18,922 results on '"A. Bollen"'
Search Results
202. ChatGPT: five priorities for research
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van Dis, Eva A. M., Bollen, Johan, Zuidema, Willem , van Rooij, Robert, and Bockting, Claudi L.
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- 2023
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203. Including uncertainties in harmonic hosting capacity calculation of a fast EV charging station utilizing Bayesian statistics and harmonic correlation
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Nakhodchi, Naser, Bakhtiari, Hamed, Bollen, Math H.J., and Rönnberg, Sarah K.
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- 2023
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204. Deep learning for power quality
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Oliveira, Roger Alves de and Bollen, Math H.J.
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- 2023
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205. A retrospective cohort study comparing differences in 30-day mortality among critically ill patients aged ≥ 70 years treated in European tax-based healthcare systems (THS) versus social health insurance systems
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Bernhard Wernly, Hans Flaatten, Michael Beil, Jesper Fjølner, Raphael Romano Bruno, Antonio Artigas, Bernardo Bollen Pinto, Joerg C. Schefold, Malte Kelm, Sviri Sigal, Peter Vernon van Heerden, Wojciech Szczeklik, Muhammed Elhadi, Michael Joannidis, Richard Rezar, Sandra Oeyen, Georg Wolff, Brian Marsh, Finn H. Andersen, Rui Moreno, Sarah Wernly, Susannah Leaver, Ariane Boumendil, Dylan W. De Lange, Bertrand Guidet, Stefan Perings, and Christian Jung
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Medicine ,Science - Abstract
Abstract In Europe, tax-based healthcare systems (THS) and social health insurance systems (SHI) coexist. We examined differences in 30-day mortality among critically ill patients aged ≥ 70 years treated in intensive care units in a THS or SHI. Retrospective cohort study. 2406 (THS n = 886; SHI n = 1520) critically ill ≥ 70 years patients in 129 ICUs. Generalized estimation equations with robust standard errors were chosen to create population average adjusted odds ratios (aOR). Data were adjusted for patient-specific variables, organ support and health economic data. The primary outcome was 30-day-mortality. Numerical differences between SHI and THS in SOFA scores (6 ± 3 vs. 5 ± 3; p = 0.002) were observed, but clinical frailty scores were similar (> 4; 17% vs. 14%; p = 0.09). Higher rates of renal replacement therapy (18% vs. 11%; p
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- 2022
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206. Home-based intensive treatment of chronic radiation-associated dysphagia in head and neck cancer survivors (HIT-CRAD trial)
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Hanne Massonet, Ann Goeleven, Leen Van den Steen, Alice Vergauwen, Margot Baudelet, Gilles Van Haesendonck, Olivier Vanderveken, Heleen Bollen, Lisette van der Molen, Fréderic Duprez, Peter Tomassen, Sandra Nuyts, and Gwen Van Nuffelen
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Dysphagia ,Head and neck cancer ,Chemoradiotherapy ,Swallowing exercises ,Tongue strengthening exercises ,Expiratory Muscle Strength Training (EMST) ,Medicine (General) ,R5-920 - Abstract
Abstract Background Chronic radiation-associated dysphagia (C-RAD) is considered to be one of the most severe functional impairments in head and neck cancer survivors treated with radiation (RT) or chemoradiation (CRT). Given the major impact of these late toxicities on patients’ health and quality of life, there is a strong need for evidence-based dysphagia management. Although studies report the benefit of strengthening exercises, transference of changes in muscle strength to changes in swallowing function often remains limited. Therefore, combining isolated strengthening exercises with functional training in patients with C-RAD may lead to greater functional gains. Methods This 3-arm multicenter randomized trial aims to compare the efficacy and possible detraining effects of mere strengthening exercises (group 1) with a combination of strengthening exercises and functional swallowing therapy (group 2) and non-invasive brain stimulation added to that combination (group 3) in 105 patients with C-RAD. Patients will be evaluated before and during therapy and 4 weeks after the last therapy session by means of swallowing-related and strength measures and quality of life questionnaires. Discussion Overall, this innovative RCT is expected to provide new insights into the rehabilitation of C-RAD to optimize post-treatment swallowing function. Trial registration International Standard Randomized Controlled Trials Number (ISRCTN) registry ID ISRCTN57028065. Registration was accepted on 15 July 2021.
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- 2022
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207. Graphical Ways to Visualize Operational Risk Results for Transmission System Contingencies
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Zunaira Nazir and Math H. J. Bollen
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contingencies ,contingency contribution ,operational risk assessment ,operational security ,power system planning ,power system security ,Electricity ,QC501-721 - Abstract
The increased complexity of the transmission grid can endanger the operational security of the grid. Operational risk assessment, a stochastic tool, helps to enhance security. Contingency analysis and its impact quantification are the main constituents of operational risk assessment. In this study, different graphical methods are proposed to visualize operational risk contingency-based detailed results: heat-map and risk-based contingency chart. Through the heat-map, the system operator can determine which contingencies contribute most to the operational risk and would therefore be the most threatening contingencies for operational security of the grid. The “risk-based contingency chart” allows the system operator to analyze contingency cases from the probability and impact aspect in one chart. Both tools may be used in the control room for improved operational planning. In this study of contingency analysis and various types of network studies of severity factor quantification, the IEEE 39-Bus sample network is used in Power-Factory to analyze the contingencies behavior under different operational scenarios.
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- 2022
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208. Quantifying collective identity online from self-defining hashtags
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Alexander T. J. Barron and Johan Bollen
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Medicine ,Science - Abstract
Abstract Mass communication over social media can drive rapid changes in our sense of collective identity. Hashtags in particular have acted as powerful social coordinators, playing a key role in organizing social movements like the Gezi park protests, Occupy Wall Street, #metoo, and #blacklivesmatter. Here we quantify collective identity from the use of hashtags as self-labels in over 85,000 actively-maintained Twitter user profiles spanning 2017–2019. Collective identities emerge from a graph model of individuals’ overlapping self-labels, producing a hierarchy of graph clusters. Each cluster is bound together and characterized semantically by specific hashtags key to its formation. We define and apply two information-theoretic measures to quantify the strength of identities in the hierarchy. First we measure collective identity coherence to determine how integrated any identity is from local to global scales. Second, we consider the conspicuousness of any identity given its vocabulary versus the global identity map. Our work reveals a rich landscape of online identity emerging from the hierarchical alignment of uncoordinated self-labeling actions.
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- 2022
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209. REPLY TO SCHMIDT ET AL. : A robust surge of cognitive distortions in historical language
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Bollen, Johan, Thij, Marijn ten, Breithaupt, Fritz, Barron, Alexander T. J., Rutter, Lauren A., Lorenzo-Luaces, Lorenzo, and Scheffer, Marten
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- 2021
210. Bioanalytical method validation and application to a phase 1, double-blind, randomized pharmacokinetic trial of a standardized Centella asiatica (L.) Urban water extract product in healthy older adults
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Kirsten M. Wright, Melissa Bollen, Jason David, Bridgette Mepham, Armando Alcázar Magaña, Christine McClure, Claudia S. Maier, Joseph F. Quinn, and Amala Soumyanath
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Centella asiatica ,pharmacokinetics ,validation ,pharmacodynamics ,Alzheimer’s disease ,caffeoylquinic acid ,Therapeutics. Pharmacology ,RM1-950 - Abstract
Introduction:Centella asiatica is an herbaceous plant reputed in Eastern medicine to improve memory. Preclinical studies have shown that C. asiatica aqueous extract (CAW) improves neuronal health, reduces oxidative stress, and positively impacts learning and cognition. This study aimed to develop and validate bioanalytical methods for detecting known bioactive compounds from C. asiatica in human biological matrices and apply them to a human pharmacokinetic trial in healthy older adults.Methods: High performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS) was used for detecting triterpenes and caffeoylquinic acids from C. asiatica, or their metabolites, in human plasma and urine. Validation parameters including linearity, precision, accuracy, recovery and thermal stability were evaluated. The method was applied to a Phase I, randomized, double-blind, crossover trial of two doses (2 or 4 g) of a standardized C. asiatica water extract product (CAP) in eight healthy older adults. Pharmacokinetic parameters were measured over a 12-h post administration period and acute safety was assessed.Results: The method satisfied US Food & Drug Administration criteria for linearity and recovery of the analytes of interest in human plasma and urine. The method also satisfied criteria for precision and accuracy at medium and high concentrations. Single administration of 2 and 4 g of CAP was well tolerated and safe in healthy older adults. The parent triterpene glycosides, asiaticoside and madecassoside, were not detected in plasma and in minimal amounts in urinary excretion analyses, while the aglycones, asiatic acid and madecassic acid, showed readily detectable pharmacokinetic profiles. Similarly, the di-caffeoylquinic acids and mono-caffeoylquinic acids were detected in low quantities, while their putative metabolites showed readily detectable pharmacokinetic profiles and urinary excretion.Discussion: This method was able to identify and calculate the concentration of triterpenes and caffeoylquinic acids from C. asiatica, or their metabolites, in human plasma and urine. The oral absorption of these key compounds from CAP, and its acute safety in healthy older adults, support the use of this C. asiatica product in future clinical trials.
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- 2023
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211. Characterization of the genetic composition and establishment of a core collection for the INERA Robusta coffee (Coffea canephora) field genebank from the Democratic Republic of Congo
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Lauren Verleysen, Robrecht Bollen, Jean-Léon Kambale, Tshimi Ebele, Benjamin Ntumba Katshela, Jonas Depecker, Valérie Poncet, Dieu-Merci Assumani, Filip Vandelook, Piet Stoffelen, Olivier Honnay, and Tom Ruttink
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Coffea canephora ,HiPlex amplicon sequencing ,genetic structure ,core collection ,ex-situ conservation ,crop wild relatives ,Nutrition. Foods and food supply ,TX341-641 ,Food processing and manufacture ,TP368-456 - Abstract
Cultivation of Robusta coffee is likely to gain importance because of its high disease resistance and climate envelope. Robusta coffee genetic resources conserved in field genebanks can play an important role to further improve its cupping quality and other agronomic traits, but such Coffea canephora collections are limited and still poorly characterized. In this study, we characterized the genetic composition of the historically important but until recently neglected INERA Coffee Collection in Yangambi (the Democratic Republic of Congo). We used GBS to discover genome-wide genetic diversity, created and validated a novel multiplex amplicon sequencing (HiPlex) screening assay to genetically screen 730 coffee shrubs of the Yangambi Coffee Collection, grouped clonal material and delineated 263 accessions with unique genetic fingerprints. Comparison to reference material of three genetic origins revealed that the majority of the Yangambi accessions were assigned a ‘Lula’ cultivar origin, four accessions were assigned to Congolese subgroup A and nine accessions were most closely related to local wild accessions. About one-quarter of the accessions was likely derived from hybridization between these groups, which could result from seed-based propagation of the collection, breeding efforts, or natural cross-pollination. Parental analyses discovered eight preferentially used accessions, which may correspond to historically selected founders, or direct descendants thereof, whose seed material was once widely used to establish coffee plantations. Finally, two core collections were proposed using the maximization strategy (CC-I; 100 accessions) and genetic distance method (CC-X; 10 accessions). Our study demonstrates a method for the genetic characterization of Robusta coffee collections in general and contributes to the re-evaluation and exploration of the Robusta coffee genetic resources in the Democratic Republic of the Congo in particular.
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- 2023
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212. The REtirement in ACTion exercise programme and its effects on elements of long term functionality in older adults
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Peter Ladlow, Max J. Western, Colin J. Greaves, Janice L. Thompson, Janet Withall, Jolanthe de Koning, Jessica C. Bollen, Sarah J. Moorlock, Jack M. Guralnik, Kenneth R. Fox, and Afroditi Stathi
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ageing ,mobility disability ,physical activity ,community ,strength ,balance ,Public aspects of medicine ,RA1-1270 - Abstract
BackgroundThe prevention of mobility-related disability amongst adults is a global healthcare priority. Cost-effective community-based strategies to improve physical function and independence in older adults with mobility limitations are needed. This study investigated the effectiveness of the REtirement in ACTion (REACT) exercise intervention on individual markers of physical function at 6-and 12-months.MethodsThe REACT multicentre randomised controlled trial assigned 777 older adults (female, 514; male 263) (mean age 77·6 [SD 6·8] years) with reduced lower limb physical functioning (Short Physical Performance Battery [SPPB] score 4–9) to receive brief healthy ageing advice or a 12-month, group-based, multimodal exercise programme delivered in local communities. Estimated differences in the three individual component scores of the SPPB (strength, balance, gait speed) and physical functional outcomes recorded at 6- and 12-months were assessed.ResultsThe intervention group demonstrated significant improvements in strength (OR = 1.88, 95% CI = 1.36–2.59, p
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- 2023
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213. Prognostic factors for multi-organ dysfunction in pediatric oncology patients admitted to the pediatric intensive care unit
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Marijn Soeteman, Marta F. Fiocco, Joppe Nijman, Casper W. Bollen, Maartje M. Marcelis, Ellen Kilsdonk, Edward E. S. Nieuwenhuis, Teus H. Kappen, Wim J. E. Tissing, and Roelie M. Wösten-van Asperen
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pediatric oncology ,intensive care unit ,multi-organ dysfunction ,critical care ,prognosis ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
BackgroundPediatric oncology patients who require admission to the pediatric intensive care unit (PICU) have worse outcomes compared to their non-cancer peers. Although multi-organ dysfunction (MOD) plays a pivotal role in PICU mortality and morbidity, risk factors for MOD have not yet been identified. We aimed to identify risk factors at PICU admission for new or progressive MOD (NPMOD) during the first week of PICU stay.MethodsThis retrospective cohort study included all pediatric oncology patients aged 0 to 18 years admitted to the PICU between June 2018 and June 2021. We used the recently published PODIUM criteria for defining multi-organ dysfunction and estimated the association between covariates at PICU baseline and the outcome NPMOD using a multivariable logistic regression model, with PICU admission as unit of study. To study the predictive performance, the model was internally validated by using bootstrap.ResultsA total of 761 PICU admissions of 571 patients were included. NPMOD was present in 154 PICU admissions (20%). Patients with NPMOD had a high mortality compared to patients without NPMOD, 14% and 1.0% respectively. Hemato-oncological diagnosis, number of failing organs and unplanned admission were independent risk factors for NPMOD. The prognostic model had an overall good discrimination and calibration.ConclusionThe risk factors at PICU admission for NPMOD may help to identify patients who may benefit from closer monitoring and early interventions. When applying the PODIUM criteria, we found some opportunities for fine-tuning these criteria for pediatric oncology patients, that need to be validated in future studies.
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- 2023
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214. Misinformation and Public Health Messaging in the Early Stages of the Mpox Outbreak: Mapping the Twitter Narrative With Deep Learning
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Andy Edinger, Danny Valdez, Eric Walsh-Buhi, Jennifer S Trueblood, Lorenzo Lorenzo-Luaces, Lauren A Rutter, and Johan Bollen
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Computer applications to medicine. Medical informatics ,R858-859.7 ,Public aspects of medicine ,RA1-1270 - Abstract
BackgroundShortly after the worst of the COVID-19 pandemic, an outbreak of mpox introduced another critical public health emergency. Like the COVID-19 pandemic, the mpox outbreak was characterized by a rising prevalence of public health misinformation on social media, through which many US adults receive and engage with news. Digital misinformation continues to challenge the efforts of public health officials in providing accurate and timely information to the public. We examine the evolving topic distributions of social media narratives during the mpox outbreak to map the tension between rapidly diffusing misinformation and public health communication. ObjectiveThis study aims to observe topical themes occurring in a large-scale collection of tweets about mpox using deep learning. MethodsWe leveraged a data set comprised of all mpox-related tweets that were posted between May 7, 2022, and July 23, 2022. We then applied Sentence Bidirectional Encoder Representations From Transformers (S-BERT) to the content of each tweet to generate a representation of its content in high-dimensional vector space, where semantically similar tweets will be located closely together. We projected the set of tweet embeddings to a 2D map by applying principal component analysis and Uniform Manifold Approximation Projection (UMAP). Finally, we group these data points into 7 topical clusters using k-means clustering and analyze each cluster to determine its dominant topics. We analyze the prevalence of each cluster over time to evaluate longitudinal thematic changes. ResultsOur deep-learning pipeline revealed 7 distinct clusters of content: (1) cynicism, (2) exasperation, (3) COVID-19, (4) men who have sex with men, (5) case reports, (6) vaccination, and (7) World Health Organization (WHO). Clusters that largely communicated erroneous or irrelevant information began earlier and grew faster, reaching a wider audience than later communications by official instances and health officials. ConclusionsWithin a few weeks of the first reported mpox cases, an avalanche of mostly false, misleading, irrelevant, or damaging information started to circulate on social media. Official institutions, including the WHO, acted promptly, providing case reports and accurate information within weeks, but were overshadowed by rapidly spreading social media chatter. Our results point to the need for real-time monitoring of social media content to optimize responses to public health emergencies.
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- 2023
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215. spread.gl: visualising pathogen dispersal in a high-performance browser application
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Li, Yimin, primary, Bollen, Nena, additional, Hong, Samuel Leandro, additional, Brusselmans, Marius, additional, Gambaro, Fabiana, additional, Suchard, Marc A., additional, Rambaut, Andrew, additional, Lemey, Philippe, additional, Dellicour, Simon, additional, and Baele, Guy, additional
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- 2024
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216. A simplified static frequency converter model for electromechanical transient stability studies of 16$\frac{2}{3}$ Hz railways
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Laury, John, Abrahamsson, Lars, and Bollen, Math H. J
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Electrical Engineering and Systems Science - Signal Processing - Abstract
With increased share of Static Frequency Converters (SFCs) in 16$\frac{2}{3}$ Hz railway grids concerns about stability have increased. Stability studies for such low-frequency railway grids are few, and models that describe SFC dynamics are especially few. This paper presents an open SFC model for electromechanical stability studies in the phasor domain, suited for 16$\frac{2}{3}$ Hz synchronous railway grids. The developed and proposed SFC model is implemented in MatLab Simulink, together with grid and loads. Numerical studies are made, in which the proposed SFC model is validated against both measured RMS-phasor amplitude of voltage and current at the railway grid side of an SFC. The SFC model developed is able to reproduce the measured RMS voltage and current with an acceptable accuracy.
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- 2018
217. A rotary frequency converter model for electromechanical transient studies of 16$\frac{2}{3}$ Hz railway systems
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Laury, John, Abrahamsson, Lars, and Bollen, Math H. J
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Electrical Engineering and Systems Science - Signal Processing - Abstract
Railway power systems operating at a nominal frequency below the frequency of the public grid (50 or 60 Hz) are special in many senses. One is that they exist in a just few countries around the world. However, for these countries such low frequency railways are a critical part of their infrastructure. The number of published dynamic models as well as stability studies regarding low frequency railways is small, compared to corresponding publications regarding 50 Hz/60 Hz public grids. Since there are two main type of low frequency railways; synchronous and asynchronous, it makes the number of available useful publications even smaller. One important reason for this is the small share of such grids on a global scale, resulting in less research and development man hours spent on low frequency grids. This work presents an open model of a (synchronous-synchronous) rotary frequency converter for electromechanical stability studies in the phasor domain, based on established synchronous machine models. The proposed model is designed such that it can be used with the available data for a rotary frequency converter. The behaviour of the model is shown through numerical electromechanical transient stability simulations of two example cases, where a fault is cleared, and the subsequent oscillations are shown. The first example is a single-fed catenary section and the second is doubly-fed catenary section.
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- 2018
218. Optimal Instrument Selection using Bayesian Model Averaging for Model Implied Instrumental Variable Two Stage Least Squares Estimators
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Henry, Teague R., Fisher, Zachary F., and Bollen, Kenneth A.
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Statistics - Methodology - Abstract
Model-Implied Instrumental Variable Two-Stage Least Squares (MIIV-2SLS) is a limited information, equation-by-equation, non-iterative estimator for latent variable models. Associated with this estimator are equation specific tests of model misspecification. One issue with equation specific tests is that they lack specificity, in that they indicate that some instruments are problematic without revealing which specific ones. Instruments that are poor predictors of their target variables (weak instruments) is a second potential problem. We propose a novel extension to detect instrument specific tests of misspecification and weak instruments. We term this the Model-Implied Instrumental Variable Two-Stage Bayesian Model Averaging (MIIV-2SBMA) estimator. We evaluate the performance of MIIV-2SBMA against MIIV-2SLS in a simulation study and show that it has comparable performance in terms of parameter estimation. Additionally, our instrument specific overidentification tests developed within the MIIV-2SBMA framework show increased power to detect specific problematic and weak instruments. Finally, we demonstrate MIIV-2SBMA using an empirical example., Comment: 31 pages, 8 figures
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- 2018
219. Does putting your emotions into words make you feel better? Measuring the minute-scale dynamics of emotions from online data
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Fan, Rui, Varamesh, Ali, Varol, Onur, Barron, Alexander, van de Leemput, Ingrid, Scheffer, Marten, and Bollen, Johan
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Computer Science - Social and Information Networks - Abstract
Studies of affect labeling, i.e. putting your feelings into words, indicate that it can attenuate positive and negative emotions. Here we track the evolution of individual emotions for tens of thousands of Twitter users by analyzing the emotional content of their tweets before and after they explicitly report having a strong emotion. Our results reveal how emotions and their expression evolve at the temporal resolution of one minute. While the expression of positive emotions is preceded by a short but steep increase in positive valence and followed by short decay to normal levels, negative emotions build up more slowly, followed by a sharp reversal to previous levels, matching earlier findings of the attenuating effects of affect labeling. We estimate that positive and negative emotions last approximately 1.25 and 1.5 hours from onset to evanescence. A separate analysis for male and female subjects is suggestive of possible gender-specific differences in emotional dynamics.
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- 2018
220. Anxiety sensitivity as a transdiagnostic risk factor for trajectories of adverse posttraumatic neuropsychiatric sequelae in the AURORA study
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Short, Nicole A., van Rooij, Sanne J.H., Murty, Vishnu P., Stevens, Jennifer S., An, Xinming, Ji, Yinyao, McLean, Samuel A., House, Stacey L., Beaudoin, Francesca L., Zeng, Donglin, Neylan, Thomas C., Clifford, Gari D., Linnstaedt, Sarah D., Germine, Laura T., Bollen, Kenneth A., Rauch, Scott L., Haran, John P., Lewandowski, Christopher, Musey, Paul I., Jr., Hendry, Phyllis L., Sheikh, Sophia, Jones, Christopher W., Punches, Brittany E., Swor, Robert A., McGrath, Meghan E., Hudak, Lauren A., Pascual, Jose L., Seamon, Mark J., Datner, Elizabeth M., Pearson, Claire, Peak, David A., Merchant, Roland C., Domeier, Robert M., Rathlev, Niels K., O'Neil, Brian J., Sergot, Paulina, Sanchez, Leon D., Bruce, Steven E., Pietrzak, Robert H., Joormann, Jutta, Barch, Deanna M., Pizzagalli, Diego A., Sheridan, John F., Smoller, Jordan W., Harte, Steven E., Elliott, James M., Kessler, Ronald C., Koenen, Karestan C., and Jovanovic, Tanja
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- 2022
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221. Voltage-sag source detection: Developing supervised methods and proposing a new unsupervised learning
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Mohammadi, Younes, Miraftabzadeh, Seyed Mahdi, Bollen, Math H.J., and Longo, Michela
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- 2022
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222. Seeking patterns in rms voltage variations at the sub-10-minute scale from multiple locations via unsupervised learning and patterns' post-processing
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Mohammadi, Younes, Mahdi Miraftabzadeh, Seyed, Bollen, Math H.J., and Longo, Michela
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- 2022
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223. Efficacy, safety, and immunogenicity of a booster regimen of Ad26.COV2.S vaccine against COVID-19 (ENSEMBLE2): results of a randomised, double-blind, placebo-controlled, phase 3 trial
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Garibaldi, Brian T., Albertson, Timothy E., Sandrock, Christian, Lee, Janet S., Looney, Mark R., Tapson, Victor F., Wiysonge, Charles Shey, Velarde, Luis Humberto Anaya, Backenroth, Daniel, Bhushanan, Jisha, Brandenburg, Börries, Cárdenas, Vicky, Chen, Bohang, Chen, Fei, Chetty, Polan, Chu, Pei-Ling, Cooper, Kimberly, Custers, Jerome, Delanghe, Hilde, Duca, Anna, Henrick, Tracy, Juraszek, Jarek, Nalpas, Catherine, Peeters, Monika, Pinheiro, Jose, Roels, Sanne, Ryser, Martin F., Salas, Jose, Santoro Matias, Samantha, Scheys, Ilse, Shetty, Pallavi, Shukarev, Georgi, Stoddard, Jeffrey, Talloen, Willem, Tran, NamPhuong, Vaissiere, Nathalie, van Son-Palmen, Elisabeth, Xu, Jiajun, Goecker, Erin A., Greninger, Alexander L., Jerome, Keith R., Roychoudhury, Pavitra, Takuva, Simbarashe G., Accini Mendoza, Jose Luis, Achtyes, Eric, Ahsan, Habibul, Alhatemi, Azhar, Allen, Nancy, Arribas, Jose R., Bahrami, Ghazaleh, Bailon, Lucia, Bajwa, Ali, Baker, Jonathan, Baron, Mira, Benet, Susana, Berdaï, Driss, Berger, Patrick, Bertoch, Todd, Bethune, Claire, Bevilacqua, Sybille, Biagioni Santos, Maria Silvia, Binnian, Ian, Bisnauthsing, Karen, Boivin, Jean-Marc, Bollen, Hilde, Bonnet, Sandrine, Borobia, Alberto M., Botelho-Nevers, Elisabeth, Bright, Phil, Britten, Vianne, Brown, Claire, Buadi, Amanda, Buntinx, Erik, Burgess, Lesley, Bush, Larry, Capeding, Maria Rosario, Carr, Quito Osuna, Carrasco Mas, Amparo, Catala, Hélène, Cathie, Katrina, Caudill, T. Shawn, Cereto Castro, Fernando, Chau, Kénora, Chavoustie, Steven, Chowdhury, Marie, Chronos, Nicolas, Cicconi, Paola, Cifuentes, Liliana, Cobo, Sara Maria, Collins, Helen, Colton, Hayley, Cuaño, Carlos Rolando G., D'Onofrio, Valentino, Dargan, Paul, Darton, Thomas, Deane, Peter, Del Pozo, Jose Luis, Derdelinckx, Inge, Desai, Amisha, Dever, Michael, Díaz-Pollán, Beatriz, DiBuono, Mark, Doust, Matthew, Duncan, Christopher, Echave-Sustaeta, Jose Maria, Eder, Frank, Ellis, Kimberly, Elzi, Stanton, Emmett, Stevan, Engelbrecht, Johannes, Evans, Mim, Farah, Theo, Felton, Timothy, Ferreira, João Pedro, Floutier, Catherine, Flume, Patrick, Ford, Stacy, Fragoso, Veronica, Freedman, Andrew, Frentiu, Emilia, Galloway, Christopher, Galtier, Florence, Garcia Diaz, Julia, García García, Irene, Garcia, Alcaide, Gardener, Zoe, Gauteul, Pascale, Geller, Steven, Gibson, Andrew, Gillet, Claudia, Girerd, Nicolas, Girodet, Pierre-Olivier, Gler, Maria Tarcela, Glover, Richard, Go, Herschel Don D., Gokani, Karishma, Gonthier, Damien, Green, Christopher, Greenberg, Richard, Griffin, Carl, Grobbelaar, Coert, Guancia, Adonis, Hakkarainen, Gloria, Harris, James, Hassman, Michael, Heimer, Deirdre, Hellstrom-Louw, Elizabeth, Herades, Yoan, Holroyd, Christopher, Hussen, Nazreen, Isidro, Marie Grace Dawn, Jackson, Yvonne, Jain, Manish, João Filho, Esaú Custódio, Johnson, Daniel, Jones, Ben, Joseph, Natasha, Jumeras, Analyn, Junquera, Patricia, Kellett-Wright, Johanna, Kennedy, Patrick, Kilgore, Paul E., Kim, Kenneth, Kimmel, Murray, Konis, George, Kutner, Mark, Lacombe, Karine, Launay, Odile, Lazarus, Rajeka, Lederman, Samuel, Lefebvre, Gigi, Lennon Collins, Katrina, Leroux-Roels, Isabel, Lim, Kenneth Wilson O., Lins, Muriel, Liu, Edward, Llewelyn, Martin, Mahomed, Akbar, Maia, Bernardo Porto, Marín-Candon, Alícia, Martínez-Gómez, Xavier, Martinot, Jean Benoit, Mazzella, Andrea, McCaughan, Frank, McCormack, Louise, McGettigan, John, Mehra, Purvi, Mejeur, Rhonda, Miller, Vicki, Mills, Anthony, Molto Marhuenda, Jose, Moodley, Prebashan, Mora-Rillo, Marta, Mothe, Beatriz, Mullan, Daniel, Munro, Alasdair, Myers, Paul, Nell, Jeremy, Newman Lobato Souza, Tamara, O'Halloran, Jane A., Ochoa Mazarro, Maria Dolores, Oliver, Abigail, Onate Gutierrez, Jose Millan, Ortega, Jessica, Oshita, Masaru, Otero Romero, Susana, Overcash, Jeffrey Scott, Owens, Daniel, Packham, Alice, Pacurar, Mihaela, Paiva de Sousa, Leonardo, Palfreeman, Adrian, Pallares, Christian José, Patel, Rahul, Patel, Suchet, Pelkey, Leslie, Peluso, Denise, Penciu, Florentina, Pinto, S. Jerry, Pounds, Kevin, Pouzar, Joe, Pragalos, Antoinette, Presti, Rachel, Price, David, Qureshi, Ehsaan, Ramalho Madruga, José Valdez, Ramesh, Mayur, Rankin, Bruce, Razat, Béatrice, Riegel Santos, Breno, Riesenberg, Robert, Riffer, Ernie, Roche, Siobhan, Rose, Katie, Rosellini, Pietro, Rossignol, Patrick, Safirstein, Beth, Salazar, Hernan, Sanchez Vallejo, Gregorio, Santhosh, Smrithi, Seco-Meseguer, Enrique, Seep, Michael, Sherry, Emma, Short, Philip, Soentjens, Patrick, Solis, Joel, Soriano Viladomiu, Alejandro, Sorli, Caroline, Spangenthal, Selwyn, Spence, Niamh, Stephenson, Elaine, Strout, Cynthia, Surowitz, Ronald, Taladua, Kristy Michelle, Tellalian, David, Thalamas, Claire, Thiriphoo, Nang, Thomas, Judith, Thomas, Nicholas, Trout, Guillermo, Urroz, Mikel, Veekmans, Bernard, Veekmans, Laurent, Villalobos, Ralph Elvi M., Warren, Sarah, Webster, Brian, White, Alexander, Williams, Gail, Williams, Hayes, Wilson, Barbara, Winston, Alan, Wiselka, Martin, Zervos, Marcus, Hardt, Karin, Vandebosch, An, Sadoff, Jerald, Le Gars, Mathieu, Truyers, Carla, Lowson, David, Van Dromme, Ilse, Vingerhoets, Johan, Kamphuis, Tobias, Scheper, Gert, Ruiz-Guiñazú, Javier, Faust, Saul N, Spinner, Christoph D, Schuitemaker, Hanneke, Van Hoof, Johan, Douoguih, Macaya, and Struyf, Frank
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- 2022
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224. Patent foramen ovale and perioperative stroke in noncardiac surgery: a systematic review and meta-analysis
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Rais, Gael, Vassallo, Paola, Schorer, Raoul, Bollen Pinto, Bernardo, and Putzu, Alessandro
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- 2022
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225. PATH-38. ROSETTE-FORMING GLIONEURONAL TUMOR IS DEFINED BY FGFR1 ACTIVATING ALTERATIONS WITH FREQUENT ACCOMPANYING PI3K AND MAPK PATHWAY MUTATIONS
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Calixto-Hope, Lucas, Lee, Julieann, Sloan, Emily, Hofmann, Jeffrey, Van Ziffle, Jessica, Onodera, Courtney, Grenert, James, Devine, Patrick, Kline, Cassie, Banerjee, Anu, Clarke, Jennifer, Taylor, Jennie, Ann Oberheim-Bush, Nancy, Buerki, Robin, Butowski, Nicholas, Chang, Susan, McDermott, Mike, Aghi, Manish, Theodosopoulos, Philip, Hervey-Jumper, Shawn, Berger, Mitchel, Raffel, Corey, Gupta, Nalin, Kleinschmidt-DeMasters, Bette, Wood, Matthew, Grafe, Marjorie, Guo, Hua, Sun, Peter, Torkildson, Joseph, Cooney, Tabitha, Fata, Cynthia, Scharnhorst, David, Samuel, David, Bannykh, Serguei, Khatib, Ziad, Maher, Ossama, Chamyan, Gabriel, Pelaez, Liset, Brathwaite, Carole, Jin, Lee-way, Lechpammer, Mirna, Born, Donald, Vogel, Hannes, Lee, Han, Phillips, Joanna, Pekmezci, Melike, Bollen, Andrew, Tihan, Tarik, Perry, Arie, and Solomon, David
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Neurosciences ,Oncology and Carcinogenesis ,Oncology & Carcinogenesis - Abstract
Abstract BACKGROUND Rosette-forming glioneuronal tumor (RGNT) is an uncommon CNS tumor originally described in the fourth ventricle characterized by a low-grade glial neoplasm admixed with a rosette-forming neurocytic component. METHODS We reviewed clinicopathologic features of 42 patients with RGNT. Targeted next-generation sequencing was performed, and genome-wide methylation profiling is underway. RESULTS The 20 male and 22 female patients had a mean age of 25 years (range 3–47) at time of diagnosis. Tumors were located within or adjacent to the lateral ventricle (n=16), fourth ventricle (15), third ventricle (9), and spinal cord (2). All 31 tumors assessed to date contained FGFR1 activating alterations, either in-frame gene fusion, kinase domain tandem duplication, or hotspot missense mutation in the kinase domain (p.N546 or p.K656). While 7 of these 31 tumors harbored FGFR1 alterations as the solitary pathogenic event, 24 contained additional pathogenic alterations within PI3-kinase or MAP kinase pathway genes: 5 with additional PIK3CA and NF1 mutations, 4 with PIK3CA mutation, 3 with PIK3R1 mutation (one of which also contained focal RAF1 amplification), 5 with PTPN11 mutation (one with additional PIK3R1 mutation), and 2 with NF1 deletion. The other 5 cases demonstrated anaplastic features including hypercellularity and increased mitotic activity. Among these anaplastic cases, 3 harbored inactivating ATRX mutations and two harbored CDKN2A homozygous deletion, in addition to the FGFR1 alterations plus other PI3-kinase and MAP kinase gene mutations seen in those RGNT without anaplasia. CONCLUSION Independent of ventricular location, RGNT is defined by FGFR1 activating mutations or rearrangements, which are frequently accompanied by mutations involving PIK3CA, PIK3R1, PTPN11, NF1, and KRAS. Whereas pilocytic astrocytoma and ganglioglioma are characterized by solitary activating MAP kinase pathway alterations (e.g. BRAF fusion or mutation), RGNT are genetically more complex with dual PI3K-Akt-mTOR and Ras-Raf-MAPK pathway activation. Rare anaplastic examples may show additional ATRX and/or CDKN2A inactivation.
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- 2019
226. Recurrent non-canonical histone H3 mutations in spinal cord diffuse gliomas.
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Sloan, Emily A, Cooney, Tabitha, Oberheim Bush, Nancy Ann, Buerki, Robin, Taylor, Jennie, Clarke, Jennifer L, Torkildson, Joseph, Kline, Cassie, Reddy, Alyssa, Mueller, Sabine, Banerjee, Anu, Butowski, Nicholas, Chang, Susan, Mummaneni, Praveen V, Chou, Dean, Tan, Lee, Theodosopoulos, Philip, McDermott, Michael, Berger, Mitchel, Raffel, Corey, Gupta, Nalin, Sun, Peter P, Li, Yi, Shah, Vinil, Cha, Soonmee, Braunstein, Steve, Raleigh, David R, Samuel, David, Scharnhorst, David, Fata, Cynthia, Guo, Hua, Moes, Gregory, Kim, John YH, Koschmann, Carl, Van Ziffle, Jessica, Onodera, Courtney, Devine, Patrick, Grenert, James P, Lee, Julieann C, Pekmezci, Melike, Phillips, Joanna J, Tihan, Tarik, Bollen, Andrew W, Perry, Arie, and Solomon, David A
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Spinal Cord ,Humans ,Glioma ,Brain Neoplasms ,Spinal Cord Neoplasms ,Histones ,Mutation ,Adolescent ,Adult ,Aged ,Middle Aged ,Child ,Child ,Preschool ,Female ,Male ,Young Adult ,Neurology & Neurosurgery ,Clinical Sciences ,Neurosciences - Published
- 2019
227. Mechanisms of Resistance to EGFR Inhibition Reveal Metabolic Vulnerabilities in Human GBM
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McKinney, Andrew, Lindberg, Olle R, Engler, Jane R, Chen, Katharine Y, Kumar, Anupam, Gong, Henry, Lu, Kan V, Simonds, Erin F, Cloughesy, Timothy F, Liau, Linda M, Prados, Michael, Bollen, Andrew W, Berger, Mitchel S, Shieh, Joseph TC, James, C David, Nicolaides, Theodore P, Yong, William H, Lai, Albert, Hegi, Monika E, Weiss, William A, and Phillips, Joanna J
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Clinical Research ,Rare Diseases ,Cancer ,Brain Disorders ,Brain Cancer ,Neurosciences ,5.1 Pharmaceuticals ,Development of treatments and therapeutic interventions ,Aetiology ,2.1 Biological and endogenous factors ,Aldehyde Dehydrogenase 1 Family ,Animals ,Brain Neoplasms ,Cell Line ,Tumor ,Cell Proliferation ,Dasatinib ,Drug Resistance ,Neoplasm ,ErbB Receptors ,Erlotinib Hydrochloride ,Glioblastoma ,Humans ,Mice ,Oxidative Stress ,Protein Kinase Inhibitors ,Retinal Dehydrogenase ,Xenograft Model Antitumor Assays ,Pharmacology and Pharmaceutical Sciences ,Oncology & Carcinogenesis ,Biochemistry and cell biology ,Oncology and carcinogenesis - Abstract
Amplification of the epidermal growth factor receptor gene (EGFR) represents one of the most commonly observed genetic lesions in glioblastoma (GBM); however, therapies targeting this signaling pathway have failed clinically. Here, using human tumors, primary patient-derived xenografts (PDX), and a murine model for GBM, we demonstrate that EGFR inhibition leads to increased invasion of tumor cells. Further, EGFR inhibitor-treated GBM demonstrates altered oxidative stress, with increased lipid peroxidation, and generation of toxic lipid peroxidation products. A tumor cell subpopulation with elevated aldehyde dehydrogenase (ALDH) levels was determined to comprise a significant proportion of the invasive cells observed in EGFR inhibitor-treated GBM. Our analysis of the ALDH1A1 protein in newly diagnosed GBM revealed detectable ALDH1A1 expression in 69% (35/51) of the cases, but in relatively low percentages of tumor cells. Analysis of paired human GBM before and after EGFR inhibitor therapy showed an increase in ALDH1A1 expression in EGFR-amplified tumors (P < 0.05, n = 13 tumor pairs), and in murine GBM ALDH1A1-high clones were more resistant to EGFR inhibition than ALDH1A1-low clones. Our data identify ALDH levels as a biomarker of GBM cells with high invasive potential, altered oxidative stress, and resistance to EGFR inhibition, and reveal a therapeutic target whose inhibition should limit GBM invasion.
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- 2019
228. Recurrent KBTBD4 small in-frame insertions and absence of DROSHA deletion or DICER1 mutation differentiate pineal parenchymal tumor of intermediate differentiation (PPTID) from pineoblastoma
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Lee, Julieann C, Mazor, Tali, Lao, Richard, Wan, Eunice, Diallo, Alpha B, Hill, Nicholas S, Thangaraj, Naina, Wendelsdorf, Katherine, Samuel, David, Kline, Cassie N, Banerjee, Anuradha, Auguste, Kurtis, Raffel, Corey, Gupta, Nalin, Berger, Mitchel, Raleigh, David R, Shai, Anny, Phillips, Joanna J, Bollen, Andrew W, Tihan, Tarik, Perry, Arie, Costello, Joseph, and Solomon, David A
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Adolescent ,Adult ,Biomarkers ,Tumor ,Brain ,Brain Neoplasms ,Carrier Proteins ,Child ,Cohort Studies ,DEAD-box RNA Helicases ,Diagnosis ,Differential ,Female ,Humans ,Infant ,Male ,Middle Aged ,Mutation ,Pineal Gland ,Pinealoma ,Ribonuclease III ,Clinical Sciences ,Neurosciences ,Neurology & Neurosurgery - Published
- 2019
229. The genetic landscape of gliomas arising after therapeutic radiation
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López, Giselle Y, Van Ziffle, Jessica, Onodera, Courtney, Grenert, James P, Yeh, Iwei, Bastian, Boris C, Clarke, Jennifer, Oberheim Bush, Nancy Ann, Taylor, Jennie, Chang, Susan, Butowski, Nicholas, Banerjee, Anuradha, Mueller, Sabine, Kline, Cassie, Torkildson, Joseph, Samuel, David, Siongco, Aleli, Raffel, Corey, Gupta, Nalin, Kunwar, Sandeep, Mummaneni, Praveen, Aghi, Manish, Theodosopoulos, Philip, Berger, Mitchel, Phillips, Joanna J, Pekmezci, Melike, Tihan, Tarik, Bollen, Andrew W, Perry, Arie, and Solomon, David A
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Biomedical and Clinical Sciences ,Clinical Sciences ,Oncology and Carcinogenesis ,Rare Diseases ,Pediatric ,Biotechnology ,Brain Cancer ,Cancer ,Human Genome ,Brain Disorders ,Pediatric Research Initiative ,Orphan Drug ,Pediatric Cancer ,Genetics ,2.1 Biological and endogenous factors ,Aetiology ,Adolescent ,Adult ,Astrocytoma ,Biomarkers ,Tumor ,Brain Neoplasms ,Child ,Child ,Preschool ,Female ,Genomics ,Glioma ,Homozygote ,Humans ,Male ,Mutation ,Sequence Deletion ,Telomerase ,Young Adult ,Secondary malignancy ,Radiation therapy ,Ionizing radiation ,Radiation-associated glioma ,Radiation-induced glioma ,DNA double-strand breaks ,Chromosome breaks ,Genomic signature ,Mutational signature ,Glioblastoma ,Ganglioglioma ,Neurosciences ,Neurology & Neurosurgery - Abstract
Radiotherapy improves survival for common childhood cancers such as medulloblastoma, leukemia, and germ cell tumors. Unfortunately, long-term survivors suffer sequelae that can include secondary neoplasia. Gliomas are common secondary neoplasms after cranial or craniospinal radiation, most often manifesting as high-grade astrocytomas with poor clinical outcomes. Here, we performed genetic profiling on a cohort of 12 gliomas arising after therapeutic radiation to determine their molecular pathogenesis and assess for differences in genomic signature compared to their spontaneous counterparts. We identified a high frequency of TP53 mutations, CDK4 amplification or CDKN2A homozygous deletion, and amplifications or rearrangements involving receptor tyrosine kinase and Ras-Raf-MAP kinase pathway genes including PDGFRA, MET, BRAF, and RRAS2. Notably, all tumors lacked alterations in IDH1, IDH2, H3F3A, HIST1H3B, HIST1H3C, TERT (including promoter region), and PTEN, which genetically define the major subtypes of diffuse gliomas in children and adults. All gliomas in this cohort had very low somatic mutation burden (less than three somatic single nucleotide variants or small indels per Mb). The ten high-grade gliomas demonstrated markedly aneuploid genomes, with significantly increased quantity of intrachromosomal copy number breakpoints and focal amplifications/homozygous deletions compared to spontaneous high-grade gliomas, likely as a result of DNA double-strand breaks induced by gamma radiation. Together, these findings demonstrate a distinct molecular pathogenesis of secondary gliomas arising after radiation therapy and identify a genomic signature that may aid in differentiating these tumors from their spontaneous counterparts.
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- 2019
230. The genetic landscape of anaplastic pleomorphic xanthoastrocytoma
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Phillips, Joanna J, Gong, Henry, Chen, Katharine, Joseph, Nancy M, van Ziffle, Jessica, Bastian, Boris C, Grenert, James P, Kline, Cassie N, Mueller, Sabine, Banerjee, Anuradha, Nicolaides, Theodore, Gupta, Nalin, Berger, Mitchel S, Lee, Han S, Pekmezci, Melike, Tihan, Tarik, Bollen, Andrew W, Perry, Arie, Shieh, Joseph TC, and Solomon, David A
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Biomedical and Clinical Sciences ,Clinical Sciences ,Oncology and Carcinogenesis ,Cancer ,Genetics ,Pediatric Research Initiative ,Human Genome ,2.1 Biological and endogenous factors ,Aetiology ,Adolescent ,Adult ,Aged ,Astrocytoma ,Brain Neoplasms ,Child ,Cyclin-Dependent Kinase Inhibitor p16 ,DNA Copy Number Variations ,Female ,Gene Expression Profiling ,Homozygote ,Humans ,Male ,Middle Aged ,Mutation ,Neoplasm Recurrence ,Local ,Proto-Oncogene Proteins B-raf ,Telomerase ,Transcriptome ,anaplastic PXA ,TERT promoter mutations ,intratumoral heterogeneity ,pediatric glioma ,glioma progression ,Neurosciences ,Neurology & Neurosurgery ,Clinical sciences - Abstract
Pleomorphic xanthoastrocytoma (PXA) is an astrocytic neoplasm that is typically well circumscribed and can have a relatively favorable prognosis. Tumor progression to anaplastic PXA (WHO grade III), however, is associated with a more aggressive biologic behavior and worse prognosis. The factors that drive anaplastic progression are largely unknown. We performed comprehensive genomic profiling on a set of 23 PXAs from 19 patients, including 15 with anaplastic PXA. Four patients had tumor tissue from multiple recurrences, including two with anaplastic progression. We find that PXAs are genetically defined by the combination of CDKN2A biallelic inactivation and RAF alterations that were present in all 19 cases, most commonly as CDKN2A homozygous deletion and BRAF p.V600E mutation but also occasionally BRAF or RAF1 fusions or other rearrangements. The third most commonly altered gene in anaplastic PXA was TERT, with 47% (7/15) harboring TERT alterations, either gene amplification (n = 2) or promoter hotspot mutation (n = 5). In tumor pairs analyzed before and after anaplastic progression, two had increased copy number alterations and one had TERT promoter mutation at recurrence. Less commonly altered genes included TP53, BCOR, BCORL1, ARID1A, ATRX, PTEN, and BCL6. All PXA in this cohort were IDH and histone H3 wildtype, and did not contain alterations in EGFR. Genetic profiling performed on six regions from the same tumor identified intratumoral genomic heterogeneity, likely reflecting clonal evolution during tumor progression. Overall, anaplastic PXA is characterized by the combination of CDKN2A biallelic inactivation and oncogenic RAF kinase signaling as well as a relatively small number of additional genetic alterations, with the most common being TERT amplification or promoter mutation. These data define a distinct molecular profile for PXA and suggest additional genetic alterations, including TERT, may be associated with anaplastic progression.
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- 2019
231. Investigating Various Severity Factor Behaviors for Operational Risk Assessment
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Zunaira Nazir and Math H. J. Bollen
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power system security ,power risk analysis ,operational risk assessment ,contingency ,severity factor ,voltage collapse ,Electricity ,QC501-721 - Abstract
Operational risk assessment is a stochastic approach to quantify the operational security of power systems. In this study, the interrelation between severity factor and operational risk, two important parameters in operational risk assessment, is analyzed. Four different definitions of severity factor, based on the results from network studies, are proposed and applied, resulting in different values for the operational risk indices. The behavior of these indices is analyzed under varying operating conditions and compared with the behavior of the severity factor for individual contingencies. This study confirms the importance of the severity factor definition and shows that multiple operational risk indices are required to obtain a clear picture of the operational security of a transmission system. One risk index may increase while another decreases.
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- 2022
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232. Noninvasive ventilation in COVID-19 patients aged ≥ 70 years—a prospective multicentre cohort study
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Kamil Polok, Jakub Fronczek, Antonio Artigas, Hans Flaatten, Bertrand Guidet, Dylan W. De Lange, Jesper Fjølner, Susannah Leaver, Michael Beil, Sigal Sviri, Raphael Romano Bruno, Bernhard Wernly, Bernardo Bollen Pinto, Joerg C. Schefold, Dorota Studzińska, Michael Joannidis, Sandra Oeyen, Brian Marsh, Finn H. Andersen, Rui Moreno, Maurizio Cecconi, Christian Jung, Wojciech Szczeklik, and COVIP Study Group
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COVID-19 ,Noninvasive ventilation ,Frailty ,Intensive care unit ,Elderly ,Medical emergencies. Critical care. Intensive care. First aid ,RC86-88.9 - Abstract
Abstract Background Noninvasive ventilation (NIV) is a promising alternative to invasive mechanical ventilation (IMV) with a particular importance amidst the shortage of intensive care unit (ICU) beds during the COVID-19 pandemic. We aimed to evaluate the use of NIV in Europe and factors associated with outcomes of patients treated with NIV. Methods This is a substudy of COVIP study—an international prospective observational study enrolling patients aged ≥ 70 years with confirmed COVID-19 treated in ICU. We enrolled patients in 156 ICUs across 15 European countries between March 2020 and April 2021.The primary endpoint was 30-day mortality. Results Cohort included 3074 patients, most of whom were male (2197/3074, 71.4%) at the mean age of 75.7 years (SD 4.6). NIV frequency was 25.7% and varied from 1.1 to 62.0% between participating countries. Primary NIV failure, defined as need for endotracheal intubation or death within 30 days since ICU admission, occurred in 470/629 (74.7%) of patients. Factors associated with increased NIV failure risk were higher Sequential Organ Failure Assessment (SOFA) score (OR 3.73, 95% CI 2.36–5.90) and Clinical Frailty Scale (CFS) on admission (OR 1.46, 95% CI 1.06–2.00). Patients initially treated with NIV (n = 630) lived for 1.36 fewer days (95% CI − 2.27 to − 0.46 days) compared to primary IMV group (n = 1876). Conclusions Frequency of NIV use varies across European countries. Higher severity of illness and more severe frailty were associated with a risk of NIV failure among critically ill older adults with COVID-19. Primary IMV was associated with better outcomes than primary NIV. Clinical Trial Registration NCT04321265 , registered 19 March 2020, https://clinicaltrials.gov .
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- 2022
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233. Association of chronic heart failure with mortality in old intensive care patients suffering from Covid‐19
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Raphael Romano Bruno, Bernhard Wernly, Georg Wolff, Jesper Fjølner, Antonio Artigas, Bernardo Bollen Pinto, Joerg C. Schefold, Detlef Kindgen‐Milles, Philipp Heinrich Baldia, Malte Kelm, Michael Beil, Sigal Sviri, Peter Vernon vanHeerden, Wojciech Szczeklik, Arzu Topeli, Muhammed Elhadi, Michael Joannidis, Sandra Oeyen, Eumorfia Kondili, Brian Marsh, Finn H. Andersen, Rui Moreno, Susannah Leaver, Ariane Boumendil, Dylan W. De Lange, Bertrand Guidet, Hans Flaatten, Christian Jung, and COVIP study group
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COVID‐19 ,Heart failure ,Elderly ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Abstract Aims Chronic heart failure (CHF) is a major risk factor for mortality in coronavirus disease 2019 (COVID‐19). This prospective international multicentre study investigates the role of pre‐existing CHF on clinical outcomes of critically ill old (≥70 years) intensive care patients with COVID‐19. Methods and results Patients with pre‐existing CHF were subclassified as having ischaemic or non‐ischaemic cardiac disease; patients with a documented ejection fraction (EF) were subclassified according to heart failure EF: reduced (HFrEF, n = 132), mild (HFmrEF, n = 91), or preserved (HFpEF, n = 103). Associations of heart failure characteristics with the 30 day mortality were analysed in univariate and multivariate logistic regression analyses. Pre‐existing CHF was reported in 566 of 3917 patients (14%). Patients with CHF were older, frailer, and had significantly higher SOFA scores on admission. CHF patients showed significantly higher crude 30 day mortality [60% vs. 48%, P
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- 2022
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234. Trajectories of Subjective Health : Testing Longitudinal Models for Self-rated Health From Adolescence to Midlife
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Bollen, Kenneth A. and Gutin, Iliya
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- 2021
235. Conclusion
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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236. Encountering Internationalism on the Circuit Around Sydney
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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237. Containing Diversity: National Distinction and International Style
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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238. Entrepreneurial Diplomacy: The Cherry Blossom Show on Tour from Tokyo
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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239. Translating Repertoire Between Melbourne and Manila
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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240. The Tourist Trade: Flying in to Singapore
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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241. Transporting Variety Through the Nightclubs of Hong Kong
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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242. Introduction
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Bollen, Jonathan, Balme, Christopher B., Series Editor, Davis, Tracy C., Series Editor, Cole, Catherine M., Series Editor, and Bollen, Jonathan
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- 2020
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243. A Conceptual Model of the Blockchain
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Bollen, Peter, Goos, Gerhard, Founding Editor, Hartmanis, Juris, Founding Editor, Bertino, Elisa, Editorial Board Member, Gao, Wen, Editorial Board Member, Steffen, Bernhard, Editorial Board Member, Woeginger, Gerhard, Editorial Board Member, Yung, Moti, Editorial Board Member, Debruyne, Christophe, editor, Panetto, Hervé, editor, Guédria, Wided, editor, Bollen, Peter, editor, Ciuciu, Ioana, editor, Karabatis, George, editor, and Meersman, Robert, editor
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- 2020
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244. The genetic landscape of ganglioglioma
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Pekmezci, Melike, Villanueva-Meyer, Javier E, Goode, Benjamin, Van Ziffle, Jessica, Onodera, Courtney, Grenert, James P, Bastian, Boris C, Chamyan, Gabriel, Maher, Ossama M, Khatib, Ziad, Kleinschmidt-DeMasters, Bette K, Samuel, David, Mueller, Sabine, Banerjee, Anuradha, Clarke, Jennifer L, Cooney, Tabitha, Torkildson, Joseph, Gupta, Nalin, Theodosopoulos, Philip, Chang, Edward F, Berger, Mitchel, Bollen, Andrew W, Perry, Arie, Tihan, Tarik, and Solomon, David A
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Biological Sciences ,Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Genetics ,Biotechnology ,Cancer ,Human Genome ,Brain Disorders ,Aetiology ,2.1 Biological and endogenous factors ,Adolescent ,Adult ,Brain Neoplasms ,Child ,Child ,Preschool ,Cohort Studies ,Cyclin-Dependent Kinase Inhibitor p16 ,Female ,Ganglioglioma ,Genetic Association Studies ,Humans ,Male ,Middle Aged ,Mitogen-Activated Protein Kinase 1 ,Mutation ,Proto-Oncogene Proteins B-raf ,Signal Transduction ,Statistics ,Nonparametric ,Young Adult ,Epilepsy ,Seizures ,Glioneuronal tumor ,Targeted next-generation sequencing ,Ras-Raf-MEK-ERK ,MAP kinase signaling pathway ,BRAF ,KRAS ,RAF1 ,NF1 ,FGFR1 ,FGFR2 ,ABL2 ,Biochemistry and Cell Biology ,Clinical Sciences ,Neurosciences ,Biochemistry and cell biology - Abstract
Ganglioglioma is the most common epilepsy-associated neoplasm that accounts for approximately 2% of all primary brain tumors. While a subset of gangliogliomas are known to harbor the activating p.V600E mutation in the BRAF oncogene, the genetic alterations responsible for the remainder are largely unknown, as is the spectrum of any additional cooperating gene mutations or copy number alterations. We performed targeted next-generation sequencing that provides comprehensive assessment of mutations, gene fusions, and copy number alterations on a cohort of 40 gangliogliomas. Thirty-six harbored mutations predicted to activate the MAP kinase signaling pathway, including 18 with BRAF p.V600E mutation, 5 with variant BRAF mutation (including 4 cases with novel in-frame insertions at p.R506 in the β3-αC loop of the kinase domain), 4 with BRAF fusion, 2 with KRAS mutation, 1 with RAF1 fusion, 1 with biallelic NF1 mutation, and 5 with FGFR1/2 alterations. Three gangliogliomas with BRAF p.V600E mutation had concurrent CDKN2A homozygous deletion and one additionally harbored a subclonal mutation in PTEN. Otherwise, no additional pathogenic mutations, fusions, amplifications, or deletions were identified in any of the other tumors. Amongst the 4 gangliogliomas without canonical MAP kinase pathway alterations identified, one epilepsy-associated tumor in the temporal lobe of a young child was found to harbor a novel ABL2-GAB2 gene fusion. The underlying genetic alterations did not show significant association with patient age or disease progression/recurrence in this cohort. Together, this study highlights that ganglioglioma is characterized by genetic alterations that activate the MAP kinase pathway, with only a small subset of cases that harbor additional pathogenic alterations such as CDKN2A deletion.
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- 2018
245. A recurrent kinase domain mutation in PRKCA defines chordoid glioma of the third ventricle
- Author
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Goode, B, Mondal, G, Hyun, M, Ruiz, DG, Lin, YH, Van Ziffle, J, Joseph, NM, Onodera, C, Talevich, E, Grenert, JP, Hewedi, IH, Snuderl, M, Brat, DJ, Kleinschmidt-Demasters, BK, Rodriguez, FJ, Louis, DN, Yong, WH, Lopes, MB, Rosenblum, MK, Butowski, N, Tihan, T, Bollen, AW, Phillips, JJ, Wiita, AP, Yeh, I, Jacobson, MP, Bastian, BC, Perry, A, and Solomon, DA
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Neurosciences ,Brain Cancer ,Genetics ,Rare Diseases ,Human Genome ,Brain Disorders ,Clinical Research ,Cancer ,2.1 Biological and endogenous factors - Abstract
Chordoid glioma is a rare brain tumor thought to arise from specialized glial cells of the lamina terminalis along the anterior wall of the third ventricle. Despite being histologically low-grade, chordoid gliomas are often associated with poor outcome, as their stereotypic location in the third ventricle makes resection challenging and efficacious adjuvant therapies have not been developed. Here we performed genomic profiling on 13 chordoid gliomas and identified a recurrent D463H missense mutation in PRKCA in all tumors, which localizes in the kinase domain of the encoded protein kinase C alpha (PKCα). Expression of mutant PRKCA in immortalized human astrocytes led to increased phospho-ERK and anchorage-independent growth that could be blocked by MEK inhibition. These studies define PRKCA as a recurrently mutated oncogene in human cancer and identify a potential therapeutic vulnerability in this uncommon brain tumor.
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- 2018
246. Risk assessment criteria for utilizing dynamic line rating in presence of electric vehicles uncertainty
- Author
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Hajeforosh, SeyedeFatemeh, Bakhtiari, Hamed, and Bollen, Math
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- 2022
- Full Text
- View/download PDF
247. Enhancing the hosting capacity of distribution transformers for using dynamic component rating
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Hajeforosh, SeyedeFatemeh, Khatun, Amena, and Bollen, Math
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- 2022
- Full Text
- View/download PDF
248. Preoperative biliary drainage in severely jaundiced patients with pancreatic head cancer: A retrospective cohort study
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van Gils, Luuk, Verbeek, Romy, Wellerdieck, Nienke, Bollen, Thomas, van Leeuwen, Maarten, Schwartz, Matthijs, Vleggaar, Frank, Molenaar, I.Q. (Quintus), van Santvoort, Hjalmar, van Hooft, Janine, Verdonk, Robert, and Weusten, Bas
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- 2022
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- View/download PDF
249. Magnification of Transients at the Voltage Dips Starting and its Impacts on DFIG-based Wind Power Plants
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Oliveira, Roger A.D. and Bollen, Math H.J.
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- 2022
- Full Text
- View/download PDF
250. Fifty years of structural equation modeling: A history of generalization, unification, and diffusion
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Bollen, Kenneth A., Fisher, Zachary, Lilly, Adam, Brehm, Christopher, Luo, Lan, Martinez, Alejandro, and Ye, Ai
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- 2022
- Full Text
- View/download PDF
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