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53. Role of Pyroptosis in Acetaminophen-Induced Hepatotoxicity

Author

Hartmut Jaeschke, David S. Umbaugh, and Anup Ramachandran

Subjects
acetaminophen, hepatotoxicity, pyroptosis, gasdermin, inflammasome, caspases, Medicine (General), R5-920
Abstract

Acetaminophen (APAP) is a widely used pain reliever that can cause liver injury or liver failure in response to an overdose. Understanding the mechanisms of APAP-induced cell death is critical for identifying new therapeutic targets. In this respect it was hypothesized that hepatocytes die by oncotic necrosis, apoptosis, necroptosis, ferroptosis and more recently pyroptosis. The latter cell death is characterized by caspase-dependent gasdermin cleavage into a C-terminal and an N-terminal fragment, which forms pores in the plasma membrane. The gasdermin pores can release potassium, interleukin-1β (IL-1β), IL-18, and other small molecules in a sublytic phase, which can be the main function of the pores in certain cell types such as inflammatory cells. Alternatively, the process can progress to full lysis of the cell (pyroptosis) with extensive cell contents release. This review discusses the experimental evidence for the involvement of pyroptosis in APAP hepatotoxicity as well as the arguments against pyroptosis as a relevant mechanism of APAP-induced cell death in hepatocytes. Based on the critical evaluation of the currently available literature and understanding of the pathophysiology, it can be concluded that pyroptotic cell death is unlikely to be a relevant contributor to APAP-induced liver injury.

Published
2022
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54. SWAG: Distribution and Kinematics of an Obscured AGB Population toward the Galactic Center

Author

Ott, Jürgen, Meier, David S., Ginsburg, Adam, Yusef-Zadeh, Farhad, Krieger, Nico, and Jäschke, Cornelia

Subjects
Astrophysics - Astrophysics of Galaxies
Abstract

Outflows from AGB stars enrich the Galactic environment with metals and inject mechanical energy into the ISM. Radio spectroscopy can recover both properties through observations of molecular lines. We present results from SWAG: "Survey of Water and Ammonia in the Galactic Center". The survey covers the entire Central Molecular Zone (CMZ), the inner 3.35deg x 0.9deg (~480 x 130pc) of the Milky Way that contains ~5x10^7 Mo of molecular gas. Although our survey primarily targets the CMZ, we observe across the entire sightline through the Milky Way. AGB stars are revealed by their signature of double peaked 22 GHz water maser lines. They are distinguished by their spectral signatures and their luminosities, which reach up to 10^-7 Lo. Higher luminosities are usually associated with Young Stellar Objects located in CMZ star forming regions. We detect a population of ~600 new water masers that can likely be associated with AGB outflows., Comment: 2 pages, 1 figure, to appear in proceedings for the IAU Symposium 343: "Why Galaxies Care About AGB Stars: A Continuing Challenge through Cosmic Time", F. Kerschbaum, M. Groenewegen, and H. Olofsson, eds

Published
2018

55. High-Order Isogeometric Methods for Compressible Flows. I. Scalar Conservation Laws

Author

Jaeschke, Andrzej and Möller, Matthias

Subjects
Mathematics - Numerical Analysis
Abstract

Isogeometric analysis was applied very successfully to many problem classes like linear elasticity, heat transfer and incompressible flow problems but its application to compressible flows is very rare. However, its ability to accurately represent complex geometries used in industrial applications makes IGA a suitable tool for the analysis of compressible flow problems that require the accurate resolution of boundary layers. The convection-diffusion solver presented in this chapter, is an indispensable step on the way to developing a compressible flow solver for complex viscous industrial flows. It is well known that the standard Galerkin finite element method and its isogeometric counterpart suffer from spurious oscillatory behaviour in the presence of shocks and steep solution gradients. As a remedy, the algebraic flux correction paradigm is generalized to B-Spline basis functions to suppress the creation of oscillations and occurrence of non-physical values in the solution. This work provides early results for scalar conservation laws and lays the foundation for extending this approach to the compressible Euler equations., Comment: Accepted for publication in the Proceedings of the 19th International Conference on Finite Elements in Flow Problems (FEF 2017)

Published
2018

56. High-Order Isogeometric Methods for Compressible Flows. II. Compressible Euler Equations

Author

Möller, Matthias and Jaeschke, Andrzej

Subjects
Mathematics - Numerical Analysis
Abstract

This work extends the high-resolution isogeometric analysis approach established for scalar transport equations to the equations of gas dynamics. The group finite element formulation is adopted to obtain an efficient assembly procedure for the standard Galerkin approximation, which is stabilized by adding artificial viscosities proportional to the spectral radius of the Roe-averaged flux-Jacobian matrix. Excess stabilization is removed in regions with smooth flow profiles with the aid of algebraic flux correction \cite{KBNII}. The underlying principles are reviewed and it is shown that linearized FCT-type flux limiting \cite{Kuzmin2009} originally derived for nodal low-order finite elements ensures positivity-preservation for high-order B-Spline discretizations., Comment: Accepted for publication in the Proceedings of the 19th International Conference on Finite Elements in Flow Problems (FEF 2017)

Published
2018

57. FDBB: Fluid Dynamics Building Blocks

Author

Möller, Matthias and Jaeschke, Andrzej

Subjects
Computer Science - Mathematical Software
Abstract

High-performance computing platforms are becoming more and more heterogeneous, which makes it very difficult for researchers and scientific software developers to keep up with the rapid changes on the hardware market. In this paper, the open-source project FDBB (Fluid Dynamics Building Blocks) is presented, which eases the development of fluid dynamics applications for heterogeneous systems. It consists of a low-level API that provides a unified interface to many different linear algebra back-ends and a lightweight and extendible high-level expression template library, which provides largely customizable fluid dynamics building blocks, like transformations between primary and secondary variables as well as expressions for Riemann invariants, equations of state, inviscid fluxes and their flux-Jacobians. The performance of the developed approach is assessed both for synthetic micro-benchmarks and within mini-applications.

Published
2018

58. Electron Spin Noise under the Conditions of Nuclei Induced Frequency Focusing

Author

Jäschke, Natalie, Anders, Frithjof B., and Glazov, Mikhail M.

Subjects
Condensed Matter - Mesoscale and Nanoscale Physics
Abstract

We study theoretically the electron spin noise in quantum dots under non-equilibrium conditions caused by the pumping by a train of circularly polarized optical pulses. In such a situation, the nuclear spins are known to adjust in such a way, that the electron spin precession frequencies become multiples of the pump pulse repetition frequency. This so called phase synchronization effect was uncovered in [Science {\bf 317}, 1896 (2007)] and termed nuclei-induced frequency focusing of electron spin coherence. Using the classical approach to the central spin model we evaluate the nuclear spin distribution function and the electron spin noise spectrum. We show that the electron spin noise spectrum consists of sharp peaks corresponding to the phase synchronization conditions and directly reveal the distribution of the nuclear spins. We discuss the effects of nuclear spin relaxation after the pumping is over and analyze the corresponding evolution of nuclear spin distributions and electron spin noise spectra., Comment: 8 pages, 5 figures

Published
2018
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59. Propagation of pericentral necrosis during acetaminophen-induced liver injury: evidence for early interhepatocyte communication and information-exchange

Author

Kennedy, Ryan C, Smith, Andrew K, Ropella, Glen EP, McGill, Mitchell R, Jaeschke, Hartmut, and Hunt, C Anthony

Subjects
Digestive Diseases, Liver Disease, Chronic Liver Disease and Cirrhosis, Oral and gastrointestinal, Acetaminophen, Activation, Metabolic, Analgesics, Non-Narcotic, Animals, Cell Communication, Chemical and Drug Induced Liver Injury, Computer Simulation, Glutathione, Hepatocytes, Male, Mice, Inbred C57BL, Models, Biological, Necrosis, Signal Transduction, Systems Biology, Time Factors, drug-induced liver injury, hepatic zonation, model mechanism, simulation, systems modeling, virtual experiment, Pharmacology and Pharmaceutical Sciences, Toxicology
Abstract

Acetaminophen (APAP)-induced liver injury is clinically significant, and APAP overdose in mice often serves as a model for drug-induced liver injury in humans. By specifying that APAP metabolism, reactive metabolite formation, glutathione depletion, and mitigation of mitochondrial damage within individual hepatocytes are functions of intralobular location, an earlier virtual model mechanism provided the first concrete multiattribute explanation for how and why early necrosis occurs close to the central vein (CV). However, two characteristic features could not be simulated consistently: necrosis occurring first adjacent to the CV, and subsequent necrosis occurring primarily adjacent to hepatocytes that have already initiated necrosis. We sought parsimonious model mechanism enhancements that would manage spatiotemporal heterogeneity sufficiently to enable meeting two new target attributes and conducted virtual experiments to explore different ideas for model mechanism improvement at intrahepatocyte and multihepatocyte levels. For the latter, evidence supports intercellular communication via exosomes, gap junctions, and connexin hemichannels playing essential roles in the toxic effects of chemicals, including facilitating or counteracting cell death processes. Logic requiring hepatocytes to obtain current information about whether downstream and lateral neighbors have triggered necrosis enabled virtual hepatocytes to achieve both new target attributes. A virtual hepatocyte that is glutathione-depleted uses that information to determine if it will initiate necrosis. When a less-stressed hepatocyte is flanked by at least two neighbors that have triggered necrosis, it too will initiate necrosis. We hypothesize that the resulting intercellular communication-enabled model mechanism is analogous to the actual explanation for APAP-induced hepatotoxicity at comparable levels of granularity.

Published
2019

60. Multistudy Research Operations in the ICU: An Interprofessional Pandemic-Informed Approach

Author

Deborah J. Cook, MD, FRCPC, Erick H. Duan, MD, FRCPC, France J. Clarke, RRT, Karlo Matic, MD, Sarah Culgin, MSc, Laurel Kelly, MSc, Katlynne S. Nelson, MSc, Christine V. Wallace, BScPhm, Mark D. Soth, MD, FRCPC, Kimberley A. Lewis, MD, FRCPC, Jill C. Rudkowski, MD, FRCPC, Dan Perri, MD, FRCPC, Tania L. Ligori, MD, FRCPC, Roman Z. Jaeschke, MD, FRCPC, Zain Chagla, MD, FRCPC, Dipayan Chaudhuri, MD, FRCPC, Angela E. Wright, PharmD, Zoe Y. Fu, PharmD, Brenda K. Reeve, MD, FRCPC, Hilary M. Lee, MD, FRCPC, Jeffrey D. Overington, MD, FRCPC, Anna Rozenberg, MD, FRCPC, Kimberly A. Bloomfield, RN, Katryn Love, RN, Jennifer L. Gain, RRT, Nicole L. Zytaruk, RN, Jason H. Cheung, MD, FRCPC, Lehana Thabane, PhD, Michelle E. Kho, PhD, for the Department of Critical Care Research Operations Committee, Waleed Alhazzani, Matthew Bell, Kimberley Bloomfield, Zain Chagla, Dipayan Chaudhuri, Jason Cheung, France Clarke, Deborah Cook, Mary Copland, Sarah Culgin, Erick Duan, Zoe Fu, Jennifer Gain, Abby Hurd, Roman Jaeschke, Hilary Lee, Katryn Love, Laurel Kelly, Michelle Kho, Kate Kim, Kimberley Lewis, Tania Ligori, Karlo Matic, Katlynne Nelson, Heather O‘Grady, Jeffrey Overington, Dan Perri, Brenda Reeve, Anna Rozenberg, Jill Rudkowski, Lois Saunders, Joanna Semrau, Mark Soth, Christine Wallace, Lily Waugh, Angela Wright, and Nicole Zytaruk

Subjects
Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9
Abstract

OBJECTIVES:. Proliferation of COVID-19 research underscored the need for improved awareness among investigators, research staff and bedside clinicians of the operational details of clinical studies. The objective was to describe the genesis, goals, participation, procedures, and outcomes of two research operations committees in an academic ICU during the COVID-19 pandemic. DESIGN:. Two-phase, single-center multistudy cohort. SETTING:. University-affiliated ICU in Hamilton, ON, Canada. PATIENTS:. Adult patients in the ICU, medical stepdown unit, or COVID-19 ward. INTERVENTIONS:. None. MEASUREMENTS AND MAIN RESULTS:. An interprofessional COVID Collaborative was convened at the pandemic onset within our department, to proactively coordinate studies, help navigate multiple authentic consent encounters by different research staff, and determine which studies would be suitable for coenrollment. From March 2020 to May 2021, five non-COVID trials continued, two were paused then restarted, and five were launched. Over 15 months, 161 patients were involved in 215 trial enrollments, 110 (51.1%) of which were into a COVID treatment trial. The overall informed consent rate (proportion agreed of those eligible and approached including a priori and deferred consent models) was 83% (215/259). The informed consent rate was lower for COVID-19 trials (110/142, 77.5%) than other trials (105/117, 89.7%; p = 0.01). Patients with COVID-19 were significantly more likely to be coenrolled in two or more studies (29/77, 37.7%) compared with other patients (13/84, 15.5%; p = 0.002). Review items for each new study were collated, refined, and evolved into a modifiable checklist template to set up each study for success. The COVID Collaborative expanded to a more formal Department of Critical Care Research Operations Committee in June 2021, supporting sustainable research operations during and beyond the pandemic. CONCLUSIONS:. Structured coordination and increased communication about research operations among diverse research stakeholders cultivated a sense of shared purpose and enhanced the integrity of clinical research operations.

Published
2022
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61. Diarrhea during critical illness: a multicenter cohort study

Author

Dionne, Joanna C., Mbuagbaw, Lawrence, Devlin, John W., Duprey, Matthew S., Cartin-Ceba, Rodrigo, Tsang, Jennifer, Sullivan, Kristen, Muscedere, John, Alshahrani, Mohammed, Szczeklik, Wojciech, Lysecki, Paul, Takaoka, Alyson, Reeve, Brenda, Campbell, Tracy, Borowska, Karolina, Serednicki, Wojciech, Cirone, Robert, Alhazzani, Waleed, Moayyedi, Paul, Armstrong, David, Thabane, Lehana, Jaeschke, Roman, Hamielec, Cindy, Karachi, Tim, and Cook, Deborah J.

Published
2022
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63. Non-equilibrium nuclear spin distribution function in quantum dots subject to periodic pulses

Author

Jäschke, Natalie, Fischer, Andreas, Evers, E., Belykh, V. V., Greilich, Alex, Bayer, Manfred, and Anders, Frithjof B.

Subjects
Condensed Matter - Mesoscale and Nanoscale Physics
Abstract

Electron spin dephasing in a singly charged semiconductor quantum dot can partially be suppressed by periodic laser pulsing. We propose a semi-classical approach describing the decoherence of the electron spin polarization governed by the hyperfine interaction with the nuclear spins as well as the probabilistic nature of the photon absorption. We use the steady-state Floquet condition to analytically derive two subclasses of resonance conditions excellently predicting the peak locations in the part of the Overhauser field distribution which is projected in the direction of the external magnetic field. As a consequence of the periodic pulsing, a non-equilibrium distribution develops as a function of time. The numerical simulation of the coupled dynamics reveals the influence of the hyperfine coupling constant distribution onto the evolution of the electron spin polarisation before the next laser pulse. Experimental indications are provided for both subclasses of resonance conditions., Comment: 21 pages, 21 figures

Published
2017
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64. Semantic Annotation for Microblog Topics Using Wikipedia Temporal Information

Author

Tran, Tuan, Tran, Nam Khanh, Asmelash, Teka Hadgu, and Jäschke, Robert

Subjects
Computer Science - Information Retrieval, I.2.7, H.3.1
Abstract

Trending topics in microblogs such as Twitter are valuable resources to understand social aspects of real-world events. To enable deep analyses of such trends, semantic annotation is an effective approach; yet the problem of annotating microblog trending topics is largely unexplored by the research community. In this work, we tackle the problem of mapping trending Twitter topics to entities from Wikipedia. We propose a novel model that complements traditional text-based approaches by rewarding entities that exhibit a high temporal correlation with topics during their burst time period. By exploiting temporal information from the Wikipedia edit history and page view logs, we have improved the annotation performance by 17-28\%, as compared to the competitive baselines., Comment: Published via ACL to EMNLP 2025

Published
2017

65. World Literature According to Wikipedia: Introduction to a DBpedia-Based Framework

Author

Hube, Christoph, Fischer, Frank, Jäschke, Robert, Lauer, Gerhard, and Thomsen, Mads Rosendahl

Subjects
Computer Science - Information Retrieval, Computer Science - Computation and Language
Abstract

Among the manifold takes on world literature, it is our goal to contribute to the discussion from a digital point of view by analyzing the representation of world literature in Wikipedia with its millions of articles in hundreds of languages. As a preliminary, we introduce and compare three different approaches to identify writers on Wikipedia using data from DBpedia, a community project with the goal of extracting and providing structured information from Wikipedia. Equipped with our basic set of writers, we analyze how they are represented throughout the 15 biggest Wikipedia language versions. We combine intrinsic measures (mostly examining the connectedness of articles) with extrinsic ones (analyzing how often articles are frequented by readers) and develop methods to evaluate our results. The better part of our findings seems to convey a rather conservative, old-fashioned version of world literature, but a version derived from reproducible facts revealing an implicit literary canon based on the editing and reading behavior of millions of people. While still having to solve some known issues, the introduced methods will help us build an observatory of world literature to further investigate its representativeness and biases., Comment: 33 pages, 6 figures, 6 tables

Published
2017

69. Ericaceous vegetation of the Bale Mountains of Ethiopia will prevail in the face of climate change

Author

Yohannes O. Kidane, Samuel Hoffmann, Anja Jaeschke, Mirela Beloiu, and Carl Beierkuhnlein

Subjects
Medicine, Science
Abstract

Abstract Climate change impacts the structure, functioning, and distribution of species and ecosystems. It will shift ecosystem boundaries, potentially affecting vulnerable ecosystems, such as tropical Africa's high mountain ecosystems, i.e., afroalpine ecosystems, and their highly susceptible uniquely adapted species. However, ecosystems along these mountains are not expected to respond similarly to the change. The ericaceous woody vegetation, located between the low-elevation broadleaf forests and high-elevation afroalpine vegetation, are anticipated to be affected differently. We hypothesize that projected climate change will result in an upward expansion and increasing dominance of ericaceous vegetation, which will negatively impact the endemic rich afroalpine ecosystems of the extensive Sanetti plateau. Hence, we modeled the impact of future climate change on the distribution of ericaceous vegetation and discussed its effect on bordering ecosystems in the Bale Mountains. We applied four familiar correlative modeling approaches: bioclim, domain, generalized linear methods, and support vector machines. We used WorldClim’s bioclimatic variables as environmental predictors and two representative concentration pathways (RCPs) of the IPCC Fifth Assessment Report climate change scenarios, namely RCP4.5 and RCP8.5 for future climate projection. The results indicate increased ericaceous vegetation cover on the midaltitude of northwestern and northern parts of the massif, and the Sanetti plateau. We observed upward range expansion and increase of close ericaceous vegetation in midaltitudes, while receding from the lower range across the massif. Moreover, the current ericaceous vegetation range correlates to the temperature and precipitation trends, reaffirming the critical role of temperature and precipitation in determining species distributions along elevational gradients. The results indicate the high likelihood of considerable changes in this biodiversity hotspot in Eastern Africa.

Published
2022
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70. Regulation of Liver Regeneration by Hepatocyte O-GlcNAcylation in MiceSummary

Author

Dakota R. Robarts, Steven R. McGreal, David S. Umbaugh, Wendena S. Parkes, Manasi Kotulkar, Sarah Abernathy, Norman Lee, Hartmut Jaeschke, Sumedha Gunewardena, Stephen A. Whelan, John A. Hanover, Natasha E. Zachara, Chad Slawson, and Udayan Apte

Subjects
Cell Death, HNF4alpha, Proliferation, Partial Hepatectomy, Regeneration, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Background & Aims: The liver has a unique capacity to regenerate after injury in a highly orchestrated and regulated manner. Here, we report that O-GlcNAcylation, an intracellular post-translational modification regulated by 2 enzymes, O-GlcNAc transferase (OGT) and O-GlcNAcase (OGA), is a critical termination signal for liver regeneration following partial hepatectomy (PHX). Methods: We studied liver regeneration after PHX on hepatocyte specific OGT and OGA knockout mice (OGT-KO and OGA-KO), which caused a significant decrease (OGT-KO) and increase (OGA-KO) in hepatic O-GlcNAcylation, respectively. Results: OGA-KO mice had normal regeneration, but the OGT-KO mice exhibited substantial defects in termination of liver regeneration with increased liver injury, sustained cell proliferation resulting in significant hepatomegaly, hepatic dysplasia, and appearance of small nodules at 28 days after PHX. This was accompanied by a sustained increase in expression of cyclins along with significant induction in pro-inflammatory and pro-fibrotic gene expression in the OGT-KO livers. RNA-sequencing studies revealed inactivation of hepatocyte nuclear 4 alpha (HNF4α), the master regulator of hepatic differentiation and a known termination signal, in OGT-KO mice at 28 days after PHX, which was confirmed by both Western blot and immunohistochemistry analysis. Furthermore, a significant decrease in HNFα target genes was observed in OGT-KO mice, indicating a lack of hepatocyte differentiation following decreased hepatic O-GlcNAcylation. Immunoprecipitation experiments revealed HNF4α is O-GlcNAcylated in normal differentiated hepatocytes. Conclusions: These studies show that O-GlcNAcylation plays a critical role in the termination of liver regeneration via regulation of HNF4α in hepatocytes.

Published
2022
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72. mGluR5 Modulation of Behavioral and Epileptic Phenotypes in a Mouse Model of Tuberous Sclerosis Complex

Author

Kelly, Elyza, Schaeffer, Samantha M, Dhamne, Sameer C, Lipton, Jonathan O, Lindemann, Lothar, Honer, Michael, Jaeschke, Georg, Super, Chloe E, Lammers, Stephen HT, Modi, Meera E, Silverman, Jill L, Dreier, John R, Kwiatkowski, David J, Rotenberg, Alexander, and Sahin, Mustafa

Subjects
Neurodegenerative, Tuberous Sclerosis, Pediatric, Behavioral and Social Science, Mental Health, Brain Disorders, Neurosciences, Rare Diseases, Intellectual and Developmental Disabilities (IDD), Epilepsy, Autism, Aetiology, 2.1 Biological and endogenous factors, Neurological, Allosteric Regulation, Animals, Autism Spectrum Disorder, Brain, Cells, Cultured, Disease Models, Animal, Excitatory Amino Acid Agents, Female, Imidazoles, Male, Mice, Transgenic, Motor Activity, Neurons, Phenotype, Pyridines, Rats, Long-Evans, Receptor, Metabotropic Glutamate 5, Tuberous Sclerosis Complex 2 Protein, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry
Abstract

Drugs targeting metabotropic glutamate receptor 5 (mGluR5) have therapeutic potential in autism spectrum disorders (ASD), including tuberous sclerosis complex (TSC). The question whether inhibition or potentiation of mGluR5 could be beneficial depends, among other factors, on the specific indication. To facilitate the development of mGluR5 treatment strategies, we tested the therapeutic utility of mGluR5 negative and positive allosteric modulators (an mGluR5 NAM and PAM) for TSC, using a mutant mouse model with neuronal loss of Tsc2 that demonstrates disease-related phenotypes, including behavioral symptoms of ASD and epilepsy. This model uniquely enables the in vivo characterization and rescue of the electrographic seizures associated with TSC. We demonstrate that inhibition of mGluR5 corrects hyperactivity, seizures, and elevated de novo synaptic protein synthesis. Conversely, positive allosteric modulation of mGluR5 results in the exacerbation of hyperactivity and epileptic phenotypes. The data suggest a meaningful therapeutic potential for mGluR5 NAMs in TSC, which warrants clinical exploration and the continued development of mGluR5 therapies.

Published
2018

75. Recommendations for the use of the acetaminophen hepatotoxicity model for mechanistic studies and how to avoid common pitfalls

Author

Hartmut Jaeschke, Olamide B. Adelusi, Jephte Y. Akakpo, Nga T. Nguyen, Giselle Sanchez-Guerrero, David S. Umbaugh, Wen-Xing Ding, and Anup Ramachandran

Subjects
Acetaminophen hepatotoxicity, Drug metabolism, Mitochondria, Apoptosis, Ferroptosis, Autophagy, Therapeutics. Pharmacology, RM1-950
Abstract

Acetaminophen (APAP) is a widely used analgesic and antipyretic drug, which is safe at therapeutic doses but can cause severe liver injury and even liver failure after overdoses. The mouse model of APAP hepatotoxicity recapitulates closely the human pathophysiology. As a result, this clinically relevant model is frequently used to study mechanisms of drug-induced liver injury and even more so to test potential therapeutic interventions. However, the complexity of the model requires a thorough understanding of the pathophysiology to obtain valid results and mechanistic information that is translatable to the clinic. However, many studies using this model are flawed, which jeopardizes the scientific and clinical relevance. The purpose of this review is to provide a framework of the model where mechanistically sound and clinically relevant data can be obtained. The discussion provides insight into the injury mechanisms and how to study it including the critical roles of drug metabolism, mitochondrial dysfunction, necrotic cell death, autophagy and the sterile inflammatory response. In addition, the most frequently made mistakes when using this model are discussed. Thus, considering these recommendations when studying APAP hepatotoxicity will facilitate the discovery of more clinically relevant interventions.

Published
2021
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76. Dual roles of p62/SQSTM1 in the injury and recovery phases of acetaminophen-induced liver injury in mice

Author

Hui Qian, Qingyun Bai, Xiao Yang, Jephte Y. Akakpo, Lili Ji, Li Yang, Thomas Rülicke, Kurt Zatloukal, Hartmut Jaeschke, Hong-Min Ni, and Wen-Xing Ding

Subjects
Autophagy, Coagulation, DILI, Liver regeneration, Macrophage, Hepatotoxicity, Therapeutics. Pharmacology, RM1-950
Abstract

Acetaminophen (APAP) overdose can induce liver injury and is the most frequent cause of acute liver failure in the United States. We investigated the role of p62/SQSTM1 (referred to as p62) in APAP-induced liver injury (AILI) in mice. We found that the hepatic protein levels of p62 dramatically increased at 24 h after APAP treatment, which was inversely correlated with the hepatic levels of APAP-adducts. APAP also activated mTOR at 24 h, which is associated with increased cell proliferation. In contrast, p62 knockout (KO) mice showed increased hepatic levels of APAP-adducts detected by a specific antibody using Western blot analysis but decreased mTOR activation and cell proliferation with aggravated liver injury at 24 h after APAP treatment. Surprisingly, p62 KO mice recovered from AILI whereas the wild-type mice still sustained liver injury at 48 h. We found increased number of infiltrated macrophages in p62 KO mice that were accompanied with decreased hepatic von Willebrand factor (VWF) and platelet aggregation, which are associated with increased cell proliferation and improved liver injury at 48 h after APAP treatment. Our data indicate that p62 inhibits the late injury phase of AILI by increasing autophagic selective removal of APAP-adducts and mitochondria but impairs the recovery phase of AILI likely by enhancing hepatic blood coagulation.

Published
2021
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77. Physical fitness of children and youth with asthma in comparison to the reference population

Author

Anke Hanssen-Doose, Robert Jaeschke, Claudia Niessner, Doris Oriwol, and Annette Worth

Subjects
Chronic disease, Health, Cardiorespiratory endurance, Muscular strength, Coordination, Physical activity, Sports medicine, RC1200-1245
Abstract

Abstract Background Physical fitness is an essential marker of health. The literature regarding the question of whether individuals with asthma have reduced physical fitness compared to their non-asthmatic peers is inconsistent and focuses on the cardiorespiratory endurance dimension. This study provides a comparison of different dimensions of physical fitness in individuals with and without asthma on the basis of the German population-based study “KiGGS” (German Health Interview and Examination Survey for Children and Adolescents) and its in-depth study “MoMo” (2009–2012: wave 1 and 2014–2017: wave 2). Methods In total, 7731 individuals aged 6–30 years were included in this cross-sectional analysis at two measurement waves, including 353 individuals with and 7378 without asthma. The 12-month prevalence of physician-diagnosed asthma was assessed by interview. Physical fitness was measured by six test items of the MoMo test profile. “Cardiorespiratory endurance” was measured by an ergometric test, “muscular strength” by standing long jump, push-ups and sit-ups and “coordination” by jumping sideways and balancing backwards. Because of the broad age range of the sample, age- and sex-specific percentiles were used. Physical activity, age, gender and general state of health were assessed by questionnaire. Results The individuals with asthma reported a poorer general state of health at both measurement waves. However, the results of the fitness tests indicated that they were as physically fit as their peers without asthma in relation to cardiorespiratory endurance and muscular strength. The mean percentiles were all within the same range. The results of the comparisons of coordination performance were inconsistent. At wave 1 they were within the same range, at wave 2 individuals with asthma showed a poorer coordination performance (p = 0.041; HL = 4.125, CI of HL 0.155–8.125). Conclusions To the best of our knowledge, this is the first study to compare the physical fitness of individuals with and without asthma by considering several dimensions of physical fitness. The study demonstrates that cardiorespiratory endurance and muscular strength are not reduced in individuals with asthma. The results of the comparisons at the two measurement waves were remarkably stable.

Published
2021
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78. Walka o prymat w stanowieniu prawa między Izbą Lordów a Izbą Gmin na początku XX wieku

Author

Andrzej Jaeschke

Subjects
xix–xx wiek, izba lordów, izba gmin, partia konserwatywna, partia liberalna, parlament brytyjski, reforma izby lordów, Political science
Abstract

Na przełomie XIX i XX wieku w parlamencie westminsterskim rozegrał się jeden z najważniejszych, trwający wiele lat akt konkurencji między obydwoma izbami parlamentu o wpływ na realizację funkcji ustawodawczej w procedurze parlamentarnej. W niniejszym artykule, będącym wynikiem znacznie szerszych studiów nad przekształceniami wewnętrznymi parlamentaryzmu brytyjskiego, przedstawiono społeczne i polityczne tło tej walki toczącej się na forum obydwu izb między dwiema siłami politycznymi: Partią Konserwatywną i Partią Liberalną, wzmocnioną przez taktycznych sojuszników. W tekście starano się przedstawić prawny wynik tego sporu w postaci słynnego Parliament Act 1911, ale także – na podstawie dzisiejszego stanu wiedzy opartego również na zachowanych stenogramach wystąpień parlamentarnych – klimat tego sporu oraz jego społeczne i polityczne tło.

Published
2021
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80. Comparison of Gonadotropin-Releasing Hormone versus Estrogen-Based Fixed-Time Artificial Insemination Protocols in Grazing Bos taurus Suckled Beef Cows

Author

Luis B. Ferré, Julian Jaeschke, Juliana Gatti, Gerardo Baladón, Ezequiel Bellocq, Gustavo Fernández, Ramiro Rearte, Michael E. Kjelland, Marcos G. Colazo, and Jordan M. Thomas

Subjects
estrus synchronization, intravaginal progesterone device, prostaglandin, presynchronization, cattle, Veterinary medicine, SF600-1100, Zoology, QL1-991
Abstract

Fixed-timed artificial insemination (FTAI) protocols for beef cattle in South America are primarily based on estradiol esters and intravaginal progesterone-releasing devices (IVPD). The objective of this study was to determine the optimal gonadotropin-releasing hormone (GnRH)-based protocol as an alternative to the use of estrogen-based protocols in grazing Bos taurus suckling beef cows. All cows received an IVPD on the day of protocol initiation and prostaglandin F2α (PG) plus equine chorionic gonadotropin (eCG) treatments at the time of IVPD removal. In Experiment 1, cows (n = 235) were randomly assigned to one of four treatments: (i) 7-day estradiol = 2 mg of estradiol benzoate (EB) at IVPD insertion on Day 9 and 1 mg of estradiol cypionate (ECP) at IVPD removal on Day 2; (ii) 7-day GnRH = 10 µg of GnRH at IVPD insertion on Day 10, IVPD removal on Day 3 and GnRH at FTAI; (iii) 7 & 7 estradiol = PG at IVPD insertion on Day 16, EB on Day 9 and ECP at IVPD removal on Day 2; (iv) 7 & 7 GnRH = PG at IVPD insertion on Day 17, GnRH on Day 10, IVPD removal on Day 3 and GnRH at FTAI. In Experiment 2, cows (n = 462) were randomly assigned to one of four treatments: (i) 6-day estradiol = EB at IVPD insertion on Day 9, IVPD removal on Day 3 and GnRH at FTAI; (ii) 7-day estradiol; (iii) 7-day GnRH; (iv) 7 & 7 GnRH. In Experiment 1, plasma progesterone concentrations and percentage of cows with a corpus luteum (CL) at IVPD removal, and pregnancy per AI (P/AI) were greater for cows subjected to GnRH-based protocols compared with cows subjected to estrogen-based protocols (p < 0.01). In Experiment 2, cows subjected to the 7 & 7 GnRH protocol had the greatest P/AI (p < 0.01). In summary, GnRH-based FTAI protocols resulted in similar or greater P/AI compared to estrogen-based FTAI protocols in grazing postpartum Bos taurus suckled beef cows. The greatest P/AI was attained with the 7 & 7 GnRH protocol.

Published
2023
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81. A non-human primate model of acute liver failure suitable for testing liver support systems

Author

Ranjeet S. Kalsi, Alina Ostrowska, Adam Olson, Mubina Quader, Melvin Deutsch, Norma J. Arbujas-Silva, Jen Symmonds, Alejandro Soto-Gutierrez, John J. Crowley, Miguel Reyes-Mugica, Giselle Sanchez-Guerrero, Hartmut Jaeschke, Bruce P. Amiot, Marilia Cascalho, Scott L. Nyberg, Jeffrey L. Platt, Edgar N. Tafaleng, and Ira J. Fox

Subjects
acute liver failure (ALF), non-human primates (NHPs), liver-directed radiation therapy, hepatic ischemia-reperfusion injury, xenogeneic hepatocyte transplantation, Medicine (General), R5-920
Abstract

Acute hepatic failure is associated with high morbidity and mortality for which the only definitive therapy is liver transplantation. Some fraction of those who undergo emergency transplantation have been shown to recover native liver function when transplanted with an auxiliary hepatic graft that leaves part of the native liver intact. Thus, transplantation could have been averted with the development and use of some form of hepatic support. The costs of developing and testing liver support systems could be dramatically reduced by the availability of a reliable large animal model of hepatic failure with a large therapeutic window that allows the assessment of efficacy and timing of intervention. Non-lethal forms of hepatic injury were examined in combination with liver-directed radiation in non-human primates (NHPs) to develop a model of acute hepatic failure that mimics the human condition. Porcine hepatocyte transplantation was then tested as a potential therapy for acute hepatic failure. After liver-directed radiation therapy, delivery of a non-lethal hepatic ischemia-reperfusion injury reliably and rapidly generated liver failure providing conditions that can enable pre-clinical testing of liver support or replacement therapies. Unfortunately, in preliminary studies, low hepatocyte engraftment and over-immune suppression interfered with the ability to assess the efficacy of transplanted porcine hepatocytes in the model. A model of acute liver failure in NHPs was created that recapitulates the pathophysiology and pathology of the clinical condition, does so with reasonably predictable kinetics, and results in 100% mortality. The model allowed preliminary testing of xenogeneic hepatocyte transplantation as a potential therapy.

Published
2022
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82. Accelerated low-intensity rTMS does not rescue anxiety behaviour or abnormal connectivity in young adult rats following chronic restraint stress

Author

Lauren A. Hennessy, Bhedita J. Seewoo, Liz A. Jaeschke, Leah A. Mackie, Abbey Figliomeni, Yasmin Arena-Foster, Sarah J. Etherington, Sarah A. Dunlop, Paul E. Croarkin, and Jennifer Rodger

Subjects
rTMS, Chronic stress, Anxiety, Animal model, MRI, Behaviour, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Currently approved repetitive transcranial magnetic stimulation (rTMS) protocols for the treatment of major depressive disorder (MDD) involve once-daily (weekday) stimulation sessions, with 10 Hz or intermittent theta burst stimulation (iTBS) frequencies, over 4–6 weeks. Recently, accelerated treatment protocols (multiple daily stimulation sessions for 1–2 weeks) have been increasingly studied to optimize rTMS treatments. Accelerated protocols might confer unique advantages for adolescents and young adults but there are many knowledge gaps related to dosing in this age group. Off-label, clinical practice frequently outpaces solid evidence as rigorous clinical trials require substantial time and resources. Murine models present an opportunity for high throughput dose finding studies to focus subsequent clinical trials in humans. This project investigated the brain and behavioural effects of an accelerated low-intensity rTMS (LI-rTMS) protocol in a young adult rodent model of chronic restraint stress (CRS). Depression and anxiety-related behaviours were induced in young adult male Sprague Dawley rats using the CRS model, followed by the 3-times-daily delivery of 10 Hz LI-rTMS, for two weeks. Behaviour was assessed using the Elevated Plus Maze and Forced Swim Test, and functional, chemical, and structural brain changes measured using magnetic resonance imaging techniques. CRS induced an agitated depression-like phenotype but therapeutic effects from the accelerated protocol were not detected. Our findings suggest that the age of rodents may impact response to CRS and LI-rTMS. Future studies should also examine higher intensities of rTMS and accelerated theta burst protocols.

Published
2022
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83. Fructose Protects Against Acetaminophen‐Induced Hepatotoxicity Mainly by Activating the Carbohydrate‐Response Element‐Binding Protein α–Fibroblast Growth Factor 21 Axis in Mice

Author

Deqiang Zhang, Sujuan Wang, Erin Ospina, Omar Shabandri, Daniel Lank, Jephte Y. Akakpo, Zifeng Zhao, Meichan Yang, Jun Wu, Hartmut Jaeschke, Pradip Saha, Xin Tong, and Lei Yin

Subjects
Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Acetaminophen (N‐acetyl‐para‐aminophenol [APAP]) overdose is the most common cause of drug‐induced liver injury in the Western world and has limited therapeutic options. As an important dietary component intake, fructose is mainly metabolized in liver, but its impact on APAP‐induced liver injury is not well established. We aimed to examine whether fructose supplementation could protect against APAP‐induced hepatotoxicity and to determine potential fructose‐sensitive intracellular mediators. We found that both high‐fructose diet feeding before APAP injection and fructose gavage after APAP injection reduced APAP‐induced liver injury with a concomitant induction of the hepatic carbohydrate‐response element‐binding protein α (ChREBPα)–fibroblast growth factor 21 (FGF21) pathway. In contrast, Chrebpα liver‐specific‐knockout (Chrebpα‐LKO) mice failed to respond to fructose following APAP overdose, suggesting that ChREBPα is the essential intracellular mediator of fructose‐induced hepatoprotective action. Primary mouse hepatocytes with deletion of Fgf21 also failed to show fructose protection against APAP hepatotoxicity. Furthermore, overexpression of FGF21 in the liver was sufficient to reverse liver toxicity in APAP‐injected Chrebpα‐LKO mice. Conclusion: Fructose protects against APAP‐induced hepatotoxicity likely through its ability to activate the hepatocyte ChREBPα–FGF21 axis.

Published
2021
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84. Liver-specific deletion of mechanistic target of rapamycin does not protect against acetaminophen-induced liver injury in mice

Author

Hua Sun, Hong-Min Ni, Jennifer M. McCracken, Jephte Y Akakpo, Sam Fulte, Tara McKeen, Hartmut Jaeschke, Hua Wang, and Wen-Xing Ding

Subjects
Acetaminophen (APAP), Autophagy, Hepatotoxicity, Liver injury, Liver regeneration, Mechanistic target of rapamycin (mTOR), Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Background: Acetaminophen (APAP) overdose can cause liver injury and liver failure, which is one of the most common causes of drug-induced liver injury in the United States. Pharmacological activation of autophagy by inhibiting mechanistic target of rapamycin (mTOR) protects against APAP-induced liver injury likely via autophagic removal of APAP-adducts and damaged mitochondria. In the present study, we aimed to investigate the role of genetic ablation of mTOR pathways in mouse liver in APAP-induced liver injury and liver repair/regeneration. Methods: Albumin-Cre (Alb-Cre) mice, mTORf/f and Raptorf/f mice (C57BL/6J background) were crossbred to produce liver-specific mTOR knockout (L-mTOR KO, Alb Cre+/-, mTORf/f) and liver-specific Raptor KO (L-Raptor, Alb Cre+/-, Raptor f/f) mice. Alb-Cre littermates were used as wild-type (WT) mice. These mice were treated with APAP for various time points for up to 48 h. Liver injury, cell proliferation, autophagy and mTOR activation were determined. Results: We found that genetic deletion of neither Raptor, an important adaptor protein in mTOR complex 1, nor mTOR, in the mouse liver significantly protected against APAP-induced liver injury despite increased hepatic autophagic flux. Genetic deletion of Raptor or mTOR in mouse livers did not affect APAP metabolism and APAP-induced c-Jun N-terminal kinase (JNK) activation, but slightly improved mouse survival likely due to increased hepatocyte proliferation. Conclusions: Our results indicate that genetic ablation of mTOR in mouse livers does not protect against APAP-induced liver injury but may slightly improve liver regeneration and mouse survival after APAP overdose.

Published
2021
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85. Mitochondrial Dynamics in Drug-Induced Liver Injury

Author

Anup Ramachandran, David S. Umbaugh, and Hartmut Jaeschke

Subjects
drug-induced liver injury, acetaminophen, mitochondrial dynamics, fusion, fission, Medicine (General), R5-920
Abstract

Mitochondria have been studied for decades from the standpoint of metabolism and ATP generation. However, in recent years mitochondrial dynamics and its influence on bioenergetics and cellular homeostasis is also being appreciated. Mitochondria undergo regular cycles of fusion and fission regulated by various cues including cellular energy requirements and pathophysiological stimuli, and the network of critical proteins and membrane lipids involved in mitochondrial dynamics is being revealed. Hepatocytes are highly metabolic cells which have abundant mitochondria suggesting a biologically relevant role for mitochondrial dynamics in hepatocyte injury and recovery. Here we review information on molecular mediators of mitochondrial dynamics and their alteration in drug-induced liver injury. Based on current information, it is evident that changes in mitochondrial fusion and fission are hallmarks of liver pathophysiology ranging from acetaminophen-induced or cholestatic liver injury to chronic liver diseases. These alterations in mitochondrial dynamics influence multiple related mitochondrial responses such as mitophagy and mitochondrial biogenesis, which are important adaptive responses facilitating liver recovery in several contexts, including drug-induced liver injury. The current focus on characterization of molecular mechanisms of mitochondrial dynamics is of immense relevance to liver pathophysiology and have the potential to provide significant insight into mechanisms of liver recovery and regeneration after injury.

Published
2021
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86. Chronic Stimulation Improves Motor Performance in an Ambulatory Rat Model of Spinal Cord Injury

Author

Jordan A. Borrell, Domenico Gattozzi, Dora Krizsan-Agbas, Matthew W. Jaeschke, Randolph J. Nudo, and Shawn B. Frost

Subjects
activity dependent stimulation, neuromodulation, spinal cord injury, closed-loop, spike-triggered intraspinal microstimulation, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Background: The purpose of this proof-of-concept feasibility study was to determine if spike-triggered intraspinal microstimulation (ISMS), a form of activity dependent stimulation (ADS), results in improved motor performance in an ambulatory rat model of spinal cord injury (SCI). Methods: Experiments were carried out in adult male Sprague Dawley rats with moderate thoracic contusion injury. Rats were assigned to one of two groups: Control or ADS therapy. Four weeks post-SCI, all rats were implanted with a recording microelectrode in the left hindlimb motor cortex and a fine-wire stimulating electrode in the contralateral lumbar spinal cord. ADS was administered for 4 hours/day, 4 days/week, for 4 weeks. During therapy sessions, single-unit spikes were discriminated in real time in the hindlimb motor cortex and used to trigger stimulation in the spinal cord ventral horn. Control rats were similarly implanted with electrodes but did not receive stimulation therapy. Results: Motor performances of each rat were evaluated before SCI contusion, once a week post-SCI for four weeks (prior to electrode implantation), and once a week post-conditioning for four weeks. Basso, Beattie, and Bresnahan (BBB) locomotor scores were significantly improved in ADS rats compared to Control rats at 1 and 2 weeks after initiation of therapy. Foot fault scores on the Horizontal Ladder were significantly improved in ADS rats compared to pre-therapy ADS and Control rats after 1 week of therapy and recovered to near pre-injury scores after 3 weeks of therapy. The Ledged Beam test showed deficits after SCI in both ADS and Control rats but there were no significant differences between groups after 4 weeks of ADS therapy. Conclusions: These results show that chronic stimulation after spinal cord injury using a methodology of spike-triggered ISMS enhances behavioral recovery of locomotor function as measured by the BBB score and the Horizontal Ladder task. However, it is still uncertain if the behavioral improvements seen were dependent on spike-triggered ISMS.

Published
2023
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88. Radiomolecular Theranostics With Fibroblast-Activation-Protein Inhibitors and Peptides.

Author

Baum, Richard P., Novruzov, Emil, Zhao, Tianzhi, Greifenstein, Lukas, Jakobsson, Vivianne, Perrone, Elisabetta, Mishra, Aditi, Eismant, Aleksandr, Ghai, Kriti, Klein, Ortwin, Jaeschke, Bastian, Benz-Zils, Daniel, Cardinale, Jens, Mori, Yuriko, Giesel, Frederik L., and Zhang, Jingjing

Abstract

The advancement of theranostics, which combines therapeutic and diagnostic capabilities in oncology, has significantly impacted cancer management. This review explores fibroblast activation protein (FAP) expression in the tumor microenvironment (TME) and its association with various malignancies, highlighting its potential as a theranostic marker for PET/CT imaging using FAP-targeted tracers and for FAP-targeted radiopharmaceutical therapy. We examine the development and clinical applications of FAP inhibitors (FAPIs) and peptides, providing insights into their diagnostic accuracy, initial therapeutic efficacy, and clinical impact across diverse cancer types, as well as the synthesis of novel FAP-targeted ligands. This review aims to showcase the promising outcomes and challenges in integrating FAP-targeted approaches into cancer management. [ABSTRACT FROM AUTHOR]

Published
2024
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89. Scale-up and sustainability of a personalized end-of-life care intervention: a longitudinal mixed-methods study

Author

Alyson Takaoka, Benjamin Tam, Meredith Vanstone, France J. Clarke, Neala Hoad, Marilyn Swinton, Feli Toledo, Anne Boyle, Anne Woods, Erick H. Duan, Diane Heels-Ansdell, Lily Waugh, Mark Soth, Jill Rudkowski, Waleed Alhazzani, Dan Perri, Tania Ligori, Roman Jaeschke, Nicole Zytaruk, and Deborah J. Cook

Subjects
Critical care, Quality improvement, Dying, Death, Palliative care, Spiritual care, Public aspects of medicine, RA1-1270
Abstract

Abstract Background Scaling-up and sustaining healthcare interventions can be challenging. Our objective was to describe how the 3 Wishes Project (3WP), a personalized end-of-life intervention, was scaled-up and sustained in an intensive care unit (ICU). Methods In a longitudinal mixed-methods study from January 12,013 - December 31, 2018, dying patients and families were invited to participate if the probability of patient death was > 95% or after a decision to withdraw life support. A research team member or bedside clinician learned more about each of the patients and their family, then elicited and implemented at least 3 personalized wishes for patients and/or family members. We used a qualitative descriptive approach to analyze interviews and focus groups conducted with 25 clinicians who cared for the enrolled patients. We used descriptive statistics to summarize patient, wish, and clinician characteristics, and analyzed outcome data in quarters using Statistical Process Control charts. The primary outcome was enrollment of terminally ill patients and respective families; the secondary outcome was the number of wishes per patient; tertiary outcomes included wish features and stakeholder involvement. Results Both qualitative and quantitative analyses suggested a three-phase approach to the scale-up of this intervention during which 369 dying patients were enrolled, having 2039 terminal wishes implemented. From a research project to clinical program to an approach to practice, we documented a three-fold increase in enrolment with a five-fold increase in total wishes implemented, without a change in cost. Beginning as a study, the protocol provided structure; starting gradually enabled frontline staff to experience and recognize the value of acts of compassion for patients, families, and clinicians. The transition to a clinical program was marked by handover from the research staff to bedside staff, whereby project catalysts mentored project champions to create staff partnerships, and family engagement became more intentional. The final transition involved empowering staff to integrate the program as an approach to care, expanding it within and beyond the organization. Conclusions The 3WP is an end-of-life intervention which was implemented as a study, scaled-up into a clinical program, and sustained by becoming integrated into practice as an approach to care.

Published
2021
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90. p53-Independent Induction of p21 Fails to Control Regeneration and Hepatocarcinogenesis in a Murine Liver Injury ModelSummary

Author

Laura Elisa Buitrago-Molina, Silke Marhenke, Diana Becker, Robert Geffers, Timo Itzel, Andreas Teufel, Hartmut Jaeschke, André Lechel, Kristian Unger, Jovana Markovic, Amar Deep Sharma, Jens U. Marquardt, Michael Saborowski, Anna Saborowski, and Arndt Vogel

Subjects
DNA Damage, Oxidative Stress Response, CHK2, HCC, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Background & Aims: A coordinated stress and regenerative response is important after hepatocyte damage. Here, we investigate the phenotypes that result from genetic abrogation of individual components of the checkpoint kinase 2/transformation-related protein 53 (p53)/cyclin-dependent kinase inhibitor 1A (p21) pathway in a murine model of metabolic liver injury. Methods: Nitisinone was reduced or withdrawn in Fah-/- mice lacking Chk2, p53, or p21, and survival, tumor development, liver injury, and regeneration were analyzed. Partial hepatectomies were performed and mice were challenged with the Fas antibody Jo2. Results: In a model of metabolic liver injury, loss of p53, but not Chk2, impairs the oxidative stress response and aggravates liver damage, indicative of a direct p53-dependent protective effect on hepatocytes. Cell-cycle control during chronic liver injury critically depends on the presence of both p53 and its downstream effector p21. In p53-deficient hepatocytes, unchecked proliferation occurs despite a strong induction of p21, showing a complex interdependency between p21 and p53. The increased regenerative potential in the absence of p53 cannot fully compensate the surplus injury and is not sufficient to promote survival. Despite the distinct phenotypes associated with the loss of individual components of the DNA damage response, gene expression patterns are dominated by the severity of liver injury, but reflect distinct effects of p53 on proliferation and the anti-oxidative stress response. Conclusions: Characteristic phenotypes result from the genetic abrogation of individual components of the DNA damage-response cascade in a liver injury model. The extent to which loss of gene function can be compensated, or affects injury and proliferation, is related to the level at which the cascade is interrupted. Accession numbers of repository for expression microarray data: GSE156983, GSE156263, GSE156852, and GSE156252.

Published
2021
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91. Coupled Oceanic and Atmospheric Controls of Deglacial Southeastern South America Precipitation and Western South Atlantic Productivity

Author

Karl J. F. Meier, Andrea Jaeschke, Janet Rethemeyer, Cristiano M. Chiessi, Ana Luiza S. Albuquerque, Vincent Wall, Oliver Friedrich, and André Bahr

Subjects
organic/inorganic geochemistry, South American Monsoon System, land-ocean teleconnection, South Atlantic Convergence Zone, last deglacial and holocene, South American Low Level Jet, Science, General. Including nature conservation, geographical distribution, QH1-199.5
Abstract

Various mechanisms were proposed as substantial drivers of (sub)tropical South American hydroclimate changes during the last deglaciation. However, the interpretation of past precipitation records from the regions affected by the South American Summer Monsoon, the dominant hydroclimatic system in (sub)tropical South America, still insufficiently consider feedbacks between oceanic and atmospheric processes evident in modern observational data. Here, we evaluate ocean-atmosphere feedbacks active in the region from 19 to 4 ka based on a multi-proxy record comprising lipid biomarker, bulk sediment elemental composition and foraminiferal geochemistry from a sediment core retrieved from the tropical western South Atlantic offshore eastern Brazil at ~22°S. Our proxy data together with existing paleoclimate records show that the consideration of large scale synoptic climatic features across South America is crucial for understanding the past spatio-temporal rainfall variability, especially during the last deglaciation. While the paleohydrological data from our study site show relatively stable precipitation across the deglaciation in the core region of the South Atlantic Convergence Zone, distinct hydroclimatic gradients developed across the continent during Heinrich Stadial 1, which climaxed at ~16 ka. By then, the prevalent atmospheric and oceanic configuration caused more frequent extreme climatic events associated with positive rainfall in the northern portion of eastern South America and in the southeastern portion of the continent. These climatic extremes resulted from substantial warming of the sub(tropical) western South Atlantic sea surface that fostered oceanic moisture transport towards the continent and the reconfiguration of quasi-stationary atmospheric patterns. We further find that enhanced continental precipitation in combination with low glacial sea level strongly impacted marine ecosystems via enhanced terrigenous organic matter input in line with augmented nutrient release to the ocean. Extreme rainfall events similar to those that occurred during Heinrich Stadial 1 are likely to recur in South America as a consequence of global warming, because the projected reduction of the intra-hemispheric temperature gradient may lead to the development of atmospheric patterns similar to those in force during Heinrich Stadial 1.

Published
2022
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92. Emerging spatial prioritization for biodiversity conservation indicated by climate change velocity

Author

Qi Lai, Samuel Hoffmann, Anja Jaeschke, and Carl Beierkuhnlein

Subjects
Climate change velocity, Europe, Natura 2000, Protected area management, Biogeographical regions, Biodiversity conservation, Ecology, QH540-549.5
Abstract

Anthropogenic climate change is challenging biodiversity conservation worldwide. Climate change metrics derived from future climate predictions help to assess potential impacts of climate change on biodiversity. Here we calculated future climate change velocities across biogeographical regions of terrestrial Europe and the Natura 2000 protected area network, the largest protected area network on Earth. We applied climate projections for the year 2070, considering two emission scenarios, six global climate models and a fine spatial resolution. Areas with very high climate change velocity were identified as climate change hotspots, while areas with very low velocity were recognized as coldspots. We further revealed where and to what extent climate change hotspots and coldspots coincide with Natura 2000 sites. We found that climate change velocities are projected highest in the Continental and Boreal regions, and lowest in the Mediterranean and Anatolian regions. However, the Alpine region will likely contain largest areal proportions of climate change hotspots, while areal proportions of coldspots are projected largest in the Mediterranean region. High mountain regions such as the Alps show a high proportion of Natura 2000 sites that coincide with climate change hotspots. Both, hotspots and coldspots, are geographically associated with areas of topographic diversity. Low topographical diversity indicates high climate change exposure. The impact of hotspots increases with spatial isolation. Oceanic climate buffers climate change exposure in contrast to continental climate. However, continental regions of Europe tend to exhibit less spatial isolation. We recommend conservation action in climate change hotspots and coldspots to simultaneously protect the most climate-exposed biodiversity as well as climate change refugia. Climate change hotspots and coldspots overlapping with Natura 2000 sites should be considered priority conservation sites because new protected areas are hard to realize in densely populated landscapes of Europe. This study directs European conservation management and policy towards meeting international conservation goals in a climate-smart way.

Published
2022
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98. Association of body surface scanner-based abdominal volume with parameters of the Metabolic Syndrome and comparison with manually measured waist circumference

Author

Lina Jaeschke, Astrid Steinbrecher, Guido Hansen, Stefan Sommer, Carolin Adler, Jürgen Janke, and Tobias Pischon

Subjects
Medicine, Science
Abstract

Abstract To investigate abdominal volume determined by a new body scanner algorithm as anthropometric marker for Metabolic Syndrome (MetS) and its parameters compared to manually measured waist circumference (WC), we performed body scans in 411 participants (38% men, 20-81 years). WC and triglyceride, HDL-cholesterol, and fasting glucose concentrations, and blood pressure were assessed as MetS parameters. We used Spearman correlations and linear regression to investigate associations and goodness-of-fit (R², BIC) of abdominal volume and WC with MetS parameters, and logistic regression to analyse the discriminative power of WC and abdominal volume to assess likelihoods of MetS components and MetS. Correlations with triglyceride, HDL-cholesterol, and glucose concentration were slightly stronger for abdominal volume (r; 0.32, −0.32, and 0.34, respectively) than for WC (0.28, −0.28, and 0.29, respectively). Explained variances in MetS parameters were slightly higher and goodness-of-fit slightly better for abdominal volume than for WC, but differences were small. Exemplarily, glucose levels were 0.28 mmol/L higher (R² = 0.25; BIC = 945.5) per 1-SD higher WC, and 0.35 mmol/L higher (R² = 0.28; BIC = 929.1) per 1-SD higher abdominal volume. The discriminative power to estimate MetS components was similar for WC and abdominal volume. Our data show that abdominal volume allows metabolic characterization comparable to established WC.

Published
2020
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100. proMAD: semiquantitative densitometric measurement of protein microarrays

Author

Anna Jaeschke, Hagen Eckert, and Laura J. Bray

Subjects
Membrane antibody array, Protein microarray, Densitometry, Web application, Python, Computer applications to medicine. Medical informatics, R858-859.7, Biology (General), QH301-705.5
Abstract

Abstract Background Protein microarrays are a versatile and widely used tool for analyzing complex protein mixtures. Membrane arrays utilize antibodies which are captured on a membrane to specifically immobilize several proteins of interest at once. Using detection antibodies, the bound protein-antibody-complex is converted into visual signals, which can be quantified using densitometry. The reliability of such densitometric assessments depends on a variety of factors, not only sample preparation and the choice of acquisition device but also the selected analysis software and the algorithms used for readout and processing data. Currently available software packages use a single image of a membrane at an optimal exposure time selected for that specific experimental framework. This selection is based on a user’s best guess and is subject to inter-user variability or the acquisition device algorithm. With modern image acquisition systems proving the capacity to collect signal development over time, this information can be used to improve densitometric measurements. Here we introduce proMAD, a toolkit for protein microarray analysis providing a novel systemic approach for the quantification of membrane arrays based on the kinetics of the analytical reaction. Results Briefly, our toolkit ensures an exact membrane alignment, utilizing basic computer vision techniques. It also provides a stable method to estimate the background light level. Finally, we model the light production over time, utilizing the knowledge about the reaction kinetics of the underlying horseradish peroxidase-based signal detection method. Conclusion proMAD incorporates the reaction kinetics of the enzyme to model the signal development over time for each membrane creating an individual, self-referencing concept. Variations of membranes within a given experimental set up can be accounted for, allowing for a better comparison of such. While the open-source library can be implemented in existing workflows and used for highly user-tailored analytic setups, the web application, on the other hand, provides easy platform-independent access to the core algorithm to a wide range of researchers. proMAD’s inherent flexibility has the potential to cover a wide range of use-cases and enables the automation of data analytic tasks.

Published
2020
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