188 research outputs found

    Recommandations pour l’utilisation de la toxine botulinique de type A (BotoxÂź) dans l’hyperactivitĂ© vĂ©sicale rĂ©fractaire idiopathique

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    RĂ©sumĂ©ObjectifsDĂ©finir des recommandations pour l’utilisation pratique de la toxine botulinique de type A (BoNTA) dans l’hyperactivitĂ© vĂ©sicale rĂ©fractaire idiopathique (HAVRI).MĂ©thodeÉlaboration de recommandations de bonne pratique par consensus formalisĂ©, validĂ©es par un groupe de 13 experts puis par un groupe de lecture indĂ©pendant.RĂ©sultatsEn cas d’infection urinaire celle-ci doit ĂȘtre traitĂ©e et l’injection reportĂ©e. Avant l’injection, il est recommandĂ© de s’assurer de la faisabilitĂ© et de l’acceptabilitĂ© de l’auto-sondage. L’injection peut ĂȘtre rĂ©alisĂ©e aprĂšs une anesthĂ©sie locale urĂ©tro-vĂ©sicale (lidocaĂŻne), Ă©ventuellement complĂ©tĂ©e par l’inhalation de protoxyde d’azote et parfois sous anesthĂ©sie gĂ©nĂ©rale. L’injection sera rĂ©alisĂ©e au bloc opĂ©ratoire ou en salle d’endoscopie. La vessie ne doit pas ĂȘtre trop remplie (risque de perforation). Le traitement doit ĂȘtre appliquĂ© en 10 à 20 injections de 0,5 à 1mL rĂ©parties de maniĂšre homogĂšne dans la vessie en restant Ă  distance des mĂ©ats urĂ©tĂ©raux. Il n’est pas recommandĂ© de laisser en place une sonde vĂ©sicale sauf en cas d’hĂ©maturie importante. Le patient doit ĂȘtre surveillĂ© jusqu’à la reprise mictionnelle. Une note d’information sur les effets indĂ©sirables Ă©ventuels doit lui ĂȘtre remise Ă  sa sortie. Une consultation doit ĂȘtre prĂ©vue 3 mois aprĂšs la premiĂšre injection (calendrier mictionnel, dĂ©bitmĂ©trie, rĂ©sidu post-mictionnel et examen cytobactĂ©riologique des urines). Un rĂ©sidu >200mL et/ou symptomatique doit faire discuter des auto-sondages. Une nouvelle injection pourra ĂȘtre envisagĂ©e lorsque le bĂ©nĂ©fice clinique de la prĂ©cĂ©dente s’estompe (entre 6 et 9 mois).ConclusionsLe respect de ces recommandations devrait permettre une utilisation optimale de la BoNTA.Niveau de preuve3.SummaryObjectivesProvide guidelines for practical usage of botulinum toxin type A (BoNTA) for refractory idiopathic Overactive Bladder management.Patients and methodsGuidelines using formalized consensus guidelines method. These guidelines have been validated by a group of 13 experts quoting proposals, subsequently reviewed by an independent group of experts.ResultsIn the case of patients with urinary tract infection, it must be treated and injection postponed. Before proposing an injection, it is recommended to ensure the feasibility and acceptability of self-catheterisation by patient. The injection can be performed after local anesthesia of the bladder and urethra (lidocaine), supplemented where necessary by nitrous oxide inhalation and sometimes under general anesthesia. Injection is performed in the operating room or endoscopy suite. The bladder should not be too filled (increased risk of perforation). Treatment should be applied in 10 to 20 injections of 0.5 to 1mL homogeneously distributed in the bladder at a distance from the urethral orifices. It is not recommended to leave a urinary catheter in place except in cases of severe hematuria. The patient should be monitored until resumption of micturition. After the first injection, an appointment must be scheduled within 3 months (micturition diary, uroflowmetry, measurement of residual urine and urine culture). Performance of self-catheterisation should be questioned in the case of a symptomatic post-void residual and/or a residue>200mL. A new injection may be considered when the clinical benefit of the previous injection diminishes (between 6 and 9 months). A period of three months must elapse between each injection.ConclusionsImplementation of these guidelines may promote best practice usage of BoNTA with optimal risk/benefit ratio

    Modelling human musculoskeletal functional movements using ultrasound imaging

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    <p>Abstract</p> <p>Background</p> <p>A widespread and fundamental assumption in the health sciences is that muscle functions are related to a wide variety of conditions, for example pain, ischemic and neurological disorder, exercise and injury. It is therefore highly desirable to study musculoskeletal contributions in clinical applications such as the treatment of muscle injuries, post-surgery evaluations, monitoring of progressive degeneration in neuromuscular disorders, and so on.</p> <p>The spatial image resolution in ultrasound systems has improved tremendously in the last few years and nowadays provides detailed information about tissue characteristics. It is now possible to study skeletal muscles in real-time during activity.</p> <p>Methods</p> <p>The ultrasound images are transformed to be congruent and are effectively compressed and stacked in order to be analysed with multivariate techniques. The method is applied to a relevant clinical orthopaedic research field, namely to describe the dynamics in the Achilles tendon and the calf during real-time movements.</p> <p>Results</p> <p>This study introduces a novel method to medical applications that can be used to examine ultrasound image sequences and to detect, visualise and quantify skeletal muscle dynamics and functions.</p> <p>Conclusions</p> <p>This new objective method is a powerful tool to use when visualising tissue activity and dynamics of musculoskeletal ultrasound registrations.</p

    Study on administration of 1,5-anhydro-D-fructose in C57BL/6J mice challenged with high-fat diet

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    1,5-Anhydro-D-fructose (AF) is a mono-saccharide directly formed from starch and glycogen by the action of α-1,4-glucan lyase (EC 4.2.2.13). Our previous study has indicated that AF increases glucose tolerance and insulin secretion in NMRI mice after administration through a gastric gavage in a single dose at 150 mg per mouse. In this study, we used high-fat feeding of C57BL/6J mice to examine the influence of long-term administration of AF on glucose-stimulated insulin secretion in vivo and in vitro. We found that 8-weeks of high-fat feeding increased body weight, fasting blood glucose and insulin levels in C57BL/6J mice when compared to mice fed normal diet. Impaired glucose tolerance was also observed in mice receiving 8-weeks of high-fat diet. In contrast, AF (1.5 g/kg/day), administered through drinking water for 8-weeks, did not affect body weight or food and water intake in mice fed either the high-fat or normal diet. There was no difference in basal blood glucose or insulin levels between AF-treated and control group. Oral glucose tolerance test (OGTT) showed that AF did not affect glucose-stimulated insulin secretion in mice. In in vitro studies with isolated islets, AF did not influence glucose-stimulated insulin secretion in mice receiving either high-fat or normal diet. We therefore conclude that when given through drinking water for 8 weeks at 1.5 g/kg/day, AF has no effect on glucose-stimulated insulin secretion in C57BL/6J mice challenged with a high-fat diet

    Noninvasive, Transient and Selective Blood-Brain Barrier Opening in Non-Human Primates In Vivo

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    The blood-brain barrier (BBB) is a specialized vascular system that impedes entry of all large and the vast majority of small molecules including the most potent central nervous system (CNS) disease therapeutic agents from entering from the lumen into the brain parenchyma. Microbubble-enhanced, focused ultrasound (ME-FUS) has been previously shown to disrupt noninvasively, selectively, and transiently the BBB in small animals in vivo. For the first time, the feasibility of transcranial ME-FUS BBB opening in non-human primates is demonstrated with subsequent BBB recovery. Sonications were combined with two different types of microbubbles (customized 4–5 ”m and DefinityÂź). 3T MRI was used to confirm the BBB disruption and to assess brain damage

    Structure determination of cyclopentane terpene derivatives by crossed NMR and MS techniques

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    3 of the 4 stereoisomers of the 1-isopropenyl 2,3-dimethylcyclopentane, obtained from the cracking of 3,7-dimethylocta-1,6-diene, were purified and characterized. Dihedral angles, between the protons of the substituted carbons, have been determined by molecular modelling. Analysis of the NMR and mass spectra allowed us to access to the structure of the different isomers
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