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1. Natural killer cells and single nucleotide polymorphisms of specific ion channels and receptor genes in myalgic encephalomyelitis/chronic fatigue syndrome

Author

Marshall-Gradisnik S, Huth T, Chacko A, Johnston S, Smith P, and Staines D

Subjects
Transient Receptor Potential Ion Channels, Acetylcholine, Chronic Fatigue Syndrome, Muscarinic Receptors, Single Nucleotide Polymorphisms, Natural Killer Cells., Medicine (General), R5-920, Genetics, QH426-470
Abstract

Sonya Marshall-Gradisnik,1,2 Teilah Huth,1,2 Anu Chacko,1,2 Samantha Johnston,1,2 Pete Smith,2 Donald Staines21School of Medical Science, 2National Centre for Neuroimmunology and Emerging Diseases, Menzies Health Institute Queensland, Griffith University, Gold Coast, QLD, Australia Aim: The aim of this paper was to determine natural killer (NK) cytotoxic activity and if single nucleotide polymorphisms (SNPs) and genotypes in transient receptor potential (TRP) ion channels and acetylcholine receptors (AChRs) were present in isolated NK cells from previously identified myalgic encephalomyelitis (ME)/chronic fatigue syndrome (CFS) patients. Subjects and methods: A total of 39 ME/CFS patients (51.69±2 years old) and 30 unfatigued controls (47.60±2.39 years old) were included in this study. Patients were defined according to the 1994 Centers for Disease Control and Prevention criteria. Flow cytometry protocols were used to examine NK cytotoxic activity. A total of 678 SNPs from isolated NK cells were examined for 21 mammalian TRP ion channel genes and for nine mammalian AChR genes via the Agena Bioscience iPlex Gold assay. SNP association and genotype was determined using analysis of variance and Plink software. Results: ME/CFS patients had a significant reduction in NK percentage lysis of target cells (17%±4.68%) compared with the unfatigued control group (31%±6.78%). Of the 678 SNPs examined, eleven SNPs for TRP ion channel genes (TRPC4, TRPC2, TRPM3, and TRPM8) were identified in the ME/CFS group. Five of these SNPs were associated with TRPM3, while the remainder were associated with TRPM8, TRPC2, and TRPC4 (P

Published
2016

2. QPACE -- a QCD parallel computer based on Cell processors

Author

Baier, H., Boettiger, H., Drochner, M., Eicker, N., Fischer, U., Fodor, Z., Frommer, A., Gomez, C., Goldrian, G., Heybrock, S., Hierl, D., Hüsken, M., Huth, T., Krill, B., Lauritsen, J., Lippert, T., Maurer, T., Mendl, B., Meyer, N., Nobile, A., Ouda, I., Pivanti, M., Pleiter, D., Ries, M., Schäfer, A., Schick, H., Schifano, F., Simma, H., Solbrig, S., Streuer, T., Sulanke, K. -H., Tripiccione, R., Vogt, J. -S., Wettig, T., and Winter, F.

Subjects
High Energy Physics - Lattice, Computer Science - Hardware Architecture
Abstract

QPACE is a novel parallel computer which has been developed to be primarily used for lattice QCD simulations. The compute power is provided by the IBM PowerXCell 8i processor, an enhanced version of the Cell processor that is used in the Playstation 3. The QPACE nodes are interconnected by a custom, application optimized 3-dimensional torus network implemented on an FPGA. To achieve the very high packaging density of 26 TFlops per rack a new water cooling concept has been developed and successfully realized. In this paper we give an overview of the architecture and highlight some important technical details of the system. Furthermore, we provide initial performance results and report on the installation of 8 QPACE racks providing an aggregate peak performance of 200 TFlops., Comment: 21 pages. Poster by T. Maurer and plenary talk by D. Pleiter presented at the "XXVII International Symposium on Lattice Field Theory", July 26-31 2009, Peking University, Beijing, China. Information on recent Green500 ranking added and list of authors extended

Published
2009

4. Status of the QPACE Project

Author

Baier, H., Boettiger, H., Drochner, M., Eicker, N., Fischer, U., Fodor, Z., Goldrian, G., Heybrock, S., Hierl, D., Huth, T., Krill, B., Lauritsen, J., Lippert, T., Maurer, T., McFadden, J., Meyer, N., Nobile, A., Ouda, I., Pivanti, M., Pleiter, D., Schäfer, A., Schick, H., Schifano, F., Simma, H., Solbrig, S., Streuer, T., Sulanke, K. H., Tripiccione, R., Wettig, T., and Winter, F.

Subjects
High Energy Physics - Lattice
Abstract

We give an overview of the QPACE project, which is pursuing the development of a massively parallel, scalable supercomputer for LQCD. The machine is a three-dimensional torus of identical processing nodes, based on the PowerXCell 8i processor. The nodes are connected by an FPGA-based, application-optimized network processor attached to the PowerXCell 8i processor. We present a performance analysis of lattice QCD codes on QPACE and corresponding hardware benchmarks., Comment: 7 pages, poster presented at the XXVI International Symposium on Lattice Field Theory, July 14-19, 2008, Williamsburg, Virginia, USA

Published
2008

5. QPACE: power-efficient parallel architecture based on IBM PowerXCell 8i

Author

Baier, H., Boettiger, H., Drochner, M., Eicker, N., Fischer, U., Fodor, Z., Frommer, A., Gomez, C., Goldrian, G., Heybrock, S., Hierl, D., Hüsken, M., Huth, T., Krill, B., Lauritsen, J., Lippert, T., Maurer, T., Mendl, B., Meyer, N., Nobile, A., Ouda, I., Pivanti, M., Pleiter, D., Ries, M., Schäfer, A., Schick, H., Schifano, F., Simma, H., Solbrig, S., Streuer, T., Sulanke, K.-H., Tripiccione, R., Vogt, J.-S., Wettig, T., and Winter, F.

Abstract

Abstract: QPACE is a novel massively parallel architecture optimized for lattice QCD simulations. Each node comprises an IBM PowerXCell 8i processor. The nodes are interconnected by a custom 3-dimensional torus network implemented on an FPGA. The architecture was systematically optimized with respect to power consumption. This put QPACE in the number one spot on the Green500 List published in November 2009. In this paper we give an overview of the architecture and highlight the steps taken to improve power efficiency.

Published
2024
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8. QPACE: power-efficient parallel architecture based on IBM PowerXCell 8i

Author

Baier, H., Boettiger, H., Drochner, M., Eicker, N., Fischer, U., Fodor, Z., Frommer, A., Gomez, C., Goldrian, G., Heybrock, S., Hierl, D., Hüsken, M., Huth, T., Krill, B., Lauritsen, J., Lippert, T., Maurer, T., Mendl, B., Meyer, N., Nobile, A., Ouda, I., Pivanti, M., Pleiter, D., Ries, M., Schäfer, A., Schick, H., Schifano, F., Simma, H., Solbrig, S., Streuer, T., Sulanke, K.-H., Tripiccione, R., Vogt, J.-S., Wettig, T., and Winter, F.

Published
2010
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22. Heat Shock Proteins and Regulatory T Cells

Author

Brenu, E. W., Staines, D. R., Tajouri, L., Huth, T., Ashton, K. J., and Marshall-Gradisnik, S. M.

Subjects
endocrine system, Article Subject, biological sciences, hemic and immune systems, chemical and pharmacologic phenomena
Abstract

Heat shock proteins (HSPs) are important molecules required for ideal protein function. Extensive research on the functional properties of HSPs indicates that HSPs may be implicated in a wide range of physiological functions including immune function. In the immune system, HSPs are involved in cell proliferation, differentiation, cytokine release, and apoptosis. Therefore, the ability of the immune system, in particular immune cells, to function optimally and in unison with other physiological systems is in part dependent on signaling transduction processes, including bidirectional communication with HSPs. Regulatory T cells (Tregs) are important T cells with suppressive functions and impairments in their function have been associated with a number of autoimmune disorders. The purpose of this paper is to examine the relationship between HSPs and Tregs. The interrelationship between cells and proteins may be important in cellular functions necessary for cell survival and expansion during diseased state.

Published
2013
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29. Palmy latitudes.

Author

Huth, T.

Subjects
HEALTH resorts
Abstract

Travels to the Two Bunch Palms spa in Southern California. Relaxation; Mineral springs; Mud baths; Massage; Aromatherapy; Food; Scenic descriptions.

Published
1990

30. A change of peso.

Author

Huth, T.

Subjects
TRAVEL
Abstract

Presents Yelapa, down the coast from Puerto Vallarta in the Mexican Pacific, a paradise for the world weary traveler. How to get there; Accommodations; Things to do.

Published
1989

32. Construction Techniques of a Molecular Hydrogen Laser.

Author

ARIZONA UNIV TUCSON DEPT OF CHEMISTRY, Babis,J S, Huth,T C, Denton,M B, ARIZONA UNIV TUCSON DEPT OF CHEMISTRY, Babis,J S, Huth,T C, and Denton,M B

Abstract

Simple techniques are described for construction of a discharge channel, and spark gap trigger electrode for a travelling-wave excited molecular hydrogen laser., Prepared in cooperation with Beckman Instruments, Irvine, CA.

Published
1985

33. Photoionization Mass Spectrometry with VUV Hydrogen Laser Source.

Author

ARIZONA UNIV TUCSON DEPT OF CHEMISTRY, Huth,T. C., Denton,M. B., ARIZONA UNIV TUCSON DEPT OF CHEMISTRY, Huth,T. C., and Denton,M. B.

Abstract

Results are presented which characterize the VUV H2 laser as a selective ion source for analytical mass spectrometry of easily ionized compounds. The types of compounds ionized below the photon energy of 7.8 eV include many pharmaceuticals and drugs of abuse, such as cocaine, heroin, phencyclidine, methamphetamine, and LSD. H2 laser photoionization has produced parent ions only, for all compounds studied thus far. The selectivity of the threshold photoionization process is very high, as compounds within as little as 0.2 eV above the threshold are completely rejected. Photoactive species can be injected as solutions in appropriate organic solvents, without interference from the solvent. At low levels, ion signals are observed, which are due to acceleration of stray electrons in the ion source. The electrons result from interaction of scattered laser radiation with metal surfaces. Additional keywords: Chemical analysis; Optical properties; Naval research. (Author)

Published
1985

37. Sea-anemone toxin ATX-II elicits A-fiber-dependent pain and enhances resurgent and persistent sodium currents in large sensory neurons

Author

Klinger Alexandra B, Eberhardt Mirjam, Link Andrea S, Namer Barbara, Kutsche Lisa K, Schuy E, Sittl Ruth, Hoffmann Tali, Alzheimer Christian, Huth Tobias, Carr Richard W, and Lampert Angelika

Subjects
Patch-clamp, Psychophysics, Differential nerve block, Sensory neurons, Itch, Sodium channels, RT-qPCR, SCN4b, Pathology, RB1-214
Abstract

Abstract Background Gain-of-function mutations of the nociceptive voltage-gated sodium channel Nav1.7 lead to inherited pain syndromes, such as paroxysmal extreme pain disorder (PEPD). One characteristic of these mutations is slowed fast-inactivation kinetics, which may give rise to resurgent sodium currents. It is long known that toxins from Anemonia sulcata, such as ATX-II, slow fast inactivation and skin contact for example during diving leads to various symptoms such as pain and itch. Here, we investigated if ATX-II induces resurgent currents in sensory neurons of the dorsal root ganglion (DRGs) and how this may translate into human sensations. Results In large A-fiber related DRGs ATX-II (5 nM) enhances persistent and resurgent sodium currents, but failed to do so in small C-fiber linked DRGs when investigated using the whole-cell patch-clamp technique. Resurgent currents are thought to depend on the presence of the sodium channel β4-subunit. Using RT-qPCR experiments, we show that small DRGs express significantly less β4 mRNA than large sensory neurons. With the β4-C-terminus peptide in the pipette solution, it was possible to evoke resurgent currents in small DRGs and in Nav1.7 or Nav1.6 expressing HEK293/N1E115 cells, which were enhanced by the presence of extracellular ATX-II. When injected into the skin of healthy volunteers, ATX-II induces painful and itch-like sensations which were abolished by mechanical nerve block. Increase in superficial blood flow of the skin, measured by Laser doppler imaging is limited to the injection site, so no axon reflex erythema as a correlate for C-fiber activation was detected. Conclusion ATX-II enhances persistent and resurgent sodium currents in large diameter DRGs, whereas small DRGs depend on the addition of β4-peptide to the pipette recording solution for ATX-II to affect resurgent currents. Mechanical A-fiber blockade abolishes all ATX-II effects in human skin (e.g. painful and itch-like paraesthesias), suggesting that it mediates its effects mainly via activation of A-fibers.

Published
2012
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38. Heat Shock Proteins and Regulatory T Cells

Author

W. Brenu, E., R. Staines, D., Tajouri, L., Huth, T., J. Ashton, K., and M. Marshall-Gradisnik, S.

Abstract

Heat shock proteins (HSPs) are important molecules required for ideal protein function. Extensive research on the functional properties of HSPs indicates that HSPs may be implicated in a wide range of physiological functions including immune function. In the immune system, HSPs are involved in cell proliferation, differentiation, cytokine release, and apoptosis. Therefore, the ability of the immune system, in particular immune cells, to function optimally and in unison with other physiological systems is in part dependent on signaling transduction processes, including bidirectional communication with HSPs. Regulatory T cells (Tregs) are important T cells with suppressive functions and impairments in their function have been associated with a number of autoimmune disorders. The purpose of this paper is to examine the relationship between HSPs and Tregs. The interrelationship between cells and proteins may be important in cellular functions necessary for cell survival and expansion during diseased state.

Published
2013
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39. Herbal toxicity and fatal hepatic failure.

Author

Hullar, T E, Sapers, B L, Ridker, P M, Jenkins, R L, Huth, T S, and Farraye, F A

Subjects
*DISEASE complications, *HEPATIC encephalopathy, *LIVER, *MEDICINAL plants, *MULTIPLE sclerosis, *TREATMENT effectiveness
Published
1999

40. A deep learning approach to real-time Markov modeling of ion channel gating.

Author

Oikonomou E, Juli Y, Kolan RR, Kern L, Gruber T, Alzheimer C, Krauss P, Maier A, and Huth T

Abstract

The patch-clamp technique allows us to eavesdrop the gating behavior of individual ion channels with unprecedented temporal resolution. The signals arise from conformational changes of the channel protein as it makes rapid transitions between conducting and non-conducting states. However, unambiguous analysis of single-channel datasets is challenging given the inadvertently low signal-to-noise ratio as well as signal distortions caused by low-pass filtering. Ion channel kinetics are typically described using hidden Markov models (HMM), which allow conclusions on the inner workings of the protein. In this study, we present a Deep Learning approach for extracting models from single-channel recordings. Two-dimensional dwell-time histograms are computed from the idealized time series and are subsequently analyzed by two neural networks, that have been trained on simulated datasets, to determine the topology and the transition rates of the HMM. We show that this method is robust regarding noise and gating events beyond the corner frequency of the low-pass filter. In addition, we propose a method to evaluate the goodness of a predicted model by re-simulating the prediction. Finally, we tested the algorithm with data recorded on a patch-clamp setup. In principle, it meets the requirements for model extraction during an ongoing recording session in real-time., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published
2024
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41. Proteomic profiling reveals CEACAM6 function in driving gallbladder cancer aggressiveness through integrin receptor, PRKCD and AKT/ERK signaling.

Author

Sugiyanto RN, Metzger C, Inal A, Truckenmueller F, Gür K, Eiteneuer E, Huth T, Fraas A, Heinze I, Kirkpatrick J, Sticht C, Albrecht T, Goeppert B, Poth T, Pusch S, Mehrabi A, Schirmacher P, Ji J, Ori A, and Roessler S

Subjects
Humans, Animals, Mice, Cell Line, Tumor, Cell Proliferation, Integrin beta1 metabolism, Integrin beta1 genetics, Cell Adhesion, Neoplasm Invasiveness, Signal Transduction, MAP Kinase Signaling System, Gene Expression Regulation, Neoplastic, Female, Male, Mice, Nude, Cell Adhesion Molecules metabolism, Cell Adhesion Molecules genetics, Gallbladder Neoplasms metabolism, Gallbladder Neoplasms pathology, Gallbladder Neoplasms genetics, Proteomics methods, GPI-Linked Proteins metabolism, GPI-Linked Proteins genetics, Proto-Oncogene Proteins c-akt metabolism, Cell Movement, Antigens, CD metabolism, Antigens, CD genetics, Protein Kinase C-delta metabolism, Protein Kinase C-delta genetics
Abstract

Gallbladder cancer (GBC) presents as an aggressive malignancy with poor patient outcome. Like other epithelial cancers, the mechanisms of GBC cancer progression remain vague and efforts in finding targeted therapies fall below expectations. This study combined proteomic analysis of formalin-fixed paraffin-embedded (FFPE) GBC samples, functional and molecular characterization of potential oncogenes and identification of potential therapeutic strategies for GBC. We identified Carcinoembryonic Antigen-related Cell Adhesion Molecule 6 (CEACAM6) as one of the significantly most upregulated proteins in GBC. CEACAM6 overexpression has been observed in other cancer entities but the molecular function remains unclear. Our functional analyses in vitro and in vivo mouse models revealed that CEACAM6 supported the initial steps of cancer progression and metastasis by decreasing cell adhesion and promoting migration and invasion of GBC cells. Conversely, CEACAM6 knockdown abolished GBC aggressiveness by increasing cell adhesion while reducing cell migration, cell proliferation, and colony formation. BirA-BioID followed by mass-spectrometry revealed Integrin Beta-1 (ITGB1) and Protein Kinase C Delta (PRKCD) as direct molecular and functional partners of CEACAM6 supporting GBC cell migration. ERK and AKT signaling and their downstream target genes were regulated by CEACAM6 and thus the treatment with AKT inhibitor capivasertib or ERK inhibitor ulixertinib mitigated the CEACAM6-induced migration. These findings demonstrate that CEACAM6 is crucially involved in gallbladder cancer progression by promoting migration and inhibiting cell adhesion through ERK and AKT signaling providing specific options for treatment of CEACAM6-positive cancers., (© 2024. The Author(s).)

Published
2024
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42. Phosphatidylinositol 4-Kinase III Alpha Governs Cytoskeletal Organization for Invasiveness of Liver Cancer Cells.

Author

Tran CS, Kersten J, Yan J, Breinig M, Huth T, Poth T, Colasanti O, Riedl T, Faure-Dupuy S, Diehl S, Verhoye L, Li TF, Lingemann M, Schult P, Ahlén G, Frelin L, Kühnel F, Vondran FWR, Breuhahn K, Meuleman P, Heikenwälder M, Schirmacher P, Bartenschlager R, Laketa V, Roessler S, Tschaharganeh DF, Sällberg M, and Lohmann V

Subjects
Humans, Animals, Mice, Phosphorylation, Hepacivirus, Cell Line, Tumor, Phosphotransferases (Alcohol Group Acceptor) metabolism, Phosphotransferases (Alcohol Group Acceptor) genetics, Hep G2 Cells, Hepatitis C pathology, Hepatitis C metabolism, Hepatitis C virology, RNA Interference, Liver Neoplasms pathology, Liver Neoplasms metabolism, Liver Neoplasms genetics, Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular metabolism, Carcinoma, Hepatocellular genetics, Cytoskeleton metabolism, Cytoskeleton pathology, Neoplasm Invasiveness, Paxillin metabolism, Signal Transduction, Cell Movement, Actin Depolymerizing Factors metabolism, Actin Depolymerizing Factors genetics
Abstract

Background & Aims: High expression of phosphatidylinositol 4-kinase III alpha (PI4KIIIα) correlates with poor survival rates in patients with hepatocellular carcinoma. In addition, hepatitis C virus (HCV) infections activate PI4KIIIα and contribute to hepatocellular carcinoma progression. We aimed at mechanistically understanding the impact of PI4KIIIα on the progression of liver cancer and the potential contribution of HCV in this process., Methods: Several hepatic cell culture and mouse models were used to study the functional importance of PI4KIIIα on liver pathogenesis. Antibody arrays, gene silencing, and PI4KIIIα-specific inhibitor were applied to identify the involved signaling pathways. The contribution of HCV was examined by using HCV infection or overexpression of its nonstructural protein., Results: High PI4KIIIα expression and/or activity induced cytoskeletal rearrangements via increased phosphorylation of paxillin and cofilin. This led to morphologic alterations and higher migratory and invasive properties of liver cancer cells. We further identified the liver-specific lipid kinase phosphatidylinositol 3-kinase C2 domain-containing subunit gamma (PIK3C2γ) working downstream of PI4KIIIα in regulation of the cytoskeleton. PIK3C2γ generates plasma membrane phosphatidylinositol 3,4-bisphosphate-enriched, invadopodia-like structures that regulate cytoskeletal reorganization by promoting Akt2 phosphorylation., Conclusions: PI4KIIIα regulates cytoskeleton organization via PIK3C2γ/Akt2/paxillin-cofilin to favor migration and invasion of liver cancer cells. These findings provide mechanistic insight into the contribution of PI4KIIIα and HCV to the progression of liver cancer and identify promising targets for therapeutic intervention., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2024
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43. Multicolor, Cell-Impermeable, and High Affinity BACE1 Inhibitor Probes Enable Superior Endogenous Staining and Imaging of Single Molecules.

Author

Stockinger F, Poc P, Möhwald A, Karch S, Häfner S, Alzheimer C, Sandoz G, Huth T, and Broichhagen J

Subjects
Humans, Animals, HEK293 Cells, Single Molecule Imaging methods, Amyloid Precursor Protein Secretases antagonists & inhibitors, Amyloid Precursor Protein Secretases metabolism, Aspartic Acid Endopeptidases antagonists & inhibitors, Aspartic Acid Endopeptidases metabolism, Fluorescent Dyes chemistry, Fluorescence Resonance Energy Transfer
Abstract

The prevailing but not undisputed amyloid cascade hypothesis places the β-site of APP cleaving enzyme 1 (BACE1) center stage in Alzheimer's Disease pathogenesis. Here, we investigated functional properties of BACE1 with novel tag- and antibody-free labeling tools, which are conjugates of the BACE1-inhibitor IV (also referred to as C3) linked to different impermeable Alexa Fluor dyes. We show that these fluorescent small molecules bind specifically to BACE1, with a 1:1 labeling stoichiometry at their orthosteric site. This is a crucial property especially for single-molecule and super-resolution microscopy approaches, allowing characterization of the dyes' labeling capabilities in overexpressing cell systems and in native neuronal tissue. With multiple colors at hand, we evaluated BACE1-multimerization by Förster resonance energy transfer (FRET) acceptor-photobleaching and single-particle imaging of native BACE1. In summary, our novel fluorescent inhibitors, termed Alexa-C3 , offer unprecedented insights into protein-protein interactions and diffusion behavior of BACE1 down to the single molecule level.

Published
2024
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44. Chromosome 8p engineering reveals increased metastatic potential targetable by patient-specific synthetic lethality in liver cancer.

Author

Huth T, Dreher EC, Lemke S, Fritzsche S, Sugiyanto RN, Castven D, Ibberson D, Sticht C, Eiteneuer E, Jauch A, Pusch S, Albrecht T, Goeppert B, Candia J, Wang XW, Ji J, Marquardt JU, Nahnsen S, Schirmacher P, and Roessler S

Subjects
Humans, Chromosome Deletion, Chromosome Aberrations, Chromosomes, CRISPR-Cas Systems, Synthetic Lethal Mutations, Liver Neoplasms genetics, Liver Neoplasms pathology
Abstract

Large-scale chromosomal aberrations are prevalent in human cancer, but their function remains poorly understood. We established chromosome-engineered hepatocellular carcinoma cell lines using CRISPR-Cas9 genome editing. A 33-mega-base pair region on chromosome 8p (chr8p) was heterozygously deleted, mimicking a frequently observed chromosomal deletion. Using this isogenic model system, we delineated the functional consequences of chr8p loss and its impact on metastatic behavior and patient survival. We found that metastasis-associated genes on chr8p act in concert to induce an aggressive and invasive phenotype characteristic for chr8p-deleted tumors. Genome-wide CRISPR-Cas9 viability screening in isogenic chr8p-deleted cells served as a powerful tool to find previously unidentified synthetic lethal targets and vulnerabilities accompanying patient-specific chromosomal alterations. Using this target identification strategy, we showed that chr8p deletion sensitizes tumor cells to targeting of the reactive oxygen sanitizing enzyme Nudix hydrolase 17. Thus, chromosomal engineering allowed for the identification of novel synthetic lethalities specific to chr8p loss of heterozygosity.

Published
2023
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45. 2D-dwell-time analysis with simulations of ion-channel gating using high-performance computing.

Author

Oikonomou E, Gruber T, Chandra AR, Höller S, Alzheimer C, Wellein G, and Huth T

Subjects
Kinetics, Markov Chains, Algorithms, Models, Biological, Ion Channels metabolism, Ion Channel Gating
Abstract

Single-channel patch-clamp recordings allow observing the action of a single protein complex in real time and hence the deduction of the underlying conformational changes in the ion-channel protein. Commonly, recordings are modeled using hidden Markov chains, connecting open and closed states in the experimental data with protein conformations. The rates between states denote transition probabilities that could be modified by membrane voltage or ligand binding. Modeling algorithms have to deal with limited recording bandwidth and a very noisy background. It was previously shown that the fit of two-dimensional (2D)-dwell-time histograms with simulations is very robust in that regard. Errors introduced by the low-pass filter or noise cancel out to a certain degree when comparing experimental and simulated data. In addition, the topology of models (that is, the chain of open and closed states) could be inferred from 2D-histograms. However, the 2D-fit was never applied to its full potential. A major reason may be the extremely time-consuming and often unreliable fitting process, due to the stochastic variability in the simulations. We have now solved these issues by introducing a message-passing interface (MPI) allowing massive parallel computing on a high-performance computing (HPC) cluster and obtaining ensemble solutions. With ensembles, we have demonstrated how important ranked solutions are for difficult tasks related to a noisy background, fast gating events beyond the corner frequency of the low-pass filter, and topology estimation of the underlying Markov model. Finally, we have shown that, by combining the objective function of the 2D-fit with the deviation of the current amplitude distributions, automatic determination of the current level of the conducting state is possible, even with an apparent current reduction due to low-pass filtering. Making use of an HPC cluster, the power of 2D-dwell-time analysis can be used to its fullest with minor input of the experimenter., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published
2023
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48. STAT1 and STAT3 Exhibit a Crosstalk and Are Associated with Increased Inflammation in Hepatocellular Carcinoma.

Author

Ploeger C, Schreck J, Huth T, Fraas A, Albrecht T, Charbel A, Ji J, Singer S, Breuhahn K, Pusch S, Köhler BC, Springfeld C, Schirmacher P, Mehrabi A, Goeppert B, and Roessler S

Abstract

Liver cancers, which are mostly hepatocellular carcinoma (HCC) and cholangiocarcinoma (CCA), are very aggressive tumors with poor prognosis. Therapeutic options with curative intent are largely limited to surgery and available systemic therapies show limited benefit. Signal transducer and activator of transcription 1 (STAT1) and 3 (STAT3) are key transcription factors activated by pro-inflammatory cytokines such as interferon-γ (IFN-γ) and interleukin-6 (IL-6). In this study, we combined in vitro cell culture experiments and immunohistochemical analyses of human HCC ( N = 124) and CCA ( N = 138) specimens. We observed that in the absence of STAT3, IL-6 induced the activation of STAT1 and its target genes suggesting that IL-6 derived from the tumor microenvironment may activate both STAT1 and STAT3 target genes in HCC tumor cells. In addition, STAT1 and STAT3 were highly activated in a subset of HCC, which exhibited a high degree of infiltrating CD8- and FOXP3-positive immune cells and PD-L1 expression. Our results demonstrate that STAT1 and STAT3 are expressed and activated in HCC and tumor infiltrating immune cells. In addition, HCC cases with high STAT1 and STAT3 expression also exhibited a high degree of immune cell infiltration, suggesting increased immunological tolerance.

Published
2022
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49. Aβ1-16 controls synaptic vesicle pools at excitatory synapses via cholinergic modulation of synapsin phosphorylation.

Author

Anni D, Weiss EM, Guhathakurta D, Akdas YE, Klueva J, Zeitler S, Andres-Alonso M, Huth T, and Fejtova A

Subjects
Animals, Calcium metabolism, Excitatory Postsynaptic Potentials drug effects, Female, Humans, Mice, Mice, Knockout, Neurons cytology, Neurons drug effects, Neurons metabolism, Neurotransmitter Agents metabolism, Nicotine pharmacology, Phosphorylation drug effects, Rats, Rats, Sprague-Dawley, Synaptic Vesicles physiology, alpha7 Nicotinic Acetylcholine Receptor deficiency, alpha7 Nicotinic Acetylcholine Receptor genetics, Amyloid beta-Peptides pharmacology, Peptide Fragments pharmacology, Synapses metabolism, Synapsins metabolism, Synaptic Vesicles drug effects, alpha7 Nicotinic Acetylcholine Receptor metabolism
Abstract

Amyloid beta (Aβ) is linked to the pathology of Alzheimer's disease (AD). At physiological concentrations, Aβ was proposed to enhance neuroplasticity and memory formation by increasing the neurotransmitter release from presynapse. However, the exact mechanisms underlying this presynaptic effect as well as specific contribution of endogenously occurring Aβ isoforms remain unclear. Here, we demonstrate that Aβ1-42 and Aβ1-16, but not Aβ17-42, increased size of the recycling pool of synaptic vesicles (SV). This presynaptic effect was driven by enhancement of endogenous cholinergic signalling via α7 nicotinic acetylcholine receptors, which led to activation of calcineurin, dephosphorylation of synapsin 1 and consequently resulted in reorganization of functional pools of SV increasing their availability for sustained neurotransmission. Our results identify synapsin 1 as a molecular target of Aβ and reveal an effect of physiological concentrations of Aβ on cholinergic modulation of glutamatergic neurotransmission. These findings provide new mechanistic insights in cholinergic dysfunction observed in AD.

Published
2021
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50. Prohibitin, STAT3 and SH2D4A physically and functionally interact in tumor cell mitochondria.

Author

Ploeger C, Huth T, Sugiyanto RN, Pusch S, Goeppert B, Singer S, Tabti R, Hausser I, Schirmacher P, Désaubry L, and Roessler S

Subjects
Humans, Prohibitins, Repressor Proteins pharmacology, Intracellular Signaling Peptides and Proteins metabolism, Mitochondria metabolism, Neoplasms genetics, Repressor Proteins therapeutic use, STAT3 Transcription Factor metabolism
Abstract

Chromosome 8p is frequently deleted in various cancer entities and has been shown to correlate with poor patient survival. SH2D4A is located on chromosome 8p and prevents the nuclear translocation of the pro-tumorigenic transcription factor STAT3. Here, we investigated the interaction of SH2D4A and STAT3 to shed light on the non-canonical functions of STAT3 in cooperation with the tumor suppressor SH2D4A. Using an immunoprecipitation-mass spectrometry (IP-MS) approach, we identified the mitochondrial scaffold proteins prohibitin 1 (PHB1) and prohibitin 2 (PHB2) among other proteins to potentially bind to SH2D4A. Co-immunoprecipitation and proximity ligation assays confirmed direct interactions of STAT3, PHB1, and SH2D4A in situ and in vitro. In addition, cell fractionation and immunofluorescence staining revealed co-localization of these proteins with mitochondria. These interactions were selectively interrupted by the small molecule and PHB ligand FL3. Furthermore, FL3 led to a reduction of STAT3 protein levels, STAT3 transcriptional activity, and HIF1α protein stabilization upon dimethyloxalylglycine (DMOG) treatment. Besides, mitochondrial fusion and fission markers, L-OPA1, Mfn1, and FIS1, were dysregulated upon FL3 treatment. This dysregulated morphology was accompanied by significant reduction of mitochondrial respiration, thus, FL3 significantly diminished mitochondrial respirational capacity. In contrast, SH2D4A knockout increased mitochondrial respiration, whereas FL3 reversed the effect of SH2D4A knockout. The here described results indicate that the interaction of SH2D4A and PHB1 is involved in the mitochondrial function and integrity. The demonstrated interaction with STAT3, accompanied by its reduction of transcriptional activity, further suggests that SH2D4A is linking STAT3 to its mitochondrial functions, and inhibition of PHB-interaction may have therapeutic effects in tumor cells with STAT3 activation.

Published
2020
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