764 results on '"Künstner A"'
Search Results
2. Genome-wide DNA methylation-analysis of blastic plasmacytoid dendritic cell neoplasm identifies distinct molecular features
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Künstner, Axel, Schwarting, Julian, Witte, Hanno M., Xing, Pengwei, Bernard, Veronica, Stölting, Stephanie, Lohneis, Philipp, Janke, Florian, Salehi, Maede, Chen, Xingqi, Kusch, Kathrin, Sültmann, Holger, Chteinberg, Emil, Fischer, Anja, Siebert, Reiner, von Bubnoff, Nikolas, Merz, Hartmut, Busch, Hauke, Feller, Alfred C., and Gebauer, Niklas
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- 2024
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3. Diagnostic management of blastic plasmacytoid dendritic cell neoplasm (BPDCN) in close interaction with therapeutic considerations
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Shumilov, Evgenii, Mazzeo, Paolo, Ghandili, Susanne, Künstner, Axel, Weidemann, Sören, Banz, Yara, Ströbel, Philipp, Pollak, Matthias, Kolloch, Lina, Beltraminelli, Helmut, Kerkhoff, Andrea, Mikesch, Jan-Henrik, Schliemann, Christoph, Haase, Detlef, Wulf, Gerald, Legros, Myriam, Lenz, Georg, Feldmeyer, Laurence, Pabst, Thomas, Witte, Hanno, Gebauer, Niklas, and Bacher, Ulrike
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- 2024
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4. Electromagnetic modeling and science reach of DMRadio-m$^3$
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DMRadio Collaboration, AlShirawi, A., Bartram, C., Benabou, J. N., Brouwer, L., Chaudhuri, S., Cho, H. -M., Corbin, J., Craddock, W., Droster, A., Foster, J. W., Fry, J. T., Graham, P. W., Henning, R., Irwin, K. D., Kadribasic, F., Kahn, Y., Keller, A., Kolevatov, R., Kuenstner, S., Kurita, N., Leder, A. F., Li, D., Ouellet, J. L., Pappas, K. M. W., Phipps, A., Rapidis, N. M., Safdi, B. R., Salemi, C. P., Simanovskaia, M., Singh, J., van Assendelft, E. C., van Bibber, K., Wells, K., Winslow, L., Wisniewski, W. J., and Young, B. A.
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High Energy Physics - Experiment ,Astrophysics - Cosmology and Nongalactic Astrophysics ,High Energy Physics - Phenomenology ,Physics - Instrumentation and Detectors - Abstract
DMRadio-m$^3$ is an experiment that is designed to be sensitive to KSVZ and DFSZ QCD axion models in the 10-200 MHz (41 neV$/c^2$ - 0.83 $\mu$eV/$c^2$) range. The experiment uses a solenoidal dc magnetic field to convert an axion dark-matter signal to an ac electromagnetic response in a coaxial copper pickup. The current induced by this axion signal is measured by dc SQUIDs. In this work, we present the electromagnetic modeling of the response of the experiment to an axion signal over the full frequency range of DMRadio-m$^3$, which extends from the low-frequency, lumped-element limit to a regime where the axion Compton wavelength is only a factor of two larger than the detector size. With these results, we determine the live time and sensitivity of the experiment. The primary science goal of sensitivity to DFSZ axions across 30-200 MHz can be achieved with a $3\sigma$ live scan time of 3.7 years., Comment: 14 pages, 6 figures
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- 2023
5. Increase in body weight is lowered when mice received fecal microbiota transfer from donor mice treated with the AT1 receptor antagonist telmisartan
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Marco L. Freschi, Axel Künstner, Gianna Huber, Ines Stölting, Hauke Busch, Misa Hirose, and Walter Raasch
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obesity ,renin-angiotensin aldosterone system (RAAS) ,telmisartan ,microbiota transfer ,desulovibrio ,weight reduction ,Therapeutics. Pharmacology ,RM1-950 - Abstract
IntroductionTreatment of rodents with the AT1 blocker (ARB) telmisartan (TEL) has an anti-adipose effect. Among other mechanisms, we also have attributed the anti-adipose action to diet-independent alterations in gut microbiota. Thus, we aimed here to confirm this mechanism by using the fecal microbiota transfer (FMT) approach.MethodsSeven weeks after initiating a high-fat diet (HFD), C57BL/6N mice received fecal microbiota for 8 weeks from donor mice by oral gavage, continuing HFD feeding. Stool samples came from mice that were treated with TEL (8 mg/kg/d by gavage, 12 weeks), thus remaining lean despite HFD feeding (BL/6>fTEL), while controls received feces samples from vehicle/HFD-treated obese mice (BL/6>fVEH). Microbiota of the stool samples from these acceptor mice was analyzed by 16S rRNA gene amplicon sequencing.ResultsWeight gain was lower in BL6>fTEL than in BL6>fVEH mice after 3 but not 8 weeks. Energy homeostasis, insulin sensitivity, and body composition did not differ between the two groups. β-diversity indicated group differences (F = 2.27, p = 0.005). Although the Firmicutes/Bacteroides ratio did not differ, abundances of distinct phyla, families, and genera varied. Among others, Ruminococcaceae and Desulfovibrionaceae, Desulfovibrionia uncl., and Lachnospiraceae uncl. were lower in BL/6>fTEL than in BL/6>fVEH mice. Moreover, the correlation between body weight and Lachnospiraceae, Desulfovibrionaceae, Desulfovibrionia uncl., or Desulfovibrio was positive in BL/6>fVEH and negative in BL/6>fTEL mice.DiscussionAs FMT from TEL-pretreated mice influences the microbiota in acceptor mice with slight weight-reducing effects, we confirm the relevance of TEL-related microbiota changes for weight reduction, most likely independent of the transferred stool-residual TEL effect on the host metabolism.
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- 2024
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6. Case report: Tenosynovial giant cell tumor
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Anke Fähnrich, Zhala Gasimova, Yamil Maluje, Fabian Ott, Helen Sievert, Stephanie Fliedner, Niklas Reimer, Axel Künstner, Niklas Gebauer, Maxim Kebenko, Nikolas von Bubnoff, Jutta Kirfel, Verena-Wilbeth Sailer, Christoph Röcken, Bjoern Konukiewitz, Wolfram Klapper, Alex Frydrychowicz, Sam Mogadas, Gerdt Huebner, Hauke Busch, and Cyrus Khandanpour
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single cell sequencing (scRNA-seq) ,RNA sequencing (RNA-seq) ,CSF1 fusion transcript ,tenosynovial giant cell tumor (TGCT) ,molecular tumor board (MTB) ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
Tenosynovial giant cell tumor (TGCT) is a rare type of tumor that originates from the synovium of joints and tendon sheaths. It is characterized by recurring genetic abnormalities, often involving the CSF1 gene. Common symptoms include pain and swelling, which are not specific to TGCT, so MRI and a pathological biopsy are needed for an accurate diagnosis. We report the case of a 45-year-old man who experienced painful swelling in his right hip for six months. Initially, this was diagnosed as Erdheim-Chester disease. However, whole exome sequencing (WES) and RNA-Sequencing revealed a CSF1::GAPDHP64 fusion, leading to a revised diagnosis of TGCT. The patient was treated with pegylated interferon and imatinib, which resulted in stable disease after three months. Single-cell transcriptome analysis identified seven distinct cell clusters, revealing that neoplastic cells expressing CSF1 attract macrophages. Analysis of ligand-receptor interactions showed significant communication between neoplastic cells and macrophages mediated by CSF1 and CSF1R. Our findings emphasize the importance of comprehensive molecular analysis in diagnosing and treating rare malignancies like TGCT.
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- 2024
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7. Quantum metrology of low frequency electromagnetic modes with frequency upconverters
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Kuenstner, Stephen E., van Assendelft, Elizabeth C., Chaudhuri, Saptarshi, Cho, Hsiao-Mei, Corbin, Jason, Henderson, Shawn W., Kadribasic, Fedja, Li, Dale, Phipps, Arran, Rapidis, Nicholas M., Simanovskaia, Maria, Singh, Jyotirmai, Yu, Cyndia, and Irwin, Kent D.
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Quantum Physics ,Physics - Instrumentation and Detectors - Abstract
We present the RF Quantum Upconverter (RQU) and describe its application to quantum metrology of electromagnetic modes between dc and the Very High Frequency band (VHF) ($\lesssim$300MHz). The RQU uses a Josephson interferometer made up of superconducting loops and Josephson junctions to implement a parametric interaction between a low-frequency electromagnetic mode (between dc and VHF) and a mode in the microwave C Band ($\sim$ 5GHz), analogous to the radiation pressure interaction between electromagnetic and mechanical modes in cavity optomechanics. We analyze RQU performance with quantum amplifier theory, and show that the RQU can operate as a quantum-limited op-amp in this frequency range. It can also use non-classical measurement protocols equivalent to those used in cavity optomechanics, including back-action evading (BAE) measurements, sideband cooling, and two-mode squeezing. These protocols enable experiments using dc--VHF electromagnetic modes as quantum sensors with sensitivity better than the Standard Quantum Limit (SQL). We demonstrate signal upconversion from low frequencies to microwave C band using an RQU and show a phase-sensitive gain (extinction ratio) of $46.9$\;dB, which is a necessary step towards the realization of full BAE., Comment: -minor rewording and clarification of arguments in abstract, introduction, and conclusion -added discussion and citations for related devices in Section IIA -renamed section II C to Quantum Amplifier Theory -added discussion of Kerr nonlinearity in II C
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- 2022
8. Dispersive readout of a high-Q encapsulated micromechanical resonator
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Bousse, Nicholas E., Kuenstner, Stephen E., Miller, James M. L., Kwon, Hyun-Keun, Vukasin, Gabrielle D., Teufel, John D., and Kenny, Thomas W.
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Physics - Applied Physics ,Physics - Instrumentation and Detectors - Abstract
Encapsulated bulk mode microresonators in the megahertz range are used in commercial timekeeping and sensing applications but their performance is limited by the current state of the art of readout methods. We demonstrate a readout using dispersive coupling between a high-Q encapsulated bulk mode micromechanical resonator and a lumped element microwave resonator that is implemented with commercially available components and standard printed circuit board fabrication methods and operates at room temperature and pressure. A frequency domain measurement of the microwave readout system yields a displacement resolution of $522 \, \mathrm{fm/\sqrt{Hz}}$, which demonstrates an improvement over the state of the art of displacement measurement in bulk-mode encapsulated microresonators. This approach can be readily implemented in cryogenic measurements, allowing for future work characterizing the thermomechanical noise of encapsulated bulk mode resonators at cryogenic temperatures.
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- 2022
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9. Bandwidth and Aliasing in the Microwave SQUID Multiplexer
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Yu, Cyndia, Ahmed, Zeeshan, Connors, Jake A., D'Ewart, J. Mitch, Dober, Bradley, Frisch, Josef C., Henderson, Shawn W., Hilton, Gene C., Hubmayr, Johannes, Kuenstner, Stephen E., Mates, J. A. Ben, Silva-Feaver, Maximiliano, Ullom, Joel N., Vale, Leila R., Van Winkle, Dan, and Young, Edward
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Physics - Instrumentation and Detectors ,Astrophysics - Instrumentation and Methods for Astrophysics - Abstract
The microwave SQUID multiplexer (umux) has enabled higher bandwidth or higher channel counts across a wide range of experiments in particle physics, astronomy, and spectroscopy. The large multiplexing factor coupled with recent commercial availability of microwave components and warm electronics readout systems make it an attractive candidate for systems requiring large cryogenic detector counts. Since the multiplexer is considered for both bolometric and calorimetric applications across several orders of magnitude of signal frequencies, understanding the bandwidth of the device and its interaction with readout electronics is key to appropriately designing and engineering systems. Here we discuss several important factors contributing to the bandwidth properties of umux systems, including the intrinsic device bandwidth, interactions with warm electronics readout systems, and aliasing. We present simulations and measurements of umux devices coupled with SLAC Microresonator RF (SMuRF) tone-tracking electronics and discuss several implications for future experimental design., Comment: Proceedings for Low Temperature Physics 2021, accepted for publication in Journal of Low Temperature Physics. 8 pages (including references), 5 figures
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- 2022
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10. Projected Sensitivity of DMRadio-m$^3$: A Search for the QCD Axion Below $1\,\mu$eV
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DMRadio Collaboration, Brouwer, L., Chaudhuri, S., Cho, H. -M., Corbin, J., Craddock, W., Dawson, C. S., Droster, A., Foster, J. W., Fry, J. T., Graham, P. W., Henning, R., Irwin, K. D., Kadribasic, F., Kahn, Y., Keller, A., Kolevatov, R., Kuenstner, S., Leder, A. F., Li, D., Ouellet, J. L., Pappas, K., Phipps, A., Rapidis, N. M., Safdi, B. R., Salemi, C. P., Simanovskaia, M., Singh, J., van Assendelft, E. C., van Bibber, K., Wells, K., Winslow, L., Wisniewski, W. J., and Young, B. A.
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High Energy Physics - Experiment ,High Energy Physics - Phenomenology ,Physics - Instrumentation and Detectors - Abstract
The QCD axion is one of the most compelling candidates to explain the dark matter abundance of the universe. With its extremely small mass ($\ll 1\,\mathrm{eV}/c^2$), axion dark matter interacts as a classical field rather than a particle. Its coupling to photons leads to a modification of Maxwell's equations that can be measured with extremely sensitive readout circuits. DMRadio-m$^3$ is a next-generation search for axion dark matter below $1\,\mu$eV using a $>4$ T static magnetic field, a coaxial inductive pickup, a tunable LC resonator, and a DC-SQUID readout. It is designed to search for QCD axion dark matter over the range $20\,\mathrm{neV}\lesssim m_ac^2\lesssim 800\,\mathrm{neV}$ ($5\,\mathrm{MHz}<\nu<200\,\mathrm{MHz}$). The primary science goal aims to achieve DFSZ sensitivity above $m_ac^2\approx 120$ neV (30 MHz), with a secondary science goal of probing KSVZ axions down to $m_ac^2\approx40\,\mathrm{neV}$ (10 MHz)., Comment: 8 pages, 4 figures. Updated to fix small errors and correct acknowledgements. Updated title and notational clarifications
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- 2022
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11. Axion Dark Matter
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Adams, C. B., Aggarwal, N., Agrawal, A., Balafendiev, R., Bartram, C., Baryakhtar, M., Bekker, H., Belov, P., Berggren, K. K., Berlin, A., Boutan, C., Bowring, D., Budker, D., Caldwell, A., Carenza, P., Carosi, G., Cervantes, R., Chakrabarty, S. S., Chaudhuri, S., Chen, T. Y., Cheong, S., Chou, A., Co, R. T., Conrad, J., Croon, D., D'Agnolo, R. T., Demarteau, M., DePorzio, N., Descalle, M., Desch, K., Di Luzio, L., Diaz-Morcillo, A., Dona, K., Drachnev, I. S., Droster, A., Du, N., Dunne, K., Döbrich, B., Ellis, S. A. R., Essig, R., Fan, J., Foster, J. W., Fry, J. T., Rosso, A. Gallo, Barceló, J. M. García, Irastorza, I. G., Gardner, S., Geraci, A. A., Ghosh, S., Giaccone, B., Giannotti, M., Gimeno, B., Grin, D., Grote, H., Guzzetti, M., Awida, M. H., Henning, R., Hoof, S., Hoshino, G., Irsic, V., Irwin, K. D., Jackson, H., Kimball, D. F. Jackson, Jaeckel, J., Jakovcic, K., Jewell, M. J., Kagan, M., Kahn, Y., Khatiwada, R., Knirck, S., Kovachy, T., Krueger, P., Kuenstner, S. E., Kurinsky, N. A., Leane, R. K., Leder, A. F., Lee, C., Lehnert, K. W., Lentz, E. W., Lewis, S. M., Liu, J., Lynn, M., Majorovits, B., Marsh, D. J. E., Maruyama, R. H., McAllister, B. T., Millar, A. J., Miller, D. W., Mitchell, J., Morampudi, S., Mueller, G., Nagaitsev, S., Nardi, E., Noroozian, O., O'Hare, C. A. J., Oblath, N. S., Ouellet, J. L., Pappas, K. M. W., Peiris, H. V., Perez, K., Phipps, A., Pivovaroff, M. J., Quílez, P., Rapidis, N. M., Robles, V. H., Rogers, K. K., Rudolph, J., Ruz, J., Rybka, G., Safdari, M., Safdi, B. R., Safronova, M. S., Salemi, C. P., Schuster, P., Schwartzman, A., Shu, J., Simanovskaia, M., Singh, J., Singh, S., Sinha, K., Sinnis, J. T., Siodlaczek, M., Smith, M. S., Snow, W. M., Sokolov, A. V., Sonnenschein, A., Speller, D. H., Stadnik, Y. V., Sun, C., Sushkov, A. O., Tait, T. M. P., Takhistov, V., Tanner, D. B., Tavecchio, F., Temples, D. J., Thomas, J. H., Tobar, M. E., Toro, N., Tsai, Y. -D., van Assendelft, E. C., van Bibber, K., Vandegar, M., Visinelli, L., Vitagliano, E., Vogel, J. K., Wang, Z., Wickenbrock, A., Winslow, L., Withington, S., Wooten, M., Yang, J., Young, B. A., Yu, F., Zhou, K., and Zhou, T.
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High Energy Physics - Experiment ,Astrophysics - Cosmology and Nongalactic Astrophysics ,High Energy Physics - Phenomenology ,Physics - Instrumentation and Detectors - Abstract
Axions are well-motivated dark matter candidates with simple cosmological production mechanisms. They were originally introduced to solve the strong CP problem, but also arise in a wide range of extensions to the Standard Model. This Snowmass white paper summarizes axion phenomenology and outlines next-generation laboratory experiments proposed to detect axion dark matter. There are vibrant synergies with astrophysical searches and advances in instrumentation including quantum-enabled readout, high-Q resonators and cavities and large high-field magnets. This white paper outlines a clear roadmap to discovery, and shows that the US is well-positioned to be at the forefront of the search for axion dark matter in the coming decade., Comment: restore and expand author list
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- 2022
12. New Horizons: Scalar and Vector Ultralight Dark Matter
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Antypas, D., Banerjee, A., Bartram, C., Baryakhtar, M., Betz, J., Bollinger, J. J., Boutan, C., Bowring, D., Budker, D., Carney, D., Carosi, G., Chaudhuri, S., Cheong, S., Chou, A., Chowdhury, M. D., Co, R. T., López-Urrutia, J. R. Crespo, Demarteau, M., DePorzio, N., Derbin, A. V., Deshpande, T., Di Luzio, L., Diaz-Morcillo, A., Doyle, J. M., Drlica-Wagner, A., Droster, A., Du, N., Döbrich, B., Eby, J., Essig, R., Farren, G. S., Figueroa, N. L., Fry, J. T., Gardner, S., Geraci, A. A., Ghalsasi, A., Ghosh, S., Giannotti, M., Gimeno, B., Griffin, S. M., Grin, D., Grote, H., Gundlach, J. H., Guzzetti, M., Hanneke, D., Harnik, R., Henning, R., Irsic, V., Jackson, H., Kimball, D. F. Jackson, Jaeckel, J., Kagan, M., Kedar, D., Khatiwada, R., Knirck, S., Kolkowitz, S., Kovachy, T., Kuenstner, S. E., Lasner, Z., Leder, A. F., Lehnert, R., Leibrandt, D. R., Lentz, E., Lewis, S. M., Liu, Z., Manley, J., Maruyama, R. H., Millar, A. J., Muratova, V. N., Musoke, N., Nagaitsev, S., Noroozian, O., O'Hare, C. A. J., Ouellet, J. L., Pappas, K. M. W., Peik, E., Perez, G., Phipps, A., Rapidis, N. M., Robinson, J. M., Robles, V. H., Rogers, K. K., Rudolph, J., Rybka, G., Safdari, M., Safronova, M. S., Salemi, C. P., Schmidt, P. O., Schumm, T., Schwartzman, A., Shu, J., Simanovskaia, M., Singh, J., Singh, S., Smith, M. S., Snow, W. M., Stadnik, Y. V., Sun, C., Sushkov, A. O., Tait, T. M. P., Takhistov, V., Tanner, D. B., Temples, D. J., Thirolf, P. G., Thomas, J. H., Tobar, M. E., Tretiak, O., Tsai, Y. -D., Tyson, J. A., Vandegar, M., Vermeulen, S., Visinelli, L., Vitagliano, E., Wang, Z., Wilson, D. J., Winslow, L., Withington, S., Wooten, M., Yang, J., Ye, J., Young, B. A., Yu, F., Zaheer, M. H., Zelevinsky, T., Zhao, Y., and Zhou, K.
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High Energy Physics - Experiment ,Astrophysics - Cosmology and Nongalactic Astrophysics ,High Energy Physics - Phenomenology ,Physics - Instrumentation and Detectors ,Quantum Physics - Abstract
The last decade has seen unprecedented effort in dark matter model building at all mass scales coupled with the design of numerous new detection strategies. Transformative advances in quantum technologies have led to a plethora of new high-precision quantum sensors and dark matter detection strategies for ultralight ($<10\,$eV) bosonic dark matter that can be described by an oscillating classical, largely coherent field. This white paper focuses on searches for wavelike scalar and vector dark matter candidates., Comment: Snowmass 2021 White Paper
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- 2022
13. Introducing DMRadio-GUT, a search for GUT-scale QCD axions
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Brouwer, L., Chaudhuri, S., Cho, H. -M., Corbin, J., Dawson, C. S., Droster, A., Foster, J. W., Fry, J. T., Graham, P. W., Henning, R., Irwin, K. D., Kadribasic, F., Kahn, Y., Keller, A., Kolevatov, R., Kuenstner, S., Leder, A. F., Li, D., Ouellet, J. L., Pappas, K. M. W., Phipps, A., Rapidis, N. M., Safdi, B. R., Salemi, C. P., Simanovskaia, M., Singh, J., van Assendelft, E. C., van Bibber, K., Wells, K., Winslow, L., Wisniewski, W. J., and Young, B. A.
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High Energy Physics - Experiment ,High Energy Physics - Phenomenology - Abstract
The QCD axion is a leading dark matter candidate that emerges as part of the solution to the strong CP problem in the Standard Model. The coupling of the axion to photons is the most common experimental probe, but much parameter space remains unexplored. The coupling of the QCD axion to the Standard Model scales linearly with the axion mass; therefore, the highly-motivated region 0.4-120 neV, corresponding to a GUT-scale axion, is particularly difficult to reach. This paper presents the design requirements for a definitive search for GUT-scale axions and reviews the technological advances needed to enable this program., Comment: 16 pages, 4 figures
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- 2022
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14. Molecularly Stratified Treatment Options in Primary Refractory DLBCL/HGBL with MYC and BCL2 or BCL6 Rearrangements (HGBL, NOS with MYC/BCL6)
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Witte, Hanno M., Riedl, Jörg, Künstner, Axel, Fähnrich, Anke, Ketzer, Julius, Fliedner, Stephanie M. J., Reimer, Niklas, Bernard, Veronica, von Bubnoff, Nikolas, Merz, Hartmut, Busch, Hauke, Feller, Alfred, and Gebauer, Niklas
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- 2023
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15. Transcriptome Profiling Associated with CARD11 Overexpression in Colorectal Cancer Implicates a Potential Role for Tumor Immune Microenvironment and Cancer Pathways Modulation via NF-κB
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Faisal Alhosani, Burcu Yener Ilce, Reem Sami Alhamidi, Poorna Manasa Bhamidimarri, Alaa Mohamed Hamad, Noura Alkhayyal, Axel Künstner, Cyrus Khandanpour, Hauke Busch, Basel Al-Ramadi, Kadria Sayed, Ali AlFazari, Riyad Bendardaf, and Rifat Hamoudi
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CARD11 ,colorectal cancer ,tumor immune microenvironment ,GSEA ,NF-κB pathway ,Biology (General) ,QH301-705.5 ,Chemistry ,QD1-999 - Abstract
The immune system plays a critical role in inflammation by initiating responses to infections or tissue damage. The nuclear factor-κB (NF-κB) pathway plays a key role in inflammation and innate immunity, as well as other cellular activities. Dysregulation of this well-choreographed pathway has been implicated in various diseases, including cancer. CARD11 is a key molecule in the BCL10-MALT1 complex, which is involved in transducing the signal downstream of the NF-κB pathway. This study aims to elucidate how CARD11 overexpression exacerbates the prognosis of colorectal cancer (CRC). To identify the cellular pathways influenced by CARD11, transcriptomic analysis in both CRC cell lines and patients was carried out on CARD11– overexpressed HCT-116 and HT-29 CRC cell lines alongside empty vector-transfected cell lines. Furthermore, a comparison of transcriptomic data from adenoma and carcinoma CRC patients with low- (CARD11–) and high-(CARD11+) CARD11 expression was carried out. Whole transcriptomics and bioinformatics analysis results indicate that CARD11 appears to play a key role in CRC progression. Absolute GSEA (absGSEA) on HCT-116 transcriptomics data revealed that CARD11 overexpression promotes cell growth and tissue remodeling and enhances immune response. Key genes co-expressed with CARD11, such as EP300, KDM5A, HIF1A, NFKBIZ, and DUSP1, were identified as mediators of these processes. In the HT-29 cell line, CARD11 overexpression activated pathways involved in chemotaxis and extracellular matrix (ECM) organization, marked by IL1RN, MDK, SPP1, and chemokines like CXCL1, CXCL3, and CCL22, which were shown to contribute to the more invasive stage of CRC. In patient samples, adenoma patients exhibited increased expression of genes associated with the tumor immune microenvironment, such as IL6ST, collagen family members, and CRC transition markers, such as GLI3 and PIEZO2, in CARD11+ adenoma patients. Carcinoma patients showed a dramatic increase in the expression of MAPK8IP2 in CARD11+ carcinoma patients alongside other cancer-related genes, including EMB, EPHB6, and CPEB4.
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- 2024
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16. Intravenous Ig Ameliorates Disease in a Murine Model of Anti–Laminin 332 Mucous Membrane Pemphigoid
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Murthy, Sripriya, Patzelt, Sabrina, Künstner, Axel, Busch, Hauke, Schmidt, Enno, and Sadik, Christian D.
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- 2024
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17. A comprehensive analysis of gut and skin microbiota in canine atopic dermatitis in Shiba Inu dogs
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Thomsen, Mirja, Künstner, Axel, Wohlers, Inken, Olbrich, Michael, Lenfers, Tim, Osumi, Takafumi, Shimazaki, Yotaro, Nishifuji, Koji, Ibrahim, Saleh M., Watson, Adrian, Busch, Hauke, and Hirose, Misa
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- 2023
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18. Uncovering the relationship between gut microbial dysbiosis, metabolomics, and dietary intake in type 2 diabetes mellitus and in healthy volunteers: a multi-omics analysis
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Al Bataineh, Mohammad Tahseen, Künstner, Axel, Dash, Nihar Ranjan, Alsafar, Habiba S., Ragab, Mohab, Schmelter, Franziska, Sina, Christian, Busch, Hauke, and Ibrahim, Saleh Mohamed
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- 2023
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19. MBECS: Microbiome Batch Effects Correction Suite
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Olbrich, Michael, Künstner, Axel, and Busch, Hauke
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- 2023
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20. Panomics reveals patient individuality as the major driver of colorectal cancer progression
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Praus, Friederike, Künstner, Axel, Sauer, Thorben, Kohl, Michael, Kern, Katharina, Deichmann, Steffen, Végvári, Ákos, Keck, Tobias, Busch, Hauke, Habermann, Jens K., and Gemoll, Timo
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- 2023
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21. Uncovering the relationship between gut microbial dysbiosis, metabolomics, and dietary intake in type 2 diabetes mellitus and in healthy volunteers: a multi-omics analysis
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Mohammad Tahseen Al Bataineh, Axel Künstner, Nihar Ranjan Dash, Habiba S. Alsafar, Mohab Ragab, Franziska Schmelter, Christian Sina, Hauke Busch, and Saleh Mohamed Ibrahim
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Medicine ,Science - Abstract
Abstract Type 2 Diabetes Mellitus has reached epidemic levels globally, and several studies have confirmed a link between gut microbial dysbiosis and aberrant glucose homeostasis among people with diabetes. While the assumption is that abnormal metabolomic signatures would often accompany microbial dysbiosis, the connection remains largely unknown. In this study, we investigated how diet changed the gut bacteriome, mycobiome and metabolome in people with and without type 2 Diabetes.1 Differential abundance testing determined that the metabolites Propionate, U8, and 2-Hydroxybutyrate were significantly lower, and 3-Hydroxyphenyl acetate was higher in the high fiber diet compared to low fiber diet in the healthy control group. Next, using multi-omics factor analysis (MOFA2), we attempted to uncover sources of variability that drive each of the different groups (bacterial, fungal, and metabolite) on all samples combined (control and DM II). Performing variance decomposition, ten latent factors were identified, and then each latent factor was tested for significant correlations with age, BMI, diet, and gender. Latent Factor1 was the most significantly correlated. Remarkably, the model revealed that the mycobiome explained most of the variance in the DM II group (12.5%) whereas bacteria explained most of the variance in the control group (64.2% vs. 10.4% in the DM II group). The latent Factor1 was significantly correlated with dietary intake (q 0.6). Alternatively, a linear regression model was fitted per disease group for each genus to visualize the relationship between the factor values and feature abundances, showing Xylose with positive weights and Propionate, U8, and 2-Hydroxybutyrate with negative weights. This data provides new information on the microbially derived changes that influence metabolic phenotypes in response to different diets and disease conditions in humans.
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- 2023
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22. A comprehensive analysis of gut and skin microbiota in canine atopic dermatitis in Shiba Inu dogs
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Mirja Thomsen, Axel Künstner, Inken Wohlers, Michael Olbrich, Tim Lenfers, Takafumi Osumi, Yotaro Shimazaki, Koji Nishifuji, Saleh M. Ibrahim, Adrian Watson, Hauke Busch, and Misa Hirose
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Canine atopic dermatitis ,Shiba Inu dogs ,16S rRNA ,Skin and gut microbiota ,Staphylococcus ,Fusobacterium ,Microbial ecology ,QR100-130 - Abstract
Abstract Background Like its human counterpart, canine atopic dermatitis (cAD) is a chronic relapsing condition; thus, most cAD-affected dogs will require lifelong treatment to maintain an acceptable quality of life. A potential intervention is modulation of the composition of gut microbiota, and in fact, probiotic treatment has been proposed and tried in human atopic dermatitis (AD) patients. Since dogs are currently receiving intensive medical care, this will be the same option for dogs, while evidence of gut dysbiosis in cAD is still missing, although skin microbial profiling in cAD has been conducted in several studies. Therefore, we conducted a comprehensive analysis of both gut and skin microbiota in cAD in one specific cAD-predisposed breed, Shiba Inu. Additionally, we evaluated the impact of commonly used medical management on cAD (Janus kinase; JAK inhibitor, oclacitinib) on the gut and skin microbiota. Furthermore, we genotyped the Shiba Inu dogs according to the mitochondrial DNA haplogroup and assessed its association with the composition of the gut microbiota. Results Staphylococcus was the most predominant bacterial genus observed in the skin; Escherichia/Shigella and Clostridium sensu stricto were highly abundant in the gut of cAD-affected dogs. In the gut microbiota, Fusobacteria and Megamonas were highly abundant in healthy dogs but significantly reduced in cAD-affected dogs. The abundance of these bacterial taxa was positively correlated with the effect of the treatment and state of the disease. Oclacitinib treatment on cAD-affected dogs shifted the composition of microbiota towards that in healthy dogs, and the latter brought it much closer to healthy microbiota, particularly in the gut. Additionally, even within the same dog breed, the mtDNA haplogroup varied, and there was an association between the mtDNA haplogroup and microbial composition in the gut and skin. Conclusions Dysbiosis of both the skin and the gut was observed in cAD in Shiba Inu dogs. Our findings provide a basis for the potential treatment of cAD by manipulating the gut microbiota as well as the skin microbiota. Video Abstract
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- 2023
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23. Update: The molecular spectrum of virus-associated high-grade B-cell non-Hodgkin lymphomas
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Witte, H., Künstner, A., and Gebauer, N.
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- 2024
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24. An Impedance-Modulated Code-Division Microwave SQUID Multiplexer
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Yu, C., Ames, A., Chaudhuri, S., Dawson, C., Irwin, K. D., Kuenstner, S. E., Li, D., and Titus, C. J.
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Physics - Instrumentation and Detectors ,Astrophysics - Instrumentation and Methods for Astrophysics - Abstract
Large arrays of cryogenic detectors, including transition-edge sensors (TESs) or magnetic micro-calorimeters (MMCs), are needed for future experiments across a wide range of applications. Complexities in integration and cryogenic wiring have driven efforts to develop cryogenic readout technologies with large multiplexing factors while maintaining minimal readout noise. One such example is the microwave SQUID multiplexer ($\mu$mux), which couples an incoming TES or magnetic calorimeter signal to a unique GHz-frequency resonance that is modulated in frequency. Here, we present a hybrid scheme combining the microwave SQUID multiplexer with code division multiplexing: the impedance-modulated code-division multiplexer (Z-CDM), which may enable an order of magnitude increase in multiplexing factor particularly for low-bandwidth signal applications., Comment: 10 pages including references, 3 figures; submitted to Engineering Research Express
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- 2020
25. Germ line variant GFI1-36N affects DNA repair and sensitizes AML cells to DNA damage and repair therapy
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Frank, Daria, Patnana, Pradeep Kumar, Vorwerk, Jan, Mao, Lianghao, Gopal, Lavanya Mokada, Jung, Noelle, Hennig, Thorben, Ruhnke, Leo, Frenz, Joris Maximillian, Kuppusamy, Maithreyan, Autry, Robert, Wei, Lanying, Sun, Kaiyan, Mohammed Ahmed, Helal Mohammed, Künstner, Axel, Busch, Hauke, Müller, Heiko, Hutter, Stephan, Hoermann, Gregor, Liu, Longlong, Xie, Xiaoqing, Al-Matary, Yahya, Nimmagadda, Subbaiah Chary, Cano, Fiorella Charles, Heuser, Michael, Thol, Felicitas, Göhring, Gudrun, Steinemann, Doris, Thomale, Jürgen, Leitner, Theo, Fischer, Anja, Rad, Roland, Röllig, Christoph, Altmann, Heidi, Kunadt, Desiree, Berdel, Wolfgang E., Hüve, Jana, Neumann, Felix, Klingauf, Jürgen, Calderon, Virginie, Opalka, Bertram, Dührsen, Ulrich, Rosenbauer, Frank, Dugas, Martin, Varghese, Julian, Reinhardt, Hans Christian, von Bubnoff, Nikolas, Möröy, Tarik, Lenz, Georg, Batcha, Aarif M. N., Giorgi, Marianna, Selvam, Murugan, Wang, Eunice, McWeeney, Shannon K., Tyner, Jeffrey W., Stölzel, Friedrich, Mann, Matthias, Jayavelu, Ashok Kumar, and Khandanpour, Cyrus
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- 2023
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26. MBECS: Microbiome Batch Effects Correction Suite
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Michael Olbrich, Axel Künstner, and Hauke Busch
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Microbiome ,Batch effects ,R-package ,phyloseq ,Bioconductor ,Computer applications to medicine. Medical informatics ,R858-859.7 ,Biology (General) ,QH301-705.5 - Abstract
Abstract Despite the availability of batch effect correcting algorithms (BECA), no comprehensive tool that combines batch correction and evaluation of the results exists for microbiome datasets. This work outlines the Microbiome Batch Effects Correction Suite development that integrates several BECAs and evaluation metrics into a software package for the statistical computation framework R.
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- 2023
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27. Methodology to assess damage mechanisms of rail steels based on small-scale experiments
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Al-Maliki, H., Künstner, D., Scheriau, S., Six, K., and Trummer, G.
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- 2023
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28. Proton pump inhibitor treatment aggravates bacterial translocation in patients with advanced cirrhosis and portal hypertension
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Lukas Sturm, Misa Hirose, Laura Stolz, Michael Schultheiss, Katharina Zoldan, Marlene Reincke, Jan Patrick Huber, Rafael Kaeser, Tobias Boettler, Robert Thimme, Elisabeth Albert, Hauke Busch, Axel Künstner, and Dominik Bettinger
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bacterial translocation ,cirrhosis ,portal hypertension ,proton pump inhibitor ,microbiome ,Microbiology ,QR1-502 - Abstract
ABSTRACT Recent studies have linked proton pump inhibitor (PPI) treatment to increased complications of cirrhosis, such as bacterial infections and hepatic encephalopathy. However, the underlying pathophysiological mechanisms remain unclear. The present study investigated the hypothesis that PPI treatment may promote adverse effects in patients with advanced cirrhosis by affecting subclinical bacterial translocation (BT) from the gut into the portal venous bloodstream. Blood samples from the portal vein were obtained during implantation of a transjugular intrahepatic portosystemic shunt (TIPS) in a total of 80 cirrhosis patients with PPI treatment (PPI group, n = 57) and without PPI treatment (no-PPI group, n = 23). BT was identified using a 16S ribosomal RNA gene (V1V2 region) polymerase chain reaction. The microbiota composition in the portal venous blood samples was further analyzed by deep amplicon sequencing. Indeed, the prevalence of BT was significantly higher in the PPI group compared to the no-PPI group (86.0% vs 52.2%, P = 0.001). Importantly, this effect was not attributable to group differences in the severity of cirrhosis, parameters of portal hypertension, or medication. Microbiome analyses showed significantly increased alpha-diversity (Shannon) in the portal venous blood of the PPI group. Taxonomic analyses revealed significantly increased Streptococcus abundances in these patients. The present study reveals aggravated BT in patients with advanced cirrhosis and portal hypertension receiving PPI therapy. Increased BT could be an important pathomechanism contributing to the adverse effects of PPI treatment in patients with cirrhosis. IMPORTANCE Long-term prescription of proton pump inhibitors (PPIs) in patients with cirrhosis is common practice. However, in recent years, several observational studies have reported increased complications and negative prognostic effects of PPI treatment in these patients. Judging the significance of these associations is complicated by the fact that a plausible underlying pathomechanism has not been identified so far. In the present study, we address this important issue by investigating the impact of PPI treatment on subclinical bacterial translocation from the gut into the blood stream in patients with advanced cirrhosis and portal hypertension. Indeed, we report significantly aggravated bacterial translocation in cirrhosis patients receiving PPI treatment. This finding is highly relevant, as bacterial translocation is known to promote the development of complications and impair prognosis in patients with cirrhosis. Hence, the present study could establish a plausible link between PPI treatment and adverse effects in cirrhosis.
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- 2023
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29. Microwave multiplexing on the Keck Array
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Cukierman, Ari, Ahmed, Zeeshan, Henderson, Shawn, Young, Edward, Yu, Cyndia, Barkats, Denis, Brown, David, Chaudhuri, Saptarshi, Cornelison, James, D'Ewart, John M., Dierickx, Marion, Dober, Bradley J., Dusatko, John, Fatigoni, Sofia, Filippini, Jeff P., Frisch, Josef C., Haller, Gunther, Halpern, Mark, Hilton, Gene C., Hubmayr, Johannes, Irwin, Kent D., Karkare, Kirit S., Karpel, Ethan, Kernasovskiy, Sarah A., Kovac, John M., Kovacs, Attila, Kuenstner, Stephen E., Kuo, Chao-Lin, Li, Dale, Mates, John A. B., Smith, Stephen, Germaine, Tyler St., Ullom, Joel N., Vale, Leila R., Van Winkle, Daniel D., Vasquez, Jesus, Willmert, Justin, Zeng, Lingzhen, Ade, P. A. R., Amiri, M., Thakur, R. Basu, Bischoff, C. A., Bock, J. J., Boenish, H., Bullock, E., Buza, V., Cheshire, J., Connors, J., Crumrine, M., Duband, L., Hall, G., Harrison, S., Hildebrandt, S. R., Hui, H., Kang, J., Kefeli, S., Lau, K., Megerian, K. G., Moncelsi, L., Namikawa, T., Nguyen, H. T., O'Brient, R., Palladino, S., Pryke, C., Racine, B., Reintsema, C. D., Richter, S., Schillaci, A., Schwarz, R., Sheehy, C. D., Soliman, A., Steinbach, B., Sudiwala, R. V., Thompson, K. L., Tucker, C., Turner, A. D., Umilta, C., Vieregg, A. G., Wandui, A., Weber, A. C., Wiebe, D. V., Wu, W. L. K., Yang, H., Yoon, K. W., and Zhang, C.
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Astrophysics - Instrumentation and Methods for Astrophysics - Abstract
We describe an on-sky demonstration of a microwave-multiplexing readout system in one of the receivers of the Keck Array, a polarimetry experiment observing the cosmic microwave background at the South Pole. During the austral summer of 2018-2019, we replaced the time-division multiplexing readout system with microwave-multiplexing components including superconducting microwave resonators coupled to radio-frequency superconducting quantum interference devices at the sub-Kelvin focal plane, coaxial-cable plumbing and amplification between room temperature and the cold stages, and a SLAC Microresonator Radio Frequency system for the warm electronics. In the range 5-6 GHz, a single coaxial cable reads out 528 channels. The readout system is coupled to transition-edge sensors, which are in turn coupled to 150-GHz slot-dipole phased-array antennas. Observations began in April 2019, and we report here on an initial characterization of the system performance., Comment: 9 pages, 11 figures, Accepted by the Journal of Low Temperature Physics (Proceedings of the 18th International Workshop on Low Temperature Detectors)
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- 2019
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30. Exclusion Limits on Hidden-Photon Dark Matter near 2 neV from a Fixed-Frequency Superconducting Lumped-Element Resonator
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Phipps, A., Kuenstner, S. E., Chaudhuri, S., Dawson, C. S., Young, B. A., FitzGerald, C. T., Froland, H., Wells, K., Li, D., Cho, H. M., Rajendran, S., Graham, P. W., and Irwin, K. D.
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Astrophysics - Cosmology and Nongalactic Astrophysics ,Physics - Instrumentation and Detectors - Abstract
We present the design and performance of a simple fixed-frequency superconducting lumped-element resonator developed for axion and hidden photon dark matter detection. A rectangular NbTi inductor was coupled to a Nb-coated sapphire capacitor and immersed in liquid helium within a superconducting shield. The resonator was transformer-coupled to a DC SQUID for readout. We measured a quality factor of $\sim$40,000 at the resonant frequency of 492.027 kHz and set a simple exclusion limit on $\sim$2 neV hidden photons with kinetic mixing angle $\varepsilon\gtrsim1.5\times10^{-9}$ based on 5.14 hours of integrated noise. This test device informs the development of the Dark Matter Radio, a tunable superconducting lumped-element resonator which will search for axions and hidden photons over the 100 Hz to 300 MHz frequency range., Comment: To appear in Proceedings of the 3rd International Workshop on Microwave Cavities and Detectors for Axion Research
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- 2019
31. Panomics reveals patient individuality as the major driver of colorectal cancer progression
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Friederike Praus, Axel Künstner, Thorben Sauer, Michael Kohl, Katharina Kern, Steffen Deichmann, Ákos Végvári, Tobias Keck, Hauke Busch, Jens K. Habermann, and Timo Gemoll
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Colorectal cancer ,Metastasis ,Panomics ,Tumour heterogeneity ,Patient individuality ,Biomarkers ,Medicine - Abstract
Abstract Background Colorectal cancer (CRC) is one of the most prevalent cancers, with over one million new cases per year. Overall, prognosis of CRC largely depends on the disease stage and metastatic status. As precision oncology for patients with CRC continues to improve, this study aimed to integrate genomic, transcriptomic, and proteomic analyses to identify significant differences in expression during CRC progression using a unique set of paired patient samples while considering tumour heterogeneity. Methods We analysed fresh-frozen tissue samples prepared under strict cryogenic conditions of matched healthy colon mucosa, colorectal carcinoma, and liver metastasis from the same patients. Somatic mutations of known cancer-related genes were analysed using Illumina's TruSeq Amplicon Cancer Panel; the transcriptome was assessed comprehensively using Clariom D microarrays. The global proteome was evaluated by liquid chromatography-coupled mass spectrometry (LC‒MS/MS) and validated by two-dimensional difference in-gel electrophoresis. Subsequent unsupervised principal component clustering, statistical comparisons, and gene set enrichment analyses were calculated based on differential expression results. Results Although panomics revealed low RNA and protein expression of CA1, CLCA1, MATN2, AHCYL2, and FCGBP in malignant tissues compared to healthy colon mucosa, no differentially expressed RNA or protein targets were detected between tumour and metastatic tissues. Subsequent intra-patient comparisons revealed highly specific expression differences (e.g., SRSF3, OLFM4, and CEACAM5) associated with patient-specific transcriptomes and proteomes. Conclusion Our research results highlight the importance of inter- and intra-tumour heterogeneity as well as individual, patient-paired evaluations for clinical studies. In addition to changes among groups reflecting CRC progression, we identified significant expression differences between normal colon mucosa, primary tumour, and liver metastasis samples from individuals, which might accelerate implementation of precision oncology in the future.
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- 2023
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32. Autoimmune pre-disease
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Bieber, Katja, Hundt, Jennifer E., Yu, Xinhua, Ehlers, Marc, Petersen, Frank, Karsten, Christian M., Köhl, Jörg, Kridin, Khalaf, Kalies, Kathrin, Kasprick, Anika, Goletz, Stephanie, Humrich, Jens Y., Manz, Rudolf A., Künstner, Axel, Hammers, Christoph M., Akbarzadeh, Reza, Busch, Hauke, Sadik, Christian D., Lange, Tanja, Grasshoff, Hanna, Hackel, Alexander M., Erdmann, Jeanette, König, Inke, Raasch, Walter, Becker, Mareike, Kerstein-Stähle, Anja, Lamprecht, Peter, Riemekasten, Gabriela, Schmidt, Enno, and Ludwig, Ralf J.
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- 2023
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33. Editorial: The molecular landscape and promising therapeutic targets in aggressive B-cell non-Hodgkin lymphomas
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Hanno Maximilian Witte, Axel Künstner, Emil Chteinberg, Francesco Piazza, Gaël Roué, and Niklas Gebauer
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aggressive B-cell lymphoma ,non-Hodgkin lymphoma ,genomics ,transcriptomics ,multi-omics ,precision oncology ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Published
- 2023
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34. Molecular profiling and specific targeting of gemcitabine-resistant subclones in heterogeneous pancreatic cancer cell populations
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Benedikt Färber, Olga Lapshyna, Axel Künstner, Michael Kohl, Thorben Sauer, Kira Bichmann, Benjamin Heckelmann, Jessica Watzelt, Kim Honselmann, Louisa Bolm, Meike ten Winkel, Hauke Busch, Hendrik Ungefroren, Tobias Keck, Timo Gemoll, Ulrich F. Wellner, and Rüdiger Braun
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pancreatic cancer ,intratumor heterogeneity ,treatment response ,gemcitabine ,chemotherapy ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
PurposeChemotherapy is pivotal in the multimodal treatment of pancreatic ductal adenocarcinoma (PDAC). Technical advances unveiled a high degree of inter- and intratumoral heterogeneity. We hypothesized that intratumoral heterogeneity (ITH) impacts response to gemcitabine treatment and demands specific targeting of resistant subclones.MethodsUsing single cell-derived cell lines (SCDCLs) from the classical cell line BxPC3 and the basal-like cell line Panc-1, we addressed the effect of ITH on response to gemcitabine treatment.ResultsIndividual SCDCLs of both parental tumor cell populations showed considerable heterogeneity in response to gemcitabine. Unsupervised PCA including the 1,000 most variably expressed genes showed a clustering of the SCDCLs according to their respective sensitivity to gemcitabine treatment for BxPC3, while this was less clear for Panc-1. In BxPC3 SCDCLs, enriched signaling pathways EMT, TNF signaling via NfKB, and IL2STAT5 signaling correlated with more resistant behavior to gemcitabine. In Panc-1 SCDCLs MYC targets V1 and V2 as well as E2F targets were associated with stronger resistance. We used recursive feature elimination for Feature Selection in order to compute sets of proteins that showed strong association with the response to gemcitabine. The optimal protein set calculated for Panc-1 comprised fewer proteins in comparison to the protein set determined for BxPC3. Based on molecular profiles, we could show that the gemcitabine-resistant SCDCLs of both BxPC3 and Panc-1 are more sensitive to the BET inhibitor JQ1 compared to the respective gemcitabine-sensitive SCDCLs.ConclusionOur model system of SCDCLs identified gemcitabine-resistant subclones and provides evidence for the critical role of ITH for treatment response in PDAC. We exploited molecular differences as the basis for differential response and used these for more targeted therapy of resistant subclones.
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- 2023
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35. PB2007: INTEGRATION OF TELEHEALTH IN DAILY CLINICAL PRACTICE IN PATIENTS WITH MYELODYSPLASTIC NEOPLASMS - STATUS QUO AND FUTURE PERSPECTIVES
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Reinhard Stauder, Adrian Lühring, Stefanie Tipelius, Gerhard Rumpold, and Patrick Künstner
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Diseases of the blood and blood-forming organs ,RC633-647.5 - Published
- 2023
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36. The landscape of the immunoglobulin repertoire in endemic pemphigus foliaceus
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Verónica Calonga-Solís, Michael Olbrich, Fabian Ott, Gabriel Adelman Cipolla, Danielle Malheiros, Axel Künstner, Ticiana D.J. Farias, Carolina M. Camargo, Maria Luiza Petzl-Erler, Hauke Busch, Anke Fähnrich, and Danillo G. Augusto
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autoimmunity ,immunoglobulin repertoire ,environmental factors ,B cells ,skin disease ,pemphigus foliaceus ,Immunologic diseases. Allergy ,RC581-607 - Abstract
IntroductionPrimarily driven by autoreactive B cells, pemphigus foliaceus (PF) is an uncommon autoimmune blistering skin disease of sporadic occurrence worldwide. However, PF reaches a prevalence of 3% in the endemic areas of Brazil, the highest ever registered for any autoimmune disease, which indicates environmental factors influencing the immune response in susceptible individuals. We aimed to provide insights into the immune repertoire of patients with PF living in the endemic region of the disease, compared to healthy individuals from the endemic region and a non-endemic area.MethodsWe characterized the B-cell repertoire in i) nontreated patients (n=5); ii) patients under immunosuppressive treatment (n=5); iii) patients in remission without treatment (n=6); and two control groups iv) from the endemic (n=6) and v) non-endemic areas in Brazil (n=4). We used total RNA extracted from peripheral blood mononuclear cells and performed a comprehensive characterization of the variable region of immunoglobulin heavy chain (IGH) in IgG and IgM using next-generation sequencing.ResultsCompared to individuals from a different area, we observed remarkably lower clonotype diversity in the B-cell immune repertoire of patients and controls from the endemic area (p < 0.02), suggesting that the immune repertoire in the endemic area is under geographically specific and intense environmental pressure. Moreover, we observed longer CDR3 sequences in patients, and we identified differential disease-specific usage of IGHV segments, including increased IGHV3-30 and decreased IGHV3-23 in patients with active disease (p < 0.04). Finally, our robust network analysis discovered clusters of CDR3 sequences uniquely observed in patients with PF.DiscussionOur results indicate that environmental factors, in addition to disease state, impact the characteristics of the repertoire. Our findings can be applied to further investigation of the environmental factors that trigger pemphigus and expand the knowledge for identifying new targeted and more effective therapies.
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- 2023
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37. Clonal evolution in tyrosine kinase inhibitor-resistance: lessons from in vitro-models
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Meike Kaehler, Pia Osteresch, Axel Künstner, Stella Juliane Vieth, Daniela Esser, Marius Möller, Hauke Busch, Inga Vater, Malte Spielmann, Ingolf Cascorbi, and Inga Nagel
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chronic myeloid leukemia ,drug resistance ,imatinib ,nilotinib ,PTPN11 ,PDGFRB ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
IntroductionResistance in anti-cancer treatment is a result of clonal evolution and clonal selection. In chronic myeloid leukemia (CML), the hematopoietic neoplasm is predominantly caused by the formation of the BCR::ABL1 kinase. Evidently, treatment with tyrosine kinase inhibitors (TKIs) is tremendously successful. It has become the role model of targeted therapy. However, therapy resistance to TKIs leads to loss of molecular remission in about 25% of CML patients being partially due to BCR::ABL1 kinase mutations, while for the remaining cases, various other mechanisms are discussed.MethodsHere, we established an in vitro-TKI resistance model against the TKIs imatinib and nilotinib and performed exome sequencing.ResultsIn this model, acquired sequence variants in NRAS, KRAS, PTPN11, and PDGFRB were identified in TKI resistance. The well-known pathogenic NRAS p.(Gln61Lys) variant provided a strong benefit for CML cells under TKI exposure visible by increased cell number (6.2-fold, p < 0.001) and decreased apoptosis (-25%, p < 0.001), proving the functionality of our approach. The transfection of PTPN11 p.(Tyr279Cys) led to increased cell number (1.7-fold, p = 0.03) and proliferation (2.0-fold, p < 0.001) under imatinib treatment.DiscussionOur data demonstrate that our in vitro-model can be used to study the effect of specific variants on TKI resistance and to identify new driver mutations and genes playing a role in TKI resistance. The established pipeline can be used to study candidates acquired in TKI-resistant patients, thereby providing new options for the development of new therapy strategies to overcome resistance.
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- 2023
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38. Crack characterization in manganese steel using a μ-bolometer camera and an air-cooled inductor
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Tuschl, Christoph, primary, Oswald-Tranta, Beate, additional, Dornig, Peter, additional, Künstner, David, additional, Pötz, Melanie, additional, and Eck, Sven, additional
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- 2024
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39. Highly-multiplexed microwave SQUID readout using the SLAC Microresonator Radio Frequency (SMuRF) Electronics for Future CMB and Sub-millimeter Surveys
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Henderson, Shawn W., Ahmed, Zeeshan, Austermann, Jason, Becker, Daniel, Bennett, Douglas A., Brown, David, Chaudhuri, Saptarshi, Cho, Hsiao-Mei Sherry, D'Ewart, John M., Dober, Bradley, Duff, Shannon M., Dusatko, John E., Fatigoni, Sofia, Frisch, Josef C., Gard, Jonathon D., Halpern, Mark, Hilton, Gene C., Hubmayr, Johannes, Irwin, Kent D., Karpel, Ethan D., Kernasovskiy, Sarah S., Kuenstner, Stephen E., Kuo, Chao-Lin, Li, Dale, Mates, John A. B., Reintsema, Carl D., Smith, Stephen R., Ullom, Joel, Vale, Leila R., Van Winkle, Daniel D., Vissers, Michael, and Yu, Cyndia
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Astrophysics - Instrumentation and Methods for Astrophysics ,Astrophysics - Cosmology and Nongalactic Astrophysics - Abstract
The next generation of cryogenic CMB and submillimeter cameras under development require densely instrumented sensor arrays to meet their science goals. The readout of large numbers ($\sim$10,000--100,000 per camera) of sub-Kelvin sensors, for instance as proposed for the CMB-S4 experiment, will require substantial improvements in cold and warm readout techniques. To reduce the readout cost per sensor and integration complexity, efforts are presently focused on achieving higher multiplexing density while maintaining readout noise subdominant to intrinsic detector noise. Highly-multiplexed cold readout technologies in active development include Microwave Kinetic Inductance Sensors (MKIDs) and microwave rf-SQUIDs. Both exploit the high quality factors of superconducting microwave resonators to densely channelize sub-Kelvin sensors into the bandwidth of a microwave transmission line. We present advancements in the development of a new warm readout system for microwave SQUID multiplexing, the SLAC Superconducting Microresonator RF electronics, or SMuRF. The SMuRF system is unique in its ability to track each tone, minimizing the total RF power required to read out each resonator, thereby significantly reducing the linearity requirements on the cold and warm readout. Here, we present measurements of the readout noise and linearity of the first full SMuRF system, including a demonstration of closed-loop tone tracking on a 528 channel cryogenic microwave SQUID multiplexer. SMuRF is being explored as a potential readout solution for several future CMB projects including Simons Observatory, BICEP Array, CCAT-prime, Ali-CPT, and CMB-S4. Parallel development of the platform is underway to adapt SMuRF to read out both MKID and fast X-ray TES calorimeter arrays., Comment: 16 pages, 5 figures
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- 2018
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40. The Simons Observatory: Science goals and forecasts
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The Simons Observatory Collaboration, Ade, Peter, Aguirre, James, Ahmed, Zeeshan, Aiola, Simone, Ali, Aamir, Alonso, David, Alvarez, Marcelo A., Arnold, Kam, Ashton, Peter, Austermann, Jason, Awan, Humna, Baccigalupi, Carlo, Baildon, Taylor, Barron, Darcy, Battaglia, Nick, Battye, Richard, Baxter, Eric, Bazarko, Andrew, Beall, James A., Bean, Rachel, Beck, Dominic, Beckman, Shawn, Beringue, Benjamin, Bianchini, Federico, Boada, Steven, Boettger, David, Bond, J. Richard, Borrill, Julian, Brown, Michael L., Bruno, Sarah Marie, Bryan, Sean, Calabrese, Erminia, Calafut, Victoria, Calisse, Paolo, Carron, Julien, Challinor, Anthony, Chesmore, Grace, Chinone, Yuji, Chluba, Jens, Cho, Hsiao-Mei Sherry, Choi, Steve, Coppi, Gabriele, Cothard, Nicholas F., Coughlin, Kevin, Crichton, Devin, Crowley, Kevin D., Crowley, Kevin T., Cukierman, Ari, D'Ewart, John M., Dünner, Rolando, de Haan, Tijmen, Devlin, Mark, Dicker, Simon, Didier, Joy, Dobbs, Matt, Dober, Bradley, Duell, Cody J., Duff, Shannon, Duivenvoorden, Adri, Dunkley, Jo, Dusatko, John, Errard, Josquin, Fabbian, Giulio, Feeney, Stephen, Ferraro, Simone, Fluxà, Pedro, Freese, Katherine, Frisch, Josef C., Frolov, Andrei, Fuller, George, Fuzia, Brittany, Galitzki, Nicholas, Gallardo, Patricio A., Ghersi, Jose Tomas Galvez, Gao, Jiansong, Gawiser, Eric, Gerbino, Martina, Gluscevic, Vera, Goeckner-Wald, Neil, Golec, Joseph, Gordon, Sam, Gralla, Megan, Green, Daniel, Grigorian, Arpi, Groh, John, Groppi, Chris, Guan, Yilun, Gudmundsson, Jon E., Han, Dongwon, Hargrave, Peter, Hasegawa, Masaya, Hasselfield, Matthew, Hattori, Makoto, Haynes, Victor, Hazumi, Masashi, He, Yizhou, Healy, Erin, Henderson, Shawn W., Hervias-Caimapo, Carlos, Hill, Charles A., Hill, J. Colin, Hilton, Gene, Hilton, Matt, Hincks, Adam D., Hinshaw, Gary, Hložek, Renée, Ho, Shirley, Ho, Shuay-Pwu Patty, Howe, Logan, Huang, Zhiqi, Hubmayr, Johannes, Huffenberger, Kevin, Hughes, John P., Ijjas, Anna, Ikape, Margaret, Irwin, Kent, Jaffe, Andrew H., Jain, Bhuvnesh, Jeong, Oliver, Kaneko, Daisuke, Karpel, Ethan D., Katayama, Nobuhiko, Keating, Brian, Kernasovskiy, Sarah S., Keskitalo, Reijo, Kisner, Theodore, Kiuchi, Kenji, Klein, Jeff, Knowles, Kenda, Koopman, Brian, Kosowsky, Arthur, Krachmalnicoff, Nicoletta, Kuenstner, Stephen E., Kuo, Chao-Lin, Kusaka, Akito, Lashner, Jacob, Lee, Adrian, Lee, Eunseong, Leon, David, Leung, Jason S. -Y., Lewis, Antony, Li, Yaqiong, Li, Zack, Limon, Michele, Linder, Eric, Lopez-Caraballo, Carlos, Louis, Thibaut, Lowry, Lindsay, Lungu, Marius, Madhavacheril, Mathew, Mak, Daisy, Maldonado, Felipe, Mani, Hamdi, Mates, Ben, Matsuda, Frederick, Maurin, Loïc, Mauskopf, Phil, May, Andrew, McCallum, Nialh, McKenney, Chris, McMahon, Jeff, Meerburg, P. Daniel, Meyers, Joel, Miller, Amber, Mirmelstein, Mark, Moodley, Kavilan, Munchmeyer, Moritz, Munson, Charles, Naess, Sigurd, Nati, Federico, Navaroli, Martin, Newburgh, Laura, Nguyen, Ho Nam, Niemack, Michael, Nishino, Haruki, Orlowski-Scherer, John, Page, Lyman, Partridge, Bruce, Peloton, Julien, Perrotta, Francesca, Piccirillo, Lucio, Pisano, Giampaolo, Poletti, Davide, Puddu, Roberto, Puglisi, Giuseppe, Raum, Chris, Reichardt, Christian L., Remazeilles, Mathieu, Rephaeli, Yoel, Riechers, Dominik, Rojas, Felipe, Roy, Anirban, Sadeh, Sharon, Sakurai, Yuki, Salatino, Maria, Rao, Mayuri Sathyanarayana, Schaan, Emmanuel, Schmittfull, Marcel, Sehgal, Neelima, Seibert, Joseph, Seljak, Uros, Sherwin, Blake, Shimon, Meir, Sierra, Carlos, Sievers, Jonathan, Sikhosana, Precious, Silva-Feaver, Maximiliano, Simon, Sara M., Sinclair, Adrian, Siritanasak, Praween, Smith, Kendrick, Smith, Stephen R., Spergel, David, Staggs, Suzanne T., Stein, George, Stevens, Jason R., Stompor, Radek, Suzuki, Aritoki, Tajima, Osamu, Takakura, Satoru, Teply, Grant, Thomas, Daniel B., Thorne, Ben, Thornton, Robert, Trac, Hy, Tsai, Calvin, Tucker, Carole, Ullom, Joel, Vagnozzi, Sunny, van Engelen, Alexander, Van Lanen, Jeff, Van Winkle, Daniel D., Vavagiakis, Eve M., Vergès, Clara, Vissers, Michael, Wagoner, Kasey, Walker, Samantha, Ward, Jon, Westbrook, Ben, Whitehorn, Nathan, Williams, Jason, Williams, Joel, Wollack, Edward J., Xu, Zhilei, Yu, Byeonghee, Yu, Cyndia, Zago, Fernando, Zhang, Hezi, and Zhu, Ningfeng
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Astrophysics - Cosmology and Nongalactic Astrophysics - Abstract
The Simons Observatory (SO) is a new cosmic microwave background experiment being built on Cerro Toco in Chile, due to begin observations in the early 2020s. We describe the scientific goals of the experiment, motivate the design, and forecast its performance. SO will measure the temperature and polarization anisotropy of the cosmic microwave background in six frequency bands: 27, 39, 93, 145, 225 and 280 GHz. The initial configuration of SO will have three small-aperture 0.5-m telescopes (SATs) and one large-aperture 6-m telescope (LAT), with a total of 60,000 cryogenic bolometers. Our key science goals are to characterize the primordial perturbations, measure the number of relativistic species and the mass of neutrinos, test for deviations from a cosmological constant, improve our understanding of galaxy evolution, and constrain the duration of reionization. The SATs will target the largest angular scales observable from Chile, mapping ~10% of the sky to a white noise level of 2 $\mu$K-arcmin in combined 93 and 145 GHz bands, to measure the primordial tensor-to-scalar ratio, $r$, at a target level of $\sigma(r)=0.003$. The LAT will map ~40% of the sky at arcminute angular resolution to an expected white noise level of 6 $\mu$K-arcmin in combined 93 and 145 GHz bands, overlapping with the majority of the LSST sky region and partially with DESI. With up to an order of magnitude lower polarization noise than maps from the Planck satellite, the high-resolution sky maps will constrain cosmological parameters derived from the damping tail, gravitational lensing of the microwave background, the primordial bispectrum, and the thermal and kinematic Sunyaev-Zel'dovich effects, and will aid in delensing the large-angle polarization signal to measure the tensor-to-scalar ratio. The survey will also provide a legacy catalog of 16,000 galaxy clusters and more than 20,000 extragalactic sources., Comment: This paper presents an overview of the Simons Observatory science goals, details about the instrument will be presented in a companion paper. The author contribution to this paper is available at https://simonsobservatory.org/publications.php (Abstract abridged) -- matching version published in JCAP
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- 2018
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41. A Spread-Spectrum SQUID Multiplexer
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Irwin, K. D., Chaudhuri, S., Cho, H. -M., Dawson, C., Kuenstner, S., Li, D., Titus, C. J., and Young, B. A.
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Physics - Instrumentation and Detectors ,Condensed Matter - Superconductivity - Abstract
The Transition-Edge Sensors (TES) is a mature, high-resolution x-ray spectrometer technology that provides a much higher efficiency than dispersive spectrometers such as gratings and crystal spectrometers. As larger arrays are developed, time-division multiplexing schemes operating at MHz frequencies are being replaced by microwave SQUID multiplexers using frequency-division multiplexing at GHz frequencies. However, the multiplexing factor achievable with microwave SQUIDs is limited by the high slew rate on the leading edge of x-ray pulses. In this paper, we propose a new multiplexing scheme for high-slew-rate TES x-ray calorimeters: the spread-spectrum SQUID multiplexer, which has the potential to enable higher multiplexing factors, especially in applications with lower photon arrival rates., Comment: 12 pages, 2 figures, Submitted to the Journal of Low Temperature Physics (Proceedings of the 17th International Workshop on Low Temperature Detectors)
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- 2018
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42. SLAC Microresonator Radio Frequency (SMuRF) Electronics for Read Out of Frequency-Division-Multiplexed Cryogenic Sensors
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Kernasovskiy, S. A., Kuenstner, S. E., Karpel, E., Ahmed, Z., Van Winkle, D. D., Smith, S., Dusatko, J., Frisch, J. C., Chaudhuri, S., Cho, H. M., Dober, B. J., Henderson, S. W., Hilton, G. C., Hubmayr, J., Irwin, K. D., Kuo, C. L., Li, D., Mates, J. A. B., Nasr, M., Tantawi, S., Ullom, J., Vale, L., and Young, B.
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Astrophysics - Instrumentation and Methods for Astrophysics - Abstract
Large arrays of cryogenic sensors for various imaging applications ranging across x-ray, gamma-ray, Cosmic Microwave Background (CMB), mm/sub-mm, as well as particle detection increasingly rely on superconducting microresonators for high multiplexing factors. These microresonators take the form of microwave SQUIDs that couple to Transition-Edge Sensors (TES) or Microwave Kinetic Inductance Detectors (MKIDs). In principle, such arrays can be read out with vastly scalable software-defined radio using suitable FPGAs, ADCs and DACs. In this work, we share plans and show initial results for SLAC Microresonator Radio Frequency (SMuRF) electronics, a next-generation control and readout system for superconducting microresonators. SMuRF electronics are unique in their implementation of specialized algorithms for closed-loop tone tracking, which consists of fast feedback and feedforward to each resonator's excitation parameters based on transmission measurements. Closed-loop tone tracking enables improved system linearity, a significant increase in sensor count per readout line, and the possibility of overcoupled resonator designs for enhanced dynamic range. Low-bandwidth prototype electronics were used to demonstrate closed-loop tone tracking on twelve 300-kHz-wide microwave SQUID resonators, spaced at $\sim$6 MHz with center frequencies $\sim$5-6 GHz. We achieve multi-kHz tracking bandwidth and demonstrate that the noise floor of the electronics is subdominant to the noise intrinsic in the multiplexer., Comment: 7 pages, 5 figures, Submitted to the Journal of Low Temperature Physics (Proceedings of the 17th International Workshop on Low Temperature Detectors)
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- 2018
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43. Integrative molecular profiling identifies two molecularly and clinically distinct subtypes of blastic plasmacytoid dendritic cell neoplasm
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Axel Künstner, Julian Schwarting, Hanno M. Witte, Veronica Bernard, Stephanie Stölting, Kathrin Kusch, Kumar Nagarathinam, Nikolas von Bubnoff, Eva Maria Murga Penas, Hartmut Merz, Hauke Busch, Alfred C. Feller, and Niklas Gebauer
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Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Published
- 2022
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44. Longitudinal Characterization of the Fungal Skin Microbiota in Healthy Subjects Over a Period of 1 Year
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Schmid, Bettina, Künstner, Axel, Fähnrich, Anke, Busch, Hauke, Glatz, Martin, and Bosshard, Philipp P.
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- 2022
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45. Dose-dependent effect of GFI1 expression in the reconstitution and the differentiation capacity of HSCs
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Xiaoqing Xie, Pradeep Kumar Patnana, Daria Frank, Judith Schütte, Yahya Al-Matary, Axel Künstner, Hauke Busch, Helal Ahmed, Longlong Liu, Daniel R. Engel, Ulrich Dührsen, Frank Rosenbauer, Nikolas Von Bubnoff, Georg Lenz, and Cyrus Khandanpour
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Gfi1 ,HSC ,dose-dependent ,engraftment ,differentiation ,Biology (General) ,QH301-705.5 - Abstract
GFI1 is a transcriptional repressor and plays a pivotal role in regulating the differentiation of hematopoietic stem cells (HSCs) towards myeloid and lymphoid cells. Serial transplantation of Gfi1 deficient HSCs repopulated whole hematopoietic system but in a competitive setting involving wild-type HSCs, they lose this ability. The underlying mechanisms to this end are poorly understood. To better understand this, we used different mouse strains that express either loss of both Gfi1 alleles (Gfi1-KO), with reduced expression of GFI1 (GFI1-KD) or wild-type Gfi1/GFI1 (Gfi1-/GFI1-WT; corresponding to the mouse and human alleles). We observed that loss of Gfi1 or reduced expression of GFI1 led to a two to four fold lower number of HSCs (defined as Lin−Sca1+c-Kit+CD150+CD48−) compared to GFI1-WT mice. To study the functional influence of different levels of GFI1 expression on HSCs function, HSCs from Gfi1-WT (expressing CD45.1 + surface antigens) and HSCs from GFI1-KD or -KO (expressing CD45.2 + surface antigens) mice were sorted and co-transplanted into lethally irradiated host mice. Every 4 weeks, CD45.1+ and CD45.2 + on different lineage mature cells were analyzed by flow cytometry. At least 16 weeks later, mice were sacrificed, and the percentage of HSCs and progenitors including GMPs, CMPs and MEPs in the total bone marrow cells was calculated as well as their CD45.1 and CD45.2 expression. In the case of co-transplantation of GFI1-KD with Gfi1-WT HSCs, the majority of HSCs (81% ± 6%) as well as the majority of mature cells (88% ± 10%) originated from CD45.2 + GFI1-KD HSCs. In the case of co-transplantation of Gfi1-KO HSCs with Gfi1-WT HSCs, the majority of HSCs originated from CD45.2+ and therefore from Gfi1-KO (61% ± 20%); however, only a small fraction of progenitors and mature cells originated from Gfi1-KO HSCs (
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- 2023
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46. Case report: Schnitzler-like syndrome without monoclonal gammopathy
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Anna Sophie Wesselmann, Axel Künstner, Anke Fähnrich, Christian Rose, Peter Lamprecht, Hauke Busch, Ralf J. Ludwig, and Andreas Recke
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case report ,Schnitzler’s syndrome ,autoinflammation ,late-onset autoinflammation ,gammopathy ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Schnitzler syndrome is a rare autoinflammatory disorder characterized by urticarial rash, joint pain, recurrent fever, leucocytosis, elevated C-reactive protein (CRP) and serum amyloid A (SAA), and monoclonal IgM or IgG gammopathy. According to the Strasbourg criteria, both urticarial rash and gammopathy are mandatorily required for the diagnosis of Schnitzler’s syndrome. However, incomplete variants lacking either skin symptoms or monoclonal gammopathy have also been described. Here, we report a case in which the diagnosis of Schnitzler-like syndrome was made despite the absence of gammopathy, based on neutrophilic dermal inflammation, episodic and excessive increase in inflammatory parameters, and prompt response to anakinra, a soluble IL1 receptor antagonist (sIL-1RA). In addition, we detected neutrophil epitheliotropism, which is highly suggestive of autoinflammatory disease. Using whole-exome sequencing, we were unable to find a causative pathogenic mutation but did find several mutations possibly related to the inflammatory processes in this patient. This and other cases highlight that the existing Strasbourg criteria are too strict to capture Schnitzler-like syndromes that may respond well and rapidly to IL1 inhibition. Recurrent episodes of disease with normalization of inflammatory symptoms in the interval, rapid response to anakinra, and neutrophilic epitheliotropism in a lesional skin biopsy may help confirm the diagnosis of Schnitzler-like syndrome.
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- 2023
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47. Corrigendum: Altered composition of the oral microbiota in depression among cigarette smokers: A pilot study
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Mohammad Tahseen Al Bataineh, Axel Künstner, Nihar Ranjan Dash, Rushud Mahmood Abdulsalam, Rafla Zaid Ali Al-Kayyali, M. Besher Adi, Habiba S. Alsafar, Hauke Busch, and Saleh Mohamed Ibrahim
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avoidance ,activation ,BADS ,metagenomics ,oral microbiome ,Psychiatry ,RC435-571 - Published
- 2023
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48. Predominance of Staphylococcus Correlates with Wound Burden and Disease Activity in Dystrophic Epidermolysis Bullosa: A Prospective Case-Control Study
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Reimer-Taschenbrecker, Antonia, Künstner, Axel, Hirose, Misa, Hübner, Stefanie, Gewert, Stella, Ibrahim, Saleh, Busch, Hauke, and Has, Cristina
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- 2022
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49. Biodiversity of mycobial communities in health and onychomycosis
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Olbrich, Michael, Ernst, Anna Lara, Beltsiou, Foteini, Bieber, Katja, Ständer, Sascha, Harder, Melanie, Anemüller, Waltraud, Köhler, Birgit, Zillikens, Detlef, Busch, Hauke, Künstner, Axel, and Ludwig, Ralf J.
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- 2022
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50. Biodiversity of mycobial communities in health and onychomycosis
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Michael Olbrich, Anna Lara Ernst, Foteini Beltsiou, Katja Bieber, Sascha Ständer, Melanie Harder, Waltraud Anemüller, Birgit Köhler, Detlef Zillikens, Hauke Busch, Axel Künstner, and Ralf J. Ludwig
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Medicine ,Science - Abstract
Abstract Onychomycosis (OM) is a common fungal nail infection. Based on the rich mycobial diversity in healthy toenails, we speculated that this is lost in OM due to the predominance of a single pathogen. We used next generation sequencing to obtain insights into the biodiversity of fungal communities in both healthy individuals and OM patients. By sequencing, a total of 338 operational-taxonomic units were found in OM patients and healthy controls. Interestingly, a classifier distinguished three distinct subsets: healthy controls and two groups within OM patients with either a low or high abundance of Trichophyton. Diversity per sample was decreased in controls compared to cases with low Trichophyton abundance (LTA), while cases with a high Trichophyton abundance (HTA) showed a lower diversity. Variation of mycobial communities between the samples showed shifts in the community structure between cases and controls—mainly driven by HTA cases. Indeed, LTA cases had a fungal β-diversity undistinguishable from that of healthy controls. Collectively, our data provides an in-depth characterization of fungal diversity in health and OM. Our findings also suggest that onychomycosis develops either through pathogen-driven mechanisms, i.e., in HTA cases, or through host and/or environmental factors, i.e., in cases with a low Trichophyton abundance.
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- 2022
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