RÉSUMÉ
In a changing environment, there is an increasing interest to monitor ecosystems to understand their responses to environmental change. Seagrass meadows are highly important ecosystems that are under constant pressure from human activities and climate impacts, with marked declines observed worldwide. Despite increasing efforts, monitoring of multispecific tropical seagrass meadows is scarce, particularly in low-income regions. Based on data from a monitoring programme in a marine protected area in Zanzibar (Tanzania), we assessed temporal changes in seagrass cover and species composition during a 10-year period in relation to local variability in environmental variables. We observed a strong, gradual decline in seagrass cover and changes in species composition, followed by a period of recovery. However, the timing and length of these temporal patterns varied in space (between transects). Multiple environmental variables-cloud cover, temperature, storm occurrence, sunspot activity, and tidal amplitude and height-influenced seagrass cover, although only to a minor extent, suggesting that the monitored seagrass meadow may be influenced by other unmeasured factors (e.g. water currents and sediment movement). Our results show that seagrass meadows can be highly dynamic at small (10-50 m) spatial scales, even in the absence of major local anthropogenic impacts. Our findings suggest that high-resolution monitoring programmes can be highly valuable for the detection of temporal changes in multispecific seagrass meadows; however, to understand the causes of change, there is a need of long-term (> 10 years) data series that include direct measurements of environmental variables and extreme events.
Sujet(s)
Alismatidae/physiologie , Changement climatique , Surveillance de l'environnement , Eau de mer , Écosystème , Humains , Tanzanie , Climat tropicalRÉSUMÉ
The treatment of obesity is an often studied subject. Although reductions in weight and improvements in cardiometabolic risk factors are important aims of obesity treatment, improvements in quality of life and eating behaviour are also relevant outcomes. In this practice-based study, we evaluated an 18-month commercial multidisciplinary obesity treatment programme and report on treatment results for weight, cardiometabolic risk factors, eating behaviour and quality of life. From a local commercial obesity treatment centre, 426 subjects (65% female; 45.4 ± 12.2 years; body mass index 40.0 ± 6.6 kg m(-2)) were recruited. Measurements of body weight, height, body composition, waist circumference and blood pressure were scheduled at baseline and every 3 months, whereas fasting blood collections were scheduled at baseline and every 6 months. At the same time points, participants were asked to fill in questionnaires on dietary intake, eating behaviour and quality of life. After 18 months of treatment programme, average weight change [mean (95% confidence interval)] was -10.9 kg (-14.8 to -7.0; P < 0.001) for the completers (n = 181) and -10.8 kg (-14.2 to -7.4; P < 0.001) for the intention-to-treat population (n = 426). Waist circumference (mean ± standard error of the mean) (-0.13 ± 0.01 cm; P < 0.001), fat mass (-7.8 ± 1.3 kg; P < 0.001) systolic (-11.4 ± 2.0; P < 0.001) and diastolic (-7.0 ± 1.3; P < 0.001) blood pressure, triglycerides (-0.4 ± 0.1; P = 0.004) and plasma glucose (-0.6 ± 0.2; P = 0.001) were significantly reduced. The PCS scale of the SF-36 and all three scales of the three-factor eating questionnaire improved significantly over the 18-month treatment period. All collected data in this study provide evidence that a multidisciplinary treatment programme based on lifestyle modification results in significant weight loss and improvements in cardiometabolic risk factors, quality of life and eating behaviour.
Sujet(s)
Obésité/thérapie , Évaluation de programme , Adulte , Glycémie/métabolisme , Indice de masse corporelle , Comportement alimentaire , Femelle , Humains , Études longitudinales , Mâle , Adulte d'âge moyen , Obésité/économie , Obésité/métabolisme , Obésité/physiopathologie , Obésité/psychologie , Qualité de vie , Tour de taille , Perte de poids , Jeune adulteRÉSUMÉ
BACKGROUND: A high dietary protein (P) content and low glycemic index (LGI) have been suggested to be beneficial for weight management, but long-term studies are scarce. OBJECTIVE: The DIOGENES randomized clinical trial investigated the effect of P and GI on weight loss maintenance in overweight or obese adults in eight centers across Europe. This study reports the 1-year results in two of the centers that extended the intervention to 1 year. METHOD: After an 8-week low-calorie diet (LCD), 256 adults (body mass index >27 kg m(-)(2)) were randomized to five ad libitum diets for 12 months: high P/LGI (HP/LGI), HP/high GI (HP/HGI), low P/LGI (LP/LGI), LP/HGI and a control diet. During the first 6 months, foods were provided for free through a shop system and during the whole 12-month period, subjects received guidance by a dietician. Primary outcome variable was the change in body weight over the 12-month intervention period. RESULTS: During the LCD period, subjects lost 11.2 (10.8, 12.0) kg (mean (95% confidence interval (CI))). Average weight regain over the 12-month intervention period was 3.9 (95% CI 3.0-4.8) kg. Subjects on the HP diets regained less weight than subjects on the LP diets. The difference in weight regain after 1 year was 2.0 (0.4, 3.6) kg (P=0.017) (completers analysis, N=139) or 2.8 (1.4, 4.1) kg (P<0.001) (intention-to-treat analysis, N=256). No consistent effect of GI on weight regain was found. There were no clinically relevant differences in changes in cardiometabolic risk factors among diet groups. CONCLUSION: A higher protein content of an ad libitum diet improves weight loss maintenance in overweight and obese adults over 12 months.
Sujet(s)
Régime amaigrissant , Protéines alimentaires/administration et posologie , Indice glycémique , Obésité/thérapie , Prise de poids , Perte de poids , , Adulte , Indice de masse corporelle , Poids , Restriction calorique , Régime pauvre en protéines , Hydrates de carbone alimentaires/administration et posologie , Ration calorique , Europe/épidémiologie , Famille , Femelle , Hyperglycémie provoquée , Humains , Mâle , Enquêtes nutritionnelles , Obésité/prévention et contrôle , Observance par le patient , Facteurs temps , Tour de tailleRÉSUMÉ
INTRODUCTION Sunitinib, an oral, multitargeted receptor tyrosine kinase inhibitor, delays disease progression, with a median overall survival (OS) of more than 2 years, improves quality of life and is becoming the first-line standard of care for metastatic renal carcinoma (mRCC). PURPOSE To assess the economic value of sunitinib as fi rst-line therapy in mRCC within the Spanish healthcare system. METHODS An adapted Markov model with a 10-year time horizon was used to analyse the cost effectiveness of sunitinib vs. sorafenib (SFN) and bevacizumab/interferon-α (BEV/IFN) as first-line mRCC therapy from the Spanish third-party payer perspective. Progression-free survival (PFS) and OS data from sunitinib, SFN and BEV/IFN pivotal trials were extrapolated to project survival and costs in 6-week cycles. Results, in progression-free life-years (PFLY), life years (LY) and quality-adjusted life-years (QALY) gained, expressed as incremental cost-effectiveness ratios (ICER) with costs and benefits discounted annually at 3%, were obtained using deterministic and probabilistic analyses. RESULTS Sunitinib was more effective and less costly than both SFN (gains of 0.52 PFLY, 0.16 LY, 0.17 QALY) and BEV/IFN (gains of 0.19 PFLY, 0.23 LY, 0.16 QALY) with average cost savings/patients of 1,124 and 23,218, respectively. Using a willingness-to-pay (WTP) threshold of 50,000/QALY, sunitinib achieved an incremental net benefit (INB) of 9,717 and 31,211 compared with SFN and BEV/IFN, respectively. At this WTP, the probability of sunitinib providing the highest INB was 75%. CONCLUSION Our analysis suggests that sunitinib is a costeffective alternative to other targeted therapies as first-line mRCC therapy in the Spanish healthcare setting.
Sujet(s)
Inhibiteurs de l'angiogenèse/économie , Néphrocarcinome/économie , Indoles/économie , Tumeurs du rein/économie , Modèles économiques , Pyrroles/économie , Inhibiteurs de l'angiogenèse/usage thérapeutique , Antiviraux/économie , Antiviraux/usage thérapeutique , Benzènesulfonates/économie , Benzènesulfonates/usage thérapeutique , Néphrocarcinome/traitement médicamenteux , Néphrocarcinome/secondaire , Essais cliniques comme sujet , Analyse coût-bénéfice , Humains , Indoles/usage thérapeutique , Interféron alpha/économie , Interféron alpha/usage thérapeutique , Tumeurs du rein/traitement médicamenteux , Tumeurs du rein/anatomopathologie , Chaines de Markov , Nicotinamide/analogues et dérivés , Phénylurées , Inhibiteurs de protéines kinases/économie , Inhibiteurs de protéines kinases/usage thérapeutique , Pyridines/économie , Pyridines/usage thérapeutique , Pyrroles/usage thérapeutique , Années de vie ajustées sur la qualité , Sorafénib , SunitinibRÉSUMÉ
INTRODUCTION Sunitinib, an oral, multitargeted receptor tyrosine kinase inhibitor, delays disease progression, with a median overall survival (OS) of more than 2 years, improves quality of life and is becoming the first-line standard of care for metastatic renal carcinoma (mRCC). PURPOSE To assess the economic value of sunitinib as fi rst-line therapy in mRCC within the Spanish healthcare system. METHODS An adapted Markov model with a 10-year time horizon was used to analyse the cost effectiveness of sunitinib vs. sorafenib (SFN) and bevacizumab/interferon-α (BEV/IFN) as first-line mRCC therapy from the Spanish third-party payer perspective. Progression-free survival (PFS) and OS data from sunitinib, SFN and BEV/IFN pivotal trials were extrapolated to project survival and costs in 6-week cycles. Results, in progression-free life-years (PFLY), life years (LY) and quality-adjusted life-years (QALY) gained, expressed as incremental cost-effectiveness ratios (ICER) with costs and benefits discounted annually at 3%, were obtained using deterministic and probabilistic analyses. RESULTS Sunitinib was more effective and less costly than both SFN (gains of 0.52 PFLY, 0.16 LY, 0.17 QALY) and BEV/IFN (gains of 0.19 PFLY, 0.23 LY, 0.16 QALY) with average cost savings/patients of 1,124 and 23,218, respectively. Using a willingness-to-pay (WTP) threshold of 50,000/QALY, sunitinib achieved an incremental net benefit (INB) of 9,717 and 31,211 compared with SFN and BEV/IFN, respectively. At this WTP, the probability of sunitinib providing the highest INB was 75%. CONCLUSION Our analysis suggests that sunitinib is a costeffective alternative to other targeted therapies as first-line mRCC therapy in the Spanish healthcare setting (AU)
Sujet(s)
Humains , Mâle , Femelle , Inhibiteurs de l'angiogenèse/économie , Néphrocarcinome/économie , Essais cliniques comme sujet/méthodes , Indoles/économie , Indoles/usage thérapeutique , Interféron alpha/économie , Tumeurs du rein/économie , Tumeurs du rein/anatomopathologie , Modèles économiques , Pyrroles/économie , Inhibiteurs de l'angiogenèse/usage thérapeutique , Antiviraux/économie , Pyrroles/usage thérapeutique , Antiviraux/usage thérapeutique , Benzènesulfonates/économie , Benzènesulfonates/usage thérapeutique , Néphrocarcinome/traitement médicamenteux , Néphrocarcinome/secondaire , Coûts et analyse des coûtsRÉSUMÉ
Usher syndrome is defined by the association of sensorineural hearing loss, retinitis pigmentosa and variable vestibular dysfunction. Many disease-causative mutations have been identified in MYO7A and USH2A genes, which play a major role in Usher syndrome type I and type II, respectively. The pathogenic nature of mutations that lead to premature stop codons is not questioned; nevertheless, additional studies are needed to verify the pathogenicity of some changes such as those putatively involved in the splice process. Five putative splice-site variants were detected in our cohort of patients: c.2283-1G>T and c.5856G>A in MYO7A and c.1841-2A>G, c.2167+5G>A and c.5298+1G>C in the USH2A gene. In this study, we analyze these changes with bioinformatic tools and investigate the expression of MYO7A and USH2A transcripts through hybrid minigene assays. Our study showed that all five mutations abolished the consensus splice site producing the skipping of involved exons. In addition, for variant c.2167+5G>A, a new donor splice site was observed. Our data reveal the pathogenic nature of the analyzed variants. The fact that splicing mutations led to in-frame or out-of-frame alterations cannot explain phenotypic differences, thus, genotype-phenotype correlations cannot be inferred.
Sujet(s)
Protéines de la matrice extracellulaire/génétique , Mutation , Myosines/génétique , Épissage des ARN/génétique , Animaux , Cellules COS , Chlorocebus aethiops , Protéines de la matrice extracellulaire/métabolisme , Femelle , Ordre des gènes , Génotype , Humains , Mâle , Myosine-VIIa , Myosines/métabolisme , Sites d'épissage d'ARN , Syndromes d'Usher/génétiqueRÉSUMÉ
PURPOSE: Inherited retinal dystrophies and hearing loss disorders have a broad clinical and genetic heterogeneity. Over the last decade there have been major advances in our understanding of the molecular pathology of these diseases; currently over 200 genes and loci are known to be involved in retinal disorders, and over 60 genes/loci are causative for hearing impairment. METHODS: Genetic testing is crucial for confirming the diagnosis at a molecular level. It also allows a more precise prognosis to be made of the future clinical evolution, as well as an accurate genetic and reproductive counselling, and raises the possibility of creating genetically homogeneous groups of patients for future clinical trials. RESULTS: The high number of genes responsible for these disorders makes molecular testing overwhelming in terms of cost, time and technical effectiveness, and no centre offers testing of all known genes. Several diagnostic tools have emerged recently to circumvent this problem. CONCLUSIONS: In this report, we review the vast genetic heterogeneity of retinal dystrophies and hypoacusis, recent advances in gene discovery, the different DNA-based microarray technologies available for molecular testing, their benefits and limitations, and novel therapeutic approaches.
Sujet(s)
Conseil génétique , Troubles de l'audition/génétique , Rétinopathies/génétique , Fécondation in vitro , Prévision , Gènes , Hétérogénéité génétique , Troubles de l'audition/diagnostic , Troubles de l'audition/prévention et contrôle , Troubles de l'audition/thérapie , Surdité neurosensorielle/diagnostic , Surdité neurosensorielle/génétique , Surdité neurosensorielle/prévention et contrôle , Surdité neurosensorielle/thérapie , Humains , Techniques de diagnostic moléculaire , Séquençage par oligonucléotides en batterie , Diagnostic préimplantatoire , Rétinopathies/diagnostic , Rétinopathies/prévention et contrôle , Rétinopathies/thérapie , Dysplasie rétinienne/diagnostic , Dysplasie rétinienne/génétique , Dysplasie rétinienne/prévention et contrôle , Dysplasie rétinienne/thérapie , Appréciation des risques , SyndromeRÉSUMÉ
Objetivo: Las enfermedades hereditarias que afectana la retina y la audición presentan una ampliaheterogeneidad clínica y genética. Durante la pasadadécada se han producido importantes avances en elconocimiento de la patogenia molecular de estasenfermedades y, actualmente, más de 200 genes yloci están implicados en enfermedades de la retina ymás de 60 son responsables de pérdida de audición.Método: El estudio genético molecular es crucialpara confirmar el diagnóstico clínico, permite, en ocasiones,conocer el pronóstico de la enfermedad, unconsejo genético y reproductivo adecuado y permitela posibilidad de crear grupos de pacientes genéticamentehomogéneos para futuros ensayos clínicos.Resultados: El elevado número de genes implicadoshace que el diagnóstico molecular no sea factibleen términos de coste, tiempo y esfuerzo técnicoy no existe ningún centro que oferte el análisis detodos los genes conocidos. Recientemente, se handesarrollado varias herramientas diagnósticas dirigidasa paliar este problema. Conclusiones: En este trabajo se ha revisado laamplia heterogeneidad genética de las distrofiasretinianas y la hipoacusia, los recientes descubrimientosde nuevos genes, las distintas herramientasdiagnósticas basadas en microchips de ADN, susventajas y limitaciones y los nuevos avances en buscade una terapia
Purpose: Inherited retinal dystrophies and hearingloss disorders have a broad clinical and geneticheterogeneity. Over the last decade there have beenmajor advances in our understanding of the molecularpathology of these diseases; currently over 200genes and loci are known to be involved in retinaldisorders, and over 60 genes/loci are causative forhearing impairment.Methods: Genetic testing is crucial for confirmingthe diagnosis at a molecular level. It also allows amore precise prognosis to be made of the future clinicalevolution, as well as an accurate genetic andreproductive counselling, and raises the possibilityof creating genetically homogeneous groups ofpatients for future clinical trials.Results: The high number of genes responsible forthese disorders makes molecular testing overwhelmingin terms of cost, time and technical effectiveness,and no centre offers testing of all knowngenes. Several diagnostic tools have emergedrecently to circumvent this problem. Conclusions: In this report, we review the vastgenetic heterogeneity of retinal dystrophies andhypoacusis, recent advances in gene discovery, thedifferent DNA-based microarray technologies availablefor molecular testing, their benefits and limitations, and novel therapeutic approaches
Sujet(s)
Humains , Mâle , Femelle , Maladies de l'oeil/génétique , Rétine/malformations , Rétine/anatomopathologie , Rétinopathies/génétique , Maladies héréditaires de l'oeil/complications , Maladies héréditaires de l'oeil/diagnostic , Maladies héréditaires de l'oeil/anatomopathologieRÉSUMÉ
Objetivo: Poner de manifiesto la existencia de una variedad de angiomiolipoma, denominada epitelioide, con propiedades diferentes tanto histológicas como clínicas. Método: Se presenta el caso de una mujer de 17 años, afecta de enfermedad de Bourneville, a la que en un control tomográfico renal se descubre la existencia de una masa sólida sugestiva de carcinoma, adyacente a otras de menor tamaño identificadas como angiomiolipomas. Resultados: Tras realizar varias tumorectomías, la sospechosa de carcinoma, de 4 cm de tamaño se diagnostica de angiomiolipoma epitelioide, con corroboración inmunohistoquímica mediante positividad para HMB45, y negatividad a vimentina y queratina. Conclusiones: A pesar de la posibilidad de coexistencia de adenocarcinoma y angiomiolipomas, no hay que descartar la existencia de la variedad epitelioide, sobre todo en pacientes con facomatosis. Los criterios quirúrgicos serán los mismos que para el resto de masas renales. Sin embargo, los criterios de seguimiento deberán ser más estrictos dada la posible evolución tórpida en cuanto a diseminación de esta infrecuente variedad de angiomilipoma (AU)
Objective: To issue the existence of a variety of angiomyolipoma, named epithelioid, with different histological and clinic properties. Methods: We report the case of a 17-year-old female, with Bourneville’s disease, who was discovered to have a solid renal mass suggestive of carcinoma in a control CT scan, adjacent to other smaller masses identified as angiomyolipomas. Results: After several tumorectomies, the suspicious mass, 4 cm in size, was diagnosed as epithelioid angiomyolipoma, with immunohistochemical confirmation of capacity for HMB45, and negative vimentin and keratin. Conclusions: Despite the possibility of coexistence of adenocarcinoma and angiomyolipoma, the existence of an epithelioid variety cannot be discarded, mainly in patients with phakomatosis. The indications for surgery are the same than for the rest of renal masses. Nevertheless, follow-up criteria must be stricter due to the possibility of torpid outcome in terms of dissemination of this infrequent variety of angiomyolipoma (AU)
Sujet(s)
Humains , Femelle , Adulte d'âge moyen , Angiomyolipome/complications , Angiomyolipome/diagnostic , Angiomyolipome/thérapie , Carcinomes/complications , Carcinomes/diagnostic , Carcinomes/thérapie , Diagnostic différentiel , Immunohistochimie/méthodes , Léiomyosarcome/complications , Léiomyome épithélioïde/complications , Hémangioendothéliome épithélioïde/complications , Syndromes neurocutanés/complications , Sarcomes/complicationsRÉSUMÉ
Mutations in the human gene encoding cadherin23 (CDH23) cause Usher syndrome type 1D (USH1D) and nonsyndromic hearing loss. Individuals with Usher syndrome type I have profound congenital deafness, vestibular areflexia and usually begin to exhibit signs of RP in early adolescence. In the present study, we carried out the mutation analysis in all 69 exons of the CDH23 gene in 56 Usher type 1 probands already screened for mutations in MYO7A. A total of 18 of 56 subjects (32.1%) were observed to have one or two CDH23 variants that are presumed to be pathologic. Twenty one different pathologic genome variants were observed of which 15 were novel. Out of a total of 112 alleles, 31 (27.7%) were considered pathologic. Based on our results it is estimated that about 20% of patients with Usher syndrome type I have CDH23 mutations.
Sujet(s)
Cadhérines/génétique , Mutation , Syndromes d'Usher/génétique , Protéines apparentées aux cadhérines , Cadhérines/composition chimique , Analyse de mutations d'ADN , Dynéines/génétique , Exons , Humains , Mutation faux-sens , Myosine-VIIa , Myosines/génétique , Structure tertiaire des protéines , Espagne , Suède , États-UnisSujet(s)
Dynéines/génétique , Mutation , Myosines/génétique , Syndromes d'Usher/génétique , Séquence d'acides aminés , Codon non-sens , République tchèque/ethnologie , Analyse de mutations d'ADN , Femelle , Humains , Italie/ethnologie , Mâle , Données de séquences moléculaires , Maroc/ethnologie , Mutagenèse par insertion , Mutation faux-sens , Myosine-VIIa , Pedigree , Mutation ponctuelle , Polymorphisme de conformation simple brin , Sites d'épissage d'ARN/génétique , Alignement de séquences , Délétion de séquence , Similitude de séquences d'acides aminés , Espagne/ethnologie , Séquences répétées en tandem , Turquie/ethnologie , Syndromes d'Usher/ethnologieRÉSUMÉ
Mutations in USH2A gene have been shown to be responsible for Usher syndrome type II, an autosomal recessive disorder characterised by hearing loss and retinitis pigmentosa. USH2A was firstly described as consisting of 21 exons, but 52 novel exons at the 3' end of the gene were recently identified. In this report, a mutation analysis of the new 52 exons of USH2A gene was carried out in 32 unrelated patients in which both disease-causing mutations could not be found after the screening of the first 21 exons of the USH2A gene. On analysing the new 52 exons, fourteen novel mutations were identified in 14 out of the 32 cases studied, including 7 missense, 5 frameshift, 1 duplication and a putative splice-site mutation.
Sujet(s)
Protéines de la matrice extracellulaire/génétique , Mutation , Syndromes d'Usher/génétique , Adolescent , Adulte , Allèles , Exons , Dépistage génétique , Humains , Isoformes de protéines/génétique , EspagneRÉSUMÉ
Usher syndrome type I is the most severe form of Usher syndrome. It is an autosomal recessive disorder characterized by profound congenital sensorineural deafness, retinitis pigmentosa, and vestibular abnormalities. Mutations in the myosin VIIA gene (MYO7A) are responsible for Usher syndrome type 1B (USH1B). This gene is thought to bear greatest responsibility for USH1 and, depending on the study, has been reported to account for between 24% and 59% of USH1 cases. In this report a mutation screening of the MYO7A gene was carried out in a series of 48 unrelated USH1 families using single strand conformation polymorphism analysis (SSCP) and direct sequencing of those fragments showed an abnormal electrophoretic pattern. Twenty-five mutations were identified in 23 out of the 48 families studied (47.9%). Twelve of these mutations were novel, including five missense mutations, three premature stop codons, three frameshift, and one putative splice-site mutation. Based on our results we can conclude there is an absence of hot spot mutations in the MYO7A gene and that this gene plays a major role in Usher syndrome.
Sujet(s)
Dynéines/génétique , Régulation de l'expression des gènes , Prédisposition génétique à une maladie , Myosines/génétique , Syndromes d'Usher/génétique , Analyse de mutations d'ADN , Humains , Modèles génétiques , Mutation , Myosine-VIIa , Polymorphisme génétique , Polymorphisme de conformation simple brin , EspagneRÉSUMÉ
Usher syndrome (USH) associates deafness and retinitis pigmentosa (RP). It is a disease both clinically and genetically heterogeneous. It is inherited as an autosomal recessive trait and its prevalence makes it the most frequent association of hearing loss and RP. Clinically Usher syndrome is divided into type I (USH1), II (USH2) and III (USH3), according to the severity of hearing loss, age of onset of RP and the existence or not of vestibular dysfunction. There are at least 7 different localizations for USH1 and 5 genes have been identified. For USH2, 3 loci and 2 genes have been reported and USH3 is due to Clarin-1 gene. Our aim is to perform a clinical and genetic characterization of all Usher syndrome patients in Spain.
Sujet(s)
Biologie moléculaire/méthodes , Syndromes d'Usher/épidémiologie , Syndromes d'Usher/génétique , Thérapie génétique/méthodes , Humains , Prévalence , Espagne/épidémiologie , Syndromes d'Usher/thérapieRÉSUMÉ
El síndrome de Usher (USH) asocia sordera y retinosis pigmentaria (RP). Es una enfermedad heterogénea tanto clínica como genéticamente. Su modo de transmisión es autosómico recesivo y su prevalencia la convierte en la asociación de sordera y ceguera de origen genético más frecuente. Clínicamente, el síndrome de Usher se divide en los tipos I (USH1), II (USH2) y III (USH3) en función de la gravedad de la sordera, la edad de aparición de la RP y la presencia o no de disfunción vestibular. Existen al menos 7 localizaciones distintas para el USH1 y se han aislado 5 genes responsables de la enfermedad. Respecto al USH2 se han localizado 3 loci y se han aislado dos genes. El USH3 está causado por el gen clarina-1. Nuestro objetivo es la caracterización clínica y genética de los pacientes con síndrome de Usher en España mediante la búsqueda de mutaciones en los genes implicados en la enfermedad y la correlación con el fenotipo
Usher syndrome (USH) associates deafness and retinitis pigmentosa (RP). It is a disease both clinically and genetically heterogeneous. It is inherited as an autosomal recessive trait and its prevalence makes it the most frequent association of hearing loss and RP. Clinically Usher syndrome is divided into type I (USH1), II (USH2) and III (USH3), according to the severity of hearing loss, age of onset of RP and the existence or not of vestibular dysfunction. There are at least 7 different localizations for USH1 and 5 genes have been identified. For USH2, 3 loci and 2 genes have been reported and USH3 is due to Clarin-1 gene. Our aim is to perform a clinical and genetic characterization of all Usher syndrome patients in Spain
Sujet(s)
Humains , Rétinite pigmentaire/génétique , Surdité/génétique , Études épidémiologiques , Rétinite pigmentaire/épidémiologie , Surdité/épidémiologie , Atteintes du nerf vestibulocochléaire/génétique , Myosine de type V/analyseRÉSUMÉ
Usher syndrome type III is an autosomal recessive disorder clinically characterized by the association of retinitis pigmentosa (RP), variable presence of vestibular dysfunction and progressive hearing loss, being the progression of the hearing impairment the critical parameter classically used to distinguish this form from Usher syndrome type I and Usher syndrome type II. Usher syndrome type III clinical subtype is the rarest form of Usher syndrome in Spain, accounting only for 6% of all Usher syndrome Spanish cases. The gene responsible for Usher syndrome type III is named clarin-1 and it is thought to be involved in hair cell and photoreceptor cell synapses. Here, we report a screening for mutations in clarin-1 gene among our series of Usher syndrome Spanish patients. Clarin-1 has been found to be responsible for the disease in only two families: the first one is a previously reported family homozygous for Y63X mutation and the second one, described here, is homozygous for C40G. This accounts for 1.7% of Usher syndrome Spanish families. It is noticeable that, whereas C40G family is clinically compatible with Usher syndrome type III due to the progression of the hearing loss, Y63X family could be diagnosed as Usher syndrome type I because the hearing impairment is profound and stable. Thus, we consider that the progression of hearing loss is not the definitive key parameter to distinguish Usher syndrome type III from Usher syndrome type I and Usher syndrome type II.
Sujet(s)
Surdité neurosensorielle/génétique , Protéines membranaires/génétique , Rétinite pigmentaire/génétique , Maladies vestibulaires/génétique , Adolescent , Adulte , Enfant , Dépistage génétique , Humains , Mâle , Mutation , Phénotype , Espagne , SyndromeRÉSUMÉ
No disponible
Sujet(s)
Adulte , Femelle , Humains , Thyroïdite subaigüe , Diagnostic différentiel , HyperthyroïdieRÉSUMÉ
A number of pyrido[1,2-c]pyrimidines bearing a nitrogen, oxygen, or sulfur functionality at C-1 were synthesized on solid-phase using the iminophosphorane methodology and tested for their effects on leukocyte functions in vitro and antiinflammatory activity. Compound 5c was found to be a strong scavenger of superoxide anion and an inhibitor of chemiluminescence induced by 12-O-tetradecanoylphorbol 13-acetate in human neutrophils. These pyrido[1,2-c]pyrimidines inhibited the generation of PGE(2) by COX-2 in RAW 264.7 macrophages stimulated with lipopolysaccharide. Compounds 7, 5f, 6, and 8 inhibited enzyme activity, whereas the remaining compounds also acted on the induction phase. In addition, 5a-f, 6, and 7 administered p.o. at a dose of 20 mg/kg showed antiinflammatory activity in the carrageenan mouse paw edema model, where they inhibited PGE(2) levels in inflamed paws without affecting the content of this eicosanoid in stomachs. Inhibition of PGE(2) production and superoxide scavenging may participate in the mechanism of the antiinflammatory action of these pyrido[1,2-c]pyrimidine derivatives.
Sujet(s)
Anti-inflammatoires non stéroïdiens/synthèse chimique , Piégeurs de radicaux libres/synthèse chimique , Macrophages/effets des médicaments et des substances chimiques , Granulocytes neutrophiles/effets des médicaments et des substances chimiques , Pyrimidines/synthèse chimique , Animaux , Anti-inflammatoires non stéroïdiens/composition chimique , Anti-inflammatoires non stéroïdiens/pharmacologie , Cellules cultivées , Cyclooxygenase 2 , Dinoprostone/antagonistes et inhibiteurs , Oedème/traitement médicamenteux , Piégeurs de radicaux libres/composition chimique , Piégeurs de radicaux libres/pharmacologie , Humains , Isoenzymes/métabolisme , Lipopolysaccharides , Mesures de luminescence , Macrophages/enzymologie , Protéines membranaires , Souris , Activation des neutrophiles , Granulocytes neutrophiles/enzymologie , Pancreatic elastase/métabolisme , Prostaglandin-endoperoxide synthases/métabolisme , Pyrimidines/composition chimique , Pyrimidines/pharmacologie , Relation structure-activité , 12-Myristate-13-acétate de phorbol/pharmacologieRÉSUMÉ
This study evaluated tolerance, local control, and short-term survival in patients with locally advanced non-small-cell lung carcinoma treated with induction chemotherapy followed by radical hyperfractionated radiotherapy with concurrent chemotherapy. Thirty-one patients with stage IIIa (N2) or IIIb tumors were treated with cis-platinum-based induction chemotherapy for 1 to 4 courses followed by radical hyperfractionated radiotherapy (69.6 Gy) with concurrent chemotherapy given at the beginning and end of radiotherapy. Induction chemotherapy produced no complete responses and 18 (58%) partial responses. After completion of radiotherapy, 4 patients had complete response (13%) and 23 patients (74%) partial response. The patterns of failure were as follows: intrathoracic, 6 patients (22%); intrathoracic + distant metastasis, 6 patients (22%); distant metastasis without thoracic failure, 5 patients (19%). Six patients of the 12 with intrathoracic failure experienced in-field radiotherapy pure local failure. At the time of this analysis, 10 patients were alive and well (4 complete and 6 partial responders). Actuarial survival projected at 39 months is 35%. No benefit was observed for those patients responding to induction chemotherapy. Toxicity was as follows: grade III neutropenic fever in 4 patients (13%), grade IV neutropenia in 13 patients (42%), pneumonia in 6 patients (19%), grade III esophagitis in 4 patients (13%) and severe clinical pneumonitis in 1 patient (3%). Induction chemotherapy followed by chemoradiotherapy is feasible, and the preliminary results are encouraging. Complete response after radiotherapy appeared to be related to short-term disease-free survival, and decisions based on the response to chemotherapy may be equivocal.
