2,709 results on '"A. Schmidt-Ott"'
Search Results
2. Converting PROMIS®-29 v2.0 profile data to SF-36 physical and mental component summary scores in patients with cardiovascular disorders
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Liegl, Gregor, H. Fischer, Felix, N. Martin, Carl, Rönnefarth, Maria, Blumrich, Annelie, Ahmadi, Michael, Boldt, Leif-Hendrik, Eckardt, Kai-Uwe, Endres, Matthias, Edelmann, Frank, Gerhardt, Holger, Grittner, Ulrike, Haghikia, Arash, Hübner, Norbert, Landmesser, Ulf, Leistner, David, Mai, Knut, Kollmus-Heege, Jil, N. Müller, Dominik, H. Nolte, Christian, K. Piper, Sophie, M. Schmidt-Ott, Kai, Pischon, Tobias, Rattan, Simrit, Rohrpasser-Napierkowski, Ira, Schönrath, Katharina, Schulz-Menger, Jeanette, Schweizerhof, Oliver, Spranger, Joachim, E. Weber, Joachim, Witzenrath, Martin, Schmidt, Sein, and Rose, Matthias
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- 2024
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3. Was ist gesichert in der Diagnostik und Therapie?: Aktuelle Highlights aus der Inneren Medizin
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Schmidt-Ott, Kai
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- 2024
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4. Früher erkennen: Prädiktoren und Alerts bei AKI
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Schenk, Heiko and Schmidt-Ott, Kai M.
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- 2024
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5. Converting PROMIS®-29 v2.0 profile data to SF-36 physical and mental component summary scores in patients with cardiovascular disorders
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Gregor Liegl, Felix H. Fischer, Carl N. Martin, Maria Rönnefarth, Annelie Blumrich, Michael Ahmadi, Leif-Hendrik Boldt, Kai-Uwe Eckardt, Matthias Endres, Frank Edelmann, Holger Gerhardt, Ulrike Grittner, Arash Haghikia, Norbert Hübner, Ulf Landmesser, David Leistner, Knut Mai, Jil Kollmus-Heege, Dominik N. Müller, Christian H. Nolte, Sophie K. Piper, Kai M. Schmidt-Ott, Tobias Pischon, Simrit Rattan, Ira Rohrpasser-Napierkowski, Katharina Schönrath, Jeanette Schulz-Menger, Oliver Schweizerhof, Joachim Spranger, Joachim E. Weber, Martin Witzenrath, Sein Schmidt, and Matthias Rose
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PROMIS-29 ,SF-36 ,Health composite scores ,Cardiovascular diseases ,Mapping ,Patient-reported outcomes ,Computer applications to medicine. Medical informatics ,R858-859.7 - Abstract
Abstract Background Health-related quality of life (HRQL) has become an important outcome parameter in cardiology. The MOS 36-ltem Short-Form Health Survey (SF-36) and the PROMIS-29 are two widely used generic measures providing composite HRQL scores. The domains of the SF-36, a well-established instrument utilized for several decades, can be aggregated to physical (PCS) and mental (MCS) component summary scores. Alternative scoring algorithms for correlated component scores (PCSc and MCSc) have also been suggested. The PROMIS-29 is a newer but increasingly used HRQL measure. Analogous to the SF-36, physical and mental health summary scores can be derived from PROMIS-29 domain scores, based on a correlated factor solution. So far, scores from the PROMIS-29 are not directly comparable to SF-36 results, complicating the aggregation of research findings. Thus, our aim was to provide algorithms to convert PROMIS-29 data to well-established SF-36 component summary scores. Methods Data from n = 662 participants of the Berlin Long-term Observation of Vascular Events (BeLOVE) study were used to estimate linear regression models with either PROMIS-29 domain scores or aggregated PROMIS-29 physical/mental health summary scores as predictors and SF-36 physical/mental component summary scores as outcomes. Data from a subsequent assessment point (n = 259) were used to evaluate the agreement between empirical and predicted SF-36 scores. Results PROMIS-29 domain scores as well as PROMIS-29 health summary scores showed high predictive value for PCS, PCSc, and MCSc (R2 ≥ 70%), and moderate predictive value for MCS (R2 = 57% and R2 = 40%, respectively). After applying the regression coefficients to new data, empirical and predicted SF-36 component summary scores were highly correlated (r > 0.8) for most models. Mean differences between empirical and predicted scores were negligible (|SMD|
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- 2024
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6. Efficacy and Safety of Ravulizumab in IgA Nephropathy: A Phase 2 Randomized Double-Blind Placebo-Controlled Trial
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Lafayette, Richard, Tumlin, James, Fenoglio, Roberta, Kaufeld, Jessica, Pérez Valdivia, Miguel Angel, Wu, Mai-Szu, Susan Huang, Shih-Han, Alamartine, Eric, Kim, Sung Gyun, Yee, Min, Kateifides, Andreas, Rice, Kara, Garlo, Katherine, Barratt, Jonathan, Ranganathan, Dwarakanathan, Wolley, Martin, Tan, Sven-Jean, Chow, Kevin, Tin Law, Mandy Man, Nichols, Kathleen, See, Emily Jan, Steinberg, Adam Glenn, Tiong, Mark, Susan Huang, Shih-Han, Jain, Arsh, Laurin, Louis-Phillipe, Lafrance, Jean-Phillipe, Lamarche, Caroline, Philibert, David, Agharazii, Mohsen, Mac-Way, Fabrice, Alamartine, Eric, Maillard, Nicolas, Mariat, Christophe, Masson, Ingrid, Boffa, Jean-Jacques, Cez, Alexandre, Esteve, Emmanuel, Marchal, Armance, Chauveau, Dominique, Belliere, Julie, Monrozeis, Pauline Bernadet, Colliou, Eloise, Faguer, Stanislas, Huart, Antoine, Ribes, David, Garrouste, Cyril, Heng, Anne-Elisabeth, Mayet, Valentin, Philipponnet, Carole, Moulin, Bruno, Parvez, Laura Braun, Vargas, Gabriela Gautier, Perrin, Peggy, Ohlmann, Sophie, Olagne, Jerome, Haller, Herman, Schmidt-Ott, Kai, Bahlmann-Kroll, Elisabeth, Kaufeld, Jessica, Reinhardt, Martin, Gaeckler, Anja, Dolff, Sebastian, Wilde, Benjamin, Schreiber, Adrian, Koch, Nadine, Seelow, Evelyn, Alberici, Federico, Affatato, Stefania, Mainardi, Allesandro, Mescia, Federica, Scolari, Francesco, Tedesco, Martina, Venturini, Margherita, Cirami, Calogero Lino, Antognoli, Giulia, Caroti, Leonardo, Gualtiero, Gabriele, Moscato, Marcos, Trivioli, Giorgio, La Manna, Gaetano, Baraldi, Olga, Campus, Anita, Stefanini, Carlo, Vischini, Gisella, Roccatello, Dario, Fenoglio, Roberta, Lalloni, Stefania, Sciascia, Savino, Nowicki, Michal, Holub, Tomasz, Kieszek, Błażej, Makówka, Agnieszka, Masajtis, Anna, Piechota, Piotr, Tylski, Maciej, Han, Seung Hyeok, Lee, Sang-Won, Lim, Beon Jin, Pyo, Jung Yoon, Kim, Sung Gyun, An, Jung Nam, Chung, Byung Ha, Kim, Jwa-Kyung, Lee, Hyung Seok, Seo, Young Il, Song, Young Rim, Lee, Hajeong, Park, Sehoon, Han, Seung Seok, Kim, Dong Ki, Kim, Yong Chul, Ryu, Hyunjin, Agraz, Irene, Bolufer, Monica, Hernandez, Josefina Cortés, Gabaldon, Maria Alejandra, Soler, Maria José, Arroyo, David, Carbayo, Javier, Diezhandino, Marian Goicoechea, Perez de Jose, Ana, Guzman, Ursula Verdalles, Moreno, Eduardo Verde, García, Olga Gracia, Albines Fiestas, Zoila Stany, Aladren Gonzalvo, Daniel Joaquin, Gonzalez, Andrea Bernal, Lou Arnal, Luis Miguel, Villarroya, Cristina Medrano, Lopez, Paula Mora, Moncasi, Eduardo Parra, Martin Conde, Maria Luisa, Gonzalez, Jorge, Jatem, Elias, Estor, Aida Moroba, Medrano, Alfons Segarra, Moreno, Antolina Rodriguez, Sanchez de la Nieta, Dolores, Garcia, Clara, Velo, Mercedes, Rocha Castilla, Jose Luis, Bermejo, Sheila, Mendoza, Manuel Lopez, Pérez Valdivia, Miguel Angel, Rojas, Remedios Toledo, Hidalgo, Pilar, Sanchez, Teresa Vazquez, Uriol Rivera, Miguel Giovanni, Fuentes, Mario Lado, Chiu, Yi-Wen, Chang, Jer-Ming, Chen, Hung-Chun, Hsiao, Mei-Ju, Hung, Chi-Chih, Hwang, Shang-Jih, Kuo, Mei Chuan, Kuo, Hung-Tien, Lim, Lee-Moay, Lee, Jia-Jung, Lai, Ping Chin, Chang, David Ray, Chang, Yun-Lun, Chen, I-Ru, Hsieh, Ming-Han, Huang, Chiu-Ching, Kuo, Huey-Liang, Wang, I-Kuan, Wu, Mai-Szu, Chen, Yu-Wei, Chiu, I-Jen, Hsu, Yung-Ho, Hung, Lie-Yee, Laio, Chia-Te, Lin, Gua-Hong, Lin, Yuh-Feng, Wu, Mei-Yi, Zheng, Cai-Mei, Lightstone, Elizabeth, Cairns, Tommy, Mcadoo, Stephen, Medjeral-Thomas, Nicholas, Pickering, Matthew, Robson, Michael, Sinha, Smeeta, Chukwu, Chukwuma, Storrar, Joshua, Ahmed, Sadiq, Cornea, Virgilius, Nadim, Amina, Sims, Tyler, Awad, Ahmed, Aldahan, Mohammed, Clark, Laurie, Lustig, Ryan, Niles, John, Jeyabalan, Anushya, Zonozi, Reza, Tumlin, James, and Paxton, William
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- 2024
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7. Empagliflozin in patients with autosomal dominant polycystic kidney disease (EMPA-PKD): study protocol for a randomised controlled trial
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Roland Schmitt, Sebastian Häckl, Armin Koch, Elisabeth Bahlmann-Kroll, Stefanie Kramer, Vera Christine Wulfmeyer, Julian Glandorf, Jessica Kaufeld, Dagmar Hartung, Bernhard M W Schmidt, and Kai Schmidt-Ott
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Medicine - Abstract
Introduction Autosomal dominant polycystic kidney disease (ADPKD) is a hereditary condition that causes the formation of cysts primarily in the kidneys. The continuous growth of multiple cysts leads to the destruction of functional parenchyma, which may progress to end-stage kidney disease. Tolvaptan is the only drug specifically approved for slowing down the progression of ADPKD. Sodium-glucose transporter 2 inhibitors might provide additional benefits but there is currently no information on safety and outcome effects of SGLT2i in patients with ADPKD, as these patients were excluded in SGLT2i trials. In particular, there has been speculation that SGLT2i might increase cyst growth and accelerate the loss of kidney function in ADPKD. The EMPA-PKD trial is assessing the safety of empagliflozin in patients with rapid progressive ADPKD with and without concomitant tolvaptan use by monitoring the total kidney volume and the loss of kidney function.Methods and analysis This is an investigator-initiated, double-blind, single-centre, placebo-controlled, randomised clinical trial including patients with rapidly progressive ADPKD (n=44). Participants will be randomly allocated (1:1) to receive a daily dose of either empagliflozin (10 mg/day) or placebo for 18 months. Patients will be stratified according to concomitant tolvaptan use. The primary endpoint is the progression of cystic kidney growth by monitoring MRI-based changes in total kidney volume and the secondary endpoint is the change in glomerular filtration rate. Additional endpoints include changes in copeptin levels, albuminuria and blood pressure.Ethics and dissemination The protocol has been approved by the German Federal Institute for Drugs and Medical Devices (BfArM) after review by the independent ethics committee Landesarztekammer Rheinland-Pfalz. Participation in this study will be voluntary and informed consent will be obtained. Regardless of the outcome, the results will be disseminated through a peer-reviewed international medical journal.Trial registration numbers EU-CT number 2023-505890-34-00, NCT06391450.
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- 2024
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8. Evaluation of Physician Knowledge of Safety and Safe Use Information for Intravitreal Aflibercept Injection in Europe: A Second Survey of Physicians Following Dissemination of Updated Risk-Minimization Materials
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Zografos, Laurie J., Andrews, Elizabeth, Wolin, Dan L., Calingaert, Brian, Davenport, Eric K., Michel, Alexander, Latocha, Margarete, Schmidt-Ott, Ursula Maria, Lovic, Nejra, Brunck, Lynne R., Johnson, Kristian T., and Suzart-Woischnik, Kiliana
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- 2024
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9. Acute kidney injury (AKI)
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Schmidt-Ott, Kai, de Groot, Kirsten, and Eckardt, Kai Uwe
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- 2024
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10. Grainyhead-like 2 Deficiency and Kidney Cyst Growth in a Mouse Model
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Yurtdas, Zeliha Yesim, Kilic, Ergin, Boor, Peter, Wyler, Emanuel, Landthaler, Markus, Jung, Klaus, and Schmidt-Ott, Kai M.
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- 2024
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11. Application of hyperspectral imaging for characterization of VOC-induced historical glass corrosion
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Sharma, Deepshikha, Schmidt-Ott, Katharina, Rothenhäusler, Ulrike, George, Sony, Joseph, Edith, and Lombardo, Tiziana
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- 2024
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12. Left Ventricular Hypertrophy After Renal Transplantation: Systematic Review and Meta-analysis
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Zhejia Tian, Kai Bergmann, Jessica Kaufeld, MD, Kai Schmidt-Ott, MD, Anette Melk, MD, PhD, and Bernhard M.W. Schmidt, MD, SM
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Surgery ,RD1-811 - Abstract
Background. Left ventricular hypertrophy (LVH) in patients with end stage renal disease undergoing renal replacement is linked to an increased risk for cardiovascular diseases. Dialysis does not completely prevent or correct this abnormality, and the evidence for kidney transplantation (KT) varies. This analysis aims to explore the relationship between KT and LVH. Methods. MEDLINE and Scopus were systematically searched in October 2023. All cross-sectional and longitudinal studies that fulfilled our inclusion criteria were included. Outcome was left ventricular mass index (LVMI) changes. We conducted a meta-analysis using a random effects model. Meta-regression was applied to examine the LVMI changes dependent on various covariates. Sensitivity analysis was used to handle outlying or influential studies and address publication bias. Results. From 7416 records, 46 studies met the inclusion criteria with 4122 included participants in total. Longitudinal studies demonstrated an improvement of LVMI after KT −0.44 g/m2 (−0.60 to −0.28). Blood pressure was identified as a predictor of LVMI change. A younger age at the time of KT and well-controlled anemia were also associated with regression of LVH. In studies longitudinally comparing patients on dialysis and renal transplant recipients, no difference was detected −0.09 g/m2 (−0.33 to 0.16). Meta-regression using changes of systolic blood pressure as a covariate showed an association between higher blood pressure and an increase in LVMI, regardless of the modality of renal replacement treatment. Conclusions. In conclusion, our results indicated a potential cardiovascular benefit, defined as the regression of LVH, after KT. This benefit was primarily attributed to improved blood pressure control rather than the transplantation itself.
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- 2024
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13. Free heme and hemopexin in acute kidney injury after cardiopulmonary bypass and transient renal ischemia
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Robert Greite, Sebastian Schott, Li Wang, Lukas Gohlke, Kirill Kreimann, Katja Derlin, Marcel Gutberlet, Martina Schmidbauer, Andreas Leffler, Igor Tudorache, Jawad Salman, Fabio Ius, Ruslan Natanov, Christine Fegbeutel, Axel Haverich, Ralf Lichtinghagen, Anne M. Hüsing, Sibylle vonVietinghoff, Roland Schmitt, Nelli Shushakova, Song Rong, Hermann Haller, Kai M. Schmidt‐Ott, Magnus Gram, Vijith Vijayan, Irina Scheffner, Wilfried Gwinner, and Stephan Immenschuh
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Therapeutics. Pharmacology ,RM1-950 ,Public aspects of medicine ,RA1-1270 - Abstract
Abstract Free heme is released from hemoproteins during hemolysis or ischemia reperfusion injury and can be pro‐inflammatory. Most studies on nephrotoxicity of hemolysis‐derived proteins focus on free hemoglobin (fHb) with heme as a prosthetic group. Measurement of heme in its free, non‐protein bound, form is challenging and not commonly used in clinical routine diagnostics. In contrast to fHb, the role of free heme in acute kidney injury (AKI) after cardiopulmonary bypass (CPB) surgery is unknown. Using an apo‐horseradish peroxidase‐based assay, we identified free heme during CPB surgery as predictor of AKI in patients undergoing cardiac valve replacement (n = 37). Free heme levels during CPB surgery correlated with depletion of hemopexin (Hx), a heme scavenger‐protein. In mice, the impact of high levels of circulating free heme on the development of AKI following transient renal ischemia and the therapeutic potential of Hx were investigated. C57BL/6 mice were subjected to bilateral renal ischemia/reperfusion injury for 15 min which did not cause AKI. However, additional administration of free heme in this model promoted overt AKI with reduced renal function, increased renal inflammation, and reduced renal perfusion on functional magnetic resonance imaging. Hx treatment attenuated AKI. Free heme administration to sham operated control mice did not cause AKI. In conclusion, free heme is a predictor of AKI in CPB surgery patients and promotes AKI in transient renal ischemia. Depletion of Hx in CPB surgery patients and attenuation of AKI by Hx in the in vivo model encourage further research on Hx therapy in patients with increased free heme levels during CPB surgery.
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- 2023
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14. Discovery of a non-canonical GRHL1 binding site using deep convolutional and recurrent neural networks
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Sebastian Proft, Janna Leiz, Udo Heinemann, Dominik Seelow, Kai M. Schmidt-Ott, and Maria Rutkiewicz
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Machine learning ,Neural networks ,Genetics ,Transcription factor binding ,Grainyhead-like 1 ,Biotechnology ,TP248.13-248.65 ,QH426-470 - Abstract
Abstract Background Transcription factors regulate gene expression by binding to transcription factor binding sites (TFBSs). Most models for predicting TFBSs are based on position weight matrices (PWMs), which require a specific motif to be present in the DNA sequence and do not consider interdependencies of nucleotides. Novel approaches such as Transcription Factor Flexible Models or recurrent neural networks consequently provide higher accuracies. However, it is unclear whether such approaches can uncover novel non-canonical, hitherto unexpected TFBSs relevant to human transcriptional regulation. Results In this study, we trained a convolutional recurrent neural network with HT-SELEX data for GRHL1 binding and applied it to a set of GRHL1 binding sites obtained from ChIP-Seq experiments from human cells. We identified 46 non-canonical GRHL1 binding sites, which were not found by a conventional PWM approach. Unexpectedly, some of the newly predicted binding sequences lacked the CNNG core motif, so far considered obligatory for GRHL1 binding. Using isothermal titration calorimetry, we experimentally confirmed binding between the GRHL1-DNA binding domain and predicted GRHL1 binding sites, including a non-canonical GRHL1 binding site. Mutagenesis of individual nucleotides revealed a correlation between predicted binding strength and experimentally validated binding affinity across representative sequences. This correlation was neither observed with a PWM-based nor another deep learning approach. Conclusions Our results show that convolutional recurrent neural networks may uncover unanticipated binding sites and facilitate quantitative transcription factor binding predictions.
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- 2023
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15. Left Ventricular Hypertrophy After Renal Transplantation: Systematic Review and Meta-analysis
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Tian, Zhejia, Bergmann, Kai, Kaufeld, Jessica, Schmidt-Ott, Kai, Melk, Anette, and Schmidt, Bernhard M.W.
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- 2024
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16. Monitoring and Understanding VOC Induced Glass Corrosion Using Multi-modal Imaging Techniques
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Sharma, Deepshikha, Rothenhaeusler, Ulrike, Schmidt-Ott, Katharina, Nurit, Marvin, Cartagena, Yuly Castro, Le-Goic, Gaetan, Joseph, Edith, George, Sony, Lombardo, Tiziana, Chaari, Fakher, Series Editor, Gherardini, Francesco, Series Editor, Ivanov, Vitalii, Series Editor, Cavas-Martínez, Francisco, Editorial Board Member, di Mare, Francesca, Editorial Board Member, Haddar, Mohamed, Editorial Board Member, Kwon, Young W., Editorial Board Member, Trojanowska, Justyna, Editorial Board Member, Furferi, Rocco, editor, Governi, Lapo, editor, Volpe, Yary, editor, and Seymour, Kate, editor
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- 2023
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17. Acute kidney injury in patients treated with immune checkpoint inhibitors
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Gupta, Shruti, Short, Samuel AP, Sise, Meghan E, Prosek, Jason M, Madhavan, Sethu M, Soler, Maria Jose, Ostermann, Marlies, Herrmann, Sandra M, Abudayyeh, Ala, Anand, Shuchi, Glezerman, Ilya, Motwani, Shveta S, Murakami, Naoka, Wanchoo, Rimda, Ortiz-Melo, David I, Rashidi, Arash, Sprangers, Ben, Aggarwal, Vikram, Malik, A Bilal, Loew, Sebastian, Carlos, Christopher A, Chang, Wei-Ting, Beckerman, Pazit, Mithani, Zain, Shah, Chintan V, Renaghan, Amanda D, De Seigneux, Sophie, Campedel, Luca, Kitchlu, Abhijat, Shin, Daniel Sanghoon, Rangarajan, Sunil, Deshpande, Priya, Coppock, Gaia, Eijgelsheim, Mark, Seethapathy, Harish, Lee, Meghan D, Strohbehn, Ian A, Owen, Dwight H, Husain, Marium, Garcia-Carro, Clara, Bermejo, Sheila, Lumlertgul, Nuttha, Seylanova, Nina, Flanders, Lucy, Isik, Busra, Mamlouk, Omar, Lin, Jamie S, Garcia, Pablo, Kaghazchi, Aydin, Khanin, Yuriy, Kansal, Sheru K, Wauters, Els, Chandra, Sunandana, Schmidt-Ott, Kai M, Hsu, Raymond K, Tio, Maria C, Mothi, Suraj Sarvode, Singh, Harkarandeep, Schrag, Deborah, Jhaveri, Kenar D, Reynolds, Kerry L, Cortazar, Frank B, Leaf, David E, Salem, Joe-Elie, Bagnis, Corinne Isnard, Rahma, Osama E, Mothi, Suraj S, Selamet, Umut, Chang, Weiting, Hirsch, Jamie S, Sakhiya, Vipulbhai, Stalbow, Daniel, Wu, Sylvia, Cennamo, Armando, Papa, Sophie, Rigg, Anne, Shaunak, Nisha, Kibbelaar, Zoe A, and Benesova, Karolina
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Kidney Disease ,6.1 Pharmaceuticals ,Evaluation of treatments and therapeutic interventions ,Renal and urogenital ,Good Health and Well Being ,Acute Kidney Injury ,Aged ,Cohort Studies ,Female ,Humans ,Immune Checkpoint Inhibitors ,Immunotherapy ,Male ,Middle Aged ,Risk Factors ,immunotherapy ,CTLA-4 antigen ,programmed cell death 1 receptor ,ICPi-AKI Consortium Investigators - Abstract
BackgroundImmune checkpoint inhibitor-associated acute kidney injury (ICPi-AKI) has emerged as an important toxicity among patients with cancer.MethodsWe collected data on 429 patients with ICPi-AKI and 429 control patients who received ICPis contemporaneously but who did not develop ICPi-AKI from 30 sites in 10 countries. Multivariable logistic regression was used to identify predictors of ICPi-AKI and its recovery. A multivariable Cox model was used to estimate the effect of ICPi rechallenge versus no rechallenge on survival following ICPi-AKI.ResultsICPi-AKI occurred at a median of 16 weeks (IQR 8-32) following ICPi initiation. Lower baseline estimated glomerular filtration rate, proton pump inhibitor (PPI) use, and extrarenal immune-related adverse events (irAEs) were each associated with a higher risk of ICPi-AKI. Acute tubulointerstitial nephritis was the most common lesion on kidney biopsy (125/151 biopsied patients [82.7%]). Renal recovery occurred in 276 patients (64.3%) at a median of 7 weeks (IQR 3-10) following ICPi-AKI. Treatment with corticosteroids within 14 days following ICPi-AKI diagnosis was associated with higher odds of renal recovery (adjusted OR 2.64; 95% CI 1.58 to 4.41). Among patients treated with corticosteroids, early initiation of corticosteroids (within 3 days of ICPi-AKI) was associated with a higher odds of renal recovery compared with later initiation (more than 3 days following ICPi-AKI) (adjusted OR 2.09; 95% CI 1.16 to 3.79). Of 121 patients rechallenged, 20 (16.5%) developed recurrent ICPi-AKI. There was no difference in survival among patients rechallenged versus those not rechallenged following ICPi-AKI.ConclusionsPatients who developed ICPi-AKI were more likely to have impaired renal function at baseline, use a PPI, and have extrarenal irAEs. Two-thirds of patients had renal recovery following ICPi-AKI. Treatment with corticosteroids was associated with improved renal recovery.
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- 2021
18. Intravitreal aflibercept 8 mg in diabetic macular oedema (PHOTON): 48-week results from a randomised, double-masked, non-inferiority, phase 2/3 trial
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Abraham, Prema, Aderman, Christopher, Akiyama, Kunihiko, Alfaro, Daniel V., Ali, Fareed A., Amini, Payam, Anzalotta, Andres Emanuelli, Bátor, György, Batlle, Ivan, Berger, Adam, Bhandari, Ramanath, Bridges, William, Brinkmann, Christian, Brown, Jamin, Burgess, Stuart, Calzada, Jorge, Capone Jr., Antonio, Cervena, Dana, Charles, Steven, Chaudhry, Nauman, Chow, David, Clark, W. Lloyd, Conrad III, Paul, Cunningham, Matthew, Dadgostar, Hajir, Dessouki, Amr, Deupree, Dana, Devine, Christopher, Eichenbaum, David, Ernest, Jan, Feltgen, Nicolas, Fenberg, Moss, Ferrone, Philip, Frenkel, Ronald, Friedman, Scott, Gasperini, Julie, Gerstenblith, Adam, Ghorayeb, Ghassan, Giunta, Michel, Goff, Mitchell, Golas, Liliya, Googe Jr., Joseph M., Goren Fein, Jordana, Hagedorn, Curtis, Hagiwara, Akira, Hahn, Paul, Hairston, Richard, Handza, Jason, Hau, Vivienne, Hayashi, Ken, Heier, Jeffrey, Hershberger, Vrinda, Higgins, Patrick, Hirano, Yoshio, Honda, Shigeru, Ikegami, Yasuko, Ishida, Yuichiro, Ishikawa, Isao, Ishii, Kiyoshi, Jablon, Eric P., Jain, Atul, Kaji, Yuichi, Kapoor, Kapil, Kerényi, Ágnes, Kimura, Kazuhiro, Kishino, Genichiro, Kiss, Katalin, Kitaoka, Takashi, Klancnik, James M., Kobayashi, Namie, Kogo, Jiro, Korda, Vladimir, Kruger, Erik, Kusuhara, Sentaro, Lara, Wilfredo, Laud, Ketan, Lee, Seong, Luu, James, Marcus, Dennis, Mein, Calvin, Meleth, Annal, Milibák, Tibor, Mitamura, Yoshinori, Murata, Toshinori, Noge, Sumiyo, Onoe, Hajime, Osher, James, Papp, András, Parschauer, Justin, Patel, Sugat, Patel, Sunil, Pezda, Matthew, Pirouz, Ashkan, Prasad, Pradeep, Punjabi, Omar, Rao, Llewelyn, Roe, Richard, Schadlu, Ramin, Schneider, Eric, Shah, Ankur, Shah, Milan, Shah, Sandeep, Shah, Sumit, Sharma, Ashish, Sheth, Veeral, Shimura, Masahiko, Singerman, Lawrence, Spital, Georg, Stoltz, Robert, Suan, Eric, Suzuma, Kiyoshi, Takahashi, Hidenori, Takamura, Yoshihiro, Takeuchi, Masaru, Tan, Jeffrey, Thomas, Benjamin, Tóth,-Molnár, Edit, Ueda, Tetsuo, Ushida, Hiroaki, Vajas, Attila, Varma, Deepali, Varsányi, Balázs, Veith, Miroslav, Weber, Pamela, Wee, Raymond, Williams, Geoff, Yamada, Haruhiko, Yonekawa, Yoshihiro, Yoshida, Shigeo, Brown, David M, Boyer, David S, Do, Diana V, Wykoff, Charles C, Sakamoto, Taiji, Win, Peter, Joshi, Sunir, Salehi-Had, Hani, Seres, András, Berliner, Alyson J, Leal, Sergio, Vitti, Robert, Chu, Karen W, Reed, Kimberly, Rao, Rohini, Cheng, Yenchieh, Sun, Wei, Voronca, Delia, Bhore, Rafia, Schmidt-Ott, Ursula, Schmelter, Thomas, Schulze, Andrea, Zhang, Xin, Hirshberg, Boaz, Yancopoulos, George D, and Sivaprasad, Sobha
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- 2024
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19. Intravitreal aflibercept 8 mg in neovascular age-related macular degeneration (PULSAR): 48-week results from a randomised, double-masked, non-inferiority, phase 3 trial
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Lanzetta, Paolo, Korobelnik, Jean-François, Heier, Jeffrey S, Leal, Sergio, Holz, Frank G, Clark, W Lloyd, Eichenbaum, David, Iida, Tomohiro, Xiaodong, Sun, Berliner, Alyson J, Schulze, Andrea, Schmelter, Thomas, Schmidt-Ott, Ursula, Zhang, Xin, Vitti, Robert, Chu, Karen W, Reed, Kimberly, Rao, Rohini, Bhore, Rafia, Cheng, Yenchieh, Sun, Wei, Hirshberg, Boaz, Yancopoulos, George D, and Wong, Tien Y
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- 2024
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20. Efficacy and safety of aldosterone synthase inhibition with and without empagliflozin for chronic kidney disease: a randomised, controlled, phase 2 trial
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Tuttle, Katherine R, Hauske, Sibylle J, Canziani, Maria Eugenia, Caramori, Maria Luiza, Cherney, David, Cronin, Lisa, Heerspink, Hiddo J L, Hugo, Christian, Nangaku, Masaomi, Rotter, Ricardo Correa, Silva, Arnold, Shah, Shimoli V, Sun, Zhichao, Urbach, Dorothea, de Zeeuw, Dick, Rossing, Peter, SZETO, Cheuk Chun, Echeverri, Diego, Martin, Edouard, Yee, Ming Li, Wah, William, Wang, Ray, Chacko, Bobby, Swaminathan, Shriram, MacIsaac, Richard, Hashimura, Hikaru, Ward, Glenn, De Vusser, Katrien, Claes, Kathleen, Kuypers, Dirk, Meijers, Björn, Van Craenenbroeck, Amaryllis, Hilbrands, Robert, Debroye, Corinne, Wissing, Karl Martin, Jadoul, Michel, Demoulin, Nathalie, Treille De Grandsaigne, Serge, Beklevic, Ishak, Marcoux, Diane, Liénart, Fabienne, Daper, Claude, De Brouckere, Véronique, Heureux, Mercédès, Felicio, Joao, Felicio, Karem Mileo, Leite, Daniella, Melo, Franciane, Queiroz, Natercia, Souza, Ana Carolina, Vieira, Jocyelle, Franco, Roberto, Mendes, Adriana, Picolli, Giovana, Canani, Luis Henrique, Sartori, Carla, Valenti, Adriana, Eliaschewitz, Freddy, Bona, Renata, Franco, Denise, Ludovico Costa de Castro, Denise, Magalhaes, Vanessa, Oliveira, Marcelo, Sampaio, Célia Regina, Visconti, Guilherme, Halpern, Bruno, Nihei, Camila, Pessoa, Bruna, Seraphim, Carlos, Santos, Daniel, Brito, Claudia, Douverny, Joao, Colella, Marina, Gazeta, Cristina, Vercia, Monique, Watanabe, Renato, Temelkova, Theodora, Kjurkchiev, Dimo, Statkova, Silviya, Popov, Iliya, Radeva, Radosveta, Arabadzhiev, Lachezar, Binova, Mariya, Bosilkov, Aleksandar, Koleva-Stoicheva, Neli, Ivanov, Ivaylo, Ivanova, Zornitsa, Kotseva, Viktoria, Spasov, Petar, Tsvetkov, Ivaylo, Jolly, Shivinder, Bailey, Gordon, Ye, Zhiming, Niu, Jianying, Li, Hongmei, Wu, Qing, Liao, Bing, Hao, Chuanming, Lai, Lingyun, Xu, Yunyu, Zhang, Min, Li, Yiwen, Liu, Bo, Shao, Lina, Chen, Wei, Wu, Haishan, Pirchala, Marian, Skarpova, Iva, Hraskova, Marketa, Soukupova, Simoneta, Veberova, Lucie, Drasnar, Tomas, Falc, Matej, Racz, Blazej, Votocek, Stepan, Weissova, Danica, Syc-Krivanova, Lenka, Slezak, Dagmar, Kantola, Ilkka, Nieminen, Sakari, Anttonen, Milla, Taurio, Jyrki, Lahtela, Jorma, Tsimihodimos, Vasileios, Balafa, Olga, Dounousi, Evangelia, Sakkou, Sissy, Tentolouris, Nikolaos, Siafarikas, Christos, Siami, Evangelia, Doupis, Ioannis, Angelopoulos, Theodoros, Georgoulias, Christodoulos, Pall, Denes, Esze, Regina, Kobling, Tamas, Varadi, Zita, Zsiros, Noemi, Vass, Viktor, Balo, Timea, Csanyi, Erika, Ory, Ivan, Pall, Istvan, Patai, Valentina, Zeak, Zsuzsanna, Takacs, Istvan, Petho, Akos, Szili, Balazs, Koranyi, Laszlo, Bezzegh, Katalin, Pauer, Jozsef, Peterfai, Eva, Konyves, Laszlo, Szoke, Brigitta, Hajdu, Csaba, Kalman, Krisztina, Yadav, Raj, Saxena, Navneet, Bhattacharya, Meenakshi, Sharma, Bal, Thomas, Nihal, K, Felix Jebasingh, Kapoor, Nitin, Kurian, Mathews E., Paul, Jinson, Ramesh, Priyadharshini, Varghese, Sheeba, Shibusawa, Nobuyuki, Nishi, Hiroshi, Noritake, Nobuyasu, Oda, Takashi, Okamoto, Hideki, Kasuga, Hirotake, Hori, Hiroshi, Ito, Yukiko, Mizukoshi, Toshihiro, Ishii, Hideto, Han, Seung Hyeok, Kim, Hyung Woo, Oh, Kook-Hwan, Han, Seung Seok, Han, Sang Youb, Cha, Dae Ryong, Cha, Jin Joo, Kwon, Soon-Kil, Cho, Hyunjeong, Kim, Hye-Young, Kim, Sun Moon, Lee, Jung Pyo, Lee, Jeonghwan, Lee, Li Yuan, Chang, Meng Lee, Laang, Shian Tuck, Tan, Zhao Zhi, Ahmad Rosdi, Hajar, Mohammad Ismail, Siti Hafizah, Simatherai, Devamalar, Tay, Ju Fan, Wong, Eddie, Fook Sem, Yakob, Suryati, Abdul Sukur, Noorhafini, Anuar, Amalina, Md. Rasid, Syaliza, Mushaddik, Irma Liyana, Mustafar, Ruslinda, Abu Shamsi, Muhammad Yusuf, Fong, Voon Ken, Kamaruzaman, Lydia, Mohd, Rozita, Wan Daud, Wan Rohaslizan, Wan Hassan, Wan Hasnul Halimi, Ab Hamid, Suhaidarwani, Abdullah, Muhammad Nabil, Yusoff, Mohd Yusran, Ramanathan, G R Letchuman, Lee, Kim Yen, Wan Ismail, Wan Fadhilah, Morales Villegas, Enrique, Ramirez Baez, Rubria, Vital Lopez, Jorge, Arias Delgadillo, Cristhian, Herrera Marmolejo, Marisol, Parra Perez, Rosa, Alpizar Salazar, Melchor, Flores Montealegre, Ana, Galvan Magaña, Jose, Gutierrez Tlapale, Minerva, Reyes Munguia, Daniela, Witczak, Bartlomiej, Gøransson, Lasse, Strand Thorsen, Inga, Caringal, Clodoaido, Villardo, Mario, Toledo, Ronaldo, Dijamco, Emerlinda Fausto, De Asis, Norman Cornelio, Kuizon, Angelica, Catindig, Elizabeth Ann, Perez, Ronald, Aquitania, Grace, Pableo, Jimrie David, Sanchez, Jay Karlou, Czernecka, Ewa, Cegiel, Aleksandra, Knychas, Dorota, Ochnio, Malgorzata, Kuligowska-Jakubowska, Monika, Cesarz, Marek, Kowalewska-Celejewska, Milena, Masajtis-Zagajewska, Anna, Jankowski, Lukasz, Ojrzanowski, Marcin, Olszewska-Jander, Magdalena, Skokowska, Ewa, Giermakowska-Samek, Malgorzata, Luchowska, Elzbieta, Patkowska, Renata, Sekulska, Marzenna, Marczuk-Krynicka, Dorota, Marciniak, Andrzej, Barwijuk, Michal, Myslicki, Marcin, Siek, Michal, Wronska, Danuta, Tomsia-Goncerz, Jadwiga, Wronski, Krzysztof, Junik, Roman, Dzialak, Szymon, Kurlapska, Ewelina, Malecha, Wieslaw, Suwala, Szymon, Branco, Patrícia, Birne, Rita, Raposo, João, Ferreira, Marta, Alexandrino, Henrique, Alves, Helena, Correia, Sara, Oliveira, Maria João, Ramalho, Diogo, Tavares, Patricia, Coetzee, Kathleen, Blignaut, Sue, Viljoen, Winifred, Potgieter, Elsje, Malherbe, Elmien, Ortiz Arduán, Alberto, Goma Garcés, Elena, Pérez, María, Santamaría, Rafael, López López, Isabel, Pendón de Mier, Victoria, Rodelo Haad, Cristian, Marques, María, Domènech, Esther, Portoles, Josep Maria, Soler, María José, Agraz, Irene, Azancot, María Antonieta, Bermejo, Sheila, Bolufer, Mónica, López, Marina, Ramos, Natalia, Toapanta, Néstor, Cigarrán Guldris, Secundino, Primo, Juan Carlos, Pérez, Luis Enrique, Rebollido Fernández, María, Holmer, Helene, Bruchfeld, Annette, Rofors, Justus, Tengmark, Bengt-Olov, Wuerzner, Gregoire, Leanizbarrutia, Garazi, Ozturk, Savas, Guler, Nurana, Safak, Seda, Lee, Keung, Campbell, Stephen, Siddiqui, Imran, Abbasi, Nadia, Tahir, Faiza, Azizad, Masoud, Jackson, Timothy, Everhart, Brian, Oliver, Michael, Rust, William, Sniezek, Matthew, Arif, Ahmed, Syed, Mohammed, Bhasin, Nitin, Bien, Michael, Gallego, Claudio, Jamal, Aamir, Moghadam, Mojtaba, Rizvi, Abid, Rizvi, Amna, Rizvi, Syed, Wong, Christopher, Lucas, Kathryn, Buery, Andrea, Chang, Ku-Lang, Presswood, Claire, Smith, Justin, Doshi, Ankur, Parikh, Manish, Wallace, Jeannine, Krishna, Arvind, Daugherty, Heidi, Fearday, Aaron, Keller, Christopher, Meng, Jerry, Nielsen, Alexandra, Rovner, Sergio, Almeida, Javier, Marranzini, Benito, Selby, Lisa, Yablon, Zachary, Jean-Louis, Daphne, Kotzker, Wayne, Perez, Chabely, Richards, Marc, Rosario, Reinaldo, Marcus, Roy, Okechukwu, Chike, Ross, Dennis, Gromala, Rachel, Reed, Matthew, Weber, Lisa, Nazeer, Imran, Kumar, Prashant, Mir, Muhammad, Shea, Heidi, Hart, Amanda, Wiebel, Jaime, Kooienga, Laura, Newsome, Britt, Suyumova, Irina, Alvarez, German, Bireddy, Venkata, Lansang, Maria, Mandry, Jose, Freire, Maria, Herrera Albornoz, Oscarina, Desai, Anant, Gandhi, Dayan, Rajan, Sibu, Raymond, Louis, Posada, Jorge, Garcia-Mayol, Luis, Gutierrez-Alsina, Rodolfo, Fernandez, Juan, Bruce, Kendaling, Cuellar, Juan, Ranz y Alvarez, Maria, Bartolacci, Ines, Pautasso, Mauro, Stoppa, Daniela, Riella, Miguel, Barbosa, Maria, Harcsa, Eleonora, Gulati, Yuvraj, Savalia, Denish, Khetan, Prakash, Sinha, Dhananjay, R, Niranjan, K, Srinivas, Pazos, Fabiola, Gacutan-Liwag, Aretha, Duszynska, Malgorzata, Antkowiak-Piatyszek, Karolina, Konieczny, Grzegorz, Sidorowicz-Bialynicka, Anna, Ciesiolkiewicz-Wojcik, Agnieszka, Dwojak, Marek, Szymkowiak, Katarzyna, Gorczyca-Siudak, Daria, Janik-Palazzolo, Marzena, Siudak, Lukasz, Opiela, Jaroslaw, Iwanow, Dariusz, Solkiewicz, Monika, Sipinska-Surzynska, Malgorzata, Olszanecka - Glinianowicz, Magdalena, Rozmilowska, Izabela, Trokis, Julian, Prozesky, Hans, Burgess, Lesley, Cyster, Henry, Jordaan, Jurie, Mohamed, Hawa, Naude, Christina, Sitsila, Thembie, Mehta, Arvind, Mocherla, Bharat, Lee, Sungchun, Boren, Kenneth, Rudolph, Lance, Benjamin, Sabrina, Sugimoto, Danny, Hammoud, Jamal, Bakleh, Muhammad, Hashish, Yaseen, Da Costa, Jonathan, Gold, Marina, Majul, Claudio, Buscema, Juan, Gatto, Maria, Lombardi, Facundo, Paez, Olga, Puleio, Pablo, Alvarisqueta, Andrés, Pajon, Vanessa, Suarez, Gabriel, Hernandez Gauna, Adrian, Pereyra, Alejandro, Reig, Moira, Gelersztein, Elizabeth, Campestri, Gina, Gonzalez Santos, Maria, Sambresqui, Julieta, Catalano, Gustavo, Igarzabal, Cecilia, Vallejos, Augusto, Escobari, Claudio, Marchetto, Rocio, Chahin, Mariano, Aguilera, Andrea, Comes, Ana, Rodriguez Segade, Silvia, Baccaro, Claudia, Larrieu Lacoste, María Verónica, Saurral, Ruben, Cristino, Alberto, Dran, Dario, Koretzky, Martin, Ponti, Juan, Porto, Alejandro, Tenaglia, Yasmin, Maldonado, Natacha, Bertollo, Natalia, Van Perdeck, Verónica, Lopau, Kai, Wanner, Christoph, Berfelo, Florieke, Contzen, Christel, Arbi, Abdulwahab, Lee-Barkey, Young Hee, Maciejewska, Aleksandra, Arelin, Katrin, Haller, Hermann, Kaufeld, Jessica, Schmidt-Ott, Kai, Heinrichs, Sven, Krüger, Thilo, Gebauer, Chris, Paliege, Alexander, Henkel, Elena, Axthelm, Christoph, Derwahl, Karl-Michael, Trevisan, Roberto, Bellante, Rosalia, Borrella, Nicolò, Corsi, Anna, Gesualdo, Loreto, Ardillo, Teodora, Ficarella, Maria, Fikry, Sameh, Mazza, Giuseppe, Poirier, Lysane, Bajaj, Harpreet, Hatziagelaki, Erifili, Katopodis, Sokratis, Katsoudas, Spiros, Yamaura, Shuichi, Shikano, Tsutomu, Tosaki, Takahiro, Miho, Otoya, Tachibana, Naoki, Yumita, Wataru, Kado, Hiroshi, Villarreal Martinez, Jesus, Soto Miranda, Ernesto, Gonzalez Rodriguez, David, Panelo, Araceli, Santos, Telma, Martins, Ana, Mateus, Catarina, Teixeira e Costa, Fernando, Barreto, Sara, Silva Costa, Joana, Ferrer, Francisco, Silva, Joana, Awad, Ahmed, Khaleel, Shatha, Lustig, Ryan, Maharjan, Gajendra, Moya, Jaynier, Johnsingh, Amit, Acosta, Idalia, Newman, George, Buckle, Anita, and Hendon, Kendra
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- 2024
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21. Discovery of a non-canonical GRHL1 binding site using deep convolutional and recurrent neural networks
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Proft, Sebastian, Leiz, Janna, Heinemann, Udo, Seelow, Dominik, Schmidt-Ott, Kai M., and Rutkiewicz, Maria
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- 2023
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22. Acquisition strategies for in-situ hyperspectral imaging of stained-glass windows: case studies from the Swiss National Museum
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Babini, Agnese, Lombardo, Tiziana, Schmidt-Ott, Katharina, George, Sony, and Hardeberg, Jon Yngve
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- 2023
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23. Acquisition strategies for in-situ hyperspectral imaging of stained-glass windows: case studies from the Swiss National Museum
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Agnese Babini, Tiziana Lombardo, Katharina Schmidt-Ott, Sony George, and Jon Yngve Hardeberg
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Stained-glass ,Hyperspectral imaging ,Transmittance ,In-situ measurement ,Fine Arts ,Analytical chemistry ,QD71-142 - Abstract
Abstract Over the last decade, hyperspectral imaging has become a popular technique for the non-invasive identification and mapping of painting materials in many typologies of artworks, thanks to the possibility of obtaining spectral information over the spatial region. A few attempts have also been made on stained-glass windows to identify the chromophore elements responsible for glass color. Hyperspectral imaging of stained glass can be complex; in most cases, stained-glass windows are an integral part of buildings, and sunlight represents the natural light source for illuminating these artifacts. While it may be considered an advantage, sunlight is not homogeneous throughout the day, and different weather conditions can affect the quality of the hyperspectral images. In addition, the presence of buildings and vegetation in the background could also modify the colors of the stained-glass windows and consequently alter the characteristic peaks of the chromophores in the spectra. This work aims to solve some of these issues and proposes different strategies to improve the results obtainable in situ. The methodology was tested on stained-glass panels displayed in the windows of the Swiss National Museum. Stained-glass panels located in windows of an internal wall were also analyzed, developing a lighting setup to account for the lack of natural light. Hyperspectral images of the selected stained glass were acquired multiple times, choosing different transmittance references for the preprocessing and exposure time to evaluate differences in the collected spectral images. The use of a diffuser sheet to mitigate the effect of external factors was also tested on some panels exposed to sunlight. Results from representative case studies will be presented to discuss the feasibility and limitations of in-situ hyperspectral imaging applications on stained glass and provide some general recommendations to consider during the acquisitions.
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- 2023
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24. Prospective Cohort Study of Soluble Urokinase Plasminogen Activation Receptor and Cardiovascular Events in Patients With CKD
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Eckardt, Kai-Uwe, Meiselbach, Heike, Schneider, Markus P., Schiffer, Mario, Prokosch, Hans-Ulrich, Bärthlein, Barbara, Beck, Andreas, Kraska, Detlef, Reis, André, Ekici, Arif B., Becker, Susanne, Alberth-Schmidt, Ulrike, Marschall, Sabine, Schefler, Eugenia, Weigel, Anke, Walz, Gerd, Köttgen, Anna, Schultheiß, Ulla T., Kotsis, Fruzsina, Meder, Simone, Mitsch, Erna, Reinhard, Ursula, Floege, Jürgen, Saritas, Turgay, Schaeffner, Elke, Baid-Agrawal, Seema, Theisen, Kerstin, Schmidt-Ott, Kai, Zeier, Martin, Sommerer, Claudia, Aykac, Mehtap, Wolf, Gunter, Busch, Martin, Paul, Rainer, Sitter, Thomas, Wanner, Christoph, Krane, Vera, Börner-Klein, Antje, Bauer, Britta, Kronenberg, Florian, Raschenberger, Julia, Kollerits, Barbara, Forer, Lukas, Schönherr, Sebastian, Weissensteiner, Hansi, Oefner, Peter, Gronwald, Wolfram, Schmid, Matthias, Nadal, Jennifer, Müller-Krebs, Sandra, Schultheiss, Ulla T., Friedrich, Nele, Nauck, Matthias, Nußhag, Christian, Reiser, Jochen, and Hayek, Salim S.
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- 2023
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25. Elektrolytstörungen in der Intensivmedizin
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Schenk, Heiko, Schmidt-Ott, Kai M., and Schmidt, Julius J.
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- 2023
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26. Was ist gesichert in der Therapie?
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Haller, Hermann and Schmidt-Ott, Kai
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- 2023
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27. Current practice of blood pressure measurement in Germany: a nationwide questionnaire-based survey in medical practices
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Christian Beger, Astrid Mayerböck, Konrad Klein, Theresa Karg, Kai M. Schmidt-Ott, Olaf Randerath, and Florian P. Limbourg
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hypertension ,blood pressure ,office blood pressure ,home blood pressure monitoring ,hbpm ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Purpose Discrepancies exist between guideline recommendations and real-world practice of blood pressure (BP) measurements. The aim of this study was to assess, with a nationwide, questionnaire-based survey, the current practice of BP measurement and associated BP values in German medical practices. Material and methods A nationwide survey in German medical practices was performed in the period from 10 May 2021 to 15 August 2021. The questionnaire was divided into five sections. The current office BP (OBP) values as well as the current drug therapy were recorded. In addition, the implementation of office BP (OBP) and home BP monitoring (HBPM) was queried. For analysis, questionnaires were scanned and automatically digitised. Results A total of 7049 questionnaires were analysed, the majority of which came from general practitioners (66%) and internal medicine practices (34%). The average OBP (SD) was 140.0 (18)/82.7 (11) mmHg. 40.8% of treated patients had OBP in the controlled range, with monotherapy (34.7%) or dual combination therapy (38.2%) prescribed in most cases. OBP was taken from a single measurement in 66.3% of cases, and in 21.8% from 23 measurements. OBP was mostly measured after a rest period (87.1%) and in a separate room (80.4%). HBPM was performed in 62.3% of patients; however, in 24.9% of the participants HBP measurements were recorded once a week or less. Conclusion In this nationwide survey in German medical practices, BP control remains at below 50%, while monotherapy is prescribed in around one third of patients. Moreover, office measurements and HBPM are often not performed according to current guideline recommendations.
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- 2023
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28. Protocol of the Berlin Long-term Observation of Vascular Events (BeLOVE): a prospective cohort study with deep phenotyping and long-term follow up of cardiovascular high-risk patients
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Ulrike Grittner, Ulf Landmesser, Matthias Endres, David M Leistner, Burkert Pieske, Kai-Uwe Eckardt, Joachim Spranger, Jeanette Schulz-Menger, Sophie K Piper, Martin Witzenrath, Geraldine Rauch, Sein Schmidt, Vasan S Ramachandran, Christian H Nolte, Tobias Pischon, Dominik N Müller, Frank Edelmann, Leif-Hendrik Boldt, Norbert Hubner, Kai M Schmidt-Ott, Bob Siegerink, Joachim E Weber, Michael Ahmadi, Holger Gerhardt, Kathrin Haubold, Jil Kollmus-Heege, Knut Mai, Simrit Rattan, Katharina Schönrath, and Oliver Schweizerhof
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Medicine - Abstract
Introduction The Berlin Long-term Observation of Vascular Events is a prospective cohort study that aims to improve prediction and disease-overarching mechanistic understanding of cardiovascular (CV) disease progression by comprehensively investigating a high-risk patient population with different organ manifestations.Methods and analysis A total of 8000 adult patients will be recruited who have either suffered an acute CV event (CVE) requiring hospitalisation or who have not experienced a recent acute CVE but are at high CV risk. An initial study examination is performed during the acute treatment phase of the index CVE or after inclusion into the chronic high risk arm. Deep phenotyping is then performed after ~90 days and includes assessments of the patient’s medical history, health status and behaviour, cardiovascular, nutritional, metabolic, and anthropometric parameters, and patient-related outcome measures. Biospecimens are collected for analyses including ‘OMICs’ technologies (e.g., genomics, metabolomics, proteomics). Subcohorts undergo MRI of the brain, heart, lung and kidney, as well as more comprehensive metabolic, neurological and CV examinations. All participants are followed up for up to 10 years to assess clinical outcomes, primarily major adverse CVEs and patient-reported (value-based) outcomes. State-of-the-art clinical research methods, as well as emerging techniques from systems medicine and artificial intelligence, will be used to identify associations between patient characteristics, longitudinal changes and outcomes.Ethics and dissemination The study was approved by the Charité—Universitätsmedizin Berlin ethics committee (EA1/066/17). The results of the study will be disseminated through international peer-reviewed publications and congress presentations.Study registration First study phase: Approved WHO primary register: German Clinical Trials Register: https://drks.de/search/de/trial/DRKS00016852; WHO International Clinical Registry Platform: http://apps.who.int/trialsearch/Trial2.aspx?TrialID=DRKS00016852. Recruitment started on July 18, 2017.Second study phase: Approved WHO primary register: German Clinical Trials Register DRKS00023323, date of registration: November 4, 2020, URL: http://www.drks.de/ DRKS00023323. Recruitment started on January 1, 2021.
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- 2023
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29. Strikingly conserved gene expression changes of polyamine regulating enzymes among various forms of acute and chronic kidney injury
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Sieckmann, Tobias, Schley, Gunnar, Ögel, Neslihan, Kelterborn, Simon, Boivin, Felix J., Fähling, Michael, Ashraf, Muhammad I., Reichel, Martin, Vigolo, Emilia, Hartner, Andrea, Lichtenberger, Falk-Bach, Breiderhoff, Tilman, Knauf, Felix, Rosenberger, Christian, Aigner, Felix, Schmidt-Ott, Kai, Scholz, Holger, and Kirschner, Karin M.
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- 2023
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30. Reported Rates of Intraocular Inflammation with Intravitreal Aflibercept Administered via Pre-Filled Syringe or from Vials in Clinical Practice Between 2012 and 2022
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Schmidt-Ott U, Fitzpatrick S, Hasanbasic Z, Leal S, Morgan-Warren P, Zhang X, and Johnson KT
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anti vegf ,eye ,injection ,ioi ,drug-related side effects and adverse reactions ,Ophthalmology ,RE1-994 - Abstract
Ursula Schmidt-Ott,1 Scott Fitzpatrick,2 Zoran Hasanbasic,3 Sergio Leal,3 Peter Morgan-Warren,4 Xin Zhang,3 Kristian T Johnson5 1Bayer AG, Berlin, Germany; 2Bayer AG, Mississauga, Canada; 3Bayer Consumer Care AG, Basel, Switzerland; 4Bayer PLC, Reading, UK; 5Bayer US LLC, Cambridge, MA, USACorrespondence: Ursula Schmidt-Ott, Bayer AG, Müllerstraße 178, Berlin, 13353, Germany, Tel +49 30 468 1111, Email ursula.schmidt-ott@bayer.comPurpose: To determine the reported rates of intraocular inflammation (IOI) in patients treated with intravitreal aflibercept (IVT-AFL) 2 mg in routine clinical practice (ie, outside interventional studies), across all indications and within all countries (excluding the United States), with access to either the vial presentation or pre-filled syringe (PFS).Patients and methods: A search was conducted using the Bayer EYLEA® Global Safety Pharmacovigilance Database for reported cases of IOI and IVT-AFL use between October 2012 and March 31, 2022.Results: With more than 10 years of post-marketing experience with the IVT-AFL vial presentation (> 25 million sold units), and over 2 years of experience with the PFS of IVT-AFL (> 6.7 million sold units) the rate of any IOI, including endophthalmitis, outside the United States was 0.3 events per 10,000 units for the PFS and 1.2 events per 10,000 units for the vial presentation. The event rates specifically for endophthalmitis were 0.1 per 10,000 units for the IVT-AFL PFS and 0.6 per 10,000 units for the IVT-AFL vial presentation.Conclusion: In patients with retinal diseases treated in routine clinical practice with IVT-AFL either from a vial or the PFS, medically important adverse events of IOI, and in particular, endophthalmitis, are infrequently reported events. Numerically, reported rates of IOI and endophthalmitis are low for the vial presentation and even lower for the PFS.Keywords: anti-VEGF, eye, injection, IOI, drug-related side effects and adverse reactions
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- 2023
31. Was ist gesichert in der Therapie der chronischen Nierenerkrankung?
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Greite, Robert and Schmidt-Ott, Kai
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- 2022
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32. Exposure to airborne SARS-CoV-2 in four hospital wards and ICUs of Cyprus. A detailed study accounting for day-to-day operations and aerosol generating procedures
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Konatzii, Rafail, Schmidt-Ott, Fabian, Palazis, Lakis, Stagianos, Panagiotis, Foka, Maria, Richter, Jan, Christodoulou, Christina, Sciare, Jean, and Pikridas, Michael
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- 2023
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33. CSF-1 and Notch signaling cooperate in macrophage instruction and tissue repair during peripheral limb ischemia
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Tamar Kapanadze, Jaba Gamrekelashvili, Stefan Sablotny, Dustin Kijas, Hermann Haller, Kai Schmidt-Ott, and Florian P. Limbourg
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macrophages ,ischemia ,inflammation ,CSF-1 ,notch signaling ,CSF-1 inhibition ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Ischemia causes an inflammatory response featuring monocyte-derived macrophages (MF) involved in angiogenesis and tissue repair. Angiogenesis and ischemic macrophage differentiation are regulated by Notch signaling via Notch ligand Delta-like 1 (Dll1). Colony stimulating factor 1 (CSF-1) is an essential MF lineage factor, but its role in ischemic macrophage development and the interaction with Notch signaling is so far unclear. Using a mouse model of hind limb ischemia with CSF-1 inhibitor studies and Dll1 heterozygous mice we show that CSF-1 is induced in the ischemic niche by a subpopulation of stromal cells expressing podoplanin, which was paralleled by the development of ischemic macrophages. Inhibition of CSF-1 signaling with small molecules or blocking antibodies impaired macrophage differentiation but prolonged the inflammatory response, resulting in impaired perfusion recovery and tissue regeneration. Yet, despite high levels of CSF-1, macrophage maturation and perfusion recovery were impaired in mice with Dll1 haploinsufficiency, while inflammation was exaggerated. In vitro, CSF-1 was not sufficient to induce full MF differentiation from donor monocytes in the absence of recombinant DLL1, while the presence of DLL1 in a dose-dependent manner stimulated MF differentiation in combination with CSF-1. Thus, CSF-1 is an ischemic niche factor that cooperates with Notch signaling in a non-redundant fashion to instruct macrophage cell fate and maturation, which is required for ischemic perfusion recovery and tissue repair.
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- 2023
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34. The aging kidney is characterized by tubuloinflammaging, a phenotype associated with MHC-II gene expression
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Julius Sinning, Nils David Funk, Inga Soerensen-Zender, Vera Christine Wulfmeyer, Chieh Ming Liao, Hermann Haller, Christian Hinze, Kai Martin Schmidt-Ott, Anette Melk, and Roland Schmitt
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aging kidney ,senescence ,tubular cell ,epithelial cell ,inflammation ,MHC-II ,Immunologic diseases. Allergy ,RC581-607 - Abstract
IntroductionEven during physiologic aging, the kidney experiences a loss of mass and a progressive functional decline. This is clinically relevant as it leads to an increased risk of acute and chronic kidney disease. The kidney tubular system plays an important role in the underlying aging process, but the involved cellular mechanisms remain largely elusive.MethodsKidneys of 3-, 12- and 24-month-old male C57BL/6J mice were used for RNA sequencing, histological examination, immunostaining and RNA-in-situ-hybridization. Single cell RNA sequencing data of differentially aged murine and human kidneys was analyzed to identify age-dependent expression patterns in tubular epithelial cells. Senescent and non-senescent primary tubular epithelial cells from mouse kidney were used for in vitro experiments.ResultsDuring normal kidney aging, tubular cells adopt an inflammatory phenotype, characterized by the expression of MHC class II related genes. In our analysis of bulk and single cell transcriptional data we found that subsets of tubular cells show an age-related expression of Cd74, H2-Eb1 and H2-Ab1 in mice and CD74, HLA-DQB1 and HLADRB1 in humans. Expression of MHC class II related genes was associated with a phenotype of tubular cell senescence, and the selective elimination of senescent cells reversed the phenotype. Exposure to the Cd74 ligand MIF promoted a prosenescent phenotype in tubular cell cultures.DiscussionTogether, these data suggest that during normal renal aging tubular cells activate a program of ‘tubuloinflammaging’, which might contribute to age-related phenotypical changes and to increased disease susceptibility.
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- 2023
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35. Aldosteronantagonisten „revisited“
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Swolinsky, Jutta and Schmidt-Ott, Kai
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- 2022
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36. Monitoring and Understanding VOC Induced Glass Corrosion Using Multi-modal Imaging Techniques
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Sharma, Deepshikha, primary, Rothenhaeusler, Ulrike, additional, Schmidt-Ott, Katharina, additional, Nurit, Marvin, additional, Cartagena, Yuly Castro, additional, Le-Goic, Gaetan, additional, Joseph, Edith, additional, George, Sony, additional, and Lombardo, Tiziana, additional
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- 2022
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37. Porphyromonas gingivalis Impairs Oral Epithelial Barrier through Targeting GRHL2
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Chen, W, Alshaikh, A, Kim, S, Kim, J, Chun, C, Mehrazarin, S, Lee, J, Lux, R, Kim, RH, Shin, KH, Park, NH, Walentin, K, Schmidt-Ott, KM, and Kang, MK
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Medical Physiology ,Biomedical and Clinical Sciences ,Dentistry ,Genetics ,Dental/Oral and Craniofacial Disease ,Rare Diseases ,Digestive Diseases ,2.1 Biological and endogenous factors ,Underpinning research ,1.1 Normal biological development and functioning ,Aetiology ,Animals ,Cells ,Cultured ,DNA-Binding Proteins ,Epithelial Cells ,Humans ,In Situ Hybridization ,Fluorescence ,Mice ,Mice ,Knockout ,Mouth Mucosa ,Porphyromonas gingivalis ,Tight Junctions ,Transcription Factors ,oral mucosa ,periodontal diseases ,tight junctions ,lipopolysaccharides ,cell adhesion ,gene knockout techniques - Abstract
Oral mucosa provides the first line of defense against a diverse array of environmental and microbial irritants by forming the barrier of epithelial cells interconnected by multiprotein tight junctions (TJ), adherens junctions, desmosomes, and gap junction complexes. Grainyhead-like 2 (GRHL2), an epithelial-specific transcription factor, may play a role in the formation of the mucosal epithelial barrier, as it regulates the expression of the junction proteins. The current study investigated the role of GRHL2 in the Porphyromonas gingivalis (Pg)-induced impairment of epithelial barrier functions. Exposure of human oral keratinocytes (HOK-16B and OKF6 cells) to Pg or Pg-derived lipopolysaccharides (Pg LPSs) led to rapid loss of endogenous GRHL2 and the junction proteins (e.g., zonula occludens, E-cadherin, claudins, and occludin). GRHL2 directly regulated the expression levels of the junction proteins and the epithelial permeability for small molecules (e.g., dextrans and Pg bacteria). To explore the functional role of GRHL2 in oral mucosal barrier, we used a Grhl2 conditional knockout (KO) mouse model, which allows for epithelial tissue-specific Grhl2 KO in an inducible manner. Grhl2 KO impaired the expression of the junction proteins at the junctional epithelium and increased the alveolar bone loss in the ligature-induced periodontitis model. Fluorescence in situ hybridization revealed increased epithelial penetration of oral bacteria in Grhl2 KO mice compared with the wild-type mice. Also, blood loadings of oral bacteria (e.g., Bacteroides, Bacillus, Firmicutes, β-proteobacteria, and Spirochetes) were significantly elevated in Grhl2 KO mice compared to the wild-type littermates. These data indicate that Pg bacteria may enhance paracellular penetration through oral mucosa in part by targeting the expression of GRHL2 in the oral epithelial cells, which then impairs the epithelial barrier by inhibition of junction protein expression, resulting in increased alveolar tissue destruction and systemic bacteremia.
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- 2019
38. Single-cell transcriptomics reveals common epithelial response patterns in human acute kidney injury
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Christian Hinze, Christine Kocks, Janna Leiz, Nikos Karaiskos, Anastasiya Boltengagen, Shuang Cao, Christopher Mark Skopnik, Jan Klocke, Jan-Hendrik Hardenberg, Helena Stockmann, Inka Gotthardt, Benedikt Obermayer, Laleh Haghverdi, Emanuel Wyler, Markus Landthaler, Sebastian Bachmann, Andreas C. Hocke, Victor Corman, Jonas Busch, Wolfgang Schneider, Nina Himmerkus, Markus Bleich, Kai-Uwe Eckardt, Philipp Enghard, Nikolaus Rajewsky, and Kai M. Schmidt-Ott
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Acute kidney injury ,Critical illness ,Single-cell sequencing ,Medicine ,Genetics ,QH426-470 - Abstract
Abstract Background Acute kidney injury (AKI) occurs frequently in critically ill patients and is associated with adverse outcomes. Cellular mechanisms underlying AKI and kidney cell responses to injury remain incompletely understood. Methods We performed single-nuclei transcriptomics, bulk transcriptomics, molecular imaging studies, and conventional histology on kidney tissues from 8 individuals with severe AKI (stage 2 or 3 according to Kidney Disease: Improving Global Outcomes (KDIGO) criteria). Specimens were obtained within 1–2 h after individuals had succumbed to critical illness associated with respiratory infections, with 4 of 8 individuals diagnosed with COVID-19. Control kidney tissues were obtained post-mortem or after nephrectomy from individuals without AKI. Results High-depth single cell-resolved gene expression data of human kidneys affected by AKI revealed enrichment of novel injury-associated cell states within the major cell types of the tubular epithelium, in particular in proximal tubules, thick ascending limbs, and distal convoluted tubules. Four distinct, hierarchically interconnected injured cell states were distinguishable and characterized by transcriptome patterns associated with oxidative stress, hypoxia, interferon response, and epithelial-to-mesenchymal transition, respectively. Transcriptome differences between individuals with AKI were driven primarily by the cell type-specific abundance of these four injury subtypes rather than by private molecular responses. AKI-associated changes in gene expression between individuals with and without COVID-19 were similar. Conclusions The study provides an extensive resource of the cell type-specific transcriptomic responses associated with critical illness-associated AKI in humans, highlighting recurrent disease-associated signatures and inter-individual heterogeneity. Personalized molecular disease assessment in human AKI may foster the development of tailored therapies.
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- 2022
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39. Urinary single-cell sequencing captures kidney injury and repair processes in human acute kidney injury
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Klocke, Jan, Kim, Seung Joon, Skopnik, Christopher M., Hinze, Christian, Boltengagen, Anastasiya, Metzke, Diana, Grothgar, Emil, Prskalo, Luka, Wagner, Leonie, Freund, Paul, Görlich, Nina, Muench, Frédéric, Schmidt-Ott, Kai M., Mashreghi, Mir-Farzin, Kocks, Christine, Eckardt, Kai-Uwe, Rajewsky, Nikolaus, and Enghard, Philipp
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- 2022
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40. Blood pressure dynamics during home blood pressure monitoring with a digital blood pressure coach—a prospective analysis of individual user data
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Christian Beger, Dominik Rüegger, Anna Lenz, Steffen Wagner, Herrmann Haller, Kai Martin Schmidt-Ott, Dirk Volland, and Florian P. Limbourg
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hypertension ,home blood pressure monitoring ,app ,eHealth ,blood pressure ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
IntroductionSelf-monitoring of blood pressure at home is a better predictor of prognosis and recommended in hypertension guidelines. However, the influence of baseline blood pressure category and measurement schedule on BP values during a period of home blood pressure monitoring (HBPM) are still poorly defined, particularly when used in conjunction with a digital application.MethodsWe analysed temporal BP changes and performed BP classification tracking in users with self-reported hypertension performing HBPM with a digital and interactive blood pressure coach.ResultsOf 3175 users who enrolled in HBPM, 74.1% completed the first measurement period. Overall, mean systolic BP dropped significantly after the first day, but stratification by BP category demonstrated that initial category influenced BP course. BP classification tracking revealed that time to reach final BP category was dependent on baseline category, with users in categories high normal and grade 1 hypertension requiring more days to decrease BP class volatility and to reach their definitive BP class. This was driven by an intense switching between directly neighbouring categories until the middle phase of the HBPM period, while more distant class switching occurred less often and only early on. Overall, >90% of users maintained their category by day 5. Omitting the first day from analysis lead to therapeutically relevant reclassification in 3.8% of users. Users who completed at least two HBPM periods (n = 864) showed a mean SBP/DBP decrease of 2.6/1.6 mmHg, which improved hypertension control from 55.6% to 68.1%.ConclusionThe optimal length of HBPM period depends on BP category. HBPM with a digital coach is associated with a reduction in average BP and improvement in BP control.
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- 2023
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41. Evolution and loss of ß-catenin and TCF-dependent axis specification in insects
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Schmidt-Ott, Urs and Yoon, Yoseop
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- 2022
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42. Insights into the enhancement of nanoparticle production throughput by atmospheric-pressure spark ablation.
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Loizidis, C., Petallidou, K. C., Maisser, A., Bezantakos, S., Pfeiffer, T. V., Schmidt-Ott, A., and Biskos, G.
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HEAT losses ,MANUFACTURING processes ,NANOPARTICLES ,MASS production ,ELECTRODES - Abstract
Spark ablation is a highly effective and versatile method for producing nanoparticles from bulk conductive electrode materials. For a number of applications, however, the production throughput of the process needs to be increased with respect to the current state of the art. Here we show that this can be achieved by decreasing the diameter of the employed bulk-material electrodes from ca. 12 to 0.15 mm, corroborating previous observations, and demonstrate that the throughput is associated with the ablation efficiency (i.e., the energy spent to produce nanoparticles per total input energy) that respectively increases by a factor of 10. It is also shown that the commonly used theory for predicting the mass of nanoparticles produced by spark ablation cannot capture this effect, and thus we extend it to account for heat losses that affect the process when electrode diameter reduces below ca. 2 mm. Through this exercise we also show that reduced heat losses associated with thinner electrodes provide an effective recipe to increase the ablation efficiency, also referred as the nanoparticle production yield. The new extended theory for estimating spark ablation nanoparticle mass production throughput is also accompanied by an empirical equation predicting its dependence on electrode diameter. [ABSTRACT FROM AUTHOR]
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- 2024
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43. Cardiac Surgery–Related Acute Kidney Injury _ Risk Factors, Clinical Course, Management Suggestions
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Just, Isabell A., Alborzi, Farnoush, Godde, Maren, Ott, Sascha, Meyer, Alexander, Stein, Julia, Mazgareanu, Stefan, van der Giet, Markus, Schmidt-Ott, Kai M., Falk, Volkmar, and Schoenrath, Felix
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- 2022
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44. Hypo- und Hypernatriämien auf der Intensivstation: Fallstricke des Volumenmanagements
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Schilling, Johannes, Compton, Friederike, and Schmidt-Ott, Kai
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- 2022
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45. Discordance between estimated and measured changes in plasma volume among patients with acute heart failure
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Jutta S. Swolinsky, Enkhtuvshin Tuvshinbat, David M. Leistner, Frank Edelmann, Fabian Knebel, Niklas P. Nerger, Caroline Lemke, Robert Roehle, Michael Haase, Maria Rosa Costanzo, Geraldine Rauch, Veselin Mitrovic, Edis Gasanin, Daniel Meier, Peter A. McCullough, Kai‐Uwe Eckardt, Bruce A. Molitoris, and Kai M. Schmidt‐Ott
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Acute heart failure ,Estimated plasma volume (ePV) ,Measured plasma volume (mPV) ,Strauss' formula ,Haematocrit ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Abstract Aims In acute heart failure (AHF), changes of venous haemoglobin (Hb) concentrations, haematocrit (Hct), and estimated plasma volume (ePV) have been proposed as surrogates of decongestion. These estimates are based on the theoretical assumptions that changes of Hb concentrations and Hct are driven by the intravascular volume status and that the intravascular Hb pool remains stable. The objective of this study was to assess the relationship of changes of measured plasma volume (mPV) with changes of Hb, Hct, and ePV in AHF. Methods and results We studied 36 AHF patients, who received two sequential assessments of mPV, measured red cell volume (mRCV) and measured total blood volume (mTBV) (48 h apart), during the course of diuretic therapy using a novel visible fluorescent injectate (VFI) technique based on the indicator dilution principle. Changes of ePV were calculated based on the Kaplan–Hakim or Strauss formula. AHF patients receiving diuretics (median intravenous furosemide equivalent 160 mg/48 h) displayed a wide range of changes of mPV (−25.4% to +37.0%). Changes in mPV were not significantly correlated with changes of Hb concentration [Pearson's r (r) = −0.241, P = 0.157], Hct (r = −0.307, P = 0.069), ePVKaplan–Hakim (r = 0.228, P = 0.182), or ePVStrauss (r = 0.237, P = 0.163). In contrast to theoretical assumptions, changes of mTBV were poorly correlated with changes of Hb concentrations and some patients displayed unanticipated variability of mRCV, suggesting an unstable intravascular red cell pool. Conclusions Changes of Hb or Hct were not reflective of directly measured changes of intravascular volume status in AHF patients. Basing clinical assessment of decongestion on changes of Hb or Hct may misguide clinical decision‐making on an individual patient level.
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- 2022
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46. Similar severity of influenza primary and re-infections in pre-school children requiring outpatient treatment due to febrile acute respiratory illness: prospective, multicentre surveillance study (2013–2015)
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Andrea Streng, Christiane Prifert, Benedikt Weissbrich, Andreas Sauerbrei, Andi Krumbholz, Ruprecht Schmidt-Ott, and Johannes G. Liese
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Influenza ,Children ,Disease severity ,IgG ,Immunology ,Infectious and parasitic diseases ,RC109-216 - Abstract
Abstract Background Influenza virus infections in immunologically naïve children (primary infection) may be more severe than in children with re-infections who are already immunologically primed. We compared frequency and severity of influenza virus primary and re-infections in pre-school children requiring outpatient treatment. Methods Influenza-unvaccinated children 1–5 years of age presenting at pediatric practices with febrile acute respiratory infection
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- 2022
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47. Zwischgold - The Secret Nanomaterial of Medieval Gilding
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Qing Wu, Karolina Soppa, Tiziana Lombardo, Katharina Schmidt-Ott, Frithjof Nolting, and Benjamin Watts
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Medieval gilding ,Nanotomography ,PXCT ,Zwischgold ,Chemistry ,QD1-999 - Published
- 2023
48. Exposure to airborne SARS-CoV-2 in four hospital wards and ICUs of Cyprus. A detailed study accounting for day-to-day operations and aerosol generating procedures
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Rafail Konatzii, Fabian Schmidt-Ott, Lakis Palazis, Panagiotis Stagianos, Maria Foka, Jan Richter, Christina Christodoulou, Jean Sciare, and Michael Pikridas
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Airborne SARS-CoV-2 fast detection ,Occupational health ,Aerosol generating procedures ,SARS-CoV-2 size distribution ,Science (General) ,Q1-390 ,Social sciences (General) ,H1-99 - Abstract
In any infectious disease, understanding the modes of transmission is key to selecting effective public health measures. In the case of COVID-19 spread, the strictness of the imposed measures outlined the lack of understanding on how SARS-CoV-2 transmits, particularly via airborne pathways. With the aim to characterize the transmission dynamics of airborne SARS-CoV-2, 165 and 62 air and environmental samples, respectively, were collected in four COVID-19 wards and ICUs in Cyprus and analyzed by RT-PCR. An alternative method for SARS-CoV-2 detection in air that provides comparable results but is less cumbersome and time demanding, is also proposed. Considering that all clinics employed 14 regenerations per hour of full fresh air inside patient rooms, it was hypothesized that the viral levels and the frequency of positive samples would be minimum outside of the rooms. However, it is shown that leaving the door opened in patient rooms hinders the efficiency of the ventilation system applied, allowing the virus to escape. As a result, the highest observed viral levels (135 copies m−3) were observed in the corridor of a ward and the frequency of positive samples in the same area was comparable to that inside a two-bed cohort. SARS-CoV-2 in that corridor was found primarily to lie in the coarse mode, at sizes between 1.8 and 10 μm. Similar to previous studies, the frequency of positive samples and viral levels were the lowest inside intensive care units. However, if a patient with sufficient viral load (Ct-value 31) underwent aerosol generating procedures, positive samples with viral levels below 45 copies m−3 were acquired within a 2 m distance of the patient. Our results suggest that a robust ventilation system can prevent unnecessary exposure to SARS-CoV-2 but with limitations related to foot traffic or the operations taking place at the time.
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- 2023
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49. Twenty-seven ZAD-ZNF genes of Drosophila melanogaster are orthologous to the embryo polarity determining mosquito gene cucoid.
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Muzi Li, Koray Kasan, Zinnia Saha, Yoseop Yoon, and Urs Schmidt-Ott
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Medicine ,Science - Abstract
The C2H2 zinc finger gene cucoid establishes anterior-posterior (AP) polarity in the early embryo of culicine mosquitoes. This gene is unrelated to genes that establish embryo polarity in other fly species (Diptera), such as the homeobox gene bicoid, which serves this function in the traditional model organism Drosophila melanogaster. The cucoid gene is a conserved single copy gene across lower dipterans but nothing is known about its function in other species, and its evolution in higher dipterans, including Drosophila, is unresolved. We found that cucoid is a member of the ZAD-containing C2H2 zinc finger (ZAD-ZNF) gene family and is orthologous to 27 of the 91 members of this family in D. melanogaster, including M1BP, ranshi, ouib, nom, zaf1, odj, Nnk, trem, Zif, and eighteen uncharacterized genes. Available knowledge of the functions of cucoid orthologs in Drosophila melanogaster suggest that the progenitor of this lineage specific expansion may have played a role in regulating chromatin. We also describe many aspects of the gene duplication history of cucoid in the brachyceran lineage of D. melanogaster, thereby providing a framework for predicting potential redundancies among these genes in D. melanogaster.
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- 2023
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50. Human Papillomavirus 16 E6 Induces FoxM1B in Oral Keratinocytes through GRHL2
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Chen, W, Shimane, T, Kawano, S, Alshaikh, A, Kim, SY, Chung, SH, Kim, RH, Shin, KH, Walentin, K, Park, NH, Schmidt-Ott, KM, and Kang, MK
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Genetics ,Cancer ,Dental/Oral and Craniofacial Disease ,Infectious Diseases ,Digestive Diseases ,Biotechnology ,Sexually Transmitted Infections ,Aetiology ,2.1 Biological and endogenous factors ,Animals ,Blotting ,Western ,Carcinogenesis ,Cell Line ,Tumor ,DNA-Binding Proteins ,Disease Models ,Animal ,Epithelial Cells ,Forkhead Box Protein M1 ,Gene Knockout Techniques ,Humans ,Immunohistochemistry ,Keratinocytes ,Oncogene Proteins ,Viral ,Oropharyngeal Neoplasms ,Palatine Tonsil ,Papillomavirus Infections ,Polymerase Chain Reaction ,Repressor Proteins ,Transcription Factors ,Tumor Cells ,Cultured ,carcinogenesis ,oncogenes ,oropharyngeal neoplasms ,tongue ,epithelial cells ,gene knockout technique ,Dentistry - Abstract
High-risk human papillomavirus (HPV) is a major risk factor for oral and pharyngeal cancers (OPCs), yet the detailed mechanisms by which HPV promotes OPCs are not understood. Forkhead box M1B (FoxM1B) is an oncogene essential for cell cycle progression and tumorigenesis, and it is aberrantly overexpressed in many tumors. We previously showed that FoxM1B was the putative target of an epithelial-specific transcription factor, Grainyhead-like 2 (GRHL2). In the current study, we demonstrate that HPV type 16 (HPV-16) E6 induces FoxM1B in human oral keratinocytes (HOKs) and tonsillar epithelial cells (TECs) in part through GRHL2. FoxM1B was barely detectable in cultured normal human oral keratinocytes (NHOKs) and progressively increased in immortalized HOKs harboring HPV-16 genome (HOK-16B) and tumorigenic HOK-16B/BaP-T cells. Retroviral expression of HPV-16 E6 and/or E7 in NHOKs, TECs, and hypopharyngeal carcinoma cells (FaDu) revealed induction of FoxM1B and GRHL2 by the E6 protein but not E7. Both GRHL2 and FoxM1B were strongly induced in the epidermis of HPV-16 E6 transgenic mice and HPV+ oral squamous cell carcinomas. Ectopic expression of FoxM1B led to acquisition of transformed phenotype in HOK-16B cells. Loss of FoxM1B by lentiviral short hairpin RNA vector or chemical inhibitor led to elimination of tumorigenic characteristics of HOK-16B/BaP-T cells. Luciferase reporter assay revealed that GRHL2 directly bound and regulated the FoxM1B gene promoter activity. Using epithelial-specific Grhl2 conditional knockout mice, we exposed wild-type (WT) and Grhl2 KO mice to 4-nitroquinolin 1-oxide (4-NQO), which led to induction of FoxM1B in the tongue tissues and rampant oral tumor development in the WT mice. However, 4-NQO exposure failed to induce tongue tumors or induction of FoxM1B expression in Grhl2 KO mice. Collectively, these results indicate that HPV-16 induces FoxM1B in part through GRHL2 transcriptional activity and that elevated FoxM1B level is required for oropharyngeal cancer development.
- Published
- 2018
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