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6. A comparison of the imaging characteristics of the new Kodak Hyper Speed G film with the current T-MAT G/RA film and the CR 9000 system

Author

P. Monnin, Francis R. Verdun, D. Lepori, Bulling S, and Daniel Gutierrez

Subjects
Materials science, Radiological and Ultrasound Technology, business.industry, Image quality, X-Ray Film, Resolution (electron density), Phosphor, Radiation, Noise (electronics), Detective quantum efficiency, Optics, Radiographic Image Interpretation, Computer-Assisted, X-Ray Intensifying Screens, Radiology, Nuclear Medicine and imaging, business, Exposure latitude
Abstract

Three standard radiation qualities (RQA 3, RQA 5 and RQA 9) and two screens, Kodak Lanex Regular and Insight Skeletal, were used to compare the imaging performance and dose requirements of the new Kodak Hyper Speed G and the current Kodak T-MAT G/RA medical x-ray films. The noise equivalent quanta (NEQ) and detective quantum efficiencies (DQE) of the four screen-film combinations were measured at three gross optical densities and compared with the characteristics for the Kodak CR 9000 system with GP (general purpose) and HR (high resolution) phosphor plates. The new Hyper Speed G film has double the intrinsic sensitivity of the T-MAT G/RA film and a higher contrast in the high optical density range for comparable exposure latitude. By providing both high sensitivity and high spatial resolution, the new film significantly improves the compromise between dose and image quality. As expected, the new film has a higher noise level and a lower signal-to-noise ratio than the standard film, although in the high frequency range this is compensated for by a better resolution, giving better DQE results--especially at high optical density. Both screen-film systems outperform the phosphor plates in terms of MTF and DQE for standard imaging conditions (Regular screen at RQA 5 and RQA 9 beam qualities). At low energy (RQA 3), the CR system has a comparable low-frequency DQE to screen-film systems when used with a fine screen at low and middle optical densities, and a superior low-frequency DQE at high optical density.

Published
2005
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8. A comparison of the performance of modern screen-film and digital mammography systems

Author

Jean-François Valley, P. Monnin, D. Lepori, Daniel Gutierrez, Francis R. Verdun, and Bulling S

Subjects
Materials science, Digital mammography, Radiological and Ultrasound Technology, medicine.diagnostic_test, Pixel, business.industry, Image quality, Phantoms, Imaging, X-Ray Film, Detector, Resolution (electron density), Detective quantum efficiency, Optics, medicine, Image Processing, Computer-Assisted, Mammography, Radiology, Nuclear Medicine and imaging, Nyquist frequency, business, Nuclear medicine, Algorithms, Software
Abstract

This work compares the detector performance and image quality of the new Kodak Min-R EV mammography screen-film system with the Fuji CR Profect detector and with other current mammography screen-film systems from Agfa, Fuji and Kodak. Basic image quality parameters (MTF, NPS, NEQ and DQE) were evaluated for a 28 kV Mo/Mo (HVL = 0.646 mm Al) beam using different mAs exposure settings. Compared with other screen-film systems, the new Kodak Min-R EV detector has the highest contrast and a low intrinsic noise level, giving better NEQ and DQE results, especially at high optical density. Thus, the properties of the new mammography film approach those of a fine mammography detector, especially at low frequency range. Screen-film systems provide the best resolution. The presampling MTF of the digital detector has a value of 15% at the Nyquist frequency and, due to the spread size of the laser beam, the use of a smaller pixel size would not permit a significant improvement of the detector resolution. The dual collection reading technology increases significantly the low frequency DQE of the Fuji CR system that can at present compete with the most efficient mammography screen-film systems.

Published
2005

15. Abstracts from the 8th Annual Meeting of the Scientific Association of Swiss Radiation Oncology (SASRO)

Author

Allal, A. S., primary, Ares, C., additional, Dulguerov, P., additional, Tschanz, E., additional, Verdan, C., additional, Mhawech, P., additional, Riesterer, O., additional, Honer, M., additional, Vuong, V., additional, Jochum, W., additional, Zingg, D., additional, Bodis, S., additional, Ametamey, S., additional, Pruschy, M., additional, Inteeworn, N., additional, Ohlerth, S., additional, Höpfl, G., additional, Roos, M., additional, Wergin, M., additional, Rohrer Bley, C., additional, Gassmann, M., additional, Kaser-Hotz, B., additional, Berthou, S., additional, Aebersold, D. M., additional, Ganapathipillai, S., additional, Streit, B., additional, Stalder, D., additional, Gruber, G., additional, Greiner, R. H., additional, Zimmer, Y., additional, Lutters, G., additional, Krek, W., additional, Tenzer, A., additional, Hofstetter, B., additional, Bonny, C., additional, Azria, A., additional, Larbouret, C., additional, Cunat, S., additional, Ozsahin, M., additional, Zouhair, A., additional, Gourgou, S., additional, Martineau, P., additional, Evans, D. B., additional, Romieu, G., additional, Pujol, P., additional, Pèlegrin, A., additional, Heuberger, J., additional, Kestenholz, P., additional, Taverna, Ch., additional, Lardinois, D., additional, Jörger, M., additional, Schneiter, D., additional, Jerman, M., additional, Weder, W., additional, Stahel, R., additional, Bodis, St., additional, Vees, H., additional, Mach, N., additional, Hügli, A., additional, Balmer Majno, S., additional, Beer, K. T., additional, Friedrich, E. E., additional, Ciernik, I. F., additional, Stanek, N., additional, Taverna, C., additional, Greiner, R., additional, Mahler, F., additional, Landmann, Ch., additional, Studer, G., additional, Bernier, J., additional, Gallino, A., additional, Juelke, Peter D., additional, Hafner, Hans-Peter, additional, Jamshidi, Peiman, additional, Erne, Paul, additional, Resink, Therese Josephine, additional, Thum, Peter, additional, Notter, M., additional, Bargetzi, M., additional, Suleiman, M., additional, Luthi, J. C., additional, Bieri, S., additional, Curschmann, J., additional, Pajic, B., additional, Kranzbühler, H., additional, Lippold, B., additional, Ueltschi, G., additional, Bonetti, M., additional, Nasi, M. L., additional, Price, K. N., additional, Castiglione-Gertsch, M., additional, Rudenstam, C.-M., additional, Holmberg, S. B., additional, Lindtner, J., additional, Gol-ouh, R., additional, Collins, J., additional, Crivellari, D., additional, Carbone, A., additional, Thürlimann, B., additional, Simoncini, E., additional, Fey, M. F., additional, Gelber, R. D., additional, Coates, A. S., additional, Goldhirsch, A., additional, Jeanneret Sozzi, W., additional, Kramar, A., additional, Mirimanoff, R. O., additional, Azria, D., additional, Taussky, D., additional, Becker, M., additional, Kranzbuehler, H., additional, Weitzel, M., additional, Bortoluzzi, L., additional, Behrensmeier, F., additional, Isaak, B., additional, Pasche, P., additional, Luthi, F., additional, Weber, D. C., additional, Lomax, A. J., additional, Rutz, H. P., additional, Pedroni, E. S., additional, Verwey, J., additional, Goitein, G., additional, Timmermann, B., additional, Lomax, A., additional, Bolsi, A., additional, Weber, D., additional, Bentzen, S. M., additional, Khalil, A. A., additional, Saunders, M. I., additional, Horiot, J. C., additional, Van den Bogaert, W., additional, Cummings, B. J., additional, Dische, S., additional, Slosman, D. O., additional, Kebdani, T., additional, Allaoua, M., additional, Stadelmann, O., additional, Stupp, R., additional, Pica, A., additional, Dubois, J. B., additional, Oehler, C., additional, Ulmer, U., additional, Lütolf, U. M., additional, Huser, M., additional, Burger, C., additional, Szekely, G., additional, Davis, J. B., additional, Gervaz, P., additional, Gertsch, P., additional, Morel, Ph., additional, Roth, A. D., additional, Zenklusen, H., additional, Schott, A., additional, Curti, G., additional, Schefer, H., additional, Kolotas, C., additional, Thalmann, G., additional, Vetterli, D., additional, Kemmerling, L., additional, Mini, R., additional, Rouzaud, M., additional, Nouet, P., additional, Mollà, M., additional, Escudé, L., additional, Miralbell, R., additional, Beer, K., additional, von Briel, C., additional, Jichlinski, P., additional, Guillou, L., additional, Fogliata, A., additional, Nicolini, G., additional, Cozzi, L., additional, Hafner, H. P., additional, Hueber, P., additional, Szczerba, D., additional, Born, E. J., additional, Dipasquale, G., additional, Jargy, C., additional, Munier, F., additional, Balmer, A., additional, Do, H. P., additional, Pasche, G., additional, Wang, H., additional, Moeckli, R., additional, Boehringer, T., additional, Coray, A., additional, Lin, S., additional, Pedroni, E., additional, Rutz, H., additional, Baumert, B. G., additional, Norton, I. A., additional, Schoenmaker, E., additional, Krayenbühl, J., additional, Bründler, M.-A., additional, Allemann, K., additional, Laluhovà, D., additional, Collen, T., additional, Coucke, P., additional, Ries, G., additional, Rufibach, K., additional, Huguenin, P., additional, Abdou, M., additional, Girardet, C., additional, Vees, H. J., additional, Bigler, R., additional, Özsoy, O., additional, Bouville, S., additional, Corminboeuf, F., additional, Betz, M., additional, Matzinger, O., additional, Tebeu, P., additional, Popowski, Y., additional, Verkooijen, H., additional, Bouchardy, C., additional, Ludicke, F., additional, Usel, M., additional, Major, A., additional, Merçay, A., additional, Pache, G., additional, Bulling, S., additional, Bressan, S., additional, Valley, J. F., additional, Motta, M., additional, Presilla, S., additional, Richetti, A., additional, Franzetti, A., additional, and Pesce, G., additional

Published
2004
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17. Mephedrone induces partial release at human dopamine transporters but full release at human serotonin transporters.

Author

Mayer FP, Niello M, Bulling S, Zhang YW, Li Y, Kudlacek O, Holy M, Kooti F, Sandtner W, Rudnick G, Schmid D, and Sitte HH

Subjects
Humans, HEK293 Cells, Central Nervous System Stimulants pharmacology, Dose-Response Relationship, Drug, Serotonin Plasma Membrane Transport Proteins metabolism, Serotonin Plasma Membrane Transport Proteins drug effects, Dopamine Plasma Membrane Transport Proteins metabolism, Dopamine Plasma Membrane Transport Proteins drug effects, Methamphetamine pharmacology, Methamphetamine analogs & derivatives
Abstract

Mephedrone (4-methylmethcathinone) is a cathinone derivative that is recreationally consumed for its energizing and empathogenic effects. The stimulating properties are believed to arise from the ability of mephedrone to interact with the high-affinity transporters for dopamine (DA) (DAT) and norepinephrine (NET), whereas the entactogenic effect presumably relies on its activity at the serotonin (5-HT) transporter (SERT). Early studies found that mephedrone acts as a releaser at NET, DAT and SERT, and thus promotes efflux of the respective monoamines. Evidence linked drug-induced reverse transport of 5-HT via SERT to prosocial effects, whereas activity at DAT is strongly correlated with abuse liability. Consequently, we sought to evaluate the pharmacology of mephedrone at human (h) DAT and SERT, heterologously expressed in human embryonic kidney 293 cells, in further detail. In line with previous studies, we report that mephedrone evokes carrier-mediated release via hDAT and hSERT. We found this effect to be sensitive to the protein kinase C inhibitor GF109203X. Electrophysiological recordings revealed that mephedrone is actively transported by hDAT and hSERT. However, mephedrone acts as a full substrate of hSERT but as a partial substrate of hDAT. Furthermore, when compared to fully efficacious releasing agents at hDAT and hSERT (i.e. S(+)-amphetamine and para-chloroamphetamine, respectively) mephedrone displays greater efficacy as a releaser at hSERT than at hDAT. In summary, this study provides additional insights into the molecular mechanism of action of mephedrone at hDAT and hSERT., Competing Interests: Declaration of competing interest None., (Copyright © 2023 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published
2023
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18. Serotonin-releasing agents with reduced off-target effects.

Author

Mayer FP, Niello M, Cintulova D, Sideromenos S, Maier J, Li Y, Bulling S, Kudlacek O, Schicker K, Iwamoto H, Deng F, Wan J, Holy M, Katamish R, Sandtner W, Li Y, Pollak DD, Blakely RD, Mihovilovic MD, Baumann MH, and Sitte HH

Subjects
Brain, Carrier Proteins, Serotonin, Dopamine
Abstract

Increasing extracellular levels of serotonin (5-HT) in the brain ameliorates symptoms of depression and anxiety-related disorders, e.g., social phobias and post-traumatic stress disorder. Recent evidence from preclinical and clinical studies established the therapeutic potential of drugs inducing the release of 5-HT via the 5-HT-transporter. Nevertheless, current 5-HT releasing compounds under clinical investigation carry the risk for abuse and deleterious side effects. Here, we demonstrate that S-enantiomers of certain ring-substituted cathinones show preference for the release of 5-HT ex vivo and in vivo, and exert 5-HT-associated effects in preclinical behavioral models. Importantly, the lead cathinone compounds (1) do not induce substantial dopamine release and (2) display reduced off-target activity at vesicular monoamine transporters and 5-HT 2B -receptors, indicative of low abuse-liability and low potential for adverse events. Taken together, our findings identify these agents as lead compounds that may prove useful for the treatment of disorders where elevation of 5-HT has proven beneficial., (© 2022. The Author(s).)

Published
2023
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19. Case Report: Treatment Planning Study to Demonstrate Feasibility of Transthoracic Ultrasound Guidance to Facilitate Ventricular Tachycardia Ablation With Protons.

Author

Perrin R, Maguire P, Garonna A, Weidlich G, Bulling S, Fargier-Voiron M, De Marco C, Rossi E, Ciocca M, Vitolo V, and Mirandola A

Abstract

Background: Cardiac arrhythmias, such as ventricular tachycardia, are disruptions in the normal cardiac function that originate from problems in the electrical conduction of signals inside the heart. Recently, a non-invasive treatment option based on external photon or proton beam irradiation has been used to ablate the arrhythmogenic structures. Especially in proton therapy, based on its steep dose gradient, it is crucial to monitor the motion of the heart in order to ensure that the radiation dose is delivered to the correct location. Transthoracic ultrasound imaging has the potential to provide guidance during this treatment delivery. However, it has to be noted that the presence of an ultrasound probe on the chest of the patient introduces constraints on usable beam angles for both protons and photon treatments. This case report investigates the possibility to generate a clinically acceptable proton treatment plan while the ultrasound probe is present on the chest of the patient., Case: A treatment plan study was performed based on a 4D cardiac-gated computed tomography scan of a 55 year-old male patient suffering from refractory ventricular tachycardia who underwent cardiac radioablation. A proton therapy treatment plan was generated for the actual treatment target in presence of an ultrasound probe on the chest of this patient. The clinical acceptability of the generated plan was confirmed by evaluating standard target dose-volume metrics, dose to organs-at-risk and target dose conformity and homogeneity., Conclusion: The generation of a clinically acceptable proton therapy treatment plan for cardiac radioablation of ventricular tachycardia could be performed in the presence of an ultrasound probe on the chest of the patient. These results establish a basis and justification for continued research and product development for ultrasound-guided cardiac radioablation., Competing Interests: PM is founder and owner of MedDevicePharma LLC. GW is founder and owner of National Medical Physics and Dosimetry Company. PM and GW are consultants to EBAMed SA. RP was previously employed and AG is still employed by EBAMed SA. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Perrin, Maguire, Garonna, Weidlich, Bulling, Fargier-Voiron, De Marco, Rossi, Ciocca, Vitolo and Mirandola.)

Published
2022
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20. Atlas Sampling for Prone Breast Automatic Segmentation of Organs at Risk: The Importance of Patients' Body Mass Index and Breast Cup Size for an Optimized Contouring of the Heart and the Coronary Vessels.

Author

Wang X, Miralbell R, Fargier-Bochaton O, Bulling S, Vallée JP, and Dipasquale G

Subjects
Body Mass Index, Breast Neoplasms pathology, Coronary Vessels anatomy & histology, Coronary Vessels radiation effects, Female, Heart anatomy & histology, Heart radiation effects, Humans, Image Processing, Computer-Assisted methods, Organs at Risk radiation effects, Patient Positioning, Tomography, X-Ray Computed methods, Breast Neoplasms diagnostic imaging, Breast Neoplasms radiotherapy, Coronary Vessels diagnostic imaging, Heart diagnostic imaging, Organs at Risk diagnostic imaging, Radiotherapy Planning, Computer-Assisted methods
Abstract

Objective: Delineation of organs at risk is a time-consuming task. This study evaluates the benefits of using single-subject atlas-based automatic segmentation of organs at risk in patients with breast cancer treated in prone position, with 2 different criteria for choosing the atlas subject. Together with laterality (left/right), the criteria used were either (1) breast volume or (2) body mass index and breast cup size., Methods: An atlas supporting different selection criteria for automatic segmentation was generated from contours drawn by a senior radiation oncologist (RO&#95;A). Atlas organs at risk included heart, left anterior descending artery, and right coronary artery. Manual contours drawn by RO&#95;A and automatic segmentation contours of organs at risk and breast clinical target volume were created for 27 nonatlas patients. A second radiation oncologist (RO&#95;B) manually contoured (M&#95;B) the breast clinical target volume and the heart. Contouring times were recorded and the reliability of the automatic segmentation was assessed in the context of 3-D planning., Results: Accounting for body mass index and breast cup size improved automatic segmentation results compared to breast volume-based sampling, especially for the heart (mean similarity indexes >0.9 for automatic segmentation organs at risk and clinical target volume after RO&#95;A editing). Mean similarity indexes for the left anterior descending artery and the right coronary artery edited by RO&#95;A expanded by 1 cm were ≥0.8. Using automatic segmentation reduced contouring time by 40%. For each parameter analyzed (eg, D 2% ), the difference in dose, averaged over all patients, between automatic segmentation structures edited by RO&#95;A and the same structure manually drawn by RO&#95;A was <1.5% of the prescribed dose. The mean heart dose was reliable for the unedited heart segmentation, and for right-sided treatments, automatic segmentation was adequate for treatment planning with 3-D conformal tangential fields., Conclusions: Automatic segmentation for prone breast radiotherapy stratified by body mass index and breast cup size improved segmentation accuracy for the heart and coronary vessels compared to breast volume sampling. A significant reduction in contouring time can be achieved by using automatic segmentation.

Published
2020
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21. Sparse proportional re-scanning with hadron beams.

Author

Amaldi U, Cuccagna C, Lo Moro A, Rizzoglio V, Bernier J, and Bulling S

Subjects
Adult, Child, Humans, Neoplasms radiotherapy, Radiotherapy Planning, Computer-Assisted, Proton Therapy methods
Abstract

Spot Scanning is a well-established technique to deliver the dose with hadron therapy systems. For many years re-scanning (called also re-painting) has been used to achieve uniform dose distribution in particular for moving organs, although it leads to an increase of the treatment time. Reducing this time is a major focus of present research. In this paper, after reviewing the current re-scanning techniques, sparse proportional re-scanning is defined and applied to 29 proton patient cases for a total of 54 fields. In this technique, only the highest weighted spot in the whole target is visited a number of times that is equal to the number N of re-scans. The number of visits of the beam spot to all remaining spots is scaled down proportionally to their weight. Sparse proportional re-scanning is advantageous especially in volumetric re-scanning. In order to quantify the potential advantages of this technique in terms of treatment time, a reduction factor of the number of scanned spots has been introduced, evaluated and analysed for 54 proton fields. The conclusion is that the reduction factor is a function of N (having values equal to 2.8 ± 0.3 and 3.6 ± 0.4 for N = 5 and N = 12 respectively) and does not depend either on the shape and volume of the target or on the distance between the scanned layers and the spot grid. The same values are approximately valid also for carbon ion treatments., (Copyright © 2019 Associazione Italiana di Fisica Medica. Published by Elsevier Ltd. All rights reserved.)

Published
2019
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22. Evidence for a role of transporter-mediated currents in the depletion of brain serotonin induced by serotonin transporter substrates.

Author

Baumann MH, Bulling S, Benaderet TS, Saha K, Ayestas MA, Partilla JS, Ali SF, Stockner T, Rothman RB, Sandtner W, and Sitte HH

Subjects
Animals, Dopamine metabolism, Extracellular Space metabolism, Fenfluramine pharmacology, Male, Membrane Potentials drug effects, Nucleus Accumbens drug effects, Nucleus Accumbens metabolism, Piperazines pharmacology, Rats, Rats, Sprague-Dawley, Synaptosomes drug effects, Synaptosomes metabolism, Time Factors, Xenopus laevis, Brain drug effects, Brain metabolism, Serotonin metabolism, Serotonin Agents pharmacology, Serotonin Plasma Membrane Transport Proteins metabolism
Abstract

Serotonin (5-HT) transporter (SERT) substrates like fenfluramine and 3,4-methylenedioxymethamphetamine cause long-term depletion of brain 5-HT, while certain other substrates do not. The 5-HT deficits produced by SERT substrates are dependent upon transporter proteins, but the exact mechanisms responsible are unclear. Here, we compared the pharmacology of several SERT substrates: fenfluramine, d-fenfluramine, 1-(m-chlorophenyl)piperazine (mCPP) and 1-(m-trifluoromethylphenyl)piperainze (TFMPP), to establish relationships between acute drug mechanisms and the propensity for long-term 5-HT depletions. In vivo microdialysis was carried out in rat nucleus accumbens to examine acute 5-HT release and long-term depletion in the same subjects. In vitro assays were performed to measure efflux of [(3)H]5-HT in rat brain synaptosomes and transporter-mediated ionic currents in SERT-expressing Xenopus oocytes. When administered repeatedly to rats (6 mg/kg, i.p., four doses), all drugs produce large sustained elevations in extracellular 5-HT (>5-fold) with minimal effects on dopamine. Importantly, 2 weeks after dosing, only rats exposed to fenfluramine and d-fenfluramine display depletion of brain 5-HT. All test drugs evoke fluoxetine-sensitive efflux of [(3)H]5-HT from synaptosomes, but d-fenfluramine and its bioactive metabolite d-norfenfluramine induce significantly greater SERT-mediated currents than phenylpiperazines. Our data confirm that drug-induced 5-HT release probably does not mediate 5-HT depletion. However, the magnitude of transporter-mediated inward current may be a critical factor in the cascade of events leading to 5-HT deficits. This hypothesis warrants further study, especially given the growing popularity of designer drugs that target SERT.

Published
2014
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23. The two Na+ sites in the human serotonin transporter play distinct roles in the ion coupling and electrogenicity of transport.

Author

Felts B, Pramod AB, Sandtner W, Burbach N, Bulling S, Sitte HH, and Henry LK

Subjects
Amino Acid Substitution, Asparagine genetics, Asparagine metabolism, Binding Sites, Biological Transport, Active physiology, Dopamine genetics, HEK293 Cells, Humans, Mutation, Missense, Serotonin Plasma Membrane Transport Proteins genetics, Dopamine metabolism, Serotonin Plasma Membrane Transport Proteins metabolism, Sodium metabolism
Abstract

Neurotransmitter transporters of the SLC6 family of proteins, including the human serotonin transporter (hSERT), utilize Na(+), Cl(-), and K(+) gradients to induce conformational changes necessary for substrate translocation. Dysregulation of ion movement through monoamine transporters has been shown to impact neuronal firing potentials and could play a role in pathophysiologies, such as depression and anxiety. Despite multiple crystal structures of prokaryotic and eukaryotic SLC transporters indicating the location of both (or one) conserved Na(+)-binding sites (termed Na1 and Na2), much remains uncertain in regard to the movements and contributions of these cation-binding sites in the transport process. In this study, we utilize the unique properties of a mutation of hSERT at a single, highly conserved asparagine on TM1 (Asn-101) to provide several lines of evidence demonstrating mechanistically distinct roles for Na1 and Na2. Mutations at Asn-101 alter the cation dependence of the transporter, allowing Ca(2+) (but not other cations) to functionally replace Na(+) for driving transport and promoting 5-hydroxytryptamine (5-HT)-dependent conformational changes. Furthermore, in two-electrode voltage clamp studies in Xenopus oocytes, both Ca(2+) and Na(+) illicit 5-HT-induced currents in the Asn-101 mutants and reveal that, although Ca(2+) promotes substrate-induced current, it does not appear to be the charge carrier during 5-HT transport. These findings, in addition to functional evaluation of Na1 and Na2 site mutants, reveal separate roles for Na1 and Na2 and provide insight into initiation of the translocation process as well as a mechanism whereby the reported SERT stoichiometry can be obtained despite the presence of two putative Na(+)-binding sites.

Published
2014
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24. Effects of computing parameters and measurement locations on the estimation of 3D NPS in non-stationary MDCT images.

Author

Miéville FA, Bolard G, Bulling S, Gudinchet F, Bochud FO, and Verdun FR

Subjects
Phantoms, Imaging, Imaging, Three-Dimensional instrumentation, Tomography, X-Ray Computed instrumentation
Abstract

The goal of this study was to investigate the impact of computing parameters and the location of volumes of interest (VOI) on the calculation of 3D noise power spectrum (NPS) in order to determine an optimal set of computing parameters and propose a robust method for evaluating the noise properties of imaging systems. Noise stationarity in noise volumes acquired with a water phantom on a 128-MDCT and a 320-MDCT scanner were analyzed in the spatial domain in order to define locally stationary VOIs. The influence of the computing parameters in the 3D NPS measurement: the sampling distances bx,y,z and the VOI lengths Lx,y,z, the number of VOIs NVOI and the structured noise were investigated to minimize measurement errors. The effect of the VOI locations on the NPS was also investigated. Results showed that the noise (standard deviation) varies more in the r-direction (phantom radius) than z-direction plane. A 25 × 25 × 40 mm(3) VOI associated with DFOV = 200 mm (Lx,y,z = 64, bx,y = 0.391 mm with 512 × 512 matrix) and a first-order detrending method to reduce structured noise led to an accurate NPS estimation. NPS estimated from off centered small VOIs had a directional dependency contrary to NPS obtained from large VOIs located in the center of the volume or from small VOIs located on a concentric circle. This showed that the VOI size and location play a major role in the determination of NPS when images are not stationary. This study emphasizes the need for consistent measurement methods to assess and compare image quality in CT., (Copyright © 2012 Associazione Italiana di Fisica Medica. Published by Elsevier Ltd. All rights reserved.)

Published
2013
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25. The mechanistic basis for noncompetitive ibogaine inhibition of serotonin and dopamine transporters.

Author

Bulling S, Schicker K, Zhang YW, Steinkellner T, Stockner T, Gruber CW, Boehm S, Freissmuth M, Rudnick G, Sitte HH, and Sandtner W

Subjects
Animals, Binding Sites, Cell Line, Dopamine Plasma Membrane Transport Proteins metabolism, Excitatory Amino Acid Antagonists metabolism, Humans, Ibogaine metabolism, Kinetics, Patch-Clamp Techniques, Radioligand Assay, Serotonin Plasma Membrane Transport Proteins metabolism, Xenopus laevis, Dopamine Plasma Membrane Transport Proteins antagonists & inhibitors, Excitatory Amino Acid Antagonists pharmacology, Ibogaine pharmacology, Serotonin Plasma Membrane Transport Proteins drug effects
Abstract

Ibogaine, a hallucinogenic alkaloid proposed as a treatment for opiate withdrawal, has been shown to inhibit serotonin transporter (SERT) noncompetitively, in contrast to all other known inhibitors, which are competitive with substrate. Ibogaine binding to SERT increases accessibility in the permeation pathway connecting the substrate-binding site with the cytoplasm. Because of the structural similarity between ibogaine and serotonin, it had been suggested that ibogaine binds to the substrate site of SERT. The results presented here show that ibogaine binds to a distinct site, accessible from the cell exterior, to inhibit both serotonin transport and serotonin-induced ionic currents. Ibogaine noncompetitively inhibited transport by both SERT and the homologous dopamine transporter (DAT). Ibogaine blocked substrate-induced currents also in DAT and increased accessibility of the DAT cytoplasmic permeation pathway. When present on the cell exterior, ibogaine inhibited SERT substrate-induced currents, but not when it was introduced into the cytoplasm through the patch electrode. Similar to noncompetitive transport inhibition, the current block was not reversed by increasing substrate concentration. The kinetics of inhibitor binding and dissociation, as determined by their effect on SERT currents, indicated that ibogaine does not inhibit by forming a long-lived complex with SERT, but rather binds directly to the transporter in an inward-open conformation. A kinetic model for transport describing the noncompetitive action of ibogaine and the competitive action of cocaine accounts well for the results of the present study.

Published
2012
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26. Unifying concept of serotonin transporter-associated currents.

Author

Schicker K, Uzelac Z, Gesmonde J, Bulling S, Stockner T, Freissmuth M, Boehm S, Rudnick G, Sitte HH, and Sandtner W

Subjects
Animals, Female, HEK293 Cells, Humans, Kinetics, Microscopy, Fluorescence, Models, Biological, Potassium metabolism, Protein Conformation drug effects, Serotonin pharmacology, Serotonin Plasma Membrane Transport Proteins chemistry, Electric Conductivity, Electrophysiological Phenomena drug effects, Serotonin Plasma Membrane Transport Proteins metabolism
Abstract

Serotonin (5-HT) uptake by the human serotonin transporter (hSERT) is driven by ion gradients. The stoichiometry of transported 5-HT and ions is predicted to result in electroneutral charge movement. However, hSERT mediates a current when challenged with 5-HT. This discrepancy can be accounted for by an uncoupled ion flux. Here, we investigated the mechanistic basis of the uncoupled currents and its relation to the conformational cycle of hSERT. Our observations support the conclusion that the conducting state underlying the uncoupled ion flux is in equilibrium with an inward facing state of the transporter with K+ bound. We identified conditions associated with accumulation of the transporter in inward facing conformations. Manipulations that increased the abundance of inward facing states resulted in enhanced steady-state currents. We present a comprehensive kinetic model of the transport cycle, which recapitulates salient features of the recorded currents. This study provides a framework for exploring transporter-associated currents.

Published
2012
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27. Feasibility and efficacy of accelerated weekly concomitant boost postoperative radiation therapy combined with concomitant chemotherapy in patients with locally advanced head and neck cancer.

Author

Pehlivan B, Luthi F, Matzinger O, Betz M, Dragusanu D, Bulling S, Bron L, Pasche P, Seelentag W, Mirimanoff RO, Zouhair A, and Ozsahin M

Subjects
Adult, Aged, Aged, 80 and over, Carcinoma, Squamous Cell pathology, Chemotherapy, Adjuvant, Combined Modality Therapy, Dose-Response Relationship, Radiation, Feasibility Studies, Female, Head and Neck Neoplasms pathology, Humans, Male, Middle Aged, Postoperative Care, Radiotherapy Dosage, Radiotherapy, Adjuvant, Treatment Outcome, Antineoplastic Agents administration & dosage, Carcinoma, Squamous Cell therapy, Cisplatin administration & dosage, Head and Neck Neoplasms therapy, Radiotherapy, Conformal
Abstract

Background: The aim of this study was to assess feasibility and efficacy of weekly concomitant boost accelerated postoperative radiation therapy (PORT) with concomitant chemotherapy (CT) in patients with locally advanced head and neck cancer (LAHNC)., Methods and Materials: Conformal or intensity-modulated 66-Gy RT was performed in 5.5 weeks in 40 patients. Cisplatin was given at days 1, 22, and 43. Median follow-up was 36 months., Results and Discussion: Grade 3 mucositis, dysphagia, and erythema was observed in ten (25%), nine (23%), and six (13%) patients, respectively. Grade 3 or more anemia was observed in two (6%) patients, and leukopenia in five (13%) patients. No grade 3 or 4 thrombocytopenia was observed. Grade 3 nephrotoxicity was observed in one patient (3%). No treatment-related mortality was observed. Grade 2 or more xerostomia and edema were observed in ten (25%) and one (3%) patient, respectively. Locoregional relapse occurred in eight patients, and seven patients developed distant metastases. Median time to locoregional relapse was 6 months. Three-year overall, disease-free survival, and locoregional control rates were 63%, 62%, and 81%, respectively. Multivariate analysis revealed that the only prognostic factor was nodal status., Conclusion: Reducing overall treatment time using accelerated PORT/CT by weekly concomitant boost (six fractions per week) combined with concomitant cisplatin CT is easily feasible with acceptable morbidity.

Published
2009
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28. Performance comparison of two commercial BGO-based PET/CT scanners using NEMA NU 2-2001.

Author

Bolard G, Prior JO, Modolo L, Delaloye AB, Kosinski M, Wastiel C, Malterre J, Bulling S, Bochud F, and Verdun FR

Subjects
Electricity, Humans, Reference Standards, Sensitivity and Specificity, Tomography, X-Ray Computed, Phantoms, Imaging, Positron-Emission Tomography
Abstract

Combined positron emission tomography and computed tomography (PET/CT) scanners play a major role in medicine for in vivo imaging in an increasing number of diseases in oncology, cardiology, neurology, and psychiatry. With the advent of short-lived radioisotopes other than 18F and newer scanners, there is a need to optimize radioisotope activity and acquisition protocols, as well as to compare scanner performances on an objective basis. The Discovery-LS (D-LS) was among the first clinical PET/CT scanners to be developed and has been extensively characterized with older National Electrical Manufacturer Association (NEMA) NU 2-1994 standards. At the time of publication of the latest version of the standards (NU 2-2001) that have been adapted for whole-body imaging under clinical conditions, more recent models from the same manufacturer, i.e., Discovery-ST (D-ST) and Discovery-STE (D-STE), were commercially available. We report on the full characterization both in the two- and three-dimensional acquisition mode of the D-LS according to latest NEMA NU 2-2001 standards (spatial resolution, sensitivity, count rate performance, accuracy of count losses, and random coincidence correction and image quality), as well as a detailed comparison with the newer D-ST widely used and whose characteristics are already published.

Published
2007
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29. Treatment of penile carcinoma: to cut or not to cut?

Author

Ozsahin M, Jichlinski P, Weber DC, Azria D, Zimmermann M, Guillou L, Bulling S, Moeckli R, Mirimanoff RO, and Zouhair A

Subjects
Adult, Aged, Aged, 80 and over, Analysis of Variance, Carcinoma, Squamous Cell pathology, Chi-Square Distribution, Humans, Male, Middle Aged, Multivariate Analysis, Neoplasm Recurrence, Local surgery, Penile Neoplasms pathology, Prognosis, Retrospective Studies, Salvage Therapy, Carcinoma, Squamous Cell radiotherapy, Carcinoma, Squamous Cell surgery, Penile Neoplasms radiotherapy, Penile Neoplasms surgery, Penis surgery
Abstract

Purpose: The aim of this study was to assess the outcome in patients with penile cancer., Methods and Materials: A total of 60 patients with penile carcinoma were included. Of the patients, 45 (n = 27) underwent surgery, and 51 underwent definitive (n = 29) or postoperative (n = 22) radiotherapy (RT). Median follow-up was 62 months., Results: Median time to locoregional relapse was 14 months. Local failure was observed in 3 of 23 patients (13%) treated with surgery with or without postoperative RT vs. in 19 of 33 patients (56%) given organ-sparing treatment (p = 0.0008). Of 22 local failures, 16 (73%) were salvaged with surgery. Of the 33 patients treated with definitive RT (n = 29) and the 4 patients refusing RT after excisional biopsy, local control was obtained with organ preservation in 13 (39%). In the remaining 20, 4 patients with local failure underwent salvage conservatively, resulting in an ultimate penis preservation rate of 17 of 33 (52%) patients treated with definitive RT. The 5-year and 10-year probability of surviving with an intact penis was 43% and 26%, respectively. There was no survival difference between the patients treated with definitive RT and primary surgery (56% vs. 53%; p = 0.16). In multivariate analysis, independent factors influencing survival were N-classification and pathologic grade. Surgery was the only independent predictor for better local control., Conclusion: Based on our study findings, in patients with penile cancer, local control is superior with surgery. However, there is no difference in survival between patients treated with surgery and those treated with definitive RT, with 52% organ preservation.

Published
2006
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30. Monte Carlo calculation of the sensitivity of a commercial dose calibrator to gamma and beta radiation.

Author

Laedermann JP, Valley JF, Bulling S, and Bochud FO

Subjects
Biophysical Phenomena, Biophysics, Humans, Models, Statistical, Monte Carlo Method, Radiometry instrumentation, Radiopharmaceuticals analysis, Sensitivity and Specificity, Software, Beta Particles, Gamma Rays, Radiometry statistics & numerical data
Abstract

The detection process used in a commercial dose calibrator was modeled using the GEANT 3 Monte Carlo code. Dose calibrator efficiency for gamma and beta emitters, and the response to monoenergetic photons and electrons was calculated. The model shows that beta emitters below 2.5 MeV deposit energy indirectly in the detector through bremsstrahlung produced in the chamber wall or in the source itself. Higher energy beta emitters (E > 2.5 MeV) deposit energy directly in the chamber sensitive volume, and dose calibrator sensitivity increases abruptly for these radionuclides. The Monte Carlo calculations were compared with gamma and beta emitter measurements. The calculations show that the variation in dose calibrator efficiency with measuring conditions (source volume, container diameter, container wall thickness and material, position of the source within the calibrator) is relatively small and can be considered insignificant for routine measurement applications. However, dose calibrator efficiency depends strongly on the inner-wall thickness of the detector.

Published
2004
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31. Influence of scatter reduction method and monochromatic beams on image quality and dose in mammography.

Author

Moeckli R, Verdun FR, Fiedler S, Pachoud M, Bulling S, Schnyder P, and Valley JF

Subjects
Computer Simulation, Dose-Response Relationship, Radiation, Equipment Design, Phantoms, Imaging, Radiation Dosage, Reproducibility of Results, Scattering, Radiation, Sensitivity and Specificity, Equipment Failure Analysis methods, Mammography instrumentation, Mammography methods, Models, Biological, Radiographic Image Enhancement instrumentation, Radiographic Image Enhancement methods, Radiometry methods
Abstract

In mammography, the image contrast and dose delivered to the patient are determined by the x-ray spectrum and the scatter to primary ratio S/P. Thus the quality of the mammographic procedure is highly dependent on the choice of anode and filter material and on the method used to reduce the amount of scattered radiation reaching the detector. Synchrotron radiation is a useful tool to study the effect of beam energy on the optimization of the mammographic process because it delivers a high flux of monochromatic photons. Moreover, because the beam is naturally flat collimated in one direction, a slot can be used instead of a grid for scatter reduction. We have measured the ratio S/P and the transmission factors for grids and slots for monoenergetic synchrotron radiation. In this way the effect of beam energy and scatter rejection method were separated, and their respective importance for image quality and dose analyzed. Our results show that conventional mammographic spectra are not far from optimum and that the use of a slot instead of a grid has an important effect on the optimization of the mammographic process. We propose a simple numerical model to quantify this effect.

Published
2003
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32. Determination of the efficiency of commercially available dose calibrators for beta-emitters.

Author

Valley JF, Bulling S, Leresche M, and Wastiel C

Subjects
Bone Neoplasms radiotherapy, Bone Neoplasms secondary, Erbium, Humans, Palliative Care, Phosphorus Radioisotopes, Radioisotopes, Radiotherapy, Strontium Radioisotopes, Yttrium Radioisotopes, Beta Particles therapeutic use, Radiation Monitoring instrumentation, Radiometry instrumentation
Abstract

Objectives: The goals of this investigation are to determine whether commercially available dose calibrators can be used to measure the activity of beta-emitting radionuclides used in pain palliation and to establish whether manufacturer-supplied calibration factors are appropriate for this purpose., Methods: Six types of commercially available dose calibrators were studied. Dose calibrator response was controlled for 5 gamma-emitters used for calibration or typically encountered in routine use. For the 4 most commonly used beta-emitters ((32)P, (90)Sr, (90)Y, and (169)Er) dose calibrator efficiency was determined in the syringe geometry used for clinical applications. Efficiency of the calibrators was also measured for (153)Sm and (186)Re, 2 beta-emitters with significant gamma-contributions. Source activities were traceable to national standards., Results: All calibrators measured gamma-emitters with a precision of +/-10%, in compliance with Swiss regulatory requirements. For beta-emitters, dose calibrator intrinsic efficiency depends strongly on the maximal energy of the beta-spectrum and is notably low for (169)Er. Manufacturer-supplied calibration factors give accurate results for beta-emitters with maximal beta-energy in the middle-energy range (1 MeV) but are not appropriate for use with low-energy ((169)Er) or high-energy ((90)Y) beta-emitters. beta-emitters with significant gamma-contributions behave like gamma-emitters., Conclusion: Commercially available dose calibrators have an intrinsic efficiency that is sufficient for the measurement of beta-emitters, including beta-emitters with a low maximum beta-energy. Manufacturer-supplied calibration factors are reliable for gamma-emitters and beta-emitters in the middle-energy range. For low- and high-energy beta-emitters, the use of manufacturer-supplied calibration factors introduces significant measurement inaccuracy.

Published
2003

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