Identification et fonction de nouvelles mutations des récepteurs à la thrombopoïétine et à l’érythropoïétine dans les néoplasmes myéloprolifératifs et les érythrocytoses.

EPOR mutations are observed in Primary familial and congenital polycythaemia (PFCP) while MPL mutations are found in myeloproliferative neoplasms (MPN). PFCP is an inherited disorder of erythroid progenitor cells resulting in elevated erythrocyte mass. Several mutations of the erythropoietin receptor (EPOR) gene have been associated with PFCP. They are all leading to a premature STOP codon and the truncation of the cytoplasmic COOH-terminal of EPOR. To examine the role of EPOR mutations in the pathogenesis of PFCP, we studied a new EPOR mutation, c.1300dupC (p.Gln434Profs*11). This mutation induced, in primary cells and cell lines, a major hypersensitivity to EPO. This phenotype was not due to the loss of negative regulation domains or an internalisation default, contrary to the current hypothesis, but rather due to conformational modification inducing the stabilisation of the mutant at the cell membrane.In the second part of this work, an EPOR mutation, Pro488Ser, was studied in a myeloproliferative neoplasms (MPN) family. Only a mild spontaneous STAT5 activation was observed in cell lines. Murine models and/or iPSC will be developed in order to test the hypothesis of a cooperation between EPOR P488S and JAK2 V617F. In the last part of this project, 2 rare MPL mutants, Tyr591Asn and Ser204Pro, identified in 3 triple negative ET patients were functionally studied. A weak gain of function was observed, suggesting that these mutants have to be associated to other genetic abnormalities to develop a phenotype.Le récepteur à l’érythropoïétine (EPOR) peut être muté dans les érythrocytoses congénitales tandis que des mutations de MPL, récepteur à la thrombopoiétine, sont observées dans certains néoplasmes myéloprolifératifs (NMP). L’érythrocytose congénitale touche exclusivement les progéniteurs érythroïdes et se traduit par une polyglobulie isolée. Des mutations d’EPOR sont décrites dans environ 12% des cas. La première partie de cette thèse reposait sur l’étude fonctionnelle d’une mutation d’EPOR, jamais décrite, c.1300dupC (p.Gln434Profs*11). Ce mutant est responsable, dans les cellules primaires et les lignées cellulaires, d’une hypersensibilité majeure à l’EPO qui n’est pas due à la perte de sites de régulation négative du signal ou à un défaut d’internalisation du récepteur, contrairement aux données de la littérature, mais à une stabilisation d’EPOR à la membrane cellulaire par probable changement conformationnel. Dans la seconde partie, un variant d’EPOR Pro488Ser a été étudié au sein d’une famille de NMP. Seule une activation spontanée faible de STAT5 a pu être mise en évidence dans les lignées cellulaires. Des modèles murins et/ou d’iPSC seront développés dans l’hypothèse d’une coopération entre EPOR P488S et JAK2V617F. Enfin, dans la dernière partie de ce travail, nous avons réalisé une étude fonctionnelle de 2 mutations rares de MPL, Tyr591Asn et Ser204Pro, identifiées chez 3 patients TE triples négatifs. Seul un gain de fonction faible a été mis en évidence, suggérant que ces mutations doivent être associées à d’autres anomalies génétiques pour entrainer l’apparition d’un phénotype

Épidémiologie de la maladie d’Alzheimer et des syndromes apparentés

La maladie d’Alzheimer et les syndromes apparentés (c’est-à-dire les autres causes de démences, essentiellement) sont devenus un problème majeur de santé publique en France et sont en passe de devenir, enfin, une priorité, en raison du vieillissement de la population. L’épidémiologie de ces affections est un des éléments essentiels pour la décision en santé publique et pour la connaissance de ces maladies et de leurs déterminants. Selon les estimations les plus raisonnables, il y aurait actuellement en France environ 850 000 cas de maladie d’Alzheimer et syndromes apparentés, et environ 220 000 nouveaux cas par an. Les progrès de la prise en charge font que la durée de la maladie augmente, ainsi que le nombre des malades. En dehors du développement d’un traitement curatif bien peu probable à court terme, seule une politique de prévention devrait permettre de contenir l’accroissement de ce nombre dans un proche avenir. Quatre pistes de prévention sont crédibles : les facteurs de risques cardiovasculaire, notamment l’hypertension artérielle ; la nutrition ; les activités stimulantes et physiques ; l’équilibre affectif et social.Alzheimer’s disease and related disorders (dementia) are a major public health problem due to the number of cases in the general population, the projections for the future, and the consequences of these diseases. We can estimate that about 850 000 cases of dementia were present in France in 2005 and this number will increase to 1 200 000 in 2020 and 2 100 000 in 2040 if the incidence and the duration of the disease did not change. The development of prevention is therefore necessary. Four ways of prevention are credible. The most important is the treatment of vascular risk factors and particularly hypertension. Other ways are nutritionnal factors, stimulating leisure activities and depression

IMRT in the treatment of locally advanced or inoperable NSCLC in the pre-durvalumab era: clinical outcomes and pattern of relapses, experience from the Oscar Lambret Center

BackgroundIntensity-modulated conformal radiotherapy (IMRT) has become the technique of choice for the treatment of locally advanced or inoperable non-small cell lung cancer (NSCLC). Nevertheless, this technique presents dosimetric uncertainties, particularly in treating moving targets such as pulmonary neoplasms. Moreover, it theoretically increases the risk of isolated nodal failure (INF) due to reduced incidental irradiation.ObjectiveThe objective of this study was to evaluate the efficacy and safety of IMRT in patients with inoperable NSCLC and to describe the pattern of relapses.MethodsPatients with locally advanced NSCLC treated with radiotherapy and chemotherapy between 2015 and 2018 at the Oscar Lambret Center were retrospectively included in the study. Overall and progression-free survival were estimated using the Kaplan–Meier method. The cumulative incidence of the different components of relapse was estimated using the Kalbfleisch and Prentice method. Prognostic factors for relapse/death were investigated using the Cox model. A comparison with literature data was performed using a one-sample log-rank test.ResultsSeventy patients were included, and 65 patients (93%) had stage III disease. All the patients received chemotherapy, most frequently with cisplatin and navelbine. The dose received was 66 Gy administered in 33 fractions. The median follow-up and survival were 49.1 and 39.1 months, respectively. A total of 35 deaths and 43 relapses, including 29 with metastatic components, were reported. The overall survival rates at 1 and 2 years were 80.2% (95% confidence interval 68.3%-88.0%) and 67.2% (95% confidence interval 54.2%-77.3%), respectively. Locoregional relapse was observed in 14 patients, including two INF, one of which was located in the lymph node area adjacent to the clinical target volume. Median relapse-free survival was 15.2 months. No variable was statistically associated with the risk of relapse/death in multivariate analysis. Seven patients (10%) experienced grade 3 or higher toxicity.ConclusionThe use of IMRT for locally advanced or inoperable NSCLC led to favorable long-term clinical outcomes. The rate of locoregional relapse, particularly isolated lymph node failure, was low and comparable with that of the three-dimensional radiotherapy series, as was the rate of early and late toxicities

Ethical challenges in preclinical Alzheimer's disease observational studies and trials:Results of the Barcelona summit

AbstractAlzheimer's disease (AD) is among the most significant health care burdens. Disappointing results from clinical trials in late-stage AD persons combined with hopeful results from trials in persons with early-stage suggest that research in the preclinical stage of AD is necessary to define an optimal therapeutic success window. We review the justification for conducting trials in the preclinical stage and highlight novel ethical challenges that arise and are related to determining appropriate risk-benefit ratios and disclosing individuals' biomarker status. We propose that to conduct clinical trials with these participants, we need to improve public understanding of AD using unified vocabulary, resolve the acceptable risk-benefit ratio in asymptomatic participants, and disclose or not biomarker status with attention to study type (observational studies vs clinical trials). Overcoming these challenges will justify clinical trials in preclinical AD at the societal level and aid to the development of societal and legal support for trial participants

What does aducanumab treatment of Alzheimer's disease mean for research on vascular cognitive disorders?

Non peer reviewe

Both common variations and rare non-synonymous substitutions and small insertion/deletions in CLU are associated with increased Alzheimer risk.

BACKGROUND: We have followed-up on the recent genome-wide association (GWA) of the clusterin gene (CLU) with increased risk for Alzheimer disease (AD), by performing an unbiased resequencing of all CLU coding exons and regulatory regions in an extended Flanders-Belgian cohort of Caucasian AD patients and control individuals (n = 1930). Moreover, we have replicated genetic findings by targeted resequencing in independent Caucasian cohorts of French (n = 2182) and Canadian (n = 573) origin and by performing meta-analysis combining our data with previous genetic CLU screenings. RESULTS: In the Flanders-Belgian cohort, we identified significant clustering in exons 5-8 of rare genetic variations leading to non-synonymous substitutions and a 9-bp insertion/deletion affecting the CLU β-chain (p = 0.02). Replicating this observation by targeted resequencing of CLU exons 5-8 in 2 independent Caucasian cohorts of French and Canadian origin identified identical as well as novel non-synonymous substitutions and small insertion/deletions. A meta-analysis, combining the datasets of the 3 cohorts with published CLU sequencing data, confirmed that rare coding variations in the CLU β-chain were significantly enriched in AD patients (OR(MH) = 1.96 [95% CI = 1.18-3.25]; p = 0.009). Single nucleotide polymorphisms (SNPs) association analysis indicated the common AD risk association (GWA SNP rs11136000, p = 0.013) in the 3 combined datasets could not be explained by the presence of the rare coding variations we identified. Further, high-density SNP mapping in the CLU locus mapped the common association signal to a more 5' CLU region. CONCLUSIONS: We identified a new genetic risk association of AD with rare coding CLU variations that is independent of the 5' common association signal identified in the GWA studies. At this stage the role of these coding variations and their likely effect on the β-chain domain and CLU protein functioning remains unclear and requires further studies.RIGHTS : This article is licensed under the BioMed Central licence at http://www.biomedcentral.com/about/license which is similar to the 'Creative Commons Attribution Licence'. In brief you may : copy, distribute, and display the work; make derivative works; or make commercial use of the work - under the following conditions: the original author must be given credit; for any reuse or distribution, it must be made clear to others what the license terms of this work are

The Vascular Impairment of Cognition Classification Consensus Study

H. Jokinen työryhmän jäsenenä.Introduction: Numerous diagnostic criteria have tried to tackle the variability in clinical manifestations and problematic diagnosis of vascular cognitive impairment (VCI) but none have been universally accepted. These criteria have not been readily comparable, impacting on clinical diagnosis rates and in turn prevalence estimates, research, and treatment. Methods: The Vascular Impairment of Cognition Classification Consensus Study (VICCCS) involved participants (81% academic researchers) from 27 countries in an online Delphi consensus study. Participants reviewed previously proposed concepts to develop new guidelines. Results: VICCCS had a mean of 122 (98-153) respondents across the study and a 67% threshold to represent consensus. VICCCS redefined VCI including classification of mild and major forms of VCI and subtypes. It proposes new standardized VCI-associated terminology and future research priorities to address gaps in current knowledge. Discussion: VICCCS proposes a consensus-based updated conceptualization of VCI intended to facilitate standardization in research. (C) 2016 the Alzheimer's Association. Published by Elsevier Inc. All rights reserved.Peer reviewe

Mild cognitive impairment and deficits in instrumental activities of daily living: a systematic review

Introduction: There is a growing body of evidence that subtle deficits in instrumental activities of daily living (IADL) may be present in mild cognitive impairment (MCI). However, it is not clear if there are IADL domains that are consistently affected across patients with MCI. In this systematic review, therefore, we aimed to summarize research results regarding the performance of MCI patients in specific IADL (sub)domains compared with persons who are cognitively normal and/or patients with dementia. Methods: The databases PsycINFO, PubMed and Web of Science were searched for relevant literature in December 2013. Publications from 1999 onward were considered for inclusion. Altogether, 497 articles were retrieved. Reference lists of selected articles were searched for potentially relevant articles. After screening the abstracts of these 497 articles, 37 articles were included in this review. Results: In 35 studies, IADL deficits (such as problems with medication intake, telephone use, keeping appointments, finding things at home and using everyday technology) were documented in patients with MCI. Financial capacity in patients with MCI was affected in the majority of studies. Effect sizes for group differences between patients with MCI and healthy controls were predominantly moderate to large. Performance-based instruments showed slight advantages (in terms of effect sizes) in detecting group differences in IADL functioning between patients with MCI, patients with Alzheimer’s disease and healthy controls. Conclusion: IADL requiring higher neuropsychological functioning seem to be most severely affected in patients with MCI. A reliable identification of such deficits is necessary, as patients with MCI with IADL deficits seem to have a higher risk of converting to dementia than patients with MCI without IADL deficits. The use of assessment tools specifically designed and validated for patients with MCI is therefore strongly recommended. Furthermore, the development of performance-based assessment instruments should be intensified, as they allow a valid and reliable assessment of subtle IADL deficits in MCI, even if a proxy is not available. Another important point to consider when designing new scales is the inclusion of technology-associated IADL. Novel instruments for clinical practice should be time-efficient and easy to administer

A Pragmatic, Data-Driven Method to Determine Cutoffs for CSF Biomarkers of Alzheimer Disease Based on Validation Against PET Imaging

OBJECTIVE: To elaborate a new algorithm to establish a standardized method to define cuff-offs for CSF biomarkers of Alzheimer's disease (AD) by validating the algorithm against CSF classification derived from PET imaging. METHODS: Low and high levels of CSF phosphorylated tau were first identified to establish optimal cut-offs for CSF amyloid-β peptide (Aβ) biomarkers. These Aβ cut-offs were then used to determine cut-offs for CSF tau and phosphorylated tau markers. We compared this algorithm to a reference method, based on tau and amyloid PET imaging status (ADNI study), and then applied the algorithm to 10 large clinical cohorts of patients. RESULTS: A total of 6,922 subjects with CSF biomarkers data were included (mean (SD) age: 70.6 (8.5) years, 51.0% women). In the ADNI study population (n=497), the agreement between classification based on our algorithm and one based on amyloid/tau PET imaging was high with Cohen's kappa coefficient between 0.87 and 0.99. Applying the algorithm to 10 large cohorts of patients (n=6,425), the proportion of persons with AD ranged from 25.9% to 43.5%. DISCUSSION: The proposed novel, pragmatic method to determine CSF biomarkers cut-offs for AD does not require assessment of other biomarkers or assumptions concerning the clinical diagnosis of patients. Use of this standardized algorithm is likely to reduce heterogeneity in AD classification