Analysis of GPCR properties of Frizzled receptors and establishment of the "in vitro" platform for screening of Frizzled agonists/antagonists as potential therapeutic agents

Morphogens of the Wnt protein family are the secreted lipoglycoprotein ligands which initiate several pathways heavily involved in the coordination of various developmental stages of organisms in the majority of animal species. Deregulation of these pathways in the adult leads to formation and sustaining of multiple types of cancer. The latter notion is reinforced by the fact that the very discovery of the first Wnt ligand was due to its role as the causative factor of carcinogenic transformation (Nusse and Varmus, 1982). Nowadays our knowledge on Wnt signaling has "moved with the times" and these pathways were identified to be often crucial for tumor formation, its interactions with the microenvironment, and promotion of the metastases (Huang and Du, 2008; Zerlin et al., 2008; Jessen, 2009). Thus the relevance of the pathway as the target for drug development has further increased in the light of modern paradigms of the complex cancer treatments which target also spreading and growth- promoting factors of tumors by specific and highly efficient substances (Pavet et al., 2010). Presently the field of the Wnt-targeting drug research is almost solely dominated by assays based on transcriptional activation induced by the signaling. This approach resulted in development of a number of promising substances (Lee et al., 2011). Despite its effectiveness, the method nevertheless suffers from several drawbacks. Among the major ones is the fact that this approach is prone to identify compounds targeting rather downstream effectors of the pathway, which are indiscriminately used by all the subtypes of the Wnt signaling. Additionally, proteins which are involved in several signaling cascades and not just the Wnt pathway turn out as targets of the new compounds. These issues increase risks of side effects due to off-target interactions and blockade of the pathway in healthy cells. In the present work we put forward a novel biochemical approach for drug development on the Wnt pathway. It targets Frizzleds (Fzs) - a family of 7-transmbembrane proteins which serve as receptors for Wnt ligands. They offer unique properties for the development of highly specific and effective drugs as they control all branches of the Wnt signaling. Recent advances in the understanding of the roles of heterotrimeric G proteins downstream from Fzs (Katanaev et al., 2005; Liu et al., 2005; Jernigan et al., 2010) suggest application of enzymatic properties of these effectors to monitor the receptor-mediated events. We have applied this knowledge in practice and established a specific and efficient method based on utilization of a novel high-throughput format of the GTP-binding assay to follow the activation of Fzs. This type of assay is a robust and well-established technology for the research and screenings on the GPCRs (Harrison and Traynor, 2003). The conventional method of detection involves the radioactively labeled non-hydrolysable GTP analog [35S]GTPyS. Its application in the large-scale screenings is however problematic which promoted development of the novel non-radioactive GTP analog GTP-Eu. The new molecule employs phenomenon of the time-resolved fluorescence to provide sensitivity comparable to the conventional radioactive substance. Initially GTP-Eu was tested only in one of many possible types of GTP-binding assays (Frang et al., 2003). In the present work we expand these limits by demonstrating the general comparability of the novel label with the radioactive method in various types of assays. We provide a biochemical characterization of GTP-Eu interactions with heterotrimeric and small GTPases and a comparative analysis of the behavior of the new label in the assays involving heterotrimeric G protein effectors. These developments in the GTP-binding assay were then applied to monitor G protein activation by the Fz receptors. The data obtained in mammalian cultured cell lines provides for the first time an unambiguous biochemical proof for direct coupling of Fzs with G proteins. The specificity of this interaction has been confirmed by the experiments with the antagonists of Fz and by the pertussis toxin-mediated deactivation. Additionally we have identified the specificity of Wnt3a towards several members of the Fz family and analyzed the properties of human Fz-1 which was found to be the receptor coupled to the Gi/o family of G proteins. Another process playing significant role in the functioning of every GPCR is endocytosis. This phenomenon can also be employed for drug screenings on GPCRs (Bickle, 2010). In the present work we have demonstrated that Drosophila Fz receptors are involved in an unusual for many GPCRs manifestation of the receptor-mediated internalization. Through combination of biochemical approaches and studies on Drosophila as the model organism we have shown that direct interactions of the Fzs and the α-subunit of the heterotrimeric G protein Go with the small GTPase Rab5 regulate internalization of the receptor in early endosomes. We provide data uncovering the decisive role of this self-promoted endocytosis in formation of a proper signaling output in the canonical as well as planar cell polarity (PCP) pathways regulated by Fz. The results of this work thus establish a platform for the high-throughput screening to identify substances active in the cancer-related Wnt pathways. This methodology has been adjusted and applied to provide the important insights in Fz functioning and will be instrumental for further investigations on the Wnt-mediated pathways.

Clinical evaluation of a method for detecting superficial surgical transitional cell carcinoma of the bladder by light-induced fluorescence of protoporphyrin IX following the topical application of 5-aminolevulinic acid: preliminary results.

BACKGROUND AND OBJECTIVE: In bladder cancer, conventional white light endoscopic examination of the bladder does not provide adequate information about the presence of "flat" urothelial lesions such as carcinoma in situ. In the present investigation, we examine a new technique for the photodetection of such lesions by the imaging of protoporphyrin IX (PpIX) fluorescence following topical application of 5-aminolevulinic acid (ALA). STUDY DESIGN/MATERIALS AND METHODS: Several hours after bladder instillation of an aqueous solution of ALA in 34 patients, a Krypton ion laser or a filtered Xenon arc-lamp was used to excite PpIX fluorescence. Tissue samples for histological analysis were taken while observing the bladder wall either by means of a video camera, or by direct endoscopic observation. RESULTS: A good correlation was found between the PpIX fluorescence and the histopathological diagnosis. On a total of 215 biopsies, 143 in fluorescent and 72 in nonfluorescent areas, all visible tumors on white light cytoscopy appeared in a bright red fluorescence with the photodetection technique. In addition, this method permitted to discover 47 unsuspected carcinomatous lesions on white light observation, among which 40% were carcinoma in situ. CONCLUSION: PpIX fluorescence induced by instillation into the bladder of 5-ALA is an efficient method of mapping the mucosa in bladder carcinoma.

Function and regulation of the scaffold protein IB1/JIP-1 in the uro-genital tract.

RESUME Ce mémoire de thèse traite de l'étude de la « scaffold »protéine ou protéine «échafaud», « Islet-Brain1/ JNK Interacting Protein 1 » (IB1/JIP-1) dans la vessie et la prostate, deux organes importants de l'appareil uro-genital. Cette protéine, mise en évidence dans notre laboratoire à la fin des année 90, a été reconnue pour réguler la voie de signalisation des « Mitogen-Activated Protein Kinases » (MAPKs), et en particulier de la MAPK appelée c-Jun N-terminal Kinase (JNK). Le réseau de voie de signalisation permet aux cellules de percevoir les changements dans le milieu extracellulaire et de permettre une réponse appropriée à ces différents stimuli. La connaissance des voies de signalisation a permis de mettre en évidence leur rôle crucial tant dans l'homéostase des tissus sains que dans des processus pathologiques comme l'oncogenèse. Parmi une vingtaine de voie de signalisation, la voie de signalisation des «MAPKinases » est une des plus importantes et a été montrée pour participer à diverses fonctions cellulaires telles que la différentiation, la motilité, la division et la mort cellulaire. La voie de signalisation des « MAPKinases » est typiquement constituée d'un module de trois kinases qui s'activent séquentiellement par phosphorylation. On note la présence d'une MAPK, d'un activateur de MAPK et d'un activateur de l'activateur de MAPK. Une fois la MAPK activée, elle permettra la régulation de différentes cibles dont certain facteur de transcription. Chez les mammifères, il existe 3 grands groupes de MAPKs : the extracellular signal-regulated kinase 1 and 2 (ERK 1/2) cascade, qui régule préférentiellement la croissance et la différentiation cellulaire, ainsi que les cascades JNK et p38 qui régulent préférentiellement la réponse à différents stress cellulaires telle que l'inflammation ou l'apoptose. JNK est activé par différents stress cellulaire telle que les cytokines inflammatoires. JNK est également requis au cours du développement embryonnaire et contribue à la mort (apoptose) ou à la prolifération cellulaire. Plusieurs études ont mis en évidence le rôle de JNK durant le processus tumoral, sans que son rôle soit clairement identifié. JNK pourrait avoir des fonctions différentes durant l'initiation puis de la progression tumorale. Chez les mammifères, les voies de signalisation intracellulaires forment un réseau complexe et elles interagissent entre elles, ce qui permet aux cellules une réponse adéquate aux multitudes de stimuli existants dans les organismes pluricellulaires. Parmi plusieurs mécanismes de régulation, les protéines dites « scaffold » ou «échafaud » jouent un rôle crucial dans l'homéostase de la voie de signalisation des «MAPKinase ». L'introduction revoit brièvement ces différents aspects, de la voie de signalisation des «MAPKinase et des connaissance sur IB1/JIP-1. Les premières études effectuées sur IB1/JIP-1 ont montré une expression relativement spécifique de cette protéine dans certains types de neurones ainsi que dans la cellule beta-sécrétrice d'insuline. IB1/JIP-1 régule la voie de signalisation JNK par interaction avec les différents composants du module, modifiant ainsi le spectre de substrats activés par JNK. La fonction précise de IB1/JIP-1 n'était pas encore élucidée, mais plusieurs travaux mettaient en lumière un rôle dans la régulation, et la sous-location cellulaire des composants de la voie de signalisation JNK, ainsi que dans la survie cellulaire à certain stress. Cette expression relativement spécifique est intrigante car elle suggère que sa présence serait nécessaire à une régulation spécifique de la MAPKinase JNK ou à certaines autres fonctions cellulaires également spécifiques de certains tissus. Le premier but de ce travail a consisté à mettre en évidence l'expression de IB1/JIP-1 dans l'appareil uro-génital et plus particulièrement dans la vessie et la prostate. Nos résultats ont montré que IB1/JIP-1 est spécifiquement exprimé au niveau de l'urothélium vésical, mais pas dans le muscle lisse. Il en est de même au niveau de la prostate où IB1/JIP-1 est exprimé spécifiquement au niveau de l'épithélium sécrétoire et absent au niveau du stroma fibro-musculaire. La vessie et la prostate sont des organes ou l'activité JNK pourrait être crucial tant dans l' homeostase tissulaire que dans le développement de pathologies bénignes ou malignes. La vessie et la prostate sont le siège fréquent de tumeur. La base pour le développement du cancer est complexe et implique plusieurs anomalies génétiques. Ce processus complexe lié au développement tumoral est encore loin d`être complètement élucidé, raison pour laquelle il est crucial de poursuivre l'étude des différents gènes pouvant être impliqué dans ces processus ou pouvant être utilisé comme outil thérapeutique. Dans l'urothelium de la vessie, la fonction de la MAPK JNK n'a été que très peu étudiée. Il existe quelques études, in vitro, suggérant une implication possible de cette voie de signalisation dans des processus telle que le développement ou la progression tumorale. Le chapitre 1 décrit une étude in vivo dans la vessie un modèle de stress mécanique, connu pour activer les MAPKinase. La dilatation vésicale, due à une obstruction urétrale, a mis en évidence une diminution de l'expression de IB1/JIP-1 ainsi qu'une activation de la MAPKinase JNK. Dans ce modèle, la régulation de IB1/JIP-1, par l'intermédiaire d'un vecteur viral, a permis de démontrer que IB1/JIP-1 régulait l'activité de JNK dans ce tissu. Pour poursuivre l'étude de cette fonction d' IB1/JIP-1 dans l'urothélium, nous avons investigué l'activité JNK dans des souris génétiquement modifiées et porteuse d'une délétion de 1 des 2 allèles du gène codant pour IB1/JIP-1, avec un contenu en IB1/JIP-1 diminué de moitié. L'activation de JNK est également augmentée dans l'urothelium au repos de ces souris, ce qui confirme la fonction régulatrice de JNK par IB1/JIP-1. Ces résultats ont permis de mettre en évidence un rôle critique de celle-ci dans l'homéostase de I`urothelium et suggère une nouvelle cible pour réguler la voie de signalisation dans ce tissu. En outre, la modulation des niveaux d'expression d'IB1/JIP-1 dans la vessie, in vivo, par l'intermédiaire de vecteurs viraux s'est révélée réalisable et indique un moyen élégant pour développer une thérapie génique dans cet organe. Un autre élément de ce travail de thèse, révélée au chapitre 2, a été d'étudier la régulation dans la vessie de rat de la communication intercellulaire de type « GAP ». Les cellules adjacentes partagent des ions, messagers secondaires et des petits métabolites par l'intermédiaire de canaux intercellulaire qui forment les jonctions de type « GAP ». Ce type de communications intercellulaire permet une activité cellulaire coordonnée, une caractéristique importante pour l'homéostase des organismes multicellulaire. Ce type de communication intercellulaire est formé de 2 demi-canaux appelés connexons. Chaque connexon est formé de six protéines appelées connexins (Cx). Il existe environ vingt connexines différentes nommées par leur poids moléculaire respectif. Les jonctions de type canaux "GAP" permettent aux cellules de communiquer avec les cellules voisines au quelles elles sont mécaniquement ou électriquement couplées. La vessie peut être particulièrement dépendante de la communication intercellulaire par les canaux « Gap » qui permettrait de coordonner la réponse de la musculature ainsi que de l'urothélium à l'augmentation de la pression transmurale du à l'accumulation d'urine, situation fréquemment observée dans le cadre de l'hyperplasie bénigne de la prostate. Dans la vessie de rat, la connexine26 est exprimée uniquement dans l'urothelium. La Cx26, a été montrée pour être un possible « tumor suppressor gene » dans le cancer de vessie. Une augmentation de la Cx26 ainsi que du couplage des cellules urothéliales a été démontré dans notre modèle de stress mécanique sur la vessie de rat et est dépendante de 2 éléments de réponses connues pour interagir avec AP-1. La régulation de IB1/JIP-1 a permis de montrer que celle-ci régulait l'activité JNK, ainsi que l'activité du facteur de transcription AP-1, composé de c-Jun lui-même cible de JNK. Cette réduction de l'activité de AP-1 est associée à une diminution de l'expression du transcipt de la Cx26. En résumé, la Cx26 pourrait être régulée par le complexe AP-1 lui-même dépendant du contenu en IB1/JIP-1. Dans le chapitre 3, l'étude de IB1/J1P-1 s'est portée sur la prostate. Cet organe, siège fréquent de pathologie telle que le cancer ou l'hyperplasie bénigne de la prostate, exprime IB1/JIP-1 au niveau de son épithélium sécrétoire. Cette expression est maintenue dans une lignée cellulaire humaine largement étudiée est reconnue comme un modèle adéquat de cellules tumorales de type androgène-sensible. IB1/JIP-1 a été investigué dans un modèle in vitro d'apoptose en réponse à un agent appelé N-(4-hydroxyphenyl)retinamide (4-HPR) qui induit une activation de la MAPK JNK ainsi que également un diminution du contenu en IB1/JIP-1. La surexpression de IB1/JIP-1 en utilisant à nouveau des virus comme vecteur a démontré que IB1/JIP-1 était capable de réguler l'activité de JNK ainsi que les taux d'apoptose. Dans le cancer de la prostate, certains travaux ont montré que la différentiation neuroendocrine des cellules tumorales est associée à la progression tumorale et à la perte de sensibilité aux androgènes. Ce travail a permis de dévoiler l'augmentation d'expression de IB1/JIP-1 dans un modèle de neurodifferentiation des cellules d'une lignée prostatique humaine (LNCaP). Les mécanismes qui permettent une expression spécifique de IB1/JIP-1 ont été partiellement investiguée dans notre laboratoire. Son promoteur humain contient un « Neuron Restricive Silencer Element » (NRSE) connu pour se lier a répresseur transcriptionel appelé « RE-1 Silencer Transcription Factor » ou « Neuron Restrictive Silencer Factor » (REST/NRSF). NRSF/REST est capable de réprimer l'expression de gènes neuronaux en dehors du système neuronal. Il prend part à la différentiation terminale des gènes neuronaux. Dans le chapitre 3, on observe que l'activité de REST/NRSF est diminuée dans les cellules LNCaP qui se transdifferencient de manière neuroendocrine, et que REST/NRSF est capable de moduler l'expression de ces gènes cibles dans ce type cellulaire. Ces travaux laissent suggérer que NRSF/REST participe à l'acquisition du phénotype neuroendocrinien et pourrait être une cible pour réguler ce phénomène. En conclusion, ce travail de thèse présente l'expression de IB1/JIP-1 dans 2 organes de l'appareil uro-génital ; la vessie et la prostate. La fonction de IB1/JIP-1 a été étudiée in vivo dans la vessie de rat, ce qui a mis en évidence sa fonction régulatrice de l'activité de la MAPKinase JNK, et de l'activité du facteur de transcription AP-1 ; ainsi que sa possible implication régulatrice de gène cible tel que la Connexin 26 (Cx26). AP-1 et la Cx26 pourraient jouer un rôle dans le processus oncologique, tant dans le control de l'invasion cellulaire ou le control de la croissance cellulaire. Dans la prostate, IB1/JIP-1 régule également l'activité JNK; crucial dans la transmission de certains stimulis pro-apoptotiques. Dans un modèle de transdifférenciation neuroendocrinienne, phénotype possiblement lié au caractère agressif du cancer de la prostate, l'expression de IB1/JIP-1 est augmenté, suggérant soit un rôle possible dans le développement du phénotype neuronal ou une implication dans une fonction anti-apoptotique. Ce travail a donc permis d'élargir nos connaissances sur la régulation et le control de la voie de signalisation des MAPKinases par IB1/JIP-1, qui pourrait avoir encore d'autres fonctions dans ces tissus.

Macronutrient composition of the diet and prospective weight change in participants of the EPIC-PANACEA study.

BACKGROUND The effect of the macronutrient composition of the usual diet on long term weight maintenance remains controversial. METHODS 373,803 subjects aged 25-70 years were recruited in 10 European countries (1992-2000) in the PANACEA project of the EPIC cohort. Diet was assessed at baseline using country-specific validated questionnaires and weight and height were measured at baseline and self-reported at follow-up in most centers. The association between weight change after 5 years of follow-up and the iso-energetic replacement of 5% of energy from one macronutrient by 5% of energy from another macronutrient was assessed using multivariate linear mixed-models. The risk of becoming overweight or obese after 5 years was investigated using multivariate Poisson regressions stratified according to initial Body Mass Index. RESULTS A higher proportion of energy from fat at the expense of carbohydrates was not significantly associated with weight change after 5 years. However, a higher proportion of energy from protein at the expense of fat was positively associated with weight gain. A higher proportion of energy from protein at the expense of carbohydrates was also positively associated with weight gain, especially when carbohydrates were rich in fibre. The association between percentage of energy from protein and weight change was slightly stronger in overweight participants, former smokers, participants ≥60 years old, participants underreporting their energy intake and participants with a prudent dietary pattern. Compared to diets with no more than 14% of energy from protein, diets with more than 22% of energy from protein were associated with a 23-24% higher risk of becoming overweight or obese in normal weight and overweight subjects at baseline. CONCLUSION Our results show that participants consuming an amount of protein above the protein intake recommended by the American Diabetes Association may experience a higher risk of becoming overweight or obese during adult life.

Fluorodeoxyglucose-positron emission tomography scan-positive recurrent papillary thyroid cancer and the prognosis and implications for surgical management.

BACKGROUND To compare outcomes for patients with recurrent or persistent papillary thyroid cancer (PTC) who had metastatic tumors that were fluorodeoxyglucose-positron emission tomography (FDG-PET) positive or negative, and to determine whether the FDG-PET scan findings changed the outcome of medical and surgical management. METHODS From a prospective thyroid cancer database, we retrospectively identified patients with recurrent or persistent PTC and reviewed data on demographics, initial stage, location and extent of persistent or recurrent disease, clinical management, disease-free survival and outcome. We further identified subsets of patients who had an FDG-PET scan or an FDG-PET/CT scan and whole-body radioactive iodine scans and categorized them by whether they had one or more FDG-PET-avid (PET-positive) lesions or PET-negative lesions. The medical and surgical treatments and outcome of these patients were compared. RESULTS Between 1984 and 2008, 41 of 141 patients who had recurrent or persistent PTC underwent FDG-PET (n = 11) or FDG-PET/CT scans (n = 30); 22 patients (54%) had one or more PET-positive lesion(s), 17 (41%) had PET-negative lesions, and two had indeterminate lesions. Most PET-positive lesions were located in the neck (55%). Patients who had a PET-positive lesion had a significantly higher TNM stage (P = 0.01), higher age (P = 0.03), and higher thyroglobulin (P = 0.024). Only patients who had PET-positive lesions died (5/22 vs. 0/17 for PET-negative lesions; P = 0.04). In two of the seven patients who underwent surgical resection of their PET-positive lesions, loco-regional control was obtained without evidence of residual disease. CONCLUSION Patients with recurrent or persistent PTC and FDG-PET-positive lesions have a worse prognosis. In some patients loco-regional control can be obtained without evidence of residual disease by reoperation if the lesion is localized in the neck or mediastinum.

L'hypnose: une ressource en soins palliatifs? Etude qualitative sur l'apport de l'hypnose chez des patients oncologique.s [Hypnosis as a resource in palliative care. A qualitative study of the contribution of hypnosis to the care of oncology patients].

Hypnosis is recognised in medicine as an effective complementary therapy. However, few qualitative data are available concerning the benefits it may bring. This qualitative exploratory study aimed to examine the contribution of hypnosis to the care of advanced cancer patients. Results demonstrate that hypnosis is an effective and efficient means of developing the resources of people suffering from serious illness. After an average of four hypnotherapy sessions, patients said they were able to locate previously unexploited resources within themselves and were able to become autonomous in the use of self-hypnosis. The major benefit reported concerned a reduction in anxiety. For patients experiencing anxiety about death, hypnosis allowed them, within a therapeutic environment perceived as safe, to explore different facets of their fears and to develop adaptive strategies. Aside from slight fatigue experienced during the sessions, no adverse side-effects were reported. In conclusion, this study exploring the effects of hypnosis allowed us to identify important benefits for patients suffering from advanced cancer. Consequently, replication on a larger scale is recommended in order to ascertain the extent to which it is possible to generalise from these results and in order better to define the characteristics of patients most likely to benefit from this therapy.

Vaccination against human papillomavirus in Switzerland: simulation of the impact on infection rates.

OBJECTIVES: Human papillomavirus (HPV) is a sexually transmitted infection of particular interest because of its high prevalence rate and strong causal association with cervical cancer. Two prophylactic vaccines have been developed and different countries have made or will soon make recommendations for the vaccination of girls. Even if there is a consensus to recommend a vaccination before the beginning of sexual activity, there are, however, large discrepancies between countries concerning the perceived usefulness of a catch-up procedure and of boosters. The main objective of this article is to simulate the impact on different vaccination policies upon the mid- and long-term HPV 16/18 age-specific infection rates. METHODS: We developed an epidemiological model based on the susceptible-infective-recovered approach using Swiss data. The mid- and long-term impact of different vaccination scenarios was then compared. RESULTS: The generalization of a catch-up procedure is always beneficial, whatever its extent. Moreover, pending on the length of the protection offered by the vaccine, boosters will also be very useful. CONCLUSIONS: To be really effective, a vaccination campaign against HPV infection should at least include a catch-up to early reach a drop in HPV 16/18 prevalence, and maybe boosters. Otherwise, the protection insured for women in their 20s could be lower than expected, resulting in higher risks to later develop cervical cancer.

Infrequent promoter methylation of the MGMT gene in liver metastases from uveal melanoma.

Uveal melanoma is associated with a high mortality rate once metastases occur, with over >90% of metastatic patients dying within less than 1 year from metastases to the liver. The intraarterial hepatic (iah) administration of the alkylating agent fotemustine holds some promise with response rates of 36% and median survival of 15 months. Here, we investigated whether the DNA-repair-protein MGMT may be involved in the variability of response to fotemustine and temozolomide in uveal melanoma. Epigenetic inactivation of MGMT has been demonstrated to be a predictive marker for benefit from alkylating agent therapy in glioblastoma. We found a methylated MGMT promoter in 6% of liver metastases from 34 uveal melanoma patients. The mean MGMT activity measured in liver metastases with negligible liver tissue content was significantly lower than in liver tissue (146 versus 523 fmol/mg protein, p = 0.002). Expression of the MGMT protein was detectable in 50% of 88 metastases by immunohistochemistry on a tissue microarray. Expression was heterogeneous, and in accordance with MGMT activity data, usually lower than in the surrounding liver. Differential MGMT activity/expression between metastasis and liver tissue and more efficient depletion of MGMT with higher doses of alkylating agent therapy using iah delivery may provide the pharmacologic window for the higher response rate. However, these results do not support MGMT methylation status or protein expression as predictive markers for treatment outcome to iah chemotherapy with alkylating agents.

Evaluation of the antitumoral effect sunitinib eluting beads in VX2 liver tumour in a rabbit model.

Background: We demonstrated that DC Bead (Biocompatibles UK, Ltd) could be loaded with sunitinib and injected intra-arterially in the rabbit without unexpected toxicity. The purpose of this study is to evaluate the antitumoral effect of sunitinib eluting beads in the VX2 tumor model of liver cancer. Methods: VX2 tumors were implanted in the left liver lobe of New-Zealand white rabbits. Animals were assigned to 3 groups: Group 1 (n=6) received 1.5mg of sunitinib loaded in 0.05ml of 100-300um DC Bead, group 2 (n=5) received 0.05ml of 100-300um DC Bead, group 3 (n=5) received 0.05ml NaCl 0.9% in the left hepatic artery. One animal in each group was sacrificed at 24 hours and the others were followed for survival until day 15. Liver enzymes were measured daily. In group 1, plasmatic sunitinib concentration were measured daily by LC MS/MS tandem mass spectroscopy. At day 15 all living animals were sacrificed. After sacrifice, the livers were harvested for determination of the VEGF receptor tyrosine kinase activity by western blot and histopathological examination. Results: In group 1, no animals died during follow-up. In group 2, 2 animals died during follow-up on day x. In control group 3, 3 animals died during follow up on day x. In group 1 plasmatic sunitinib levels remained under therapeutic concentration throughout the experiment. Very high concentrations of sunitinib were measured in the liver tissue 24 and 15 days after embolization. Inhibition of the phosphorylation of the RTK was demonstrated at 24h and 15 days in groups 1. Sunitinib eluting beads seemed to penetrate in the tumor more effectively and there was more necrosis around the beads than their bland counterparts. Conclusions: Administration of sunitinib eluting beads in VX2 carrying rabbits resulted invery high drug concentrations at the site of embolization with minimal systemic passage. Despite the very high tissular sunitinib concentration we did not observe any additional toxicity with loaded beads. Sunitinib eluting beads inhibit the activation of RTK's triggered by ischemia and seem to prolong survival of the treated animals. Therefore we consider that local treatment with sunitinib may provide a promising approach for the treatment of liver cancer.

Optical spectroscopy of the bladder washout fluid to optimize fluorescence cystoscopy with Hexvix®.

Fluorescence cystoscopy enhances detection of early bladder cancer. Water used to inflate the bladder during the procedure rapidly contains urine, which may contain fluorochromes. This frequently degradesfluorescence images. Samples of bladder washout fluid (BWF) or urine were collected (15 subjects). We studiedtheir fluorescence properties and assessed changes induced by pH (4 to 9) and temperature (15°C to 41°C).A typical fluorescence spectrum of BWF features a main peak (excitation/emission: 320∕420 nm, FWHM =50∕100 nm) and a weaker (5% to 20% of main peak intensity), secondary peak (excitation/emission: 455∕525 nm, FWHM = 80∕50 nm). Interpatient fluctuations of fluorescence intensity are observed. Fluorescence intensity decreases when temperature increases (max 30%) or pH values vary (max 25%). Neither approach is compatible with clinical settings. Fluorescence lifetime measurements suggest that 4-pyridoxic acid/riboflavin is the most likely molecule responsible for urine's main/secondary fluorescence peak. Our measurements give an insight into the spectroscopy of the detrimental background fluorescence. This should be included in the optical design of fluorescence cystoscopes. We estimate that restricting the excitation range from 370-430 nm to 395-415 nm would reduce the BWF background by a factor 2.

Die Reichweite von Theorien als Indikator für ihre Umsetzbarkeit in der Praxis [The scope as an indicator of the applicability of nursing theories to practice]

In der Pflegewissenschaft geben der Einsatz von Theorien und der daraus folgende Gewinn immer wieder Anlass zu Diskussionen. Ein Hauptvorwurf ist, dass Pflegetheorien als sehr abstrakt und wenig praxisnah gelten. Jedoch gibt es wenige Indikatoren, um das Abstraktionsniveau von Theorien und die damit verbundene Reichweite zu bestimmen. Im vorliegenden Artikel werden Fragen basierend auf die Definitionen und Grundannahmen von Theorien erstellt. Damit werden anschließend drei ausgesuchte Theorien auf ihr Abstraktionsniveau und Reichweite untersucht. Es wurden 18 Fragen zu den drei Bereichen ,,Zweck der Theorie", ,,Aufgabe der Theorie" und ,,Beschreibung der Theorie" entwickelt. Diese 18 Fragen wurden auf die Theorie der Adaptation von Sister Callista Roy, die Theorie zur Unsicherheit von Merle M. Mishel und die Theorie der Omnipräsenz von Krebs von Maya Shaha angewendet. [The use of nursing theories and their associated benefits remain an area of repeated discussion in nursing. One of the main objections is that nursing theories are abstract and therefore cannot be easily applied to practice. However, only few indicators exist to help identify a theory's level of abstraction or its scope. In this article, questions based on definitions and assumptions of theories have been developed. These questions have then been applied to three selected theories to investigate their level of abstraction and scope. A total of 18 questions divided into three domains were developed. The three categories were: ,,the purpose of the theory", ,,the aim of the theory" and ,,the description of the theory". The theory of Adaptation by Sister Callista Roy, the Theory of Uncertainty by Merle M. Mishel and the Theory of the Omnipresence of Cancer by Maya Shaha were selected to be analysed following the three domains with the 18 questions.]

Study of the effectiveness of first-line treatment in renal cell carcinoma.

The emergence of novel drugs corresponds with the determination of the effectiveness of the current treatments used in clinical practice. A retrospective observational study was conducted to evaluate the effectiveness of first-line treatments and to test the influence of the prognostic factors established using the Memorial Sloan-Kettering Cancer Center (MSKCC) and the analysis of Mekhail's study for two or more metastatic sites. The primary endpoints were median progression-free survival (mPFS) and median overall survival (mOS) times. A total of 65 patients were enrolled and the mPFS and mOS of the patients treated with sunitinib (n=51) were 9.0 and 20.1 months, respectively, and for the patients treated with temsirolimus (n=14) these were 3.0 and 6.2 months, respectively. In the poor-prognosis (PP) group, a difference of 1.2 months (P=0.049) was found in mPFS depending on the first-line treatment. A difference of 4.1 months (P=0.023) was also found in mPFS when classified by histology (clear verses non-clear cell) in the sunitinib-treatment group. When stratified by the prognostic group, differences of >7 months (P<0.001) were found between the groups. Therefore, it was concluded that the effectiveness of the treatments was reduced compared to previous studies and differences were found in the PP group when classified by first-line drug and histology. Additionally, the influence of prognostic factors on OS and the value of stratifying patients using these factors have been confirmed.

Evaluation of the efficacy and safety of lanreotide in combination with targeted therapies in patients with neuroendocrine tumours in clinical practice: a retrospective cross-sectional analysis.

BACKGROUND Based on the mechanism of action, combining somatostatin analogues (SSAs) with mTOR inhibitors or antiangiogenic agents may provide synergistic effects for the treatment of patients with neuroendocrine tumours (NETs). Herein, we investigate the use of these treatment combinations in clinical practice. METHODS This retrospective cross-sectional analysis of patients with NETs treated with the SSA lanreotide and targeted therapies at 35 Spanish hospitals evaluated the efficacy and safety of lanreotide treatment combinations in clinical practice. The data of 159 treatment combinations with lanreotide in 133 patients was retrospectively collected. RESULTS Of the 133 patients, with a median age of 59.4 (16-83) years, 70 (52.6 %) patients were male, 64 (48.1 %) had pancreatic NET, 23 (17.3 %) had ECOG PS ≥2, 41 (30.8 %) had functioning tumours, 63 (47.7 %) underwent surgery of the primary tumour, 45 (33.8 %) had received prior chemotherapy, and 115 (86.5 %) had received prior SSAs. 115 patients received 1 lanreotide treatment combination and 18 patients received between 2 and 5 combinations. Lanreotide was mainly administered in combination with everolimus (73 combinations) or sunitinib (61 combinations). The probability of being progression-free was 78.5 % (6 months), 68.6 % (12 months) and 57.0 % (18 months) for patients who only received everolimus plus lanreotide (n = 57) and 89.3 % (6 months), 73.0 % (12 months), and 67.4 % (18 months) for patients who only received sunitinib and lanreotide (n = 50). In patients who only received everolimus plus lanreotide the median time-to-progression from the initiation of lanreotide combination treatment was 25.8 months (95 % CI, 11.3, 40.3) and it had not yet been reached among the subgroup of patients only receiving sunitinib plus lanreotide. The safety profile of the combination treatment was comparable to that of the targeted agent alone. CONCLUSIONS The combination of lanreotide and targeted therapies, mainly everolimus and sunitinib, is widely used in clinical practice without unexpected toxicities and suggests efficacy that should be explored in randomized prospective clinical trials.

Use of the comet test to assess DNA damage in children with ataxia-telangiectasia and their relatives.

The electrophoresis of cells in alkaline medium (comet assay) is a valid technique for quantifying DNA damage in patients with ataxia-telangiectasia and their relatives.

New insights into the role of the immune microenvironment in breast carcinoma.

Recently, immune edition has been recognized as a new hallmark of cancer. In this respect, some clinical trials in breast cancer have reported imppressive outcomes related to laboratory immune findings, especially in the neoadjuvant and metastatic setting. Infiltration by tumor infiltrating lymphocytes (TIL) and their subtypes, tumor-associated macrophages (TAM) and myeloid-derived suppressive cells (MDSC) seem bona fide prognostic and even predictive biomarkers, that will eventually be incorporated into diagnostic and therapeutic algorithms of breast cancer. In addition, the complex interaction of costimulatory and coinhibitory molecules on the immune synapse and the different signals that they may exert represent another exciting field to explore. In this review we try to summarize and elucidate these new concepts and knowledge from a translational perspective focusing on breast cancer, paying special attention to those aspects that might have more significance in clinical practice and could be useful to design successful therapeutic strategies in the future.