LEJEUNE
1 E RUE DE TRIANON, 76300 SOTTEVILLE LES ROUEN
Secteur de conventionnement non disponible (médecin hospitalier ou non présent dans l'Annuaire santé CNAM des libéraux conventionnés).
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Lien Doctolib = recherche Google site:doctolib.fr (le 1er résultat est presque toujours le profil correct s'il existe).
Journal of medical genetics · 2013
Background PTEN hamartoma tumour syndrome (PHTS) encompasses several clinical syndromes with germline mutations in the PTEN tumour suppressor gene, including Cowden syndrome which is characterised by an increased risk of breast and thyroid cancers. Because PHTS is rare, data regarding cancer risks and genotype–phenotype correlations are limited. The objective of this study was to better define cancer risks in this syndrome with respect to the type and location of PTEN mutations. Methods 154 PHTS individuals with a deleterious germline PTEN mutation were recruited from the activity of the Institut Bergonié genetic laboratory. Detailed phenotypic information was obtained for 146 of them. Age and sex adjusted standardised incidence ratio (SIR) calculations, cumulative cancer risk estimations, and genotype–phenotype analyses were performed. Results Elevated SIRs were found mainly for female breast cancer (39.1, 95% CI 24.8 to 58.6), thyroid cancer in women (43.2, 95% CI 19.7 to 82.1) and in men (199.5, 95% CI 106.39 to 342.03), melanoma in women (28.3, 95% CI 7.6 to 35.4) and in men (39.4, 95% CI 10.6 to 100.9), and endometrial cancer (48.7, 95% CI 9.8 to 142.3). Cumulative cancer risks at age 70 were 85% (95% CI 70% to 95%) for any cancer, 77% (95% CI 59% to 91%) for female breast cancer, and 38% (95% CI 25% to 56%) for thyroid cancer. The risk of cancer was two times greater in women with PHTS than in men with PHTS (p<0.05). Conclusions This study shows a considerably high cumulative risk of cancer for patients with PHTS, mainly in women without clear genotype–phenotype correlation for this cancer risk. New recommendations for the management of PHTS patients are proposed.
Journal of medical genetics · 2017
Oral–facial–digital syndromes (OFDS) gather rare genetic disorders characterised by facial, oral and digital abnormalities associated with a wide range of additional features (polycystic kidney disease, cerebral malformations and several others) to delineate a growing list of OFDS subtypes. The most frequent, OFD type I, is caused by a heterozygous mutation in the OFD1 gene encoding a centrosomal protein. The wide clinical heterogeneity of OFDS suggests the involvement of other ciliary genes. For 15 years, we have aimed to identify the molecular bases of OFDS. This effort has been greatly helped by the recent development of whole-exome sequencing (WES). Here, we present all our published and unpublished results for WES in 24 cases with OFDS. We identified causal variants in five new genes (C2CD3, TMEM107, INTU, KIAA0753 and IFT57) and related the clinical spectrum of four genes in other ciliopathies (C5orf42, TMEM138, TMEM231 and WDPCP) to OFDS. Mutations were also detected in two genes previously implicated in OFDS. Functional studies revealed the involvement of centriole elongation, transition zone and intraflagellar transport defects in OFDS, thus characterising three ciliary protein modules: the complex KIAA0753-FOPNL-OFD1, a regulator of centriole elongation; the Meckel-Gruber syndrome module, a major component of the transition zone; and the CPLANE complex necessary for IFT-A assembly. OFDS now appear to be a distinct subgroup of ciliopathies with wide heterogeneity, which makes the initial classification obsolete. A clinical classification restricted to the three frequent/well-delineated subtypes could be proposed, and for patients who do not fit one of these three main subtypes, a further classification could be based on the genotype.
Journal of medical genetics · 2019
Background Subtelomeres are variable regions between telomeres and chromosomal-specific regions. One of the most studied pathologies linked to subtelomeric imbalance is facioscapulohumeral dystrophy (FSHD). In most cases, this disease involves shortening of an array of D4Z4 macrosatellite elements at the 4q35 locus. The disease also segregates with a specific A-type haplotype containing a degenerated polyadenylation signal distal to the last repeat followed by a repetitive array of β-satellite elements. This classification applies to most patients with FSHD. A subset of patients called FSHD2 escapes this definition and carries a mutation in the SMCHD1 gene. We also recently described patients carrying a complex rearrangement consisting of a cis-duplication of the distal 4q35 locus identified by molecular combing. Methods Using this high-resolution technology, we further investigated the organisation of the 4q35 region linked to the disease and the 10q26 locus presenting with 98% of homology in controls and patients. Results Our analyses reveal a broad variability in size of the different elements composing these loci highlighting the complexity of these subtelomeres and the difficulty for genomic assembly. Out of the 1029 DNA samples analysed in our centre in the last 7 years, we also identified 54 cases clinically diagnosed with FSHD carrying complex genotypes. This includes mosaic patients, patients with deletions of the proximal 4q region and 23 cases with an atypical chromosome 10 pattern, infrequently found in the control population and never reported before. Conclusion Overall, this work underlines the complexity of these loci challenging the diagnosis and genetic counselling for this disease.
Source PubMed · Recherche par auteur (homonymes possibles, vérifier l'affiliation).
Gut · 2025 · Journal Article
Hollenbach M, Heise C, Abou-Ali E, Gulla A, et al.
Therapie · 2021 · Letter
Chappuy M, Peyrat M, Lejeune O, Duvernay N, et al.
Journal of medical genetics · 2019 · Journal Article
Nguyen K, Broucqsault N, Chaix C, Roche S, et al.
Clinical genetics · 2018 · Case Reports
Mehawej C, Hoischen A, Farah RA, Marey I, et al.
Journal of medical genetics · 2017 · Journal Article
Bruel AL, Franco B, Duffourd Y, Thevenon J, et al.
Journal of medical genetics · 2013 · Journal Article
Thauvin-Robinet C, Munck A, Huet F, de Becdelièvre A, et al.
Journal of medical genetics · 2013 · Journal Article
Bubien V, Bonnet F, Brouste V, Hoppe S, et al.
Acta clinica Belgica · 1984 · Case Reports
Buysschaert M, Lejeune D, Esselinckx W, Lebacq EG
The American journal of geriatric psychiatry : official journal of the American Association for Geriatric Psychiatry · 2025 · Journal Article
Desmidt T, Santiago-Ribeiro MJ, Robert G, Blanc F, et al.
Neuro-Chirurgie · 2020 · Journal Article
Proust F, Bracard S, Thines L, Pelissou-Guyotat I, et al.
Neuro-Chirurgie · 2010 · Case Reports
Proust F, Bracard S, Thines L, Leclerc X, et al.
Neuro-Chirurgie · 2018 · Journal Article
Proust F, Bracard S, Lejeune JP, Thines L, et al.
Neuro-Chirurgie · 2010 · Case Reports
Proust F, Bracard S, Thines L, Leclerc X, et al.
Microorganisms · 2023 · Journal Article
Dulermo T, Lejeune C, Aybeke E, Abreu S, et al.
Neuro-Chirurgie · 2018 · Journal Article
Proust F, Bracard S, Lejeune JP, Thines L, et al.
The American journal of geriatric psychiatry : official journal of the American Association for Geriatric Psychiatry · 2025 · Journal Article
Desmidt T, Santiago-Ribeiro MJ, Robert G, Blanc F, et al.
Source : DataCite — DOIs pour datasets, logiciels, protocoles, registres patient. Hors articles (déjà couverts).