Influence of inter-electrode distance, contraction type, and muscle on the relationship between the sEMG power spectrum and contraction force.

INTRODUCTION: Spectral frequencies of the surface electromyogram (sEMG) increase with contraction force, but debate still exists on whether this increase is affected by various methodological and anatomical factors. This study aimed to investigate the influence of inter-electrode distance (IED) and contraction modality (step-wise vs. ramp) on the changes in spectral frequencies with increasing contraction strength for the vastus lateralis (VL) and vastus medialis (VM) muscles. METHODS: Twenty healthy male volunteers were assessed for isometric sEMG activity of the VM and VL, with the knee at 90° flexion. Subjects performed isometric ramp contractions in knee extension (6-s duration) with the force gradually increasing from 0 to 80 % MVC. Also, subjects performed 4-s step-wise isometric contractions at 10, 20, 30, 40, 50, 60, 70, and 80 % MVC. Interference sEMG signals were recorded simultaneously at different IEDs: 10, 20, 30, and 50 mm. The mean (F mean) and median (F median) frequencies and root mean square (RMS) of sEMG signals were calculated. RESULTS: For all IEDs, contraction modalities, and muscles tested, spectral frequencies increased significantly with increasing level of force up to 50-60 % MVC force. Spectral indexes increased systematically as IED was decreased. The sensitivity of spectral frequencies to changes in contraction force was independent of IED. The behaviour of spectral indexes with increasing contraction force was similar for step-wise and ramp contractions. CONCLUSIONS: In the VL and VM muscles, it is highly unlikely that a particular inter-electrode distance or contraction modality could have prevented the observation of the full extent of the increase in spectral frequencies with increasing force level.

Alcohol and nonlethal injuries: a Swiss emergency department study on the risk relationship between acute alcohol consumption and type of injury.

BACKGROUND: Acute alcohol consumption has been reported to be an important risk factor for injury, but clear scientific evidence on issues such as injury type is not available. The present study aims to improve the knowledge of the importance of alcohol consumption as an injury determinant with regards to two dimensions of the type of injury, namely the nature and the body region involved. METHODS: Risk relationships between two injury type components and acute alcohol use were estimated through multinomial and logistic regression models based on data from 7,529 patients-among whom 3,682 had injury diagnoses-gathered in a Swiss emergency department. RESULTS: Depending on the type of injury, between 31.1% and 48.7% of casualties report alcohol use before emergency department attendance. The multinomial regression models show that even low alcohol levels are consistently associated with nearly all natures of injury and body regions. A persistent dose-response effect between alcohol levels and risk associations was observed for almost all injury types. CONCLUSIONS: The results highlight the importance and consistency of the risk association between low and moderate levels of acute alcohol consumption and all types of injury. None of the body regions and natures of injury could pride on absence of association between alcohol and injury. Public health, prevention, and care implications are considered.

Multi-stage garnet in the internal Brianconnais basement (Ambin massif, Savoy): New petrological constraints on the blueschist-facies metamorphism in the Western Alps and tectonic implications

Three types of garnet have been distinguished in pelitic schists from an epidote-blueschist-facies unit of the Ambin and South Vanoise Brianconnais massifs on the basis of texture, chemical zoning and mineral inclusion characterization. Type-1 garnet cores with high Mn/Ca ratios are interpreted as pre-Alpine relicts, whereas Type-1 garnet rims, Type-2 inclusion-rich porphyroblasts and smaller Type-3 garnets are Alpine. The latter are all characterized by low Mn/Ca ratios and a coexisting mineral assemblage of blue amphibole, high-Si phengite, epidote and quartz. Prograde growth conditions during Alpine D-1 high-pressure (HP) metamorphism are recorded by a decrease in Mn and increase in Fe (+/-Ca) in the Type-2 garnets, culminating in peak P-T conditions of 14-16 kbar and 500degreesC in the deepest parts of the Ambin dome. The multistage growth history of Type-1 garnets indicates a polymetamorphic history for the Ambin and South Vanoise massifs; unfortunately, no age constraints are available. The new metamorphic constraints on the Alpine event in the massifs define a metamorphic T `gap' between them and their surrounding cover (Brianconnais and upper Schistes Lustres units), which experienced metamorphism only in the stability field of carpholite-lawsonite (T < 400degreesC). These data and supporting structural studies confirm that the Ambin and South Vanoise massifs are slices of `eclogitized' continental crust tectonically extruded within the Schistes Lustres units and Brianconnais covers. The corresponding tectonic contacts with top-to-east movement are responsible for the juxtaposition of lower-grade metamorphic units on the Ambin and South Vanoise massifs.

Influence of cassette type on the DQE of CR systems.

In our recent paper by Monnin et al. [Med. Phys. 33, 411-420 (2006)], an objective analysis of the relative performance of a computed radiography (CR) system using both standard single-side (ST-VI) and prototype dual-side read (ST-BD) plates was reported. The presampled modulation transfer function (MTF), noise power spectrum (NPS), and detective quantum efficiency (DQE) for the systems were determined at three different beam qualities representative of paediatric chest radiography, at an entrance detector air kerma of 5 microGy. Experiments demonstrated that, compared to the standard single-side read system, the MTF for the dual-side read system was slightly reduced, but a significant decrease in image noise resulted in a marked increase in DQE (+40%) in the low spatial frequency range. However, the DQE improvement for the ST-BD plate decreased with increasing spatial frequency, and, at spatial frequencies above 2.2 mm(-1), the DQE of the dual-side read system was lower than that of the single-side one.

Effect of computerisation on the quality and safety of chemotherapy prescription.

BACKGROUND: Chemotherapy is prescribed according to protocols of several cycles. These protocols include not only therapeutic agents but also adjuvant solvents and inherent supportive care measures. Multiple errors can occur during the prescription, the transmission of documents and the drug delivery processes, and lead to potentially serious consequences. OBJECTIVE: To assess the effect of a computerised physician order entry (CPOE) system on the number of errors in prescription recorded by the centralised chemotherapy unit of a pharmacy service in a university hospital. PATIENTS AND METHODS: Existing chemotherapy protocols were standardised by a multidisciplinary team (composed of a doctor, a pharmacist and a nurse) and a CPOE system was developed from a File Maker Pro database. Chemotherapy protocols were progressively introduced into the CPOE system. The effect of the system on prescribing errors was measured over 15 months before and 21 months after starting computerised protocol prescription. Errors were classified as major (dosage and drug name) and minor (volume or type of infusion solution). RESULTS: Before computerisation, 141 errors were recorded for 940 prescribed chemotherapy regimens (15%). After introduction of the CPOE system, 75 errors were recorded for 1505 prescribed chemotherapy regimens (5%). Of these errors, 69 (92%) were recorded in prescriptions that did not use a computerised protocol. A dramatic decrease in the number of errors was noticeable when 50% of the chemotherapy protocols were prescribed through the CPOE system. CONCLUSION: Errors in chemotherapy prescription nearly disappeared after implementation of CPOE. The safety of chemotherapy prescription was markedly improved.

Effects of muscle fibre shortening on the characteristics of surface motor unit potentials.

Traditionally, studies dealing with muscle shortening have concentrated on assessing its impact on conduction velocity, and to this end, electrodes have been located between the end-plate and tendon regions. Possible morphologic changes in surface motor unit potentials (MUPs) as a result of muscle shortening have not, as yet, been evaluated or characterized. Using a convolutional MUP model, we investigated the effects of muscle shortening on the shape, amplitude, and duration characteristics of MUPs for different electrode positions relative to the fibre-tendon junction and for different depths of the MU in the muscle (MU-to-electrode distance). It was found that the effects of muscle shortening on MUP morphology depended not only on whether the electrodes were between the end-plate and the tendon junction or beyond the tendon junction, but also on the specific distance to this junction. When the electrodes lie between the end-plate and tendon junction, it was found that (1) the muscle shortening effect is not important for superficial MUs, (2) the sensitivity of MUP amplitude to muscle shortening increases with MU-to-electrode distance, and (3) the amplitude of the MUP negative phase is not affected by muscle shortening. This study provides a basis for the interpretation of the changes in MUP characteristics in experiments where both physiological and geometrical aspects of the muscle are varied.

A descriptive study on the surgery and the microbiology of Gustilo type III fractures in an university hospital in Switzerland.

OBJECTIVE: To describe the epidemiology, the surgical treatment, the microbiology, the antibiotic prophylaxis and the outcome of patients with the most severe type of open fractures. METHODS: Retrospective chart reviews of patients with Gustilo type III open fracture admitted to an university hospital in Switzerland between January 2007 and December 2011. The patient's and fracture's characteristics, surgery, antibiotic prophylaxis, and microbiology findings at the initial and at the revision surgery were described. RESULTS: Thirty patients were included (83% male, mean age 41 years). More than half of the patients had polytrauma. In all patients, debridement and stabilization surgery (70% using external fixation) were performed at admission. Soft tissue reconstruction was performed in 87% and in 23% immediate bone graft was performed. Antibiotic prophylaxis were given in all patients for a median duration of 9 days (60% received amoxicillin/clavulanic acid). Positive bacterial culture was found in 53% of the patients at initial surgery and in 88% at revision surgery. At initial and revision surgery, 47% and 88% of the pathogens were amoxicillin/clavulanic acid-resistant. Treatment outcome was favorable in 24 of 30 patients (80%) and in six cases (20%) an amputation had to be performed. None of the patients had chronic bone infection. CONCLUSIONS: Positive cultures were found often in open fractures. Amoxicillin/clavulanic acid which is often mentioned in many guidelines as prophylaxis in open fractures does not cover the most common isolated organisms. The combination of surgery and antibiotic prophylaxis leads to good outcome in Gustilo type III fracture.

On the Use of a Test to Exhaustion Specific to Tennis (TEST) with Ball Hitting by Elite Players

PURPOSE: We aimed to a) introduce a new Test to Exhaustion Specific to Tennis (TEST) and compare performance (test duration) and physiological responses to those obtained during the 20-m multistage shuttle test (MSST), and b) determine to which extent those variables correlate with performance level (tennis competitive ranking) for both test procedures. METHODS: Twenty-seven junior players (8 males, 19 females) members of the national teams of the French Tennis Federation completed MSST and TEST, including elements of the game (ball hitting, intermittent activity, lateral displacement), in a randomized order. Cardiorespiratory responses were compared at submaximal (respiratory compensation point) and maximal loads between the two tests. RESULTS: At the respiratory compensation point oxygen uptake (50.1 +/- 4.7 vs. 47.5 +/- 4.3 mL.min-1.kg-1, p = 0.02), but not minute ventilation and heart rate, was higher for TEST compared to MSST. However, load increment and physiological responses at exhaustion did not differ between the two tests. Players' ranking correlated negatively with oxygen uptake measured at submaximal and maximal loads for both TEST (r = -0.41; p = 0.01 and -0.55; p = 0.004) and MSST (r = -0.38; P = 0.05 and -0.51; p = 0.1). CONCLUSION: Using TEST provides a tennis-specific assessment of aerobic fitness and may be used to prescribe aerobic exercise in a context more appropriate to the game than MSST. Results also indicate that VO2 values both at submaximal and maximal load reached during TEST and MSST are moderate predictors of players competitive ranking.

Clinical review: practical recommendations on the management of perioperative heart failure in cardiac surgery.

Acute cardiovascular dysfunction occurs perioperatively in more than 20% of cardiosurgical patients, yet current acute heart failure (HF) classification is not applicable to this period. Indicators of major perioperative risk include unstable coronary syndromes, decompensated HF, significant arrhythmias and valvular disease. Clinical risk factors include history of heart disease, compensated HF, cerebrovascular disease, presence of diabetes mellitus, renal insufficiency and high-risk surgery. EuroSCORE reliably predicts perioperative cardiovascular alteration in patients aged less than 80 years. Preoperative B-type natriuretic peptide level is an additional risk stratification factor. Aggressively preserving heart function during cardiosurgery is a major goal. Volatile anaesthetics and levosimendan seem to be promising cardioprotective agents, but large trials are still needed to assess the best cardioprotective agent(s) and optimal protocol(s). The aim of monitoring is early detection and assessment of mechanisms of perioperative cardiovascular dysfunction. Ideally, volume status should be assessed by 'dynamic' measurement of haemodynamic parameters. Assess heart function first by echocardiography, then using a pulmonary artery catheter (especially in right heart dysfunction). If volaemia and heart function are in the normal range, cardiovascular dysfunction is very likely related to vascular dysfunction. In treating myocardial dysfunction, consider the following options, either alone or in combination: low-to-moderate doses of dobutamine and epinephrine, milrinone or levosimendan. In vasoplegia-induced hypotension, use norepinephrine to maintain adequate perfusion pressure. Exclude hypovolaemia in patients under vasopressors, through repeated volume assessments. Optimal perioperative use of inotropes/vasopressors in cardiosurgery remains controversial, and further large multinational studies are needed. Cardiosurgical perioperative classification of cardiac impairment should be based on time of occurrence (precardiotomy, failure to wean, postcardiotomy) and haemodynamic severity of the patient's condition (crash and burn, deteriorating fast, stable but inotrope dependent). In heart dysfunction with suspected coronary hypoperfusion, an intra-aortic balloon pump is highly recommended. A ventricular assist device should be considered before end organ dysfunction becomes evident. Extra-corporeal membrane oxygenation is an elegant solution as a bridge to recovery and/or decision making. This paper offers practical recommendations for management of perioperative HF in cardiosurgery based on European experts' opinion. It also emphasizes the need for large surveys and studies to assess the optimal way to manage perioperative HF in cardiac surgery.

Expression of a functional single chain antibody on the surface of extracellular enveloped vaccinia virus as a step towards selective tumour cell targeting.

Recombinant vaccinia virus with tumour cell specificity may provide a versatile tool either for direct lysis of cancer cells or for the targeted transfer of genes encoding immunomodulatory molecules. We report the expression of a single chain antibody on the surface of extracellular enveloped vaccinia virus. The wild-type haemagglutinin, an envelope glycoprotein which is not required for viral infection and replication, was replaced by haemagglutinin fusion molecules carrying a single chain antibody directed against the tumour-associated antigen ErbB2. ErbB2 is an epidermal growth factor receptor-related tyrosine kinase overexpressed in a high percentage of human adenocarcinomas. Two fusion proteins carrying the single chain antibody at different NH2-terminal positions were expressed and exposed at the envelope of the corresponding recombinant viruses. The construct containing the antibody at the site of the immunoglobulin-like loop of the haemagglutinin was able to bind solubilized ErbB2. This is the first report of replacement of a vaccinia virus envelope protein by a specific recognition structure and represents a first step towards modifying the host cell tropism of the virus.

Interactive Epistemology and Reasoning: On the Foundations of Game Theory

Game theory describes and analyzes strategic interaction. It is usually distinguished between static games, which are strategic situations in which the players choose only once as well as simultaneously, and dynamic games, which are strategic situations involving sequential choices. In addition, dynamic games can be further classified according to perfect and imperfect information. Indeed, a dynamic game is said to exhibit perfect information, whenever at any point of the game every player has full informational access to all choices that have been conducted so far. However, in the case of imperfect information some players are not fully informed about some choices. Game-theoretic analysis proceeds in two steps. Firstly, games are modelled by so-called form structures which extract and formalize the significant parts of the underlying strategic interaction. The basic and most commonly used models of games are the normal form, which rather sparsely describes a game merely in terms of the players' strategy sets and utilities, and the extensive form, which models a game in a more detailed way as a tree. In fact, it is standard to formalize static games with the normal form and dynamic games with the extensive form. Secondly, solution concepts are developed to solve models of games in the sense of identifying the choices that should be taken by rational players. Indeed, the ultimate objective of the classical approach to game theory, which is of normative character, is the development of a solution concept that is capable of identifying a unique choice for every player in an arbitrary game. However, given the large variety of games, it is not at all certain whether it is possible to device a solution concept with such universal capability. Alternatively, interactive epistemology provides an epistemic approach to game theory of descriptive character. This rather recent discipline analyzes the relation between knowledge, belief and choice of game-playing agents in an epistemic framework. The description of the players' choices in a given game relative to various epistemic assumptions constitutes the fundamental problem addressed by an epistemic approach to game theory. In a general sense, the objective of interactive epistemology consists in characterizing existing game-theoretic solution concepts in terms of epistemic assumptions as well as in proposing novel solution concepts by studying the game-theoretic implications of refined or new epistemic hypotheses. Intuitively, an epistemic model of a game can be interpreted as representing the reasoning of the players. Indeed, before making a decision in a game, the players reason about the game and their respective opponents, given their knowledge and beliefs. Precisely these epistemic mental states on which players base their decisions are explicitly expressible in an epistemic framework. In this PhD thesis, we consider an epistemic approach to game theory from a foundational point of view. In Chapter 1, basic game-theoretic notions as well as Aumann's epistemic framework for games are expounded and illustrated. Also, Aumann's sufficient conditions for backward induction are presented and his conceptual views discussed. In Chapter 2, Aumann's interactive epistemology is conceptually analyzed. In Chapter 3, which is based on joint work with Conrad Heilmann, a three-stage account for dynamic games is introduced and a type-based epistemic model is extended with a notion of agent connectedness. Then, sufficient conditions for backward induction are derived. In Chapter 4, which is based on joint work with Jérémie Cabessa, a topological approach to interactive epistemology is initiated. In particular, the epistemic-topological operator limit knowledge is defined and some implications for games considered. In Chapter 5, which is based on joint work with Jérémie Cabessa and Andrés Perea, Aumann's impossibility theorem on agreeing to disagree is revisited and weakened in the sense that possible contexts are provided in which agents can indeed agree to disagree.

On the use of reporter bacteria for measuring availability of organic contaminants

Natural environments are constantly challenged by the release of hydrophobic organic contaminants, which represent a threat for both the ecosystem and human health. Despite a substantial degradation by naturally occurring micro-organisms, a non negligible fraction of these pollutants tend to persist in soil and sediments due to their reduced accessibility to microbial degraders. This lack of 'bioavailability' is acknowledged as a key parameter for the natural and stimulated clean-up (bioremediation) of contaminated sites. We developed a bacterial bioreporter that responds to the presence of polyaromatic hydrocarbons (PAHs) by the production of the green fluorescent protein (GFP), based on the PAH-degrading bacterium Burkholderia sartisoli. We showed in this study that the bacterial biosensor B. sartisoli strain RP037 was faithfully reporting the degradation of naphthalene and phenanthrene (two PAHs of low molecular weight) via the production of GFP. What is more, the magnitude of GFP induction was influenced by change in the PAH flux triggered by a variety of physico-chemical parameters, such as the contact surface between the pollutant and the aqueous suspension. Further experiments permitted to test the influence of dissolved organic matter, which is an important component of natural habitats and can interact with organic pollutants. In addition, we tested the influence of two types of biosurfactants (tensio-active agents produced by living organisms) on phenanthrene's degradation by RP037. Interestingly, the surfactant's effects on the biodegradation rate appeared to depend on the type of biosurfactant and probably on the type of bacterial strain. Finally, we tagged B. sartisoli strain RP037 with a constitutively expressed mCherry fluorescent protein. The presence of mCherry allowed us to visualize the bacteria in complex samples even when GFP production was not induced. The new strain RP037-mChe embedded in a gel patch was used to detect PAH fluxes from a point source, such as a non-aqueous liquid or particles of contaminated soil. In parallel, we also developed and tested a so-called multiwell bacterial biosensor platform, which permitted the simultaneous use of four different reporter strains for the detection of major crude oil components (e.g., saturated hydrocarbons, mono- and polyaromatics) in aqueous samples. We specifically constructed the strain B. sartisoli RP007 (pPROBE-phn-luxAB) for the detection of naphthalene and phenanthrene. It was equipped with a reporter plasmid similar to the one in strain RP037, except that the gfp gene was replaced by the genes luxAB, which encoded the bacterial luciferase. The strain was implemented in the biosensor platform and detected an equivalent naphthalene concentration in oil spilled-sea water. We also cloned the gene for the transcriptional activator AlkS and the operator/promoter region of the operon alkSB1GHJ from the alkane-degrader bacterium Alcanivorax borkumensis strain SK2 in order to construct a new bacterial biosensor with higher sensitivity towards long-chain alkanes. However, the resulting strain showed no increased light emission in presence of tetradecane (C14), while it still efficiently reported low concentrations of octane (C8). RÉSUMÉ : Les écosystèmes naturels sont constamment exposés à nombre de contaminants organiques hydrophobes (COHs) d'origine industrielle, agricole ou même naturelle. Les COHs menacent à la fois l'environnement, le bien-être des espèces animales et végétales et la santé humaine, mais ils peuvent être dégradés par des micro-organismes tels que les bactéries et les champignons, qui peuvent être capables des les transformer en produits inoffensifs comme le gaz carbonique et l'eau. La biodégradation des COHs est cependant fréquemment limitée par leur pauvre disponibilité envers les organismes qui les dégradent. Ainsi, bien que la biodégradation opère partiellement, les COHs persistent dans l'environnement à de faibles concentrations qui potentiellement peuvent encore causer des effets toxiques chroniques. Puisque la plupart des COHs peuvent être métabolisés par l'activité microbienne, leur persistance a généralement pour origine des contraintes physico-chimiques plutôt que biologiques. Par exemple, leur solubilité dans l'eau très limitée réduit leur prise par des consommateurs potentiels. De plus, l'adsorption à la matière organique et la séquestration dans les micropores du sol participent à réduire leur disponibilité envers les microbes. Les processus de biodisponibilité, c'est-à-dire les processus qui gouvernent la dissolution et la prise de polluants par les organismes vivants, sont généralement perçus comme des paramètres clés pour la dépollution (bioremédiation) naturelle et stimulée des sites contaminés. Les hydrocarbures aromatiques polycycliques (HAPs) sont un modèle de COH produits par les activités aussi bien humaines que naturelles, et listés comme des contaminants chroniques de l'air, des sols et des sédiments. Ils peuvent être dégradés par un vaste nombre d'espèces bactériennes mais leur taux de biodégradation est souvent limité par les contraintes mentionnées ci-dessus. Afin de comprendre les processus de biodisponibilité pour les cellules bactériennes, nous avons décidé d'utiliser les bactéries elles-mêmes pour détecter et rapporter les flux de COH. Ceci a été réalisé par l'application d'une stratégie de conception visant à produire des bactéries `biocapteurs-rapporteurs', qui littéralement s'allument lorsqu'elles détectent un composé cible pour lequel elles ont été conçues. En premier lieu, nous nous sommes concentrés sur Burkholderia sartisoli (souche RP007), une bactérie isolée du sol et consommatrice de HAP .Cette souche a servi de base à la construction d'un circuit génétique permettant la formation de la protéine autofluorescente GFP dès que les cellules détectent le naphtalène ou le phénanthrène, deux HAP de faible masse moléculaire. En effet, nous avons pu montrer que la bactérie obtenue, la souche RP037 de B. sartisoli, produit une fluorescence GFP grandissante lors d'une exposition en culture liquide à du phénanthrène sous forme cristalline (0.5 mg par ml de milieu de culture). Nous avons découvert que pour une induction optimale il était nécessaire de fournir aux cellules une source additionnelle de carbone sous la forme d'acétate, ou sinon seul un nombre limité de cellules deviennent induites. Malgré cela, le phénanthrène a induit une réponse très hétérogène au sein de la population de cellules, avec quelques cellules pauvrement induites tandis que d'autres l'étaient très fortement. La raison de cette hétérogénéité extrême, même dans des cultures liquides mélangées, reste pour le moment incertaine. Plus important, nous avons pu montrer que l'amplitude de l'induction de GFP dépendait de paramètres physiques affectant le flux de phénanthrène aux cellules, tels que : la surface de contact entre le phénanthrène solide et la phase aqueuse ; l'ajout de surfactant ; le scellement de phénanthrène à l'intérieur de billes de polymères (Model Polymer Release System) ; la dissolution du phénanthrène dans un fluide gras immiscible à l'eau. Nous en avons conclu que la souche RP037 détecte convenablement des flux de phénantrène et nous avons proposé une relation entre le transfert de masse de phénanthrène et la production de GFP. Nous avons par la suite utilisé la souche afin d'examiner l'effet de plusieurs paramètres chimiques connus dans la littérature pour influencer la biodisponibilité des HAP. Premièrement, les acides humiques. Quelques rapports font état que la disponibilité des HAP pourrait être augmentée par la présence de matière organique dissoute. Nous avons mesuré l'induction de GFP comme fonction de l'exposition des cellules RP037 au phénanthrène ou au naphtalène en présence ou absence d'acides humiques dans la culture. Nous avons testé des concentrations d'acides humiques de 0.1 et 10 mg/L, tandis que le phénanthrène était ajouté via l'heptamethylnonane (HMN), un liquide non aqueux, ce qui au préalable avait produit le plus haut flux constant de phénanthrène aux cellules. De plus, nous avons utilisé des tests en phase gazeuse avec des concentrations d'acides humiques de 0.1, 10 et 1000 mg/L mais avec du naphtalène. Contrairement à ce que décrit la littérature, nos résultats ont indiqué que dans ces conditions l'expression de GFP en fonction de l'exposition au phénanthrène dans des cultures en croissance de la souche RP037 n'était pas modifiée par la présence d'acides humiques. D'un autre côté, le test en phase gazeuse avec du naphtalène a montré que 1000 mg/L d'acides humiques abaissent légèrement mais significativement la production de GFP dans les cellules de RP037. Nous avons conclu qu'il n'y a pas d'effet général des acides humiques sur la disponibilité des HAP pour les bactéries. Par la suite, nous nous sommes demandé si des biosurfactants modifieraient la disponibilité du phénanthrène pour les bactéries. Les surfactants sont souvent décrits dans la littérature comme des moyens d'accroître la biodisponibilité des COHs. Les surfactants sont des agents tensio-actifs qui augmentent la solubilité apparente de COH en les dissolvant à l'intérieur de micelles. Nous avons ainsi testé si des biosurfactants (des surfactants produits par des organismes vivants) peuvent être utilisé pour augmenter la biodisponibilité du phénanthrène pour la souche B. sartisoli RP037. Premièrement, nous avons tenté d'obtenir des biosurfactants produits par une autre bactérie vivant en co-culture avec les biocapteurs bactériens. Deuxièmement, nous avons utilisé des biosurfactants purifiés. La co-cultivation en présence de la bactérie productrice de lipopeptide Pseudomonas putida souche PCL1445 a augmenté l'expression de GFP induite par le phénanthrène chez B. sartisoli en comparaison des cultures simples, mais cet effet n'était pas significativement différent lorsque la souche RP037 était co-cultivée avec un mutant de P. putida ne produisant pas de lipopeptides. L'ajout de lipopeptides partiellement purifiés dans la culture de RP037 a résulté en une réduction de la tension de surface, mais n'a pas provoqué de changement dans l'expression de GFP. D'un autre côté, l'ajout d'une solution commerciale de rhamnolipides (un autre type de biosurfactants produits par Pseudomonas spp.) a facilité la dégradation du phénanthrène par la souche RP037 et induit une expression de GFP élevée dans une plus grande proportion de cellules. Nous avons ainsi conclu que les effets des biosurfactants sont mesurables à l'aide de la souche biocapteur, mais que ceux-ci sont dépendants du type de surfactant utilisé conjointement avec le phénanthrène. La question suivante que nous avons abordée était si les tests utilisant des biocapteurs peuvent être améliorés de manière à ce que les flux de HAP provenant de matériel contaminé soient détectés. Les tests en milieu liquide avec des échantillons de sol ne fournissant pas de mesures, et sachant que les concentrations de HAP dans l'eau sont en général extrêmement basses, nous avons conçu des tests de diffusion dans lesquels nous pouvons étudier l'induction par les HAPs en fonction de la distance aux cellules. Le biocapteur bactérien B. sartisoli souche RP037 a été marqué avec une seconde protéine fluorescente (mCherry), qui est constitutivement exprimée dans les cellules et leur confère une fluorescence rouge/rose. La souche résultante RP037-mChe témoigne d'une fluorescence rouge constitutive mais n'induit la fluorescence verte qu'en présence de naphtalène ou de phénanthrène. La présence d'un marqueur fluorescent constitutif nous permet de visualiser les biocapteurs bactériens plus facilement parmi des particules de sol. Un test de diffusion a été conçu en préparant un gel fait d'une suspension de cellules mélangées à 0.5 % d'agarose. Des bandes de gel de dimensions 0.5 x 2 cm x 1 mm ont été montées dans des chambres d'incubation et exposées à des sources de HAP (soit dissouts dans du HMN ou en tant que matériel solide, puis appliqués à une extrémité de la bande). En utilisant ce montage expérimental, le naphtalène ou le phénanthrène (dissouts dans du HMN à une concentration de 2.5 µg/µl) ont induit un gradient d'intensité de fluorescence GFP après 24 heures d'incubation, tandis que la fluorescence mCherry demeurait comparable. Un sol contaminé par des HAPs (provenant d'un ancien site de production de gaz) a induit la production de GFP à un niveau comparable à celui du naphtalène. Des biocapteurs bactériens individuels ont également détecté un flux de phénanthrène dans un gel contenant des particules de sol amendées avec 1 et 10 mg/g de phénanthrène. Ceci a montré que le test de diffusion peut être utilisé pour mesurer des flux de HAP provenant de matériel contaminé. D'un autre côté, la sensibilité est encore très basse pour plusieurs sols contaminés, et l'autofluorescence de certains échantillons rend difficile l'identification de la réponse de la GFP chez les cellules. Pour terminer, un des points majeurs de ce travail a été la production et la validation d'une plateforme multi-puits de biocapteurs bactériens, qui a permis l'emploi simultané de plusieurs souches différentes de biocapteurs pour la détection des constituants principaux du pétrole. Pour cela nous avons choisi les alcanes linéaires, les composés mono-aromatiques, les biphényls et les composés poly-aromatiques. De plus, nous avons utilisé un capteur pour la génotoxicité afin de détecter la `toxicité globale' dans des échantillons aqueux. Plusieurs efforts d'ingénierie ont été investis de manière à compléter ce set. En premier lieu, chaque souche a été équipée avec soit gfp, soit luxAB en tant que signal rapporteur. Deuxièmement, puisqu'aucune souche de biocapteur n'était disponible pour les HAP ou pour les alcanes à longues chaînes, nous avons spécifiquement construit deux nouveaux biocapteurs. L'un d'eux est également basé sur B. sartisoli RP007, que nous avons équipé avec le plasmide pPROBE-phn-luxAB pour la détection du naphtalène et du phénanthrène mais avec production de luciférase bactérienne. Un autre est un nouveau biocapteur bactérien pour les alcanes. Bien que nous possédions une souche Escherichia coli DHS α (pGEc74, pJAMA7) détectant les alcanes courts de manière satisfaisante, la présence des alcanes à longues chaînes n'était pas rapportée efficacement. Nous avons cloné le gène de l'activateur transcriptionnel A1kS ainsi que la région opérateur/promoteur de l'opéron alkSB1GHJ chez la bactérie dégradant les alcanes Alcanivorax borkumensis souche SK2, afin de construire un nouveau biocapteur bactérien bénéficiant d'une sensibilité accrue envers les alcanes à longues chaînes. Cependant, la souche résultante E. coli DHSα (pAlk3} n'a pas montré d'émission de lumière augmentée en présence de tétradécane (C14), tandis qu'elle rapportait toujours efficacement de basses concentrations d'octane (C8). De manière surprenante, l'utilisation de A. borkumensis en tant que souche hôte pour le nouveau plasmide rapporteur basé sur la GFP a totalement supprimé la sensibilité pour l'octane, tandis que la détection de tétradécane n'était pas accrue. Cet aspect devra être résolu dans de futurs travaux. Pour calibrer la plateforme de biocapteurs, nous avons simulé une fuite de pétrole en mer dans une bouteille en verre ouverte de 5L contenant 2L d'eau de mer contaminée avec 20 ml (1%) de pétrole brut. La phase aqueuse a été échantillonée à intervalles réguliers après la fuite durant une période allant jusqu'à une semaine tandis que les principaux contaminants pétroliers étaient mesurés via les biocapteurs. L'émission de bioluminescence a été mesurée de manière à déterminer la réponse des biocapteurs et une calibration intégrée faite avec des inducteurs types a servi à calculer des concentrations d'équivalents inducteurs dans l'échantillon. E. coli a été utilisée en tant que souche hôte pour la plupart des spécificités des biocapteurs, à l'exception de la détection du naphtalène et du phénanthrène pour lesquels nous avons utilisé B. sartisoli. Cette souche, cependant, peut être employée plus ou moins selon la même procédure. Il est intéressant de noter que le pétrole répandu a produit une apparition séquentielle de composés dissouts dans la phase aqueuse, ceux-ci .étant détectables par les biocapteurs. Ce profil contenait d'abord les alcanes à courtes chaînes et les BTEX (c'est-à dire benzène, toluène, éthylbenzène et xylènes), apparaissant entre des minutes et des heures après que le pétrole a été versé. Leurs concentrations aqueuses ont par la suite fortement décru dans l'eau échantillonnée après 24 heures, à cause de la volatilisation ou de la biodégradation. Après quelques jours d'incubation, ces composés sont devenus indétectables. Les HAPs, en revanche, sont apparus plus tard que les alcanes et les BTEX, et leur concentration a augmenté de pair avec un temps d'incubation prolongé. Aucun signal significatif n'a été mis en évidence avec le biocapteur pour le biphényl ou pour la génotoxicité. Ceci démontre l'utilité de ces biocapteurs, spécifiquement pour la détection des composés pétroliers, comprenant les alcanes à courtes chaînes, les BTEX et les HAPs légers.

Influence of the primary cleft palate closure on the future need for orthognathic surgery in unilateral cleft lip and palate patients.

The aim of the study was to determine the influence of the dissection of the palate during primary surgery and the type of orthognathic surgery needed in cases of unilateral total cleft. The review concerns 58 children born with a complete unilateral cleft lip and palate and treated between 1994 and 2008 at the appropriate age for orthognathic surgery. This is a retrospective mixed-longitudinal study. Patients with syndromes or associated anomalies were excluded. All children were treated by the same orthodontist and by the same surgical team. Children are divided into 2 groups: the first group includes children who had conventional primary cleft palate repair during their first year of life, with extensive mucoperiosteal undermining. The second group includes children operated on according to the Malek surgical protocol. The soft palate is closed at the age of 3 months, and the hard palate at 6 months with minimal mucoperiosteal undermining. Lateral cephalograms at ages 9 and 16 years and surgical records were compared. The need for orthognathic surgery was more frequent in the first than in the second group (60% vs 47.8%). Concerning the type of orthognathic surgery performed, 2- or 3-piece Le Fort I or bimaxillary osteotomies were also less required in the first group. Palate surgery following the Malek procedure results in an improved and simplified craniofacial outcome. With a minimal undermining of palatal mucosa, we managed to reduce the amount of patients who required an orthognathic procedure. When this procedure was indicated, the surgical intervention was also greatly simplified.

Active mitral ring for post-surgical remote correction of residual mitral regurgitation on the beating heart.

OBJECTIVES: Residual mitral regurgitation after valve repair worsens patients' clinical outcome. Postimplant adjustable mitral rings potentially address this issue, allowing the reshaping of the annulus on the beating heart under echocardiography control. We developed an original mitral ring allowing valve geometry remodelling after the implantation and designed an animal study to assess device effectiveness in correcting residual mitral regurgitation. METHODS: The device consists of two concentric rings: one internal and flexible, sutured to the mitral annulus and a second external and rigid. A third conic element slides between the two rings, modifying the shape of the flexible ring. This sliding element is remotely activated with a rotating tool. Animal model: in adult swine, under cardio pulmonary bypass and cardiac arrest, we shortened the primary chordae of P2 segment to reproduce Type III regurgitation and implanted the active ring. We used intracardiac ultrasound to assess mitral regurgitation and the efficacy of the active ring to correct it. RESULTS: Severe mitral regurgitation (3+ and 4+) was induced in eight animals, 54 ± 6 kg in weight. Vena contracta width decreased from 0.8 ± 0.2 to 0.1 cm; proximal isovelocity surface area radius decreased from 0.8 ± 0.2 to 0.1 cm and effective regurgitant orifice area decreased from 0.50 ± 0.1 to 0.1 ± 0.1 cm(2). Six animals had a reversal of systolic pulmonary flow that normalized following the activation of the device. All corrections were reversible. CONCLUSIONS: Postimplant adjustable mitral ring corrects severe mitral regurgitation through the reversible modification of the annulus geometry on the beating heart. It addresses the frequent and morbid issue of recurrent mitral valve regurgitation.