Incidence et traitement des lymphocèles après greffe rénale

1.1. La greffe de rein La greffe d'organes a révolutionné la médecine. De tout le temps elle a suscité les fantasmes et les rêves : la pratique est ancestrale ; elle remonte au 3ème siècle lorsque Saint Côme et Saint Damien réalisent pour la première fois une greffe de jambe de Maure sur un patient. Il faudra néanmoins attendre le 20ème siècle pour voir la transplantation se réaliser plus concrètement avec succès et se généraliser. A Vienne, en 1902, le Dr. Ulmann (1861-1937) pratique la toute première autogreffe de rein sur un chien. Il replace le rein de l'animal au niveau du cou, pratiquant une anastomose vasculaire. Depuis, les tentatives se multiplient et peu après le Dr. Von Decastello, pratique la première transplantation chien-chien. Par la suite, en associa- tion avec le Dr. Ulmann la première greffe entre un chien et une chèvre aura lieu, avec un certain succès. En effet, elle a permis à l'animal receveur de produire de l'urine. L'avancée majeure durant ce début de siècle fut le développement d'une nouvelle technique de suture vasculaire par le Dr. Carrel, qui obtiendra le prix Nobel en 1912. Son élève, le Dr. Jaboulay (1860-1913) a réalisé plusieurs tentatives de xénogreffes rénales. Il pratiquera en 1906 les deux premières xénogreffes en utilisant un cochon et une chèvre comme donneurs. Le greffon fut respectivement placé au niveau de la cuisse et du bras des patients. La fonction rénale durera une heure. En 1909 Ernest Unger (1875-1938) transplanta un rein de fox-terrier sur un boxer, avec une production d'urine pendant 14 jours. Durant la même année le Dr. Unger a pratiqué une xénogreffe en transplantant un rein de nouveau né sur un babouin, cette intervention se terminant par la mort de l'animal. Un autre essai de greffe singe à humain, pratiqué sur une femme mourant de défaillance rénale, a fait comprendre à Unger qu'il y a des barrières biologiques dans la transplantation, mais que la greffe rénale est techniquement faisable. En 1914, J.B. Murphy découvre l'importance de la rate et de la moelle osseuse dans la réponse immune. En 1933 et 1949 en Ukraine, les premières allogreffes humaines de reins sont pratiquées par le chirurgien soviétique Yu Yu Voronoy. Malheureuse- ment aucune fonction rénale des greffons n'a été observée. Après une période de « stagnation scientifique » générale qui durera à peu près 10 ans, l'intérêt pour la transplantation refait surface dans les années 1950. Deux équipes de chirurgien se forment : une à Boston et l'autre à Paris. De nombreux cas d'allogreffes humaines sans immunosuppression sont documentés de 1950 à 1953. Malheureusement chaque opération aboutit à un échec, ceci dû aux phénomènes du rejet. M. Simonsen et WJ. Dempster découvrent qu'un mécanisme immun est à la base du rejet. Ils établissent aussi que la position pelvienne était meilleure que la position plus superficielle. Grâce aux découvertes dans le domaine du rejet et les nombreux progrès techniques, une allogreffe entre vrais jumeaux est pratiquée à Boston en 1954. L'opération est un succès total et permet de contrer toutes les hypothèses négatives avancées par certains groupes de travail. Depuis 1948, de nombreux travaux dans le domaine de l'immunosuppression ont été entrepris. La découverte de l'action immunosuppressive de la cortisone permet son instauration dans le traitement anti-rejet, malheureusement avec peu de succès. En effet, l'irradiation totale reste la méthode de choix jusqu'en 1962, date de l'apparition de l'Azaothioprine (Imuran®). La découverte de l'Azaothioprine, permet d'avancer de nouvelles hypothèses concernant le rejet : en évitant le rejet post-opératoire aigu, une protection et une adaptation au receveur pourraient être modulées par l'immunosuppression. Dans les années 1960, l'apparition des immunosuppresseurs de synthèse permet de développer de nouvelles lignes de traitement. Le Dr.Starzl et ses collègues, découvrent l'efficacité d'un traitement combiné de Prednisone et d'Azathioprine qui devient alors le standard d'immunosuppression post greffe durant cette période. Les années 60 et 70 sont des années d'optimisme. La prise en charge des patients s'améliore, le développement de la dialyse permet de maintenir en vie les patients avant la greffe, les techniques de conservation des organes s'améliorent, la transplantation élargit son domaine d'action avec la première greffe de coeur en 1968. Le typage tissulaire permet de déterminer le type d'HLA et la compatibilité entre le re- ceveur et le donneur afin de minimiser les risques de rejet aigu. Les années 1970 se caractérisent par deux amélioration majeures : celle du typage HLA-DR et l'apparition des inhibiteurs de la calcineurine (Cyclosporine A). Ce dernier restera l'agent de premier choix jusqu'aux alentours des années 1990 où apparaissaient de nouveaux immunosuppresseurs, tels que les inhibiteurs mTOR (siroli- mus) et les inhibiteurs de l'inosine monophosphate déshydrogénase (mycophénolate mofétil), par exemple. En conclusion, la transplantation rénale a été une des premières transplantations d'organes solides pratiquées sur l'homme avec de nombreux essais cliniques impliquant une multitude d'acteurs. Malgré des périodes de hauts et de bas, les avancements techniques ont été notables, ce qui a été très favorable en terme de survie pour les patients nécessitant une greffe. 1.2. Le lymphocèle La greffe rénale, comme toute autre acte chirurgical, comporte des risques et une morbidité spécifique. Le lymphocèle a la prévalence la plus élevée, qui peut aller de 0.6 à 51% 1-3 avec des variations entre les études. Le lymphocèle est défini comme une collection post opératoire de liquide lymphatique dans une cavité non épithélialisée et n'est pas causée par une fuite urinaire ou une hémorragie1, 4. Historiquement, le lymphocèle a été décrit pour la première fois dans la littérature médicale dans les années 1950, par Kobayashi et Inoue5 en chirurgie gynécologique. Par la suite Mori et al.6 en 1960 documentent la première série d'analyse de lymphocèles. En 1969 le lymphocèle est décrit pour la première fois par Inociencio et al.7 en tant que complication de greffe rénale. Sa pathogénèse n'est pas complètement élucidée, cependant plusieurs facteurs de risque ont été identifiés tels que : la ligature inadéquate des vaisseaux lymphatiques lors de la dissection des vaisseaux iliaques du donneur et de la préparation du greffon, le BMI, les diurétiques, l'anticoagulation (héparine), les hautes doses de stéoïdes, certains agents immunosuppresseurs (sirolimus), le diabète, les problèmes de cicatrisation, une hypoalbuminémie, une chirurgie rétropéritonéale préalable et le rejet aigu de greffe. (Tableau 1) Une symptomatologie peut être présente ou absente : elle découle directement de la localisation et de la taille de la collection8, 9, 10. Lorsqu'on se trouve devant un tableau de lymphocèle asymptomatique, la découverte se fait de manière fortuite lors d'un contrôle de suivi de greffe11, 12 cliniquement ou par échographie. En cas de lymphocèle non significatif cela ne requiert aucun traitement. Au contraire, lorsqu'il atteint une certaines taille il provoque un effet de masse et de compression qui provoque la symptomatologie. Cette dernière est peu spécifique et apparait en moyenne entre 2 semaines et 6 mois 13 après la greffe. Le patient va se présenter avec un tableau pouvant aller de la simple douleur abdominale en passant par un oedème du membre inférieur ou, dans de plus rares cas, une thrombose veineuse profonde sera le seul signe consécutif au lymphocèle14, 15. La plupart du temps on observera des valeurs de créatinine élevées, signant une souffrance rénale. Le diagnostic du lymphocèle peut se faire selon plusieurs techniques. La plus utilisée est la ponction à l'aiguille fine sous guidage ultrasonographique4. L'analyse du liquide ponctionné permet de différencier un lymphocèle d'un urinome. Les autres techniques existantes sont : la ponction après injection de carmin d'indigo15, un pyelogramme intraveineux et un lymphangiogramme16, le CT-Scan ou l'IRM15. Le dosage sanguin d'IL6 et IL8 est parfois utilisé pour déterminer si le lymphocèle est infecté.15 Suite à l'apparition d'une collection symptomatique; le rein transplanté peut être dans une situation à risque pour laquelle un traitement doit être entrepris. A l'heure actuelle, il n'existe pas de solution universelle dans la prévention et le traitement de ce type de complication. Les solutions sont multiples et dépendent principalement de la localisation et de la taille de la collection. Pendant de nombreuses années, le seul traitement du lymphocèle a été celui de l'aspiration percutanée simple. Cette dernière conduit cependant à un taux de récidive de presque 100%.17 Cette technique reste une solution utilisée principalement à visée diagnostique18, 19, 20, 21 ou pour soulager les patients à court terme15. Pour améliorer l'efficacité de cette technique on a fait appel à des agents sclérosants comme l'éthanol, la povidone-iodine, la tétracycline, la doxycycline ou de la colle de fibrine. Des complications chirurgicales ont cependant été rapportées, pouvant aller jusqu'au rejet de greffe22. La fenestration par laparoscopie a été décrite pour la première fois en 1991 par McCullough et al.23 Cette technique reste, de nos jours, la technique la plus utilisée pour le traitement du lymphocèle. Elle a de nombreux avantages : un temps de convalescence court, des pertes de sang minimes et une réalimentation rapide24, 25. On constate en outre la quasi absence de récidives après traitement11, 26. L'évaluation radiologique est très importante, car la marsupialisation par laparoscopie est limitée par l'emplacement et le volume de la collection. Ainsi, on évitera ce type de traite- ment lorsque la collection se situera postérieurement, à proximité de la vessie, de l'uretère ou du hile rénal. Dans ces situations, la laparotomie s'impose malgré l'augmentation de la morbidité liée à cette technique24. Actuellement on cherche à trouver une technique universelle du traitement des lymphocèles avec la chirurgie la moins invasive possible et le taux de récidive le plus faible possible. Malgré ses li- mites, la fenestration par laparoscopie apparaît comme une très bonne solution. Cette étude consiste en une évaluation rétrospective des traitements chirurgicaux de cette complication post-opératoire de la greffe rénale au CHUV (Centre Hospitalier Universitaire Vaudois) de 2003 à 2011. Le but est de recenser et analyser les différentes techniques que l'on observe actuellement dans la littérature et pouvoir ainsi proposer une technique idéale pour le CHUV.

Mutant prominin 1 found in patients with macular degeneration disrupts photoreceptor disk morphogenesis in mice.

Familial macular degeneration is a clinically and genetically heterogeneous group of disorders characterized by progressive central vision loss. Here we show that an R373C missense mutation in the prominin 1 gene (PROM1) causes 3 forms of autosomal-dominant macular degeneration. In transgenic mice expressing R373C mutant human PROM1, both mutant and endogenous PROM1 were found throughout the layers of the photoreceptors, rather than at the base of the photoreceptor outer segments, where PROM1 is normally localized. Moreover, the outer segment disk membranes were greatly overgrown and misoriented, indicating defective disk morphogenesis. Immunoprecipitation studies showed that PROM1 interacted with protocadherin 21 (PCDH21), a photoreceptor-specific cadherin, and with actin filaments, both of which play critical roles in disk membrane morphogenesis. Collectively, our results identify what we believe to be a novel complex involved in photoreceptor disk morphogenesis and indicate a possible role for PROM1 and PCDH21 in macular degeneration.

Use of 2D Sensitivity Encoding for Slow-Infusion Contrast-Enhanced Isotropic 3-T Whole-Heart Coronary MR Angiography.

OBJECTIVE. The purpose of this study was to improve the blood-pool signal-to-noise ratio (SNR) and blood-myocardium contrast-to-noise ratio (CNR) of slow-infusion 3-T whole-heart coronary MR angiography (MRA).SUBJECTS AND METHODS. In 2D sensitivity encoding (SENSE), the number of acquired k-space lines is reduced, allowing less radiofrequency excitation per cardiac cycle and a longer TR. The former can be exploited for signal enhancement with a higher radiofrequency excitation angle, and the latter leads to noise reduction due to lower data-sampling bandwidth. Both effects contribute to SNR gain in coronary MRA when spatial and temporal resolution and acquisition time remain identical. Numeric simulation was performed to select the optimal 2D SENSE pulse sequence parameters and predict the SNR gain. Eleven patients underwent conventional unenhanced and the proposed 2D SENSE contrast-enhanced coronary MRA acquisition. Blood-pool SNR, blood-myocardium CNR, visible vessel length, vessel sharpness, and number of side branches were evaluated.RESULTS. Consistent with the numeric simulation, using 2D SENSE in contrast-enhanced coronary MRA resulted in significant improvement in aortic blood-pool SNR (unenhanced vs contrast-enhanced, 37.5 +/- 14.7 vs 121.3 +/- 44.0; p < 0.05) and CNR (14.4 +/- 6.9 vs 101.5 +/- 40.8; p < 0.05) in the patient sample. A longer length of left anterior descending coronary artery was visualized, but vessel sharpness, coronary artery coverage, and image quality score were not improved with the proposed approach.CONCLUSION. In combination with contrast administration, 2D SENSE was found effective in improving SNR and CNR in 3-T whole-heart coronary MRA. Further investigation of cardiac motion compensation is necessary to exploit the SNR and CNR advantages and to achieve submillimeter spatial resolution.

RHAMM-R3 peptide vaccination in patients with acute myeloid leukemia, myelodysplastic syndrome, and multiple myeloma elicits immunologic and clinical responses.

The receptor for hyaluronic acid-mediated motility (RHAMM) is an antigen eliciting both humoral and cellular immune responses in patients with acute myeloid leukemia (AML), myelodysplastic syndrome (MDS), and multiple myeloma (MM). We initiated a phase 1 clinical trial vaccinating 10 patients with R3 (ILSLELMKL), a highly immunogenic CD8(+) T-cell epitope peptide derived from RHAMM. In 7 of 10 patients, we detected an increase of CD8(+)/HLA-A2/RHAMM R3 tetramer(+)/CD45RA(+)/CCR7(-)/CD27(-)/CD28(-) effector T cells in accordance with an increase of R3-specific CD8(+) T cells in enzyme linked immunospot (ELISpot) assays. In chromium release assays, a specific lysis of RHAMM-positive leukemic blasts was shown. Three of 6 patients with myeloid disorders (1/3 AML, 2/3 MDS) achieved clinical responses: one patient with AML and one with MDS showed a significant reduction of blasts in the bone marrow after the last vaccination. One patient with MDS no longer needed erythrocyte transfusions after 4 vaccinations. Two of 4 patients with MM showed a reduction of free light chain serum levels. Taken together, RHAMM-R3 peptide vaccination induced both immunologic and clinical responses, and therefore RHAMM constitutes a promising target for further immunotherapeutic approaches. This study is registered at http://ISRCTN.org as ISRCTN32763606 and is registered with EudraCT as 2005-001706-37.

Regional coronary endothelial function is closely related to local early coronary atherosclerosis in patients with mild coronary artery disease: pilot study.

BACKGROUND: Coronary endothelial function is abnormal in patients with established coronary artery disease and was recently shown by MRI to relate to the severity of luminal stenosis. Recent advances in MRI now allow the noninvasive assessment of both anatomic and functional (endothelial function) changes that previously required invasive studies. We tested the hypothesis that abnormal coronary endothelial function is related to measures of early atherosclerosis such as increased coronary wall thickness. METHODS AND RESULTS: Seventeen arteries in 14 healthy adults and 17 arteries in 14 patients with nonobstructive coronary artery disease were studied. To measure endothelial function, coronary MRI was performed before and during isometric handgrip exercise, an endothelial-dependent stressor, and changes in coronary cross-sectional area and flow were measured. Black blood imaging was performed to quantify coronary wall thickness and indices of arterial remodeling. The mean stress-induced change in cross-sectional area was significantly higher in healthy adults (13.5%±12.8%, mean±SD, n=17) than in those with mildly diseased arteries (-2.2%±6.8%, P<0.0001, n=17). Mean coronary wall thickness was lower in healthy subjects (0.9±0.2 mm) than in patients with coronary artery disease (1.4±0.3 mm, P<0.0001). In contrast to healthy subjects, stress-induced changes in cross-sectional area, a measure of coronary endothelial function, correlated inversely with coronary wall thickness in patients with coronary artery disease (r=-0.73, P=0.0008). CONCLUSIONS: There is an inverse relationship between coronary endothelial function and local coronary wall thickness in patients with coronary artery disease but not in healthy adults. These findings demonstrate that local endothelial-dependent functional changes are related to the extent of early anatomic atherosclerosis in mildly diseased arteries. This combined MRI approach enables the anatomic and functional investigation of early coronary disease.

Steady-state equilibrium phase inversion recovery ON-resonant water suppression (IRON) MR angiography in conjunction with superparamagnetic nanoparticles. A robust technique for imaging within a wide range of contrast agent dosages.

PURPOSE: To investigate the ability of inversion recovery ON-resonant water suppression (IRON) in conjunction with P904 (superparamagnetic nanoparticles which consisting of a maghemite core coated with a low-molecular-weight amino-alcohol derivative of glucose) to perform steady-state equilibrium phase MR angiography (MRA) over a wide dose range. MATERIALS AND METHODS: Experiments were approved by the institutional animal care committee. Rabbits (n = 12) were imaged at baseline and serially after the administration of 10 incremental dosages of 0.57-5.7 mgFe/Kg P904. Conventional T1-weighted and IRON MRA were obtained on a clinical 1.5 Tesla (T) scanner to image the thoracic and abdominal aorta, and peripheral vessels. Contrast-to-noise ratios (CNR) and vessel sharpness were quantified. RESULTS: Using IRON MRA, CNR and vessel sharpness progressively increased with incremental dosages of the contrast agent P904, exhibiting constantly higher contrast values than T1 -weighted MRA over a very wide range of contrast agent doses (CNR of 18.8 ± 5.6 for IRON versus 11.1 ± 2.8 for T1 -weighted MRA at 1.71 mgFe/kg, P = 0.02 and 19.8 ± 5.9 for IRON versus -0.8 ± 1.4 for T1-weighted MRA at 3.99 mgFe/kg, P = 0.0002). Similar results were obtained for vessel sharpness in peripheral vessels, (Vessel sharpness of 46.76 ± 6.48% for IRON versus 33.20 ± 3.53% for T1-weighted MRA at 1.71 mgFe/Kg, P = 0.002, and of 48.66 ± 5.50% for IRON versus 19.00 ± 7.41% for T1-weighted MRA at 3.99 mgFe/Kg, P = 0.003). CONCLUSION: Our study suggests that quantitative CNR and vessel sharpness after the injection of P904 are consistently higher for IRON MRA when compared with conventional T1-weighted MRA. These findings apply for a wide range of contrast agent dosages.

Shedding light on proteolytic cleavage of CD44: the responsible sheddase and functional significance of shedding.

CD44 is the major cell-surface receptor for hyaluronan, which is implicated in cell-cell and cell-matrix adhesion, cell migration, and signaling. Studies have shown that CD44-dependent migration requires CD44 to be shed from the cell surface and that matrix metalloproteinase-mediated cleavage may provide an underlying mechanism. However, the full spectrum of proteases that may participate in CD44 shedding has yet to be defined. In this issue, Anderegg et al. demonstrate that ADAM10, but not ADAM17 or MMP14, mediates constitutive shedding of CD44 in human melanoma cells and that knockdown of ADAM10 blocks the antiproliferative activity of the soluble proteolytic cleavage product of CD44.

Mirror extreme BMI phenotypes associated with gene dosage at the chromosome 16p11.2 locus.

Both obesity and being underweight have been associated with increased mortality. Underweight, defined as a body mass index (BMI) ≤ 18.5 kg per m(2) in adults and ≤ -2 standard deviations from the mean in children, is the main sign of a series of heterogeneous clinical conditions including failure to thrive, feeding and eating disorder and/or anorexia nervosa. In contrast to obesity, few genetic variants underlying these clinical conditions have been reported. We previously showed that hemizygosity of a ∼600-kilobase (kb) region on the short arm of chromosome 16 causes a highly penetrant form of obesity that is often associated with hyperphagia and intellectual disabilities. Here we show that the corresponding reciprocal duplication is associated with being underweight. We identified 138 duplication carriers (including 132 novel cases and 108 unrelated carriers) from individuals clinically referred for developmental or intellectual disabilities (DD/ID) or psychiatric disorders, or recruited from population-based cohorts. These carriers show significantly reduced postnatal weight and BMI. Half of the boys younger than five years are underweight with a probable diagnosis of failure to thrive, whereas adult duplication carriers have an 8.3-fold increased risk of being clinically underweight. We observe a trend towards increased severity in males, as well as a depletion of male carriers among non-medically ascertained cases. These features are associated with an unusually high frequency of selective and restrictive eating behaviours and a significant reduction in head circumference. Each of the observed phenotypes is the converse of one reported in carriers of deletions at this locus. The phenotypes correlate with changes in transcript levels for genes mapping within the duplication but not in flanking regions. The reciprocal impact of these 16p11.2 copy-number variants indicates that severe obesity and being underweight could have mirror aetiologies, possibly through contrasting effects on energy balance.

The amphioxus genome illuminates vertebrate origins and cephalochordate biology.

Cephalochordates, urochordates, and vertebrates evolved from a common ancestor over 520 million years ago. To improve our understanding of chordate evolution and the origin of vertebrates, we intensively searched for particular genes, gene families, and conserved noncoding elements in the sequenced genome of the cephalochordate Branchiostoma floridae, commonly called amphioxus or lancelets. Special attention was given to homeobox genes, opsin genes, genes involved in neural crest development, nuclear receptor genes, genes encoding components of the endocrine and immune systems, and conserved cis-regulatory enhancers. The amphioxus genome contains a basic set of chordate genes involved in development and cell signaling, including a fifteenth Hox gene. This set includes many genes that were co-opted in vertebrates for new roles in neural crest development and adaptive immunity. However, where amphioxus has a single gene, vertebrates often have two, three, or four paralogs derived from two whole-genome duplication events. In addition, several transcriptional enhancers are conserved between amphioxus and vertebrates--a very wide phylogenetic distance. In contrast, urochordate genomes have lost many genes, including a diversity of homeobox families and genes involved in steroid hormone function. The amphioxus genome also exhibits derived features, including duplications of opsins and genes proposed to function in innate immunity and endocrine systems. Our results indicate that the amphioxus genome is elemental to an understanding of the biology and evolution of nonchordate deuterostomes, invertebrate chordates, and vertebrates.

Diet and the risk of head and neck cancer: a pooled analysis in the INHANCE consortium.

We investigated the association between diet and head and neck cancer (HNC) risk using data from the International Head and Neck Cancer Epidemiology (INHANCE) consortium. The INHANCE pooled data included 22 case-control studies with 14,520 cases and 22,737 controls. Center-specific quartiles among the controls were used for food groups, and frequencies per week were used for single food items. A dietary pattern score combining high fruit and vegetable intake and low red meat intake was created. Odds ratios (OR) and 95% confidence intervals (CI) for the dietary items on the risk of HNC were estimated with a two-stage random-effects logistic regression model. An inverse association was observed for higher-frequency intake of fruit (4th vs. 1st quartile OR = 0.52, 95% CI = 0.43-0.62, p (trend) < 0.01) and vegetables (OR = 0.66, 95% CI = 0.49-0.90, p (trend) = 0.01). Intake of red meat (OR = 1.40, 95% CI = 1.13-1.74, p p (trend) < 0.01) was positively associated with HNC risk. Higher dietary pattern scores, reflecting high fruit/vegetable and low red meat intake, were associated with reduced HNC risk (per score increment OR = 0.90, 95% CI = 0.84-0.97).

Non-invasive detection of coronary endothelial response to sequential handgrip exercise in coronary artery disease patients and healthy adults.

OBJECTIVES: Our objective is to test the hypothesis that coronary endothelial function (CorEndoFx) does not change with repeated isometric handgrip (IHG) stress in CAD patients or healthy subjects. BACKGROUND: Coronary responses to endothelial-dependent stressors are important measures of vascular risk that can change in response to environmental stimuli or pharmacologic interventions. The evaluation of the effect of an acute intervention on endothelial response is only valid if the measurement does not change significantly in the short term under normal conditions. Using 3.0 Tesla (T) MRI, we non-invasively compared two coronary artery endothelial function measurements separated by a ten minute interval in healthy subjects and patients with coronary artery disease (CAD). METHODS: Twenty healthy adult subjects and 12 CAD patients were studied on a commercial 3.0 T whole-body MR imaging system. Coronary cross-sectional area (CSA), peak diastolic coronary flow velocity (PDFV) and blood-flow were quantified before and during continuous IHG stress, an endothelial-dependent stressor. The IHG exercise with imaging was repeated after a 10 minute recovery period. RESULTS: In healthy adults, coronary artery CSA changes and blood-flow increases did not differ between the first and second stresses (mean % change ±SEM, first vs. second stress CSA: 14.8%±3.3% vs. 17.8%±3.6%, p = 0.24; PDFV: 27.5%±4.9% vs. 24.2%±4.5%, p = 0.54; blood-flow: 44.3%±8.3 vs. 44.8%±8.1, p = 0.84). The coronary vasoreactive responses in the CAD patients also did not differ between the first and second stresses (mean % change ±SEM, first stress vs. second stress: CSA: -6.4%±2.0% vs. -5.0%±2.4%, p = 0.22; PDFV: -4.0%±4.6% vs. -4.2%±5.3%, p = 0.83; blood-flow: -9.7%±5.1% vs. -8.7%±6.3%, p = 0.38). CONCLUSION: MRI measures of CorEndoFx are unchanged during repeated isometric handgrip exercise tests in CAD patients and healthy adults. These findings demonstrate the repeatability of noninvasive 3T MRI assessment of CorEndoFx and support its use in future studies designed to determine the effects of acute interventions on coronary vasoreactivity.

Merlin, a "Magic" Linker between Extracellular Cues and Intracellular Signaling Pathways that Regulate Cell Motility, Proliferation, and Survival.

Genetic alterations of neurofibromatosis type 2 (NF2) gene lead to the development of schwannomas, meningiomas, and ependymomas. Mutations of NF2 gene were also found in thyroid cancer, mesothelioma, and melanoma, suggesting that it functions as a tumor suppressor in a wide spectrum of cells. The product of NF2 gene is merlin (moesin-ezrin-radixin-like protein), a member of the Band 4.1 superfamily proteins. Merlin shares significant sequence homology with the ERM (Ezrin-Radixin-Moesin) family proteins and serves as a linker between transmembrane proteins and the actin-cytoskeleton. Merlin is a multifunctional protein and involved in integrating and regulating the extracellular cues and intracellular signaling pathways that control cell fate, shape, proliferation, survival, and motility. Recent studies showed that merlin regulates the cell-cell and cell-matrix adhesions and functions of the cell surface adhesion/extracellular matrix receptors including CD44 and that merlin and CD44 antagonize each other's function and work upstream of the mammalian Hippo signaling pathway. Furthermore, merlin plays important roles in stabilizing the contact inhibition of proliferation and in regulating activities of several receptor tyrosine kinases. Accumulating data also suggested an emerging role of merlin as a negative regulator of growth and progression of several non-NF2 associated cancer types. Together, these recent advances have improved our basic understanding about merlin function, its regulation, and the major signaling pathways regulated by merlin and provided the foundation for future translation of these findings into the clinic for patients bearing the cancers in which merlin function and/or its downstream signaling pathways are impaired or altered.

Flow structures at an idealized bifurcation : a numerical experiment

River bifurcations are key nodes within braided river systems controlling the flow and sediment partitioning and therefore the dynamics of the river braiding process. Recent research has shown that certain geometrical configurations induce instabilities that lead to downstream mid-channel bar formation and the formation of bifurcations. However, we currently have a poor understanding of the flow division process within bifurcations and the flow dynamics in the downstream bifurcates, both of which are needed to understand bifurcation stability. This paper presents results of a numerical sensitivity experiment undertaken using computational fluid dynamics (CFD) with the purpose of understanding the flow dynamics of a series of idealized bifurcations. A geometric sensitivity analysis is undertaken for a range of channel slopes (0.005 to 0.03), bifurcation angles (22 degrees to 42 degrees) and a restricted set of inflow conditions based upon simulating flow through meander bends with different curvature on the flow field dynamics through the bifurcation. The results demonstrate that the overall slope of the bifurcation affects the velocity of flow through the bifurcation and when slope asymmetry is introduced, the flow structures in the bifurcation are modified. In terms of bifurcation evolution the most important observation appears to be that once slope asymmetry is greater than 0.2 the flow within the steep bifurcate shows potential instability and the potential for alternate channel bar formation. Bifurcation angle also defines the flow structures within the bifurcation with an increase in bifurcation angle increasing the flow velocity down both bifurcates. However, redistributive effects of secondary circulation caused by upstream curvature can very easily counter the effects of local bifurcation characteristics. Copyright (C) 2011 John Wiley & Sons, Ltd.

Estimating and explaining the effect of education and income on head and neck cancer risk : INHANCE consortium pooled analysis of 31 case-control studies from 27 countries

Low socioeconomic status has been reported to be associated with head and neck cancer risk. However, previous studies have been too small to examine the associations by cancer subsite, age, sex, global region, and calendar time, and to explain the association in terms of behavioural risk factors. Individual participant data of 23,964 cases with head and neck cancer and 31,954 controls from 31 studies in 27 countries pooled with random effects models. Overall, low education was associated with an increased risk of head and neck cancer (OR = 2·50; 95%CI 2·02- 3·09). Overall one-third of the increased risk was not explained by differences in the distribution of cigarette smoking and alcohol behaviours; and it remained elevated among never users of tobacco and non-drinkers (OR = 1·61; 95%CI 1·13 - 2·31). More of the estimated education effect was not explained by cigarette smoking and alcohol behaviours: in women than in men, in older than younger groups, in the oropharynx than in other sites, in South/Central America than in Europe/North America, and was strongest in countries with greater income inequality. Similar findings were observed for the estimated effect of low vs high household income. The lowest levels of income and educational attainment were associated with more than 2-fold increased risk of head and neck cancer, which is not entirely explained by differences in the distributions of behavioural risk factors for these cancers, and which varies across cancer sites, sexes, countries, and country income inequality levels. © 2014 Wiley Periodicals, Inc.