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2. Microwave spectroscopy of interacting Andreev spins

Author

Wesdorp, J. J., Matute-Caňadas, F. J., Vaartjes, A., Grünhaupt, L., Laeven, T., Roelofs, S., Splitthoff, L. J., Pita-Vidal, M., Bargerbos, A., van Woerkom, D. J., Krogstrup, P., Kouwenhoven, L. P., Andersen, C. K., Yeyati, A. Levy, van Heck, B., and de Lange, G.

Subjects
Condensed Matter - Mesoscale and Nanoscale Physics, Condensed Matter - Superconductivity, Quantum Physics
Abstract

Andreev bound states are fermionic states localized in weak links between superconductors which can be occupied with spinful quasiparticles. Microwave experiments using superconducting circuits with InAs/Al nanowire Josephson junctions have recently enabled probing and coherent manipulation of Andreev states but have remained limited to zero or small fields. Here we use a flux-tunable superconducting circuit in external magnetic fields up to 1T to perform spectroscopy of spin-polarized Andreev states up to ~250 mT, beyond which the spectrum becomes gapless. We identify singlet and triplet states of two quasiparticles occupying different Andreev states through their dispersion in magnetic field. These states are split by exchange interaction and couple via spin-orbit coupling, analogously to two-electron states in quantum dots. We also show that the magnetic field allows to drive a direct spin-flip transition of a single quasiparticle trapped in the junction. Finally, we measure a gate- and field-dependent anomalous phase shift of the Andreev spectrum, of magnitude up to approximately $0.7\pi$. Our observations demonstrate new ways to manipulate Andreev states in a magnetic field and reveal spin-polarized triplet states that carry supercurrent.

Published
2022
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4. Event generators for high-energy physics experiments

Author

J. M. Campbell, M. Diefenthaler, T. J. Hobbs, S. Höche, J. Isaacson, F. Kling, S. Mrenna, J. Reuter, S. Alioli, J. R. Andersen, C. Andreopoulos, A. M. Ankowski, E. C. Aschenauer, A. Ashkenazi, M. D. Baker, J. L. Barrow, M. van Beekveld, G. Bewick, S. Bhattacharya, C. Bierlich, E. Bothmann, P. Bredt, A. Broggio, A. Buckley, A. Butter, J. M. Butterworth, E. P. Byrne, C. M. Carloni-Calame, S. Chakraborty, X. Chen, M. Chiesa, J. T. Childers, J. Cruz-Martinez, J. Currie, N. Darvishi, M. Dasgupta, A. Denner, F. A. Dreyer, S. Dytman, B. K. El-Menoufi, T. Engel, S. Ferrario Ravasio, D. Figueroa, L. Flower, J. R. Forshaw, R. Frederix, A. Friedland, S. Frixione, H. Gallagher, K. Gallmeister, S. Gardiner, R. Gauld, J. Gaunt, A. Gavardi, T. Gehrmann, A. Gehrmann-De Ridder, L. Gellersen, W. Giele, S. Gieseke, F. Giuli, E. W. N. Glover, M. Grazzini, A. Grohsjean, C. Gütschow, K. Hamilton, T. Han, R. Hatcher, G. Heinrich, I. Helenius, O. Hen, V. Hirschi, M. Höfer, J. Holguin, A. Huss, P. Ilten, S. Jadach, A. Jentsch, S. P. Jones, W. Ju, S. Kallweit, A. Karlberg, T. Katori, M. Kerner, W. Kilian, M. M. Kirchgaeßer, S. Klein, M. Knobbe, C. Krause, F. Krauss, J. Lang, J. -N. Lang, G. Lee, S. W. Li, M. A. Lim, J. M. Lindert, D. Lombardi, L. Lönnblad, M. Löschner, N. Lurkin, Y. Ma, P. Machado, V. Magerya, A. Maier, I. Majer, F. Maltoni, M. Marcoli, G. Marinelli, M. R. Masouminia, P. Mastrolia, O. Mattelaer, J. Mazzitelli, J. McFayden, R. Medves, P. Meinzinger, J. Mo, P. F. Monni, G. Montagna, T. Morgan, U. Mosel, B. Nachman, P. Nadolsky, R. Nagar, Z. Nagy, D. Napoletano, P. Nason, T. Neumann, L. J. Nevay, O. Nicrosini, J. Niehues, K. Niewczas, T. Ohl, G. Ossola, V. Pandey, A. Papadopoulou, A. Papaefstathiou, G. Paz, M. Pellen, G. Pelliccioli, T. Peraro, F. Piccinini, L. Pickering, J. Pires, W. Placzek, S. Plätzer, T. Plehn, S. Pozzorini, S. Prestel, C. T. Preuss, A. C. Price, S. Quackenbush, E. Re, D. Reichelt, L. Reina, C. Reuschle, P. Richardson, M. Rocco, N. Rocco, M. Roda, A. Rodriguez Garcia, S. Roiser, J. Rojo, L. Rottoli, G. P. Salam, M. Schönherr, S. Schuchmann, S. Schumann, R. Schürmann, L. Scyboz, M. H. Seymour, F. Siegert, A. Signer, G. Singh Chahal, A. Siódmok, T. Sjöstrand, P. Skands, J. M. Smillie, J. T. Sobczyk, D. Soldin, D. E. Soper, A. Soto-Ontoso, G. Soyez, G. Stagnitto, J. Tena-Vidal, O. Tomalak, F. Tramontano, S. Trojanowski, Z. Tu, S. Uccirati, T. Ullrich, Y. Ulrich, M. Utheim, A. Valassi, A. Verbytskyi, R. Verheyen, M. Wagman, D. Walker, B. R. Webber, L. Weinstein, O. White, J. Whitehead, M. Wiesemann, C. Wilkinson, C. Williams, R. Winterhalder, C. Wret, K. Xie, T-Z. Yang, E. Yazgan, G. Zanderighi, S. Zanoli, K. Zapp

Subjects
Physics, QC1-999
Abstract

We provide an overview of the status of Monte-Carlo event generators for high-energy particle physics. Guided by the experimental needs and requirements, we highlight areas of active development, and opportunities for future improvements. Particular emphasis is given to physics models and algorithms that are employed across a variety of experiments. These common themes in event generator development lead to a more comprehensive understanding of physics at the highest energies and intensities, and allow models to be tested against a wealth of data that have been accumulated over the past decades. A cohesive approach to event generator development will allow these models to be further improved and systematic uncertainties to be reduced, directly contributing to future experimental success. Event generators are part of a much larger ecosystem of computational tools. They typically involve a number of unknown model parameters that must be tuned to experimental data, while maintaining the integrity of the underlying physics models. Making both these data, and the analyses with which they have been obtained accessible to future users is an essential aspect of open science and data preservation. It ensures the consistency of physics models across a variety of experiments.

Published
2024
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7. The Danish Heart Failure Registry: A Validation Study of Content

Author

Andersen C, Schjødt I, Nakano A, Johnsen SP, Egstrup K, and Løgstrup BB

Subjects
heart failure, database, epidemiology, registries, danish heart failure registry, Infectious and parasitic diseases, RC109-216
Abstract

Christina Andersen,1 Inge Schjødt,1 Anne Nakano,2 Søren Paaske Johnsen,3 Kenneth Egstrup,4 Brian B Løgstrup1,5 1Department of Cardiology, Aarhus University Hospital, Aarhus, Denmark; 2The Danish Clinical Registries (RKKP), Aarhus, Denmark; 3Danish Center for Clinical Health Services Research (DACS), Department of Clinical Medicine, Aalborg University, Aalborg, Denmark; 4Department of Cardiology, Odense University Hospital, Svendborg, Denmark; 5Institute of Clinical Medicine, Aarhus University, Aarhus, DenmarkCorrespondence: Brian B Løgstrup, Department of Cardiology, Aarhus University Hospital, Palle Juul-Jensens Boulevard 99, Aarhus, 8200, Denmark, Email bbl@skejby.rm.dkBackground: The Danish Heart Failure Registry (DHFR) is a clinical quality database established to monitor and improve the quality of heart failure (HF) care in Denmark.Objective: We examined the validity of the content of the DHFR.Methods: In a random sample of patients registered in DHFR between the 1st of January 2016 to the 31st of December 2018, we determined the agreement between the information entered in the database and information in the medical records regarding 1) content; 2) sensitivity; 3) specificity; 4) positive predictive values (PPV) as well as negative predictive values (NPV) of all patient characteristics and performance measures obtained in the DHFR.Results: The study population included 453 patients. In general, the content of the DHFR was accurate. Patient characteristics showed high PPV between 93.0% and 99.5% for all variables. Sensitivity ranged from 81.0% to 95.2%, specificity from 79.8% to 99.5% and NPV ranged from 81.4% to 99.0%. The pharmacological performance measures showed high agreement regarding sensitivity (77.4% to 98.6%) and PPV (84.0% to 94.0%). Further, the specificity ranged from 66.7% to 98.0% and NPP ranged from 90.1% to 96.5%. For the non-pharmacological performance measures, patient education showed high sensitivity (98.0%, 95% CI 96.1– 99.1) and PPV (94.9% CI: 93.0– 96.3), whereas referral to exercise training had a lower sensitivity of 77.8% (CI: 71.6– 83.1) and a PPV of 74.5% (CI: 69.6– 78.6).Conclusion: Overall, the Danish Heart Failure Registry have a high degree of completeness and validity, making it a valuable tool for clinical epidemiological research in HF.Keywords: heart failure, database, epidemiology, registries, Danish Heart Failure Registry

Published
2022

13. Microwave spectroscopy of interacting Andreev spins

Author

Wesdorp, J. J., Matute-cañadas, F. J., Vaartjes, A., Grünhaupt, L., Laeven, T., Roelofs, S., Splitthoff, L. J., Pita-vidal, M., Bargerbos, A., Van Woerkom, D. J., Krogstrup, P., Kouwenhoven, L. P., Andersen, C. K., Yeyati, A. Levy, Van Heck, B., De Lange, G., Wesdorp, J. J., Matute-cañadas, F. J., Vaartjes, A., Grünhaupt, L., Laeven, T., Roelofs, S., Splitthoff, L. J., Pita-vidal, M., Bargerbos, A., Van Woerkom, D. J., Krogstrup, P., Kouwenhoven, L. P., Andersen, C. K., Yeyati, A. Levy, Van Heck, B., and De Lange, G.

Published
2024

14. The intrafollicular concentrations of biologically active cortisol in women rise abruptly shortly before ovulation and follicular rupture

Author

Johannsen, M. L., Poulsen, L. C., Mamsen, L. S., Grøndahl, M. L., Englund, A. L. M., Lauritsen, N. L., Carstensen, E. C., Styrishave, B., Andersen, C. Yding, Johannsen, M. L., Poulsen, L. C., Mamsen, L. S., Grøndahl, M. L., Englund, A. L. M., Lauritsen, N. L., Carstensen, E. C., Styrishave, B., and Andersen, C. Yding

Abstract

STUDY QUESTION: What is the temporal activity and the concentration in follicular fluid (FF) of the anti-inflammatory steroid cortisol during the ovulatory process in humans? SUMMARY ANSWER: Intrafollicular concentrations of cortisol become massively upregulated close to ovulation concomitant with an exceptionally high biological activity securing a timely and efficient termination of inflammatory processes. WHAT IS KNOWN ALREADY: Ovulation has been described as a local, controlled inflammatory process resulting in the degeneration of the follicle wall which facilitate oocyte extrusion. Ovulation also affects the glucocorticoid metabolism of granulosa cells (GCs) and although de novo synthesis of cortisol only occurs in the adrenal cortex, the mid-cycle surge has been shown to induce a change from high expression of HSD11B2, inactivating cortisol to cortisone, to high expression of HSD11B1 which reversibly catalyses cortisol production from cortisone. Furthermore, high concentrations of progesterone and 17OH-proges-terone within follicles may cause dislodging of cortisol from cortisol binding protein (CBP) thereby activating the biological activity of cortisol. STUDY DESIGN, SIZE, DURATION: This prospective cohort study included 50 women undergoing fertility treatment according to a standard antagonist protocol at a university hospital-affiliated fertility clinic in Denmark. PARTICIPANTS/MATERIALS, SETTING, METHODS: Women donated FF and GCs from one follicle for research purpose aspirated at one of four time points during the process of final maturation of follicles: T ¼ 0 h, T ¼ 12 h, T ¼ 17 h, T ¼ 32 h. A second sample was collected at oocyte pick up at T ¼ 36 h. The concentration of cortisol and cortisone together with a range of sex steroids was measured by LC-MS/MS in FF collected at the five time points mentioned above. Whole genome microarray data, validated by q-PCR analysis, was used to evaluate gene expression of CYP11B1, CYP21A2, HSD11B1, HSD11B2, and

Published
2024

15. Microwave spectroscopy of interacting Andreev spins

Author

Wesdorp, J. J., primary, Matute-Cañadas, F. J., additional, Vaartjes, A., additional, Grünhaupt, L., additional, Laeven, T., additional, Roelofs, S., additional, Splitthoff, L. J., additional, Pita-Vidal, M., additional, Bargerbos, A., additional, van Woerkom, D. J., additional, Krogstrup, P., additional, Kouwenhoven, L. P., additional, Andersen, C. K., additional, Yeyati, A. Levy, additional, van Heck, B., additional, and de Lange, G., additional

Published
2024
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16. EE215 Estimation of 10-Year Healthcare Costs of Patients Diagnosed With Myeloproliferative Neoplasms in Denmark

Author

Stenling, A., primary, Friis Christensen, S., additional, Skovgaard Svingel, L., additional, Kjærsgaard, A., additional, Paulsson, B., additional, Lykkegaard Andersen, C., additional, Fynbo Christiansen, C., additional, Stentoft, J., additional, Starklint, J., additional, Tang Severinsen, M., additional, Borg Clausen, M., additional, Hagemann Hilsøe, M., additional, Hasselbalch, H.C., additional, Mikkelsen, E.M., additional, and Bak, M., additional

Published
2023
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17. Accelerometer-measured physical activity in patients with heart failure and reduced ejection fraction: determinants and relationship with patient-reported health status

Author

Larsen, J H, primary, Andersen, C F, additional, Omar, M, additional, Kistorp, C M, additional, Tuxen, C D, additional, Gustafsson, F, additional, Koeber, L, additional, Poulsen, M I, additional, Broend, J C, additional, Moeller, J E, additional, Schou, M, additional, and Jensen, J, additional

Published
2023
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23. The intrafollicular concentrations of biologically active cortisol in women rise abruptly shortly before ovulation and follicular rupture.

Author

Johannsen, M L, Poulsen, L C, Mamsen, L S, Grøndahl, M L, Englund, A L M, Lauritsen, N L, Carstensen, E C, Styrishave, B, and Andersen, C Yding

Subjects
OVULATION, HYDROCORTISONE, INDUCED ovulation, GRANULOSA cells, ADRENAL cortex
Abstract

STUDY QUESTION What is the temporal activity and the concentration in follicular fluid (FF) of the anti-inflammatory steroid cortisol during the ovulatory process in humans? SUMMARY ANSWER Intrafollicular concentrations of cortisol become massively upregulated close to ovulation concomitant with an exceptionally high biological activity securing a timely and efficient termination of inflammatory processes. WHAT IS KNOWN ALREADY Ovulation has been described as a local, controlled inflammatory process resulting in the degeneration of the follicle wall which facilitate oocyte extrusion. Ovulation also affects the glucocorticoid metabolism of granulosa cells (GCs) and although de novo synthesis of cortisol only occurs in the adrenal cortex, the mid-cycle surge has been shown to induce a change from high expression of HSD11B2, inactivating cortisol to cortisone, to high expression of HSD11B1 which reversibly catalyses cortisol production from cortisone. Furthermore, high concentrations of progesterone and 17OH-progesterone within follicles may cause dislodging of cortisol from cortisol binding protein (CBP) thereby activating the biological activity of cortisol. STUDY DESIGN, SIZE, DURATION This prospective cohort study included 50 women undergoing fertility treatment according to a standard antagonist protocol at a university hospital-affiliated fertility clinic in Denmark. PARTICIPANTS/MATERIALS, SETTING, METHODS Women donated FF and GCs from one follicle for research purpose aspirated at one of four time points during the process of final maturation of follicles: T  = 0 h, T  = 12 h, T  = 17 h, T  = 32 h. A second sample was collected at oocyte pick up at T  = 36 h. The concentration of cortisol and cortisone together with a range of sex steroids was measured by LC-MS/MS in FF collected at the five time points mentioned above. Whole genome microarray data, validated by q-PCR analysis, was used to evaluate gene expression of CYP11B1 , CYP21A2 , HSD11B1 , HSD11B2 , and NR3C1 in GCs at the same time points. MAIN RESULTS AND THE ROLE OF CHANCE The concentration of cortisol was significantly increased from a few nM at 0 h to around 100–140 nM (P  ≤ 0.0001) at 32–36 h, whilst cortisone was almost constant from 0 to 17 h at a concentration of between 90 and 100 nM being significantly reduced to 25–40 nM (P  ≤ 0.0001) at 32–36 h. This was paralleled by a 690-fold upregulation of HSD11B1 from 0 to 12 h increasing to a more than 20.000-fold change at 36 h. HSD11B2 was quickly downregulated 15- to 20-fold after ovulation induction. Concentrations of progesterone and 17OH-progesterone increased during the ovulatory process to high levels which in essence displaces cortisol from its binding protein CBP due to similar binding affinities. Furthermore, a significant decrease in 11-deoxycortisol expression was seen, but CYP11B1 expression was below detection limit in GCs. LIMITATIONS, REASONS FOR CAUTION The study included women undergoing ovarian stimulation and results may differ from the natural cycle. More observations at each specific time point may have strengthened the conclusions. Furthermore, we have not been able to measure the actual active biological concentration of cortisol. WIDER IMPLICATIONS OF THE FINDINGS For the first time, this study collectively evaluated the temporal pattern of cortisol and cortisone concentrations during human ovulation, rendering a physiological framework for understanding potential dysregulations in the inflammatory reaction of ovulation. STUDY FUNDING/COMPETING INTEREST(S) This research was supported by the University Hospital of Copenhagen, Rigshospitalet, and Novo Nordisk Foundation grant number NNF21OC00700556. Interreg V ÔKS through ReproUnion (www.reprounion.eu); Region Zealand Research Foundation. The funders had no role in study design, collection of data, analyses, writing of the article, or the decision to submit it for publication. The authors have no conflicts of interest to declare. TRIAL REGISTRATION NUMBER N/A. [ABSTRACT FROM AUTHOR]

Published
2024
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26. Accumulated dose implications from systematic dose-rate transients in gated treatments with Viewray MRIdian accelerators

Author

Klavsen, M. F., Ankjærgaard, C., Boye, K., Behrens, C. P., Vogelius, I. R., Ehrbar, S., Baumgartl, M., Rippke, C., Buchele, C., Renkamp, C. K., Santurio, G. V., Andersen, C. E., Klavsen, M. F., Ankjærgaard, C., Boye, K., Behrens, C. P., Vogelius, I. R., Ehrbar, S., Baumgartl, M., Rippke, C., Buchele, C., Renkamp, C. K., Santurio, G. V., and Andersen, C. E.

Abstract

The combination of magnetic resonance (MR) imaging and linear accelerators (linacs) into MR-Linacs enables continuous MR imaging and advanced gated treatments of patients. Previously, a dose-rate transient (∼8% reduced dose rate during the initial 0.5 s of each beam) was identified for a Viewray MRIdian MR-Linac (Klavsen et al 2022 Radiation Measurement 106759). Here, the dose-rate transient is studied in more detail at four linacs of the same type at different hospitals. The implications of dose-rate transients were examined for gated treatments. The dose-rate transients were investigated using dose-per pulse measurements with organic plastic scintillators in three experiments: (i) A gated treatment with the scintillator placed in a moving target in a dynamic phantom, (ii) a gated treatment with the same dynamic conditions but with the scintillator placed in a stationary target, and (iii) measurements in a water-equivalent material to examine beam quality deviations at a dose-per-pulse basis. Gated treatments (i) compared with non-gated treatments with a static target in the same setup showed a broadening of accumulated dose profiles due to motion (dose smearing). The linac with the largest dose-rate transient had a reduced accumulated dose of up to (3.1 ± 0.65) % in the center of the PTV due to the combined dose smearing and dose-rate transient effect. Dose-rate transients were found to vary between different machines. Two MR-Linacs showed initial dose-rate transients that could not be identified from conventional linearity tests. The source of the transients includes an initial change in photon fluence rate and an initial change in x-ray beam quality. For gated treatments, this caused a reduction of more than 1% dose delivered at the central part of the beam for the studied, cyclic-motion treatment plan. Quality assurance of this effect should be considered when gated treatment with the Viewray MRIdian is implemented clinically.

Published
2023

27. Eight weeks of androgen priming by daily low-dose hCG injections before ICSI treatment in women with low ovarian reserve

Author

Friis Wang, N., Bogstad, J. W., Pors, S. E., Petersen, M. R., Pinborg, A., Yding Andersen, C., Løssl, K., Friis Wang, N., Bogstad, J. W., Pors, S. E., Petersen, M. R., Pinborg, A., Yding Andersen, C., and Løssl, K.

Abstract

STUDY QUESTION: Does 8 weeks of continuous low-dose hCG administration increase the proportion of antral follicles that reach the preovulatory state during ovarian stimulation (OS) in women with low ovarian reserve? SUMMARY ANSWER: The proportion of antral follicles (2-10 mm) that reached the preovulatory state did not increase. WHAT IS KNOWN ALREADY: The administration of androgens prior to OS might upregulate FSH receptor (FSHR) expression on granulosa cells, making follicles more responsive to exogenous FSH stimulation during OS. LH and hCG stimulate the local follicular androgen synthesis in theca cells and may be used as an endogenous androgen priming method. Exogenous priming by testosterone and dehydroepiandrosterone (DHEA) have been shown to increase the number of retrieved oocytes and live birth rate but the studies are small, and their use is associated with side effects. STUDY DESIGN, SIZE, DURATION: A prospective, paired, non-blinded single-center study including 20 women serving as their own controls conducted between January 2021 and July 2021 at The University Hospital Copenhagen Rigshospitalet, Denmark. PARTICIPANTS/MATERIALS, SETTING, METHODS: Participants underwent two identical consecutive IVF/ICSI treatments, a Control cycle and a Study cycle, separated by ∼8 weeks (two menstrual cycles) of daily injections of 260 IU recombinant hCG (rhCG). A freeze-all strategy was applied in the Control cycle. Both IVF/ICSI cycles were performed in a fixed GnRH antagonist protocol using a daily dose of 300 IU recombinant FSH (rFSH) and GnRH antagonist 0.25 mg from stimulation days 5-6. MAIN RESULTS AND THE ROLE OF CHANCE: Follicular output rate, defined as the number of follicles >16 mm on hCG trigger day divided by the antral follicle count (2-10 mm) at baseline, did not increase after 8 weeks of hCG priming (P = 0.8). The mean number of oocytes retrieved was significantly higher after the hCG priming being 4.7 (2.8) vs 3.2 (1.7) in the Study and Control

Published
2023

31. The association of loneliness and social isolation with healthcare utilization in Denmark

Author

Christensen, J., Pedersen, S. S., Andersen, C. M., Qualter, P., Lund, R., and Lasgaard, M.

Subjects
Public Health, Environmental and Occupational Health
Abstract

Objectives The present prospective cohort study investigated the association of loneliness and social isolation (SI) with healthcare utilization (HCU) in the general population over time. Methods Data from the 2013 Danish “How are you?’ survey (n = 29,472) were combined with individual-level register data from the National Danish Patient Registry and the Danish National Health Service Registry over a 6-year follow-up period (2013-2018). Negative binomial regression analyses were performed while adjusting for baseline demographics and chronic disease. Results Loneliness measured at baseline was significantly associated with more GP contacts (incident-rate ratio (IRR) = 1.03, 95% confidence interval (CI) [1.02, 1.04]), more emergency treatments (IRR = 1.06, 95% CI [1.03, 1.10]), more emergency admissions (IRR = 1.06, 95% CI [1.03, 1.06]), and hospital admission days (IRR=1.05, 95% CI [1.00, 1.11]) across the 6-year follow-up period. No significant associations were found between social isolation and HCU with one minor exception, in which SI was associated with fewer planned outpatient treatments (IRR = .97, 95% CI [.94, .99]). Conclusions Our findings suggest that loneliness is a risk factor for certain types of HCU, independent of social isolation, baseline demographics, and chronic disease. Key messages

Published
2022
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35. Direct effects of empagliflozin on erythropoiesis in heart failure: data from the Empire HF trial

Author

Andersen, C, primary, Omar, M, additional, Glenthoej, A, additional, Fassi, D E, additional, Moeller, H J, additional, Styrishave, B, additional, Kistorp, C, additional, Tuxen, C, additional, Poulsen, M K, additional, Faber, J, additional, Koeber, L, additional, Gustafsson, F, additional, Moeller, J E, additional, Schou, M, additional, and Jensen, J, additional

Published
2022
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39. Androgen and inhibin B levels during ovarian stimulation before and after 8 weeks of low-dose hCG priming in women with low ovarian reserve.

Author

Wang, N Friis, Bogstad, J W, Petersen, M R, Pinborg, A, Andersen, C Yding, and Løssl, K

Subjects
INDUCED ovulation, OVARIAN reserve, BLASTOCYST, OVARIAN follicle, INTRACYTOPLASMIC sperm injection, OOCYTE retrieval
Abstract

STUDY QUESTION Does 8 weeks of daily low-dose hCG administration affect androgen or inhibin B levels in serum and/or follicular fluid (FF) during the subsequent IVF/ICSI cycle in women with low ovarian reserve? SUMMARY ANSWER Androgen levels in serum and FF, and inhibin B levels in serum, decreased following 8 weeks of hCG administration. WHAT IS KNOWN ALREADY Recently, we showed that 8 weeks of low-dose hCG priming, in between two IVF/ICSI treatments in women with poor ovarian responder (anti-Müllerian hormone (AMH) <6.29 pmol/l), resulted in more follicles of 2–5 mm and less of 6–10-mm diameter at the start of stimulation and more retrieved oocytes at oocyte retrieval. The duration of stimulation and total FSH consumption was increased in the IVF/ICSI cycle after priming. Hypothetically, hCG priming stimulates intraovarian androgen synthesis causing upregulation of FSH receptors (FSHR) on granulosa cells. It was therefore unexpected that antral follicles were smaller and the stimulation time longer after hCG priming. This might indicate a different mechanism of action than previously suggested. STUDY DESIGN, SIZE, DURATION Blood samples were drawn on stimulation day 1, stimulation days 5–6, trigger day, day of oocyte retrieval, and oocyte retrieval + 5 days in the IVF/ICSI cycles before and after hCG priming (the control and study cycles, respectively). FF was collected from the first aspirated follicle on both sides during oocyte retrieval in both cycles. The study was conducted as a prospective, paired, non-blinded, single-center study conducted between January 2021 and July 2021 at a tertiary care center. The 20 participants underwent two identical IVF/ICSI treatments: a control cycle including elective freezing of all blastocysts and a study cycle with fresh blastocyst transfer. The control and study cycles were separated by 8 weeks (two menstrual cycles) of hCG priming by daily injections of 260 IU recombinant hCG. PARTICIPANTS/MATERIALS, SETTING, METHODS Women aged 18–40 years with cycle lengths of 23–35 days and AMH <6.29 pmol/l were included. Control and study IVF/ICSI cycles were performed in a fixed GnRH-antagonist protocol. MAIN RESULTS AND THE ROLE OF CHANCE Inhibin B was lower on stimulation day 1 after hCG priming (P  = 0.05). Dehydroepiandrosterone sulfate (DHEAS) was significantly lower on stimulation day 1 (P  = 0.03), and DHEAS and androstenedione were significantly lower on stimulation days 5–6 after priming (P  = 0.02 and P  = 0.02) The testosterone level in FF was significantly lower in the study cycle (P  = 0.008), while the concentrations of inhibin B and androstenedione in the FF did not differ between the study and control cycles. A lower serum inhibin B in the study cycle corresponds with the antral follicles being significantly smaller after priming, and this probably led to a longer stimulation time in the study cycle. This contradicts the theory that hCG priming increases the intraovarian androgen level, which in turn causes more FSHR on developing (antral up to preovulatory) follicles. However, based on this study, we cannot rule out that an increased intra-follicular androgen level was present at initiation of the ovarian stimulation, without elevating the androgen level in serum and that an increased androgen level may have rescued some small antral follicles that would have otherwise undergone atresia by the end of the previous menstrual cycle. We retrieved significantly more oocytes in the Study cycle, and the production of estradiol per follicle ≥10-mm diameter on trigger day was comparable in the study and control cycles, suggesting that the rescued follicles were competent in terms of producing oocytes and steroid hormones. LIMITATIONS, REASONS FOR CAUTION The sample size was small, and the study was not randomized. Our study design did not allow for the measurement and comparison of androgen levels or FSHR expression in small antral follicles before and immediately after the hCG-priming period. WIDER IMPLICATIONS OF THE FINDINGS The results make us question the mechanism of action behind hCG priming prior to IVF. It is important to design a study with the puncture of small antral follicles before and immediately after priming to investigate the proposed hypothesis. Improved cycle outcomes, i.e. more retrieved oocytes, must be confirmed in a larger, preferably randomized study. STUDY FUNDING/COMPETING INTEREST(S) This study was funded by an unrestricted grant from Gedeon Richter awarded to the institution. A.P. reports personal consulting fees from PregLem SA, Novo Nordisk A/S, Ferring Pharmaceuticals A/S, Gedeon Richter Nordics AB, Cryos International, and Merck A/S outside the submitted work and payment or honoraria for lectures from Gedeon Richter Nordics AB, Ferring Pharmaceuticals A/S, Merck A/S, and Theramex and Organon & Co and payment for participation in an advisory board for Preglem. Grants to the institution have been provided by Gedeon Richter Nordics AB, Ferring Pharmaceuticals A/S, and Merck A/S, and equipment and travel support has been given to the institution by Gedeon Richter Nordics AB. The remaining authors have no conflicts of interest to declare. TRIAL REGISTRATION NUMBER ClinicalTrials.gov Identifier: NCT04643925. [ABSTRACT FROM AUTHOR]

Published
2023
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41. Inhaled Corticosteroids in Patients with Chronic Obstructive Pulmonary Disease and Risk of Acquiring Streptococcus Pneumoniae Infection. A Multiregional Epidemiological study

Author

Kjer Heerfordt, C, primary, Eklöf, J, additional, Sivapalan, P, additional, Ingebrigtsen, T S, additional, Biering-Sørensen, T, additional, Barrella Harboe, Z, additional, Petersen, J K, additional, Andersen, C Ø, additional, Boel, J B, additional, Bock, A K, additional, Mathioudakis, A G, additional, Hurst, J R, additional, Kolekar, S, additional, Johansson, S L, additional, Bangsborg, J M, additional, Jarløv, J O, additional, Dessau, R, additional, Laursen, C B, additional, Perch, M, additional, and Jensen, J S, additional

Published
2022
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44. P-468 Organotypic culture of testicular tissue from infant boys with cryptorchidism

Author

Wang, D., Hildorf, Simone Engmann, Ntemou, Elissavet, Dong, L., Pors, S., Mamsen, L, Fedder, Jens, Hoffmann, Eva, Clasen-Linde, Erik, Cortes, Dina, Thorup, Jørgen, and Andersen, C.

Subjects
Reproductive Medicine, Rehabilitation, Obstetrics and Gynecology
Abstract

Study question Can organotypic culture support the survival and maturation of germ cells and niche-related cells within testicular tissue from infant boys with cryptorchidism? Summary answer The testicular structure and the number of germ cells were maintained during organotypic culture, whereas Sertoli cells and peritubular myoid cells (PTMCs) matured. What is known already Testicular tissue cryopreservation (TTC) is a strategy to safeguard the fertility of prepubertal boys who face a risk of infertility. Organotypic culture of immature testicular tissue from mice achieved production of spermatozoa. Similarly, the culture of human fetal gonads resulted in the generation of competent spermatids. However , in vitro spermatogenesis by organotypic culture of human prepubertal testicular tissue has not been achieved. It is also unknown whether germ cells as well as its niche-related cells, in testicular tissue from infant boys with cryptorchidism, can maintain and mature under in vitro conditions. Study design, size, duration Testicular tissue was cryopreserved from four infant boys with bilateral cryptorchidism undergoing orchidopexy (age range: 0.5-1.4 years), as part of a fertility preservation program. Culture media with and without retinoic acid were tested. Testicular fragments were harvested at 30 days and 60 days after culture and evaluated by histological assessment of tissue structure, germ cell development, and immunohistochemical staining for germ cell and somatic cell markers. Participants/materials, setting, methods Cryopreserved-thawed testicular tissue was cut into fragments (1-2 mm3) and placed on top of agarose gel stands and cultured at 34oC with 5% CO2 in Minimum Essential Medium-alpha supplemented with knockout serum replacement, human umbilical cord plasma, Activin A, hormones, growth factors, with or without retinoic acid. Immunohistochemical analyses were performed using germ cell markers (MAGE-A, GAGE, and VASA), Sertoli cell maturation markers (AMH, AR, SOX9), PTMC marker (alpha-SMA). Main results and the role of chance Following the 60-day culture, the lumen of the seminiferous tubules had developed. The number of germ cells per tubule remained stable during this period. However, no further germ cell maturation was observed. Germ cells showed different phenotypes of MAGEA, GAGE, and VASA expression with no significant difference in number. The number of SOX9-positive Sertoli cells was significantly increased from 30 days to 60 days of culture (p Limitations, reasons for caution The small number of testicular biopsies available is a limitation. Wider implications of the findings Our organotypic culture conditions support the long-term survival of germ cells in testicular tissue from infant boys with cryptorchidism. Thus, further studies are needed to induce the maturation of germ cells under similar experimental conditions. Trial registration number not applicable

Published
2022
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45. Variants in PHF8 cause a spectrum of X-linked neurodevelopmental disorders and facial dysmorphology

Author

Sobering, A.K., Bryant, L.M., Li, D., McGaughran, J., Maystadt, I., Moortgat, S., Graham, J.M., Haeringen, A. van, Ruivenkamp, C., Cuperus, R., Vogt, J., Morton, J., Brasch-Andersen, C., Steenhof, M., Hansen, L.K., Adler, E., Lyonnet, S., Pingault, V., Sandrine, M., Ziegler, A., Donald, T., Nelson, B., Holt, B., Petryna, O., Firth, H., McWalter, K., Zyskind, J., Telegrafi, A., Juusola, J., Person, R., Bamshad, M.J., Earl, D., Tsai, A.C.H., Yearwood, K.R., Marco, E., Nowak, C., Douglas, J., Hakonarson, H., Bhoj, E.J., and Univ Washington Ctr Mendelian Geno

Subjects
histone demethylation, PHF8, Molecular Medicine, orofacial clefting, Genetics (clinical), epigenetic gene regulation, X-linked intellectual disability
Abstract

Loss-of-function variants in PHD Finger Protein 8 (PHF8) cause Siderius X-linked intellectual disability (ID) syndrome, hereafter called PHF8-XLID. PHF8 is a histone demethylase that is important for epigenetic regulation of gene expression. PHF8-XLID is an under-characterized disorder with only five previous reports describing different PHF8 predicted loss-of-function variants in eight individuals. Features of PHF8-XLID include ID and craniofacial dysmorphology. In this report we present 16 additional individuals with PHF8-XLID from 11 different families of diverse ancestry. We also present five individuals from four different families who have ID and a variant of unknown significance in PHF8 with no other explanatory variant in another gene. All affected individuals exhibited developmental delay and all but two had borderline to severe ID. Of the two who did not have ID, one had dyscalculia and the other had mild learning difficulties. Craniofacial findings such as hypertelorism, microcephaly, elongated face, ptosis, and mild facial asymmetry were found in some affected individuals. Orofacial clefting was seen in three individuals from our cohort, suggesting that this feature is less common than previously reported. Autism spectrum disorder and attention deficit hyperactivity disorder, which were not previously emphasized in PHF8-XLID, were frequently observed in affected individuals. This series expands the clinical phenotype of this rare ID syndrome caused by loss of PHF8 function.

Published
2022
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46. Genotype-Phenotype Comparison in POGZ-Related Neurodevelopmental Disorders by Using Clinical Scoring

Author

Nagy, D., Verheyen, S., Wigby, K.M., Borovikov, A., Sharkov, A., Slegesky, V., Larson, A., Fagerberg, C., Brasch-Andersen, C., Kibæk, M., Bader, I., Hernan, R., High, F.A., Chung, W.K., Schieving, J.H., Behunova, J., Smogavec, M., Laccone, F., Witsch-Baumgartner, M., Zobel, J., Duba, H.C., Weis, D., Nagy, D., Verheyen, S., Wigby, K.M., Borovikov, A., Sharkov, A., Slegesky, V., Larson, A., Fagerberg, C., Brasch-Andersen, C., Kibæk, M., Bader, I., Hernan, R., High, F.A., Chung, W.K., Schieving, J.H., Behunova, J., Smogavec, M., Laccone, F., Witsch-Baumgartner, M., Zobel, J., Duba, H.C., and Weis, D.

Abstract

Contains fulltext : 248217.pdf (Publisher’s version ) (Open Access), POGZ-related disorders (also known as White-Sutton syndrome) encompass a wide range of neurocognitive abnormalities and other accompanying anomalies. Disease severity varies widely among POGZ patients and studies investigating genotype-phenotype association are scarce. Therefore, our aim was to collect data on previously unreported POGZ patients and perform a large-scale phenotype-genotype comparison from published data. Overall, 117 POGZ patients' genotype and phenotype data were included in the analysis, including 12 novel patients. A severity scoring system was developed for the comparison. Mild and severe phenotypes were compared with the types and location of the variants and the predicted presence or absence of nonsense-mediated RNA decay (NMD). Missense variants were more often associated with mild phenotypes (p = 0.0421) and truncating variants predicted to escape NMD presented with more severe phenotypes (p < 0.0001). Within this group, variants in the prolin-rich region of the POGZ protein were associated with the most severe phenotypes (p = 0.0004). Our study suggests that gain-of-function or dominant negative effect through escaping NMD and the location of the variants in the prolin-rich domain of the protein may play an important role in the severity of manifestations of POGZ-associated neurodevelopmental disorders.

Published
2022

47. Loss-of-function variants in SRRM2 cause a neurodevelopmental disorder

Author

Cuinat, S., Nizon, M., Isidor, B., Stegmann, Alexander, Jaarsveld, R.H. van, Gassen, K.L.I. van, Smagt, J.J. van der, Volker-Touw, C.M., Holwerda, S.J.B., Terhal, P.A., Schuhmann, S., Vasileiou, G., Khalifa, M., Nugud, A.A., Yasaei, H., Ousager, L.B., Brasch-Andersen, C., Deb, W., Besnard, T., Simon, M.E., Amsterdam, K.H., Verbeek, N.E., Matalon, D., Dykzeul, N., White, S., Spiteri, E., Devriendt, K., Boogaerts, A., Willemsen, M.H., Brunner, H.G., Sinnema, M., Vries, B.B. de, Gerkes, E.H., Pfundt, R.P., Izumi, K., Krantz, I.D., Xu, Z.L., Murrell, J.R., Valenzuela, I., Cusco, I., Rovira-Moreno, E., Yang, Y., Bizaoui, V., Patat, O., Faivre, L., Tran-Mau-Them, F., Vitobello, A., Denommé-Pichon, A.S., Philippe, C., Bezieau, S., Cogné, B., Cuinat, S., Nizon, M., Isidor, B., Stegmann, Alexander, Jaarsveld, R.H. van, Gassen, K.L.I. van, Smagt, J.J. van der, Volker-Touw, C.M., Holwerda, S.J.B., Terhal, P.A., Schuhmann, S., Vasileiou, G., Khalifa, M., Nugud, A.A., Yasaei, H., Ousager, L.B., Brasch-Andersen, C., Deb, W., Besnard, T., Simon, M.E., Amsterdam, K.H., Verbeek, N.E., Matalon, D., Dykzeul, N., White, S., Spiteri, E., Devriendt, K., Boogaerts, A., Willemsen, M.H., Brunner, H.G., Sinnema, M., Vries, B.B. de, Gerkes, E.H., Pfundt, R.P., Izumi, K., Krantz, I.D., Xu, Z.L., Murrell, J.R., Valenzuela, I., Cusco, I., Rovira-Moreno, E., Yang, Y., Bizaoui, V., Patat, O., Faivre, L., Tran-Mau-Them, F., Vitobello, A., Denommé-Pichon, A.S., Philippe, C., Bezieau, S., and Cogné, B.

Abstract

Contains fulltext : 282702.pdf (Publisher’s version ) (Closed access), PURPOSE: SRRM2 encodes the SRm300 protein, a splicing factor of the SR-related protein family characterized by its serine- and arginine-enriched domains. It promotes interactions between messenger RNA and the spliceosome catalytic machinery. This gene, predicted to be highly intolerant to loss of function (LoF) and very conserved through evolution, has not been previously reported in constitutive human disease. METHODS: Among the 1000 probands studied with developmental delay and intellectual disability in our database, we found 2 patients with de novo LoF variants in SRRM2. Additional families were identified through GeneMatcher. RESULTS: Here, we report on 22 patients with LoF variants in SRRM2 and provide a description of the phenotype. Molecular analysis identified 12 frameshift variants, 8 nonsense variants, and 2 microdeletions of 66 kb and 270 kb. The patients presented with a mild developmental delay, predominant speech delay, autistic or attention-deficit/hyperactivity disorder features, overfriendliness, generalized hypotonia, overweight, and dysmorphic facial features. Intellectual disability was variable and mild when present. CONCLUSION: We established SRRM2 as a gene responsible for a rare neurodevelopmental disease.

Published
2022

48. Protocol describing a systematic review and mixed methods consensus process to define the deteriorated ward patient.

Author

Malycha, J, Andersen, C, Redfern, OC, Peake, S, Subbe, C, Dykes, L, Phillips, A, Ludbrook, G, Young, D, Watkinson, PJ, Flabouris, A, Jones, D, Malycha, J, Andersen, C, Redfern, OC, Peake, S, Subbe, C, Dykes, L, Phillips, A, Ludbrook, G, Young, D, Watkinson, PJ, Flabouris, A, and Jones, D

Abstract

INTRODUCTION: Most patients admitted to hospital recover with treatments that can be administered on the general ward. A small but important group deteriorate however and require augmented organ support in areas with increased nursing to patient ratios. In observational studies evaluating this cohort, proxy outcomes such as unplanned intensive care unit admission, cardiac arrest and death are used. These outcome measures introduce subjectivity and variability, which in turn hinders the development and accuracy of the increasing numbers of electronic medical record (EMR) linked digital tools designed to predict clinical deterioration. Here, we describe a protocol for developing a new outcome measure using mixed methods to address these limitations. METHODS AND ANALYSIS: We will undertake firstly, a systematic literature review to identify existing generic, syndrome-specific and organ-specific definitions for clinically deteriorated, hospitalised adult patients. Secondly, an international modified Delphi study to generate a short list of candidate definitions. Thirdly, a nominal group technique (NGT) (using a trained facilitator) will take a diverse group of stakeholders through a structured process to generate a consensus definition. The NGT process will be informed by the data generated from the first two stages. The definition(s) for the deteriorated ward patient will be readily extractable from the EMR. ETHICS AND DISSEMINATION: This study has ethics approval (reference 16399) from the Central Adelaide Local Health Network Human Research Ethics Committee. Results generated from this study will be disseminated through publication and presentation at national and international scientific meetings.

Published
2022

49. Personalized circulating tumor DNA in patients with hepatocellular carcinoma:a pilot study

Author

Pommergaard, H. C., Yde, C. W., Ahlborn, L. B., Andersen, C. L., Henriksen, T., Hasselby, J. P., Rostved, A. A., Sorensen, C. L., Rohrberg, K. S., Nielsen, F. C., Rasmussen, A., Pommergaard, H. C., Yde, C. W., Ahlborn, L. B., Andersen, C. L., Henriksen, T., Hasselby, J. P., Rostved, A. A., Sorensen, C. L., Rohrberg, K. S., Nielsen, F. C., and Rasmussen, A.

Abstract

Background Mutational analysis of circulating tumor DNA (ctDNA) can potentially be used for early detection of recurrence after resection for hepatocellular carcinoma (HCC). Mutations from tumor may be identified in plasma as an early sign of recurrence. We conducted a pilot study investigating if somatic mutations could be detected in plasma in patients undergoing liver resection for HCC and in patients with advanced non-resectable HCC. Methods and results We prospectively included patients undergoing curative liver resection for HCC. Tumor tissue was investigated with whole exome sequencing and preoperative blood samples were evaluated for ctDNA using targeted next-generation sequencing (NGS) with TruSight Oncology 500 including 523 cancer-associated genes. Subsequently, the method was evaluated in patients with advanced HCC. We included eight patients curatively resected for HCC, where tumor tissue mutations were identified in seven patients. However, only in one patient tumor specific mutations were found in the preoperative blood sample. In all three patients with advanced HCC, tumor mutations were detected in the blood. Conclusions In patients with resectable HCC, ctDNA could not be reliably detected using the applied targeted NGS method. In contrast, ctDNA was detected in all patients with advanced HCC. Small tumors, tumor heterogeneity and limited sequencing coverage may explain the lack of detectable ctDNA.

Published
2022

50. Ovarian Tissue Banking to Postpone Menopause

Author

Grynberg, Michael, Patrizio, Pasquale, Yding Andersen, C., Jouhari, S., Mamsen, L. S., Skouby, S. O., Grynberg, Michael, Patrizio, Pasquale, Yding Andersen, C., Jouhari, S., Mamsen, L. S., and Skouby, S. O.

Abstract

The rising life expectancy far beyond any historical records presents serious demographic and socioeconomic changes to society with critical challenges for healthy aging. The burden of the menopause-related diseases will invariably increase in the coming years including the risk of osteoporosis, cardiovascular disease, dementia and cognitive decline. The main reason is loss of ovarian function and circulating concentrations of sex steroids. Existing therapies to reduce the burden of menopause-related diseases (i.e. hormone therapy, lifestyle changes and alternative medications) apparently have their shortcomings and are only partly capable of solving the problem, implying that new alternative solutions are warranted. The present review emphasizes that ovarian follicles are present in huge surplus during most of the reproductive active years and that current technology allows cryopreservation of resting follicles, apparently with little consequences for the woman’s reproductive abilities. Based on the multitude and complexity of oestrogen and progestin signalling pathways active and its intricate control in target cells throughout the body, we suggest that ovarian tissue transplanted back into the woman herself after menopause will allow for continued menstrual cycles with the whole armamentarium of hormones and growth factors released naturally from the follicle and the corpus luteum. This option has been termed cellular hormone replacement therapy. This new solution needs to be backed by clinical trials, extensive research and investigations of potential side effects to qualify as a valid alternative to existing therapies.

Published
2022

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