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2. Femtosecond diffractive imaging with a soft-X-ray free-electron laser

Author

Chapman, HN, Barty, A, Bogan, MJ, Boutet, S, Frank, M, Hau-Riege, SP, Marchesini, S, Woods, BW, Bajt, S, Benner, WH, London, RA, Plönjes, E, Kuhlmann, M, Treusch, R, Düsterer, S, Tschentscher, T, Schneider, JR, Spiller, E, Möller, T, Bostedt, C, Hoener, M, Shapiro, DA, Hodgson, KO, Van Der Spoel, D, Burmeister, F, Bergh, M, Caleman, C, Huldt, G, Seibert, MM, Maia, FRNC, Lee, RW, Szöke, A, Timneanu, N, and Hajdu, J

Subjects
physics.optics, Biomedical Imaging, Fluids & Plasmas, Mathematical Sciences, Physical Sciences
Abstract

Theory predicts that, with an ultrashort and extremely bright coherent X-ray pulse, a single diffraction pattern may be recorded from a large macromolecule, a virus or a cell before the sample explodes and turns into a plasma. Here we report the first experimental demonstration of this principle using the FLASH soft-X-ray free-electron laser. An intense 25 fs, 4×10 13 W cm -2 pulse, containing 10 12 photons at 32 nm wavelength, produced a coherent diffraction pattern from a nanostructured non-periodic object, before destroying it at 60,000 K. A novel X-ray camera assured single-photon detection sensitivity by filtering out parasitic scattering and plasma radiation. The reconstructed image, obtained directly from the coherent pattern by phase retrieval through oversampling, shows no measurable damage, and is reconstructed at the diffraction-limited resolution. A three-dimensional data set may be assembled from such images when copies of a reproducible sample are exposed to the beam one by one. © 2006 Nature Publishing Group.

Published
2006

5. Femtosecond electronic response of atoms to ultra-intense X-rays

Author

Young, L., Kanter, E.P., Krassig, B., Li, Y., March, A.M., Pratt, S.T., Santra, R., Southworth, S.H., Rohringer, N., DiMauro, L.F., Doumy, G., Roedig, C.A., Berrah, N., Fang, L., Hoener, M., Bucksbaum, P.H., Cryan, J.P., Ghimire, S., Glownia, J.M., Reis, D.A., Bozek, J.D., Bostedt, C., and Messerschmidt, M.

Subjects
Atoms -- Properties -- Research -- Usage, X-rays -- Usage -- Research, Free electron lasers -- Usage
Abstract

An era of exploring the interactions of high-intensity, hard X-rays with matter has begun with the start-up of a hard-X-ray free-electron laser, the Linac Coherent Light Source (LCLS). Understanding how electrons in matter respond to ultra-intense X-ray radiation is essential for all applications. Here we reveal the nature of the electronic response in a free atom to unprecedented high-intensity, short-wavelength, high-fluence radiation (respectively [10.sup.18] W [cm.sup.-2], 1.5-0.6 nm, ~[10.sup.5] X-ray photons per [Å.sup.2]). At this fluence, the neon target inevitably changes during the course of a single femtosecond-duration X-ray pulse--by sequentially ejecting electrons--to produce fully-stripped neon through absorption of six photons. Rapid photoejection of inner-shell electrons produces 'hollow' atoms and an intensity-induced X-ray transparency. Such transparency, due to the presence of inner-shell vacancies, can be induced in all atomic, molecular and condensed matter systems at high intensity. Quantitative comparison with theory allows us to extract LCLS fluence and pulse duration. Our successful modelling of X-ray/atom interactions using a straightforward rate equation approach augurs favourably for extension to complex systems., X-ray crystallography has been the foundation of structural science for the past century. Indeed, almost all the atomic-scale structural knowledge that we have today has been acquired through diffraction within [...]

Published
2010
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11. Short-pulse laser induced transient structure formation and ablation studied with time-resolved coherent XUV-scattering

Author

Sokolowski-Tinten, Klaus, Barty, Anton, Boutet, Sebastien, Shymanovich, Uladzimir, Chapman, Henry, Bogan, Mike, Marchesini, Stefano, Hau-Riege, Stefan, Stojanovic, Nikola, Bonse, Jörn, Rosandi, Yudi, Urbassek, Herbert M., Tobey, Ra’anan, Ehrke, Henri, Cavalleri, Andrea, Düsterer, Stefan, Redlin, Harald, Frank, Matthias, Bajt, Sasa, Schulz, Joachim, Seibert, Marvin, Hajdu, Janos, Treusch, Rolf, Bostedt, Christoph, Hoener, M., and Möeller, T.

Published
2009
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13. A pressurized flow reactor combustion experiment interfaced with synchrotron double imaging photoelectron photoion coincidence spectroscopy.

Author

Hoener, M., Kaczmarek, D., Bierkandt, T., Bodi, A., Hemberger, P., and Kasper, T.

Subjects
*SYNCHROTRON radiation, *PHOTOIONIZATION, *CHEMICAL models, *COMBUSTION, *COINCIDENCE, *LIGHT sources, *PHOTOELECTRONS
Abstract

A new pressurized low-temperature combustion experiment has been commissioned at the Swiss Light Source, Paul Scherrer Institute. The experiment uses photoionization with tunable synchrotron radiation and double imaging photoelectron photoion coincidence (i2PEPICO) detection at the vacuum ultraviolet beamline. The experimental setup is described, including the high-pressure reactor experiment, sampling interface, and reactant delivery system. The CRF-PEPICO (Combustion Reactions Followed by Photoelectron Photoion Coincidence) endstation and VUV beamline are briefly elaborated. The novel aspects of the apparatus and the new components are elucidated in detail, such as the fluid supply system to the reactor and the reactor integration into the endstation. We also present a system overview of the experimental setup. The technical details are followed by a description of the experimental procedure used to operate the pressurized flow reactor setup. Finally, first experimental results demonstrating the capability of the setup are provided and analyzed. A major advantage of this new experiment is that the excellent isomer resolution capabilities of the i2PEPICO technique can be transferred to the investigation of reactions at elevated pressures of several bars. This enables the investigation of pressure effects on the reactivity of fuel mixtures and covers more realistic conditions found in technical combustors. The capability to obtain quantitative oxidation data is confirmed, and the main and certain intermediate species are quantified for a selected condition. The results show excellent agreement with a chemical kinetics model and previously published reference measurements performed with a gas chromatography setup. [ABSTRACT FROM AUTHOR]

Published
2020
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14. Experimental determination of the ionization potentials of the first five members of the nanodiamond series.

Author

Lenzke, K., Landt, L., Hoener, M., Thomas, H., Dahl, J. E., Liu, S. G., Carlson, R. M. K., Möller, T., and Bostedt, C.

Subjects
IONIZATION (Atomic physics), NANODIAMONDS, SPECTRUM analysis, FULLERENES, CARBON, NUCLEAR isomers
Abstract

The ionization potentials of size- and isomer-selected diamondoids (nanodiamond containing one to five crystal cages) have been measured by means of total-ion-yield spectroscopy. We find a monotonic decrease of the ionization potential with increasing diamondoid size. This experimental result is compared to recent theoretical predictions and comparable investigations on related carbon clusters, the fullerenes, which show isomer effects to be stronger than size dependence. [ABSTRACT FROM AUTHOR]

Published
2007
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15. Pharmacological characterization of designer cathinones in vitro.

Author

Simmler L, Buser T, Donzelli M, Schramm Y, Dieu LH, Huwyler J, Chaboz S, Hoener M, Liechti M, Simmler, L D, Buser, T A, Donzelli, M, Schramm, Y, Dieu, L-H, Huwyler, J, Chaboz, S, Hoener, M C, and Liechti, M E

Abstract

Background and Purpose: Designer β-keto amphetamines (e.g. cathinones, 'bath salts' and 'research chemicals') have become popular recreational drugs, but their pharmacology is poorly characterized.Experimental Approach: We determined the potencies of cathinones to inhibit DA, NA and 5-HT transport into transporter-transfected HEK 293 cells, DA and 5-HT efflux from monoamine-preloaded cells, and monoamine receptor binding affinity.Key Results: Mephedrone, methylone, ethylone, butylone and naphyrone acted as non-selective monoamine uptake inhibitors, similar to cocaine. Mephedrone, methylone, ethylone and butylone also induced the release of 5-HT, similar to 3,4-methylenedioxymethamphetamine (MDMA, ecstasy) and other entactogens. Cathinone, methcathinone and flephedrone, similar to amphetamine and methamphetamine, acted as preferential DA and NA uptake inhibitors and induced the release of DA. Pyrovalerone and 3,4-methylenedioxypyrovalerone (MDPV) were highly potent and selective DA and NA transporter inhibitors but unlike amphetamines did not evoke the release of monoamines. The non-β-keto amphetamines are trace amine-associated receptor 1 ligands, whereas the cathinones are not. All the cathinones showed high blood-brain barrier permeability in an in vitro model; mephedrone and MDPV exhibited particularly high permeability.Conclusions and Implications: Cathinones have considerable pharmacological differences that form the basis of their suggested classification into three groups. The predominant action of all cathinones on the DA transporter is probably associated with a considerable risk of addiction. [ABSTRACT FROM AUTHOR]

Published
2013
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16. Ultra-fast and ultra-intense x-ray sciences: first results from the Linac Coherent Light Source free-electron laser.

Author

Bostedt, C., Bozek, J. D., Bucksbaum, P. H., Coffee, R. N., Hastings, J. B., Z. Huang, Lee, R. W., Schorb, S., Corlett, J. N., Denes, P., Emma, P., Falcone, R. W., Schoenlein, R. W., Doumy, G., Kanter, E. P., Kraessig, B., Southworth, S., L. Young, L. Fang, and Hoener, M.

Subjects
LINEAR accelerators, COHERENCE (Optics), LIGHT sources, FREE electron lasers, ELECTRON spectroscopy, X-rays
Abstract

X-ray free-electron lasers (FELs) produce femtosecond x-ray pulses with unprecedented intensities that are uniquely suited for studying many phenomena in atomic, molecular, and optical (AMO) physics. A compilation of the current developments at the Linac Coherent Light Source (LCLS) and future plans for the LCLS-II and Next Generation Light Source (NGLS) are outlined. The AMO instrumentation at LCLS and its performance parameters are summarized. A few selected experiments representing the rapidly developing field of ultra-fast and peak intensity x-ray AMO sciences are discussed. These examples include fundamental aspects of intense x-ray interaction with atoms, nonlinear atomic physics in the x-ray regime, double core-hole spectroscopy, quantum control experiments with FELs and ultra-fast x-ray induced dynamics in clusters. These experiments illustrate the fundamental aspects of the interaction of intense short pulses of x-rays with atoms, molecules and clusters that are probed by electron and ion spectroscopies as well as ultra-fast x-ray scattering. [ABSTRACT FROM AUTHOR]

Published
2013
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17. Molecular frame Auger electron energy spectrum from N2.

Author

Cryan, J. P., Glownia, J. M., Andreasson, J., Belkacem, A., Berrah, N., Blaga, C. I., Bostedt, C., Bozek, J., Cherepkov, N. A., DiMauro, L. F., Fang, L., Gessner, O., Gühr, M., Hajdu, J., Hertlein, M. P., Hoener, M., Kornilov, O., Marangos, J. P., March, A. M., and McFarland, B. K.

Subjects
AUGER electron spectroscopy, NITROGEN, PHOTOIONIZATION, PHOTONS, ELECTRON emission, ANGULAR distribution (Nuclear physics)
Abstract

Here we present the first angle-resolved, non-resonant (normal) Auger spectra for impulsively aligned nitrogen molecules. We have measured the angular pattern of Auger electron emission following K-shell photoionization by 1.1 keV photons from the Linac Coherent Light Source (LCLS). Using strong-field-induced molecular alignment to make molecular frame measurements is equally effective for both repulsive and quasi-bound final states. The capability to resolve Auger emission angular distributions in the molecular frame of reference provides a new tool for spectral assignments in congested Auger electron spectra that takes advantage of the symmetries of the final diction states. Based on our experimental results and theoretical predictions, we propose the assignment of the spectral features in the Auger electron spectrum. [ABSTRACT FROM AUTHOR]

Published
2012
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18. Non-linear processes in the interaction of atoms and molecules with intense EUV and X-ray fields from SASE free electron lasers (FELs).

Author

Berrah, N., Bozek, J., Costello, J. T., Dusterer, S., Fang, L., Feldhaus, J., Fukuzawa, H., Hoener, M., Jiang, Y. H., Johnsson, P., Kennedy, E. T., Meyer, M., Moshammer, R., Radcliffe, P., Richter, M., Rouzée, A., Rudenko, A., Sorokin, A. A., Tiedtke, K., and Ueda, K.

Subjects
FREE electron lasers, NONLINEAR optics, X-rays, ATOMS, ELECTRONS
Abstract

The advent of free electron laser (FEL) facilities capable of delivering high intensity pulses in the extreme-UV to X-ray spectral range has opened up a wide vista of opportunities to study and control light matter interactions in hitherto unexplored parameter regimes. In particular, current short wavelength FELs can uniquely drive non-linear processes mediated by inner shell electrons and in fields where the photon energy can be as high as 10 keV and so the corresponding optical period reaches below one attosecond. Combined with ultrafast optical lasers, or simply employing wavefront division, pump probe experiments can be performed with femtosecond time resolution. As single photon ionization of atoms and molecules is by now very well understood, they provide the ideal targets for early experiments by which not only FELs can be characterised and benchmarked but can also be the natural departure point in the hunt for non-linear behaviour of atomistic systems bathed in laser fields of ultrahigh photon energy. In this topical review we illustrate with specific examples the gamut of apposite experiments in atomic, molecular physics currently underway at the SCSS Test Accelerator (Japan), FLASH (Hamburg) and LCLS (Stanford). [ABSTRACT FROM AUTHOR]

Published
2010
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19. Role played by sodium in activity-dependent secretion of neurotrophins - revisited.

Author

Hoener, M. C.

Subjects
*NEUROSECRETION, *NERVE growth factor, *SODIUM in the body, *IONOPHORES, *NEURON development
Abstract

AbstractIn previous experiments, a causal relationship between sodium influx and secretion of nerve growth factor (NGF) was deduced from the observation that the sodium substitute N-methyl-d-glucamine (NMDG) abolished any activity-mediated NGF secretion that depends on intact internal calcium stores. However, all available experimental evidence speaks against sodium-mediated calcium mobilization from these stores under physiological conditions. We now report that rapid sodium influx initiated by monensin or ouabain did not induce brain-derived neurotrophic factor (BDNF) secretion from either native hippocampal slices or BDNF-transduced hippocampal neuronal cultures. Additionally, we found marked differences between the replacement of sodium by NMDG and sucrose on the one hand, and choline and lithium on the other. Replacement of 100% (and as little as 10%) sodium by NMDG or sucrose not only blocked the activity-mediated neurotrophin secretion, but itself led to a rapid and substantial increase of neurotrophin secretion. In contrast, the replacement of sodium (10% and 100%) by lithium and choline did not result in a release of neurotrophins, and only 100% replacement blocked the activity-mediated neurotrophin secretion. We conclude that the blocking effects of NMDG and sucrose on neurotrophin secretion do not reflect the sodium replacement, but instead represent an independent blocking effect. These differences were also reflected in part by electrophysiological investigations in individually patched hippocampal neurons. The importance of the present observations lies not only in the reevaluation of the involvement of sodium in activity-dependent neurotrophin secretion, but also in the demonstration that sodium replacement may initiate ‘side effects’ that are unrelated to sodium replacement. [ABSTRACT FROM AUTHOR]

Published
2000
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25. Single-Photon Multiple Detachment in Fullerene Negative Ions: Absolute Ionization Cross Sections and the Role of the Extra Electron.

Author

Bilodeau, R. C., Gibson, N. D., Walter, C. W., Esteves-Macaluso, D. A., Schippers, S., Müller, A., Phaneuf, R. A., Aguilar, A., Hoener, M., Rost, J. M., and Berrah, N.

Subjects
*PHOTONS, *DETACHMENT reactions, *FULLERENES, *ANIONS, *ELECTRONS
Abstract

We have obtained experimental photo-double- and photo-triple-detachment cross sections for the fullerene negative ion using Advanced Light Source photons of 17-90 eV. The cross sections are 2 and 2.5 times larger than those for C60 and appear to be compressed and shifted in photon energy as compared to C60. Our analysis reveals that the additional electron in C60- primarily produces screening which is responsible for the modification of the spectrum. Both screening effects, the shift and the compression, can be quantitatively accounted for by a linear transformation of the energy axis. Applying the transformation allows us to map the neutral and negative ion cross sections onto each other, pointing out the close relationship of correlated few-electron dynamics in neutral and negatively charged extended systems. In contrast, dynamics of neutral and negatively charged atoms or small molecules are typically not closely related. [ABSTRACT FROM AUTHOR]

Published
2013
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26. Explosions of Xenon Clusters in Ultraintense Femtosecond X-Ray Pulses from the LCLS Free Electron Laser.

Author

Thomas, H., Helal, A., Hoffmann, K., Kandadai, N., Keto, J., Andreasson, J., Iwan, B., Seibert, M., Timneanu, N., Hajdu, J., Adolph, M., Gorkhover, T., Rupp, D., Schorb, S., Möller, T., Doumy, G., DiMauro, L. F., Hoener, M., Murphy, B., and Berrah, N.

Subjects
*XENON, *FEMTOSECOND pulses, *X-rays, *PHOTON emission, *LIGHT sources, *HYDRODYNAMICS, *PHOTOIONIZATION, *FREE electron lasers
Abstract

Explosions of large Xe clusters (〈N〉) ∼ 11 000) irradiated by femtosecond pulses of 850 eV x-ray photons focused to an intensity of up to 1017 W/cm2 from the Linac Coherent Light Source were investigated experimentally. Measurements of ion charge-state distributions and energy spectra exhibit strong evidence for the formation of a Xe nanoplasma in the intense x-ray pulse. This x-ray produced Xe nanoplasma is accompanied by a three-body recombination and hydrodynamic expansion. These experimental results appear to be consistent with a model in which a spherically exploding nanoplasma is formed inside the Xe cluster and where the plasma temperature is determined by photoionization heating. [ABSTRACT FROM AUTHOR]

Published
2012
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27. Molecular frame Auger electron energy spectrum from N2.

Author

Cryan, J. P., Glownia, J. M., Andreasson, J., Belkacem, A., Berrah, N., Blaga, C. I., Bostedt, C., Bozek, J., Cherepkov, N. A., DiMauro, L. F., Fang, L., Gessner, O., Gühr, M., Hajdu, J., Hertlein, M. P., Hoener, M., Kornilov, O., Marangos, J. P., March, A. M., and McFarland, B. K.

Subjects
*AUGER electron spectroscopy, *NITROGEN, *PHOTOIONIZATION, *PHOTONS, *ELECTRON emission, *ANGULAR distribution (Nuclear physics)
Abstract

Here we present the first angle-resolved, non-resonant (normal) Auger spectra for impulsively aligned nitrogen molecules. We have measured the angular pattern of Auger electron emission following K-shell photoionization by 1.1 keV photons from the Linac Coherent Light Source (LCLS). Using strong-field-induced molecular alignment to make molecular frame measurements is equally effective for both repulsive and quasi-bound final states. The capability to resolve Auger emission angular distributions in the molecular frame of reference provides a new tool for spectral assignments in congested Auger electron spectra that takes advantage of the symmetries of the final diction states. Based on our experimental results and theoretical predictions, we propose the assignment of the spectral features in the Auger electron spectrum. [ABSTRACT FROM AUTHOR]

Published
2012
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28. Ultrafast X-Ray Scattering of Xenon Nanoparticles: Imaging Transient States of Matter.

Author

Bostedt, C., Eremina, E., Rupp, D., Adolph, M., Thomas, H., Hoener, M., De Castro, A. R. B., Tiggesbäumker, J., Meiwes-Broer, K. H., Laarmann, T., Wabnitz, H., Plönjes, E., Treusch, R., Schneider, J. R., and Möller, T.

Subjects
*X-ray scattering, *XENON, *NANOPARTICLES, *FEMTOSECOND lasers, *CLUSTER analysis (Statistics), *OPTICAL constants, *X-ray diffraction
Abstract

Femtosecond x-ray laser flashes with power densities of up to 1014 W/cm2 at 13.7 nm wavelength were scattered by single xenon clusters in the gas phase. Similar to light scattering from atmospheric microparticles, the x-ray diffraction patterns carry information about the optical constants of the objects. However, the high flux of the x-ray laser induces severe transient changes of the electronic configuration, resulting in a tenfold increase of absorption in the developing nanoplasma. The modification in opaqueness can be correlated to strong atomic charging of the particle leading to excitation of Xe4+. It is shown that single-shot single-particle scattering on femtosecond time scales yields insight into ultrafast processes in highly excited systems where conventional spectroscopy techniques are inherently blind. [ABSTRACT FROM AUTHOR]

Published
2012
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29. Unveiling and Driving Hidden Resonances with High-Fluence, High-Intensity X-Ray Pulses.

Author

Kanter, E. P., Krässig, B., Li, Y., March, A. M., Ho, P., Rohringer, N., Santra, R., Southworth, S. H., DiMauro, L. F., Doumy, G., Roedig, C. A., Berrah, N., Fang, L., Hoener, M., Bucksbaum, P. H., Ghimire, S., Reis, D. A., Bozek, J. D., Bostedt, C., and Messerschmidt, M.

Subjects
*X-ray lasers, *FREE electron lasers, *SYNCHROTRONS, *RESONANCE, *ELECTRONS, *LIGHT absorption, *PHOTONS
Abstract

We show that high fluence, high-intensity x-ray pulses from the world's first hard x-ray free-electron laser produce nonlinear phenomena that differ dramatically from the linear x-ray--matter interaction processes that are encountered at synchrotron x-ray sources. We use intense x-ray pulses of sub-10-fs duration to first reveal and subsequently drive the 1s ⇔ 2p resonance in singly ionized neon. This photondriven cycling of an inner-shell electron modifies the Auger decay process, as evidenced by line shape modification. Our work demonstrates the propensity of high-fluence, femtosecond x-ray pulses to alter the target within a single pulse, i.e., to unveil hidden resonances, by cracking open inner shells energetically inaccessible via single-photon absorption, and to consequently trigger damaging electron cascades at unexpectedly low photon energies. [ABSTRACT FROM AUTHOR]

Published
2011
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30. Translational molecular imaging and drug development in Parkinson's disease.

Author

Haider A, Elghazawy NH, Dawoud A, Gebhard C, Wichmann T, Sippl W, Hoener M, Arenas E, and Liang SH

Subjects
Animals, alpha-Synuclein, Dopamine, Molecular Imaging, Drug Development, Parkinson Disease pathology, Parkinsonian Disorders
Abstract

Parkinson's disease (PD) is a progressive neurodegenerative disorder that primarily affects elderly people and constitutes a major source of disability worldwide. Notably, the neuropathological hallmarks of PD include nigrostriatal loss and the formation of intracellular inclusion bodies containing misfolded α-synuclein protein aggregates. Cardinal motor symptoms, which include tremor, rigidity and bradykinesia, can effectively be managed with dopaminergic therapy for years following symptom onset. Nonetheless, patients ultimately develop symptoms that no longer fully respond to dopaminergic treatment. Attempts to discover disease-modifying agents have increasingly been supported by translational molecular imaging concepts, targeting the most prominent pathological hallmark of PD, α-synuclein accumulation, as well as other molecular pathways that contribute to the pathophysiology of PD. Indeed, molecular imaging modalities such as positron emission tomography (PET) and single-photon emission computed tomography (SPECT) can be leveraged to study parkinsonism not only in animal models but also in living patients. For instance, mitochondrial dysfunction can be assessed with probes that target the mitochondrial complex I (MC-I), while nigrostriatal degeneration is typically evaluated with probes designed to non-invasively quantify dopaminergic nerve loss. In addition to dopaminergic imaging, serotonin transporter and N-methyl-D-aspartate (NMDA) receptor probes are increasingly used as research tools to better understand the complexity of neurotransmitter dysregulation in PD. Non-invasive quantification of neuroinflammatory processes is mainly conducted by targeting the translocator protein 18 kDa (TSPO) on activated microglia using established imaging agents. Despite the overwhelming involvement of the brain and brainstem, the pathophysiology of PD is not restricted to the central nervous system (CNS). In fact, PD also affects various peripheral organs such as the heart and gastrointestinal tract - primarily via autonomic dysfunction. As such, research into peripheral biomarkers has taken advantage of cardiac autonomic denervation in PD, allowing the differential diagnosis between PD and multiple system atrophy with probes that visualize sympathetic nerve terminals in the myocardium. Further, α-synuclein has recently gained attention as a potential peripheral biomarker in PD. This review discusses breakthrough discoveries that have led to the contemporary molecular concepts of PD pathophysiology and how they can be harnessed to develop effective imaging probes and therapeutic agents. Further, we will shed light on potential future trends, thereby focusing on potential novel diagnostic tracers and disease-modifying therapeutic interventions., (© 2023. The Author(s).)

Published
2023
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31. Secreted retrovirus-like GAG-domain-containing protein PEG10 is regulated by UBE3A and is involved in Angelman syndrome pathophysiology.

Author

Pandya NJ, Wang C, Costa V, Lopatta P, Meier S, Zampeta FI, Punt AM, Mientjes E, Grossen P, Distler T, Tzouros M, Martí Y, Banfai B, Patsch C, Rasmussen S, Hoener M, Berrera M, Kremer T, Dunkley T, Ebeling M, Distel B, Elgersma Y, and Jagasia R

Subjects
Animals, Cell Movement, Child, Preschool, Extracellular Vesicles metabolism, Extracellular Vesicles ultrastructure, Female, Humans, Induced Pluripotent Stem Cells pathology, Male, Mice, Inbred C57BL, Neurons metabolism, Neurons pathology, Proteasome Endopeptidase Complex metabolism, Protein Domains, Retroelements genetics, Stress Granules metabolism, Stress Granules ultrastructure, Transcriptome genetics, Mice, Angelman Syndrome metabolism, Angelman Syndrome physiopathology, Apoptosis Regulatory Proteins metabolism, DNA-Binding Proteins metabolism, Gene Products, gag chemistry, RNA-Binding Proteins metabolism, Retroviridae metabolism, Ubiquitin-Protein Ligases metabolism
Abstract

Angelman syndrome (AS) is a neurodevelopmental disorder caused by the loss of maternal UBE3A , a ubiquitin protein ligase E3A. Here, we study neurons derived from patients with AS and neurotypical individuals, and reciprocally modulate UBE3A using antisense oligonucleotides. Unbiased proteomics reveal proteins that are regulated by UBE3A in a disease-specific manner, including PEG10, a retrotransposon-derived GAG protein. PEG10 protein increase, but not RNA, is dependent on UBE3A and proteasome function. PEG10 binds to both RNA and ataxia-associated proteins (ATXN2 and ATXN10), localizes to stress granules, and is secreted in extracellular vesicles, modulating vesicle content. Rescue of AS patient-derived neurons by UBE3A reinstatement or PEG10 reduction reveals similarity in transcriptome changes. Overexpression of PEG10 during mouse brain development alters neuronal migration, suggesting that it can affect brain development. These findings imply that PEG10 is a secreted human UBE3A target involved in AS pathophysiology., Competing Interests: N.J.P., V.C., C.W., P.L., S.M., P.G., T.D., M.T., Y.M., B.B., C.P., S.R., M.H., M.B., T.K., T.D., M.E., and R.J. are employed by F. Hoffmann-La Roche. Parts of the work in this study have been filed in the patent WO2020/148310. The remaining authors declare no competing financial interests., (© 2021 The Authors.)

Published
2021
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32. Threshold photoionization shows no sign of nitryl hydride in methane oxidation with nitric oxide.

Author

Hoener M, Bodi A, Hemberger P, Endres T, and Kasper T

Abstract

Methane was doped with nitric oxide and oxidized in a high-pressure flow reactor. The nitrogen chemistry during partial oxidation was studied using photoelectron photoion coincidence spectroscopy with vacuum ultraviolet synchrotron radiation. The adiabatic ionization energy of nitrous acid, HONO, has been determined as 10.95 ± 0.03 eV. The HONO breakdown diagram was plotted based solely on the measured parent signal and the computed Franck-Condon envelope of trans-HONO, confirming the trans-HONO dissociative photoionization threshold to NO+ + ˙OH at 11.34 eV. The spectra show strong indication for the presence of cis-HONO. We expected the m/z 47 photoion mass selected threshold photoelectron signal to rebound near 12 eV, i.e., at the ionization energy of nitryl hydride, the third HNO2 isomer. Recent computational studies suggest nitryl hydride is formed at a rate similar to trans-HONO, is more thermally stable than nitrous acid, its cation is bound, and its photoelectron spectrum is predicted to exhibit a strong origin band near 12 eV. The absence of its mass selected threshold photoelectron signal shows that nitryl hydride is either not formed in measurable amounts or is consumed faster than nitrous acid, for instance by isomerization to trans-HONO.

Published
2021
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33. A partial trace amine-associated receptor 1 agonist exhibits properties consistent with a methamphetamine substitution treatment.

Author

Pei Y, Asif-Malik A, Hoener M, and Canales JJ

Subjects
Amphetamine-Related Disorders, Animals, Dopamine metabolism, Male, Nucleus Accumbens drug effects, Nucleus Accumbens metabolism, Rats, Rats, Long-Evans, Reinforcement, Psychology, Reward, Behavior, Animal drug effects, Central Nervous System Stimulants administration & dosage, Drug-Seeking Behavior drug effects, Methamphetamine administration & dosage, Oxazoles pharmacology, Receptors, G-Protein-Coupled agonists, Self Administration
Abstract

Recent evidence suggests that the trace amine-associated receptor 1 (TAAR1) plays a pivotal role in the regulation of dopamine (DA) transmission and psychostimulant action. Several selective TAAR1 agonists have previously shown efficacy in models of cocaine addiction. However, the effects of TAAR1 activation on methamphetamine (METH)-induced behaviours are less well understood, as indeed are the underlying neurochemical mechanisms mediating potential interactions between TAAR1 and METH. Here, in a progressive ratio schedule of reinforcement the partial TAAR1 agonist, RO5263397, reduced the break-point for METH self-administration, while significantly increasing responding maintained by food reward. Following self-administration and extinction training, RO5263397 completely blocked METH-primed reinstatement of METH seeking. Moreover, when used as a substitute, unlike a low dose of METH, which sustained vigorous responding when substituting for the training dose of METH, RO5263397 was not self-administered at any dose, thus exhibiting no apparent abuse liability. Fast-scan cyclic voltammetry experiments showed that RO5263397 prevented METH-induced DA overflow in slices of the nucleus accumbens, while having no effect on DA transmission in its own right. Collectively, the present observations demonstrate that partial TAAR1 activation decreases the motivation to self-administer METH, blocks METH-primed reinstatement of METH seeking and prevents METH-induced DA elevations in the nucleus accumbens, and strongly support the candidacy of TAAR1-based medications as potential substitute treatment in METH addiction., (© 2016 Society for the Study of Addiction.)

Published
2017
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34. Transient X-ray fragmentation: probing a prototypical photoinduced ring opening.

Author

Petrović VS, Siano M, White JL, Berrah N, Bostedt C, Bozek JD, Broege D, Chalfin M, Coffee RN, Cryan J, Fang L, Farrell JP, Frasinski LJ, Glownia JM, Gühr M, Hoener M, Holland DM, Kim J, Marangos JP, Martinez T, McFarland BK, Minns RS, Miyabe S, Schorb S, Sension RJ, Spector LS, Squibb R, Tao H, Underwood JG, and Bucksbaum PH

Subjects
Photochemical Processes, Spectrophotometry, Ultraviolet, Thermodynamics, X-Rays, Alkenes chemistry, Cyclization radiation effects, Cyclohexenes chemistry, Polyenes chemistry
Abstract

We report the first study of UV-induced photoisomerization probed via core ionization by an x-ray laser. We investigated x-ray ionization and fragmentation of the cyclohexadiene-hexatriene system at 850 eV during the ring opening. We find that the ion-fragmentation patterns evolve over a picosecond, reflecting a change in the state of excitation and the molecular geometry: the average kinetic energy per ion fragment and H(+)-ion count increase as the ring opens and the molecule elongates. We discuss new opportunities for molecular photophysics created by optical pump x-ray probe experiments.

Published
2012
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35. Ultrafast absorption of intense x rays by nitrogen molecules.

Author

Buth C, Liu JC, Chen MH, Cryan JP, Fang L, Glownia JM, Hoener M, Coffee RN, and Berrah N

Abstract

We devise a theoretical description for the response of nitrogen molecules (N(2)) to ultrashort and intense x rays from the free electron laser Linac Coherent Light Source (LCLS). We set out from a rate-equation description for the x-ray absorption by a nitrogen atom. The equations are formulated using all one-x-ray-photon absorption cross sections and the Auger and radiative decay widths of multiply-ionized nitrogen atoms. Cross sections are obtained with a one-electron theory and decay widths are determined from ab initio computations using the Dirac-Hartree-Slater (DHS) method. We also calculate all binding and transition energies of nitrogen atoms in all charge states with the DHS method as the difference of two self-consistent field (SCF) calculations (ΔSCF method). To describe the interaction with N(2), a detailed investigation of intense x-ray-induced ionization and molecular fragmentation are carried out. As a figure of merit, we calculate ion yields and the average charge state measured in recent experiments at the LCLS. We use a series of phenomenological models of increasing sophistication to unravel the mechanisms of the interaction of x rays with N(2): a single atom, a symmetric-sharing model, and a fragmentation-matrix model are developed. The role of the formation and decay of single and double core holes, the metastable states of N(2)(2+), and molecular fragmentation are explained.

Published
2012
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36. Nonlinear atomic response to intense ultrashort x rays.

Author

Doumy G, Roedig C, Son SK, Blaga CI, DiChiara AD, Santra R, Berrah N, Bostedt C, Bozek JD, Bucksbaum PH, Cryan JP, Fang L, Ghimire S, Glownia JM, Hoener M, Kanter EP, Krässig B, Kuebel M, Messerschmidt M, Paulus GG, Reis DA, Rohringer N, Young L, Agostini P, and DiMauro LF

Abstract

The nonlinear absorption mechanisms of neon atoms to intense, femtosecond kilovolt x rays are investigated. The production of Ne(9+) is observed at x-ray frequencies below the Ne(8+), 1s(2) absorption edge and demonstrates a clear quadratic dependence on fluence. Theoretical analysis shows that the production is a combination of the two-photon ionization of Ne(8+) ground state and a high-order sequential process involving single-photon production and ionization of transient excited states on a time scale faster than the Auger decay. We find that the nonlinear direct two-photon ionization cross section is orders of magnitude higher than expected from previous calculations., (© 2011 American Physical Society)

Published
2011
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37. Auger electron angular distribution of double core-hole states in the molecular reference frame.

Author

Cryan JP, Glownia JM, Andreasson J, Belkacem A, Berrah N, Blaga CI, Bostedt C, Bozek J, Buth C, DiMauro LF, Fang L, Gessner O, Guehr M, Hajdu J, Hertlein MP, Hoener M, Kornilov O, Marangos JP, March AM, McFarland BK, Merdji H, Petrović VS, Raman C, Ray D, Reis D, Tarantelli F, Trigo M, White JL, White W, Young L, Bucksbaum PH, and Coffee RN

Subjects
Light, Nitrogen chemistry, Quantum Theory, Spectrum Analysis, Time Factors, Electrons, Physical Phenomena
Abstract

The Linac Coherent Light Source free electron laser is a source of high brightness x rays, 2×10(11) photons in a ∼5 fs pulse, that can be focused to produce double core vacancies through rapid sequential ionization. This enables double core vacancy Auger electron spectroscopy, an entirely new way to study femtosecond chemical dynamics with Auger electrons that probe the local valence structure of molecules near a specific atomic core. Using 1.1 keV photons for sequential x-ray ionization of impulsively aligned molecular nitrogen, we observed a rich single-site double core vacancy Auger electron spectrum near 413 eV, in good agreement with ab initio calculations, and we measured the corresponding Auger electron angle dependence in the molecular frame.

Published
2010
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38. Double core-hole production in N2: beating the Auger clock.

Author

Fang L, Hoener M, Gessner O, Tarantelli F, Pratt ST, Kornilov O, Buth C, Gühr M, Kanter EP, Bostedt C, Bozek JD, Bucksbaum PH, Chen M, Coffee R, Cryan J, Glownia M, Kukk E, Leone SR, and Berrah N

Subjects
Lasers, Photoelectron Spectroscopy, Quantum Theory, Synchrotrons, X-Rays, Electrons, Nitrogen, Physical Phenomena
Abstract

We investigate the creation of double K-shell holes in N2 molecules via sequential absorption of two photons on a time scale shorter than the core-hole lifetime by using intense x-ray pulses from the Linac Coherent Light Source free electron laser. The production and decay of these states is characterized by photoelectron spectroscopy and Auger electron spectroscopy. In molecules, two types of double core holes are expected, the first with two core holes on the same N atom, and the second with one core hole on each N atom. We report the first direct observations of the former type of core hole in a molecule, in good agreement with theory, and provide an experimental upper bound for the relative contribution of the latter type.

Published
2010
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39. Time-resolved pump-probe experiments at the LCLS.

Author

Glownia JM, Cryan J, Andreasson J, Belkacem A, Berrah N, Blaga CI, Bostedt C, Bozek J, DiMauro LF, Fang L, Frisch J, Gessner O, Gühr M, Hajdu J, Hertlein MP, Hoener M, Huang G, Kornilov O, Marangos JP, March AM, McFarland BK, Merdji H, Petrovic VS, Raman C, Ray D, Reis DA, Trigo M, White JL, White W, Wilcox R, Young L, Coffee RN, and Bucksbaum PH

Subjects
Equipment Design, Optical Fibers, Time Factors, X-Rays, Electrons, Lasers, Synchrotrons
Abstract

The first time-resolved x-ray/optical pump-probe experiments at the SLAC Linac Coherent Light Source (LCLS) used a combination of feedback methods and post-analysis binning techniques to synchronize an ultrafast optical laser to the linac-based x-ray laser. Transient molecular nitrogen alignment revival features were resolved in time-dependent x-ray-induced fragmentation spectra. These alignment features were used to find the temporal overlap of the pump and probe pulses. The strong-field dissociation of x-ray generated quasi-bound molecular dications was used to establish the residual timing jitter. This analysis shows that the relative arrival time of the Ti:Sapphire laser and the x-ray pulses had a distribution with a standard deviation of approximately 120 fs. The largest contribution to the jitter noise spectrum was the locking of the laser oscillator to the reference RF of the accelerator, which suggests that simple technical improvements could reduce the jitter to better than 50 fs.

Published
2010
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40. Ultraintense x-ray induced ionization, dissociation, and frustrated absorption in molecular nitrogen.

Author

Hoener M, Fang L, Kornilov O, Gessner O, Pratt ST, Gühr M, Kanter EP, Blaga C, Bostedt C, Bozek JD, Bucksbaum PH, Buth C, Chen M, Coffee R, Cryan J, Dimauro L, Glownia M, Hosler E, Kukk E, Leone SR, McFarland B, Messerschmidt M, Murphy B, Petrovic V, Rolles D, and Berrah N

Abstract

Sequential multiple photoionization of the prototypical molecule N2 is studied with femtosecond time resolution using the Linac Coherent Light Source (LCLS). A detailed picture of intense x-ray induced ionization and dissociation dynamics is revealed, including a molecular mechanism of frustrated absorption that suppresses the formation of high charge states at short pulse durations. The inverse scaling of the average target charge state with x-ray peak brightness has possible implications for single-pulse imaging applications.

Published
2010
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41. Multistep ionization of argon clusters in intense femtosecond extreme ultraviolet pulses.

Author

Bostedt C, Thomas H, Hoener M, Eremina E, Fennel T, Meiwes-Broer KH, Wabnitz H, Kuhlmann M, Plönjes E, Tiedtke K, Treusch R, Feldhaus J, de Castro AR, and Möller T

Abstract

The interaction of intense extreme ultraviolet femtosecond laser pulses (lambda = 32.8 nm) from the FLASH free electron laser (FEL) with clusters has been investigated by means of photoelectron spectroscopy and modeled by Monte Carlo simulations. For laser intensities up to 5x10(13) W/cm(2), we find that the cluster ionization process is a sequence of direct electron emission events in a developing Coulomb field. A nanoplasma is formed only at the highest investigated power densities where ionization is frustrated due to the deep cluster potential. In contrast with earlier studies in the IR and vacuum ultraviolet spectral regime, we find no evidence for electron emission from plasma heating processes.

Published
2008
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42. Similar patterns of mitochondrial vulnerability and rescue induced by genetic modification of alpha-synuclein, parkin, and DJ-1 in Caenorhabditis elegans.

Author

Ved R, Saha S, Westlund B, Perier C, Burnam L, Sluder A, Hoener M, Rodrigues CM, Alfonso A, Steer C, Liu L, Przedborski S, and Wolozin B

Subjects
3-Hydroxybutyric Acid pharmacology, Amino Acid Sequence, Animals, Animals, Genetically Modified, Antioxidants pharmacology, Apoptosis, Benzoates pharmacology, Benzothiazoles, Bile Acids and Salts metabolism, Cholagogues and Choleretics pharmacology, Copper chemistry, Disease Models, Animal, Electron Transport Complex I antagonists & inhibitors, Gene Deletion, Gene Library, Genetic Techniques, Humans, Immunoblotting, Intracellular Signaling Peptides and Proteins, Ions, Iron chemistry, Molecular Sequence Data, Mutagenesis, Mutation, Neurons metabolism, Oxygen Consumption, Paraquat pharmacology, Parkinson Disease pathology, Polyenes pharmacology, Probucol pharmacology, Protein Deglycase DJ-1, Pyrazoles pharmacology, Pyridazines pharmacology, RNA, Small Interfering metabolism, Rotenone pharmacology, Sequence Homology, Amino Acid, Sodium Azide pharmacology, Taurochenodeoxycholic Acid pharmacology, Thiazoles pharmacology, Time Factors, Transgenes, Caenorhabditis elegans metabolism, Gene Expression Regulation, Mitochondria metabolism, Oncogene Proteins genetics, Ubiquitin-Protein Ligases genetics, alpha-Synuclein genetics
Abstract

How genetic and environmental factors interact in Parkinson disease is poorly understood. We have now compared the patterns of vulnerability and rescue of Caenorhabditis elegans with genetic modifications of three different genetic factors implicated in Parkinson disease (PD). We observed that expressing alpha-synuclein, deleting parkin (K08E3.7), or knocking down DJ-1 (B0432.2) or parkin produces similar patterns of pharmacological vulnerability and rescue. C. elegans lines with these genetic changes were more vulnerable than nontransgenic nematodes to mitochondrial complex I inhibitors, including rotenone, fenperoximate, pyridaben, or stigmatellin. In contrast, the genetic manipulations did not increase sensitivity to paraquat, sodium azide, divalent metal ions (Fe(II) or Cu(II)), or etoposide compared with the nontransgenic nematodes. Each of the PD-related lines was also partially rescued by the antioxidant probucol, the mitochondrial complex II activator, D-beta-hydroxybutyrate, or the anti-apoptotic bile acid tauroursodeoxycholic acid. Complete protection in all lines was achieved by combining d-beta-hydroxybutyrate with tauroursodeoxycholic acid but not with probucol. These results show that diverse PD-related genetic modifications disrupt the mitochondrial function in C. elegans, and they raise the possibility that mitochondrial disruption is a pathway shared in common by many types of familial PD.

Published
2005
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43. Geldanamycin restores a defective heat shock response in vivo.

Author

Winklhofer KF, Reintjes A, Hoener MC, Voellmy R, and Tatzelt J

Subjects
Animals, Benzoquinones, Blotting, Western, Cell Division drug effects, DNA-Binding Proteins biosynthesis, Detergents pharmacology, Dimerization, Fluorescent Antibody Technique, Indirect, Gene Expression Regulation, HSP72 Heat-Shock Proteins, HSP90 Heat-Shock Proteins metabolism, Heat Shock Transcription Factors, Heat-Shock Proteins biosynthesis, Kinetics, Lactams, Macrocyclic, Luciferases metabolism, Mice, Models, Biological, Phosphorylation, Plasmids metabolism, Protein Binding, Recombinant Proteins metabolism, Scrapie metabolism, Stress, Physiological, Temperature, Time Factors, Transcription Factors, Transfection, Tumor Cells, Cultured, beta-Galactosidase metabolism, Enzyme Inhibitors pharmacology, Hot Temperature, Quinones pharmacology
Abstract

Induced expression of heat shock proteins (Hsps) plays a central role in promoting cellular survival after environmental and physiological stress. We have previously shown that scrapie-infected mouse neuroblastoma (ScN2a) cells fail to induce the expression of Hsp72 and Hsp28 after various stress conditions. Here we present evidence that this impaired stress response is due to an altered regulation of HSF1 activity. Upon stress in ScN2a cells, HSF1 was converted into hyperphosphorylated trimers but failed to acquire transactivation competence. A kinetic analysis of HSF1 activation revealed that in ScN2a cells trimer formation after stress was efficient, but disassembly of trimers proceeded much faster than in the uninfected cell line. Geldanamycin, a Hsp90-binding drug, significantly delayed disassembly of HSF1 trimers after a heat shock and restored stress-induced expression of Hsp72 in ScN2a cells. Heat-induced Hsp72 expression required geldanamycin to be present; following removal of the drug ScN2a cells again lost their ability to mount a stress response. Thus, our studies show that a defective stress response can be pharmacologically restored and suggest that the HSF1 deactivation pathway may play an important role in the regulation of Hsp expression.

Published
2001
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44. Are there differences between the secretion characteristics of NGF and BDNF? Implications for the modulatory role of neurotrophins in activity-dependent neuronal plasticity.

Author

Griesbeck O, Canossa M, Campana G, Gärtner A, Hoener MC, Nawa H, Kolbeck R, and Thoenen H

Subjects
Animals, Brain-Derived Neurotrophic Factor genetics, Calcium metabolism, Cells, Cultured, Female, Gene Transfer Techniques, Genetic Vectors genetics, Hippocampus cytology, Male, Microscopy, Confocal, Nerve Growth Factors genetics, Neurons cytology, Neurons drug effects, Potassium metabolism, Rats, Rats, Wistar, Time Factors, Brain-Derived Neurotrophic Factor metabolism, Hippocampus metabolism, Nerve Growth Factors metabolism, Neurons physiology
Abstract

In previous experiments the activity-dependent secretion of nerve growth factor (NGF) from native hippocampal slices and from NGF-cDNA transfected hippocampal neurons showed unusual characteristics [Blochl and Thoenen (1995) Eur J Neurosci 7:1220-1228; (1996) Mol Cell Neurosci 7:173-190]. In both hippocampal slices and cultured hippocampal neurons the activity-dependent secretion proved to be independent of extracellular calcium, but dependent on the release of calcium from intracellular stores. Under different experimental conditions, Goodman et al. [(1996) Mol Cell Neurosci 7:222-238] reported that the high potassium-mediated secretion of brain-derived neurotrophic factor (BDNF) from hippocampal cultures was dependent on extracellular calcium. Mowla et al. [(1997) Proc 27th Annu Meet Soc Neurosci New Orleans 875.10] reported on even further-reaching differences between NGF and BDNF secretion, namely, that in hippocampal neurons and in pituitary cell lines NGF was secreted exclusively according to the constitutive pathway, whereas BDNF was exclusively sorted according to the activity-dependent regulated pathway. In view of the crucial importance of such potential differences between the processing, sorting, and secretory mechanisms of different neurotrophins for their modulatory roles in activity-dependent neuronal plasticity, a thorough analysis under comparable experimental conditions was mandatory. We demonstrate that in native hippocampal slices and adenoviral-transduced hippocampal neurons there are no differences between NGF and BDNF with respect to the subcellular distribution and mechanism of secretion; that the activity-dependent secretion of both NGF and BDNF is dependent on intact intracellular calcium stores; and that the differences between our own observations and those of Goodman et al. (ibid.) regarding the dependence on extracellular calcium do not reflect differences between NGF and BDNF sorting and secretion, but reflect the differing experimental conditions used.

Published
1999
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45. Partial cortical devascularization results in elevations of cortical nerve growth factor and increases nerve growth factor protein within basal forebrain cholinergic neurons.

Author

Conner JM, Hoener MC, and Varon S

Subjects
Animals, Basal Ganglia metabolism, Basal Ganglia pathology, Cerebral Arteries physiology, Cerebral Cortex pathology, Cerebral Infarction pathology, Enzyme-Linked Immunosorbent Assay, Female, Functional Laterality, Immunohistochemistry, Ischemia pathology, Neurons pathology, Prosencephalon pathology, Rats, Rats, Sprague-Dawley, Regional Blood Flow, Time Factors, Cerebral Cortex blood supply, Cerebral Cortex metabolism, Cerebral Infarction metabolism, Ischemia metabolism, Nerve Growth Factors biosynthesis, Neurons metabolism, Prosencephalon metabolism
Abstract

Previous studies have demonstrated that partial cortical devascularization results in increased levels of nerve growth factor protein within the tissue immediately surrounding the infarcted region. In the present study, we have used this lesion model to further characterize the nerve growth factor increase by investigating: (i) the time course for this phenomenon; (ii) the impact of the devascularizing lesion on cortical regions not directly impinged upon by the lesion; and (iii) the response of nerve growth factor-sensitive nucleus basalis neurons providing afferent cortical innervation to the increased availability of nerve growth factor within their target territory. Our results indicate that, within the infarcted cortex, nerve growth factor levels increase rapidly following the lesion (up 51% by one day post lesion), reach a maximum of 136% above controls by three days and undergo a slow decline back to baseline levels by 23 days. Within the frontal and cingulate cortices, which are not devascularized by the lesion and show no signs of pathological damage, nerve growth factor levels increase over a similar time course, and with a similar magnitude, to those in the lesioned cortex. Nerve growth factor-sensitive nucleus basalis neurons on the side ipsilateral to the lesion respond to increased cortical nerve growth factor levels with an increased accumulation of nerve growth factor within their cell bodies (revealed by nerve growth factor immunohistochemistry and quantitative enzyme-linked immunosorbent assay) which was apparent at three days following the lesion, but no longer discernible at seven or 14 days or later. The present study investigated a model of cortical devascularization for its ability to alter nerve growth factor levels within the cortex. Nerve growth factor levels were rapidly increased within the infarcted cortical tissue beneath the lesion but were also elevated to a similar extent, and with a similar time course, in cortical regions not directly impinged upon by the lesion. The retrograde impact of elevated cortical nerve growth factor levels was demonstrated by an increased accumulation of nerve growth factor within the cell bodies of nucleus basalis neurons providing innervation to the cortex. This lesion model should provide a potential avenue for investigating the functional role(s) of nerve growth factor in the intact and lesioned adult central nervous system, as well as the internal mechanisms for regulating its synthesis, release, uptake, and degradation.

Published
1998
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46. Reversible sedimentation and masking of nerve growth factor (NGF) antigen by high molecular weight fractions from rat brain.

Author

Hoener MC and Varon S

Subjects
Animals, Centrifugation, Chromatography, Gel, Enzyme-Linked Immunosorbent Assay, Female, Humans, Hydrogen-Ion Concentration, Logistic Models, Mice, Molecular Weight, Rats, Rats, Sprague-Dawley, Recombinant Proteins isolation & purification, Solubility, Antigens isolation & purification, Brain immunology, Nerve Growth Factors immunology
Abstract

Nerve growth factor (NGF) was recently found to be largely associated with sedimentable fractions of adult rat brain and treatments of the fractions by alkaline pH increased the measurable amount of their NGF antigen as well as its solubilization [M.C. Hoener, E. Hewitt, J.M. Conner, J.W. Costello and S. Varon, Nerve growth factor (NGF) content in adult rat brain tissues is several-fold higher than generally reported and is largely associated with sedimentable fractions, Brain Res., 728 (1996) 47-56; M.C. Hoener and S. Varon, Effects of sodium chloride, Triton X-100, and alkaline pH on the measurable contents and sedimentability of the nerve growth factor (NGF) antigen in adult rat hippocampal tissue extracts, J. Neurosci. Res., in press (1997); C. Zettler, D.C.McL. Bridges, X.-F. Zhou and R.A. Rush, Detection of increased tissue concentrations of nerve growth factor with improved extraction procedure, J. Neurosci. Res., 46 (1996) 581-594]. We have further investigated the reversibility of these pH effects. Reversal of the pH of an adult rat hippocampal tissue extract from 10.5 to 7.4 led to an almost complete transfer of NGF back from nonsedimentable to sedimentable fractions and to a remasking of the previously unmasked portion of NGF antigen. Thus, molecules causing masking and sedimentation of NGF at pH 7.4 were likely to be present in the alkaline extract. A gel filtration column in PBS, pH 10.5 was used to separate such putative binding molecules from the NGF. All of the NGF antigen from rat hippocampal alkaline extract was found to elute with 19 kDa fractions. The same apparent molecular weight was found for mouse submaxillary beta-NGF and recombinant human beta-NGF. Masking and sedimentation no longer occurred when newly generated 19 kDa rat brain NGF was returned to pH 7.4. When high molecular weight fractions derived from the same gel filtration (in PBS, pH 10.5) were added back to the 19 kDa NGF pool at pH 7.4 and the mixture incubated and centrifuged, the measurability of 19 kDa rat brain NGF antigen was markedly reduced and half of the antigen was recovered in sedimentable fractions. Similar but less dramatic results were obtained when mixing the same high molecular weight fractions with 19 kDa mouse or human beta-NGF. These findings provide new opportunities to identify molecules to which NGF may be bound within intact brain tissues.

Published
1997
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47. Effects of sodium chloride, Triton X-100, and alkaline pH on the measurable contents and sedimentability of the nerve growth factor (NGF) antigen in adult rat hippocampal tissue extracts.

Author

Hoener MC and Varon S

Subjects
Alkalies, Animals, Enzyme-Linked Immunosorbent Assay, Female, Hydrogen-Ion Concentration, Rats, Rats, Sprague-Dawley, Solubility, Sonication, Tissue Extracts analysis, Tissue Extracts chemistry, Detergents, Hippocampus chemistry, Nerve Growth Factors analysis, Octoxynol, Sodium Chloride
Abstract

Nerve growth factor (NGF) was found to be largely associated with sedimentable fractions of hippocampal and other neural tissues of the adult rat (Hoener et al.: Brain Res 728:47-56, 1996), verified by both bioassay and ELISA techniques. In the present study, the ELISA assay conditions were improved and simplified. Bovine serum albumin was needed in the phosphate buffered saline for maximal measurability of NGF antigen. Hippocampal tissue sonicates were separated into nonsedimentable supernatant and sedimentable pellet fractions. Individual or combined treatments with sodium chloride, Triton X-100, and pH were applied to the samples for possible effects on the i) measurable content of NGF antigen and ii) distribution of sedimentable and nonsedimentable forms. The amount of measurable NGF antigen was found to be increased in a dose dependent fashion by sodium chloride between 0.15 and 0.35 M, Triton X-100 between 0 and 0.5%, and pH between 8.5 and 10.5. The same treatment that led to maximal measurable NGF levels (0.7% Triton X-100 and pH 10.5) also caused the release of the NGF antigen from sedimentable to nonsedimentable fractions. Similar findings regarding maximal NGF antigen levels and release were seen for treatments applied to the sonicate before separation into a supernatant and pellet fraction.

Published
1997

48. Nerve growth factor (NGF) content in adult rat brain tissues is several-fold higher than generally reported and is largely associated with sedimentable fractions.

Author

Hoener MC, Hewitt E, Conner JM, Costello JW, and Varon S

Subjects
Animals, Antigens analysis, Biological Assay, Centrifugation, Chemical Fractionation, Chick Embryo, Enzyme-Linked Immunosorbent Assay, Female, Nerve Growth Factors immunology, Rats, Rats, Sprague-Dawley, Solubility, Sonication, Brain Chemistry physiology, Nerve Growth Factors analysis
Abstract

Initial studies had revealed that the bioactivity of nerve growth factor (NGF) in sonicates of adult rat hippocampal formation (HF) is several-fold greater in their pellet than their supernatant fractions. Such observations have prompted an analysis of NGF antigen (NGF-Ag) contents in pellets and supernatants from a variety of adult rat CNS tissues, both in the absence and the presence of exogenous beta-NGF. With HF tissues, NGF-Ag in the supernatants was comparable to most literature values, but pellet NGF-Ag was 3 to 5 times that amount. All other CNS tissue sonicates also revealed 3-6 fold higher NGF-Ag in their pellets than their supernatants, hence overall NGF-Ag contents were greatly in excess of reported ones. Presentation of mouse beta-NGF to a tissue, its sonicate, or its standard pellet resulted in a transfer to the final pellet of 30-50% of the added soluble NGF-Ag (and 30% of the added bioactivity). This percentage is much lower than that present in native pellets (80%), suggesting that the association of endogenous NGF with particulate matter may involve at least two compartments. Treatments of pellets with salt, alkaline pH, and/or the detergent Triton X-100 have revealed a third subset, namely additional pellet NGF-Ag that was not initially recognized by the antibody in our ELISA assay. The treatments also caused substantial release of NGF from pellet to supernatant. Further studies should clarify the nature of the association between NGF and the three subsets of pellet NGF and allow the investigation of the pellet molecules responsible for it.

Published
1996

49. Glycosyl-phosphatidylinositol-specific phospholipase D. Interaction with and stimulation by apolipoprotein A-I.

Author

Hoener MC, Bolli R, and Brodbeck U

Subjects
Acetylcholinesterase metabolism, Animals, Cattle, Centrifugation, Density Gradient, Chromatography, Affinity, Enzyme Activation, Protein Binding, Apolipoprotein A-I metabolism, Phospholipase D metabolism
Abstract

Glycosyl-phosphatidylinositol-specific phospholipase D (GPI-PLD) is an amphiphilic protein which, in serum, is associated with high-density lipoproteins (HDL). It is shown that the major component of the HDL fraction, apolipoprotein A-I (apo A-I), is responsible for this association. In the absence of apo A-I, purified GPI-PLD occurred as virtually inactive aggregates which became disaggregated by apo A-I. The enzyme/apo A-I complex efficiently hydrolyzed the solubilized GPI-anchored substrate, acetylcholinesterase. Triton X-100 was also able to dissociate aggregated GPI-PLD, however, it strongly inhibited enzyme activity at detergent concentrations above the critical micellar concentration.

Published
1993
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50. Phosphatidylinositol-glycan-specific phospholipase D is an amphiphilic glycoprotein that in serum is associated with high-density lipoproteins.

Author

Hoener MC and Brodbeck U

Subjects
Amino Acid Sequence, Animals, Cattle, Centrifugation, Density Gradient, Chemical Phenomena, Chemistry, Physical, Cyanogen Bromide, Glycoside Hydrolases metabolism, Humans, Milk enzymology, Milk, Human enzymology, Molecular Sequence Data, Peptide Fragments chemistry, Phospholipase D cerebrospinal fluid, Phospholipase D chemistry, Lipoproteins, HDL blood, Phospholipase D blood
Abstract

Phosphatidylinositol (PtdIns)-glycan-specific phospholipase D was purified from bovine and human serum by phase separation in Triton X-114 and by chromatography on DEAE-cellulose, octyl-Sepharose, concanavalin-A-Sepharose, and hydroxyapatite. The purification of the two enzymes was approximately 1200-fold with a recovery of 3-5%. Bovine serum contained about 40 micrograms/ml of PtdIns-glycan-specific phospholipase D, about 10 times more than the amount determined in human serum. PtdIns-glycan-specific phospholipase D is also present in mammalian cerebrospinal fluid and in mammalian milk but to a much lesser extent than in serum. Enzyme from bovine and human serum displayed amphiphilic properties as revealed by sucrose density gradient centrifugation and gel filtration in the absence and presence of detergent. On density gradient centrifugation, both enzymes sedimented with an apparent sedimentation coefficient of about 6.0 S in the presence of 0.1% Triton X-100, and formed aggregates up to 14.5 S in the absence of detergent. Upon gel filtration, the bovine and human enzymes migrated with a Stokes' radius of 6.5 nm and 6.6 nm, respectively, in the presence of Triton X-100. In the absence of Triton X-100, both enzymes gave a Stokes' radius of 8.8 nm. Serial centrifugation of serum at increasing NaBr concentrations revealed that the majority of the enzyme is contained in the high-density lipoprotein fraction. PtdIns-glycan-specific phospholipase D from bovine and human serum contained 27 and 28 N-acetylglucosamine residues, respectively. Treatment with N-glycosidase F decreased the apparent molecular mass of the bovine and human enzyme from 115 and 123 kDa to 91 and 87 kDa, respectively. Sequence analysis of peptides derived from PtdIns-glycan-specific phospholipase D of bovine serum by CNBr cleavage gave 100% identity to the sequence published for the bovine liver enzyme while there was 83% similarity and 74% identity to the sequence of peptides obtained from the human serum enzyme.

Published
1992
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