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2. Early long-term administration of the CSF1R inhibitor PLX3397 ablates microglia and reduces accumulation of intraneuronal amyloid, neuritic plaque deposition and pre-fibrillar oligomers in 5XFAD mouse model of Alzheimer’s disease

Author

Justyna Sosna, Stephan Philipp, Ricardo Albay, Jorge Mauricio Reyes-Ruiz, David Baglietto-Vargas, Frank M. LaFerla, and Charles G. Glabe

Subjects
Alzheimer’s disease, Amyloid beta, Plaques, Intraneuronal amyloid, Microglia, Neuroinflammation, Neurology. Diseases of the nervous system, RC346-429, Geriatrics, RC952-954.6
Abstract

Abstract Background Besides the two main classical features of amyloid beta aggregation and tau-containing neurofibrillary tangle deposition, neuroinflammation plays an important yet unclear role in the pathophysiology of Alzheimer’s disease (AD). Microglia are believed to be key mediators of neuroinflammation during AD and responsible for the regulation of brain homeostasis by balancing neurotoxicity and neuroprotective events. We have previously reported evidence that neuritic plaques are derived from dead neurons that have accumulated intraneuronal amyloid and further recruit Iba1-positive cells, which play a role in either neuronal demise or neuritic plaque maturation or both. Methods To study the impact of microglia on neuritic plaque development, we treated two-month-old 5XFAD mice with a selective colony stimulation factor 1 receptor (CSF1R) inhibitor, PLX3397, for a period of 3 months, resulting in a significant ablation of microglia. Directly after this treatment, we analyzed the amount of intraneuronal amyloid and neuritic plaques and performed behavioral studies including Y-maze, fear conditioning and elevated plus maze. Results We found that early long-term PLX3397 administration results in a dramatic reduction of both intraneuronal amyloid as well as neuritic plaque deposition. PLX3397 treated young 5XFAD mice also displayed a significant decrease of soluble fibrillar amyloid oligomers in brain lysates, a depletion of soluble pre-fibrillar oligomers in plasma and an improvement in cognitive function measured by fear conditioning tests. Conclusions Our findings demonstrate that CSF1R signaling, either directly on neurons or mediated by microglia, is crucial for the accumulation of intraneuronal amyloid and formation of neuritic plaques, suggesting that these two events are serially linked in a causal pathway leading to neurodegeneration and neuritic plaque formation. CSF1R inhibitors represent potential preventative or therapeutic approach that target the very earliest stages of the formation of intraneuronal amyloid and neuritic plaques.

Published
2018
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4. Viki LibraRy

Author

Babbili, Shaduan, primary, Bönisch, Kevin, additional, Heinrich, Yannick, additional, Stephan, Philipp, additional, Abrami, Giuseppe, additional, and Mehler, Alexander, additional

Published
2023
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7. Structure-based inhibitors of amyloid beta core suggest a common interface with tau

Author

Sarah L Griner, Paul Seidler, Jeannette Bowler, Kevin A Murray, Tianxiao Peter Yang, Shruti Sahay, Michael R Sawaya, Duilio Cascio, Jose A Rodriguez, Stephan Philipp, Justyna Sosna, Charles G Glabe, Tamir Gonen, and David S Eisenberg

Subjects
amyloid beta, tau, inhibitor, MicroED, amyloid, cross-seeding, Medicine, Science, Biology (General), QH301-705.5
Abstract

Alzheimer’s disease (AD) pathology is characterized by plaques of amyloid beta (Aβ) and neurofibrillary tangles of tau. Aβ aggregation is thought to occur at early stages of the disease, and ultimately gives way to the formation of tau tangles which track with cognitive decline in humans. Here, we report the crystal structure of an Aβ core segment determined by MicroED and in it, note characteristics of both fibrillar and oligomeric structure. Using this structure, we designed peptide-based inhibitors that reduce Aβ aggregation and toxicity of already-aggregated species. Unexpectedly, we also found that these inhibitors reduce the efficiency of Aβ-mediated tau aggregation, and moreover reduce aggregation and self-seeding of tau fibrils. The ability of these inhibitors to interfere with both Aβ and tau seeds suggests these fibrils share a common epitope, and supports the hypothesis that cross-seeding is one mechanism by which amyloid is linked to tau aggregation and could promote cognitive decline.

Published
2019
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9. Vorderer und Mittlerer Orient

Author

Asmus, Sebastian, Borchardt, Ulrike, Hensell, Stephan, Ihlau, Dagmar, Huwe, Stephan-Philipp, Endres, Jürgen, Schlaphoff, Marc, Conrad, Burkhard, Stock, Franziska, Mößner, Nicola, Rabehl, Thomas, editor, and Schreiber, Wolfgang, editor

Published
2001
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10. Atomic structures of fibrillar segments of hIAPP suggest tightly mated β-sheets are important for cytotoxicity

Author

Pascal Krotee, Jose A Rodriguez, Michael R Sawaya, Duilio Cascio, Francis E Reyes, Dan Shi, Johan Hattne, Brent L Nannenga, Marie E Oskarsson, Stephan Philipp, Sarah Griner, Lin Jiang, Charles G Glabe, Gunilla T Westermark, Tamir Gonen, and David S Eisenberg

Subjects
islet amyloid polypeptide, amyloid fibril, cytotoxicity, MicroED, Type-II Diabetes, Medicine, Science, Biology (General), QH301-705.5
Abstract

hIAPP fibrils are associated with Type-II Diabetes, but the link of hIAPP structure to islet cell death remains elusive. Here we observe that hIAPP fibrils are cytotoxic to cultured pancreatic β-cells, leading us to determine the structure and cytotoxicity of protein segments composing the amyloid spine of hIAPP. Using the cryoEM method MicroED, we discover that one segment, 19–29 S20G, forms pairs of β-sheets mated by a dry interface that share structural features with and are similarly cytotoxic to full-length hIAPP fibrils. In contrast, a second segment, 15–25 WT, forms non-toxic labile β-sheets. These segments possess different structures and cytotoxic effects, however, both can seed full-length hIAPP, and cause hIAPP to take on the cytotoxic and structural features of that segment. These results suggest that protein segment structures represent polymorphs of their parent protein and that segment 19–29 S20G may serve as a model for the toxic spine of hIAPP.

Published
2017
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11. Vorderer und Mittlerer Orient

Author

Hänlein, Rüdiger, Neukirch, Claus, Rabehl, Thomas, Trines, Stefan, Huwe, Stephan-Philipp, Endres, Jürgen, Dorenwendt, Thomas, Schmitt, Mathias, and Rabehl, Thomas, editor

Published
1999
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12. Asien

Author

Wilke, Boris, Schneider, Nils-Thomas, Rabehl, Thomas, Segelcken, Iris, Huwe, Stephan-Philipp, Köllmann, Thomas, Böge, Volker, Scholz, Sonja, Franke, Jens Peter, and Rabehl, Thomas, editor

Published
1999
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16. No association of the BDNF val66met polymorphism with implicit associative vocabulary and motor learning.

Author

Nils Freundlieb, Stephan Philipp, Susanne A Schneider, Norbert Brüggemann, Christine Klein, Christian Gerloff, and Friedhelm C Hummel

Subjects
Medicine, Science
Abstract

Brain-derived neurotrophic factor (BDNF) has been suggested to play a major role in plasticity, neurogenesis and learning in the adult brain. The BDNF gene contains a common val66met polymorphism associated with decreased activity-dependent excretion of BDNF and a potential influence on behaviour, more specifically, on motor learning. The objective of this study was to determine the influence of the BDNF val66met polymorphism on short-term implicit associative learning and whether its influence is cognitive domain-specific (motor vs. language). A sample of 38 young healthy participants was genotyped, screened for background and neuropsychological differences, and tested with two associative implicit learning paradigms in two different cognitive domains, i.e., motor and vocabulary learning. Subjects performed the serial reaction time task (SRTT) to determine implicit motor learning and a recently established associative vocabulary learning task (AVL) for implicit learning of action and object words. To determine the influence of the BDNF polymorphism on domain-specific implicit learning, behavioural improvements in the two tasks were compared between val/val (n = 22) and met carriers (val/met: n = 15 and met/met: n = 1). There was no evidence for an impact of the BDNF val66met polymorphism on the behavioural outcome in implicit short-term learning paradigms in young healthy subjects. Whether this polymorphism plays a relevant role in long-term training paradigms or in subjects with impaired neuronal plasticity or reduced learning capacity, such as aged individuals, demented patients or patients with brain lesions, has to be determined in future studies.

Published
2012
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22. TRPC1- and TRPC3-dependent Ca2+signaling in mouse cortical astrocytes affects injury-evoked astrogliosisin vivo

Author

Stephan Philipp, Andreas Keller, Frank Kirchhoff, Veit Flockerzi, Thabet Belkacemi, Anja Scheller, Ulrich Wissenbach, Eckart Meese, Lutz Birnbaumer, Alexander Niermann, Petra Weissgerber, Petra Leidinger, Andreas Beck, Xianshu Bai, Laura Hofmann, and Christina Backes

Subjects
0301 basic medicine, biology, medicine.disease, Astrogliosis, TRPC1, 03 medical and health sciences, Cellular and Molecular Neuroscience, Transient receptor potential channel, 030104 developmental biology, 0302 clinical medicine, TRPC3, medicine.anatomical_structure, Neurology, Gliosis, medicine, Glutamate aspartate transporter, biology.protein, medicine.symptom, Neuroscience, 030217 neurology & neurosurgery, TRPC, Astrocyte
Abstract

Following brain injury astrocytes change into a reactive state, proliferate and grow into the site of lesion, a process called astrogliosis, initiated and regulated by changes in cytoplasmic Ca2+ . Transient receptor potential canonical (TRPC) channels may contribute to Ca2+ influx but their presence and possible function in astrocytes is not known. By RT-PCR and RNA sequencing we identified transcripts of Trpc1, Trpc2, Trpc3, and Trpc4 in FACS-sorted glutamate aspartate transporter (GLAST)-positive cultured mouse cortical astrocytes and subcloned full-length Trpc1 and Trpc3 cDNAs from these cells. Ca2+ entry in cortical astrocytes depended on TRPC3 and was increased in the absence of Trpc1. After co-expression of Trpc1 and Trpc3 in HEK-293 cells both proteins co-immunoprecipitate and form functional heteromeric channels, with TRPC1 reducing TRPC3 activity. In vitro, lack of Trpc3 reduced astrocyte proliferation and migration whereas the TRPC3 gain-of-function moonwalker mutation and Trpc1 deficiency increased astrocyte migration. In vivo, astrogliosis and cortex edema following stab wound injury were reduced in Trpc3-/- but increased in Trpc1-/- mice. In summary, our results show a decisive contribution of TRPC3 to astrocyte Ca2+ signaling, which is even augmented in the absence of Trpc1, in particular following brain injury. Targeted therapies to reduce TRPC3 channel activity in astrocytes might therefore be beneficial in traumatic brain injury.

Published
2017
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23. Author response: Structure-based inhibitors of amyloid beta core suggest a common interface with tau

Author

Stephan Philipp, Sarah Griner, David Eisenberg, Duilio Cascio, Jose A. Rodriguez, Shruti Sahay, Kevin A. Murray, Tamir Gonen, Paul M. Seidler, Justyna Sosna, Jeannette Bowler, Charles G. Glabe, Michael R. Sawaya, and Tianxiao Peter Yang

Subjects
Core (optical fiber), Materials science, biology, Interface (Java), Amyloid beta, Biophysics, biology.protein, Structure based
Published
2019
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24. P4‐697: ATOMIC STRUCTURES OF A SINGLE CHAIN ANTIBODY THAT BINDS AND INHIBITS SEEDING BY TAU OLIGOMERS

Author

Romany Abskharon, Duilio Cascio, Charles G. Glabe, David Eisenberg, Paul M. Seidler, Michael R. Sawaya, and Stephan Philipp

Subjects
biology, Epidemiology, Chemistry, Health Policy, Single chain, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Biophysics, biology.protein, Seeding, Neurology (clinical), Geriatrics and Gerontology, Antibody
Published
2019
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25. Effects of climate change on regional energy systems

Author

Hausl, Stephan Philipp, Hamacher, Thomas (Prof. Dr.), and Streicher, Wolfgang (Prof. Dr.)

Subjects
Ingenieurwissenschaften, ddc:620, Climate change, Energy system modelling, Regional energy systems, Regional climate models, Energy system optimisation, Space heating demand, Cooling demand, Renewable energies, GIS, RESRO, Klimawandel, Energiesystemmodellierung, Regionale Energiesysteme, Regionale Klimamodelle, Energiesystemoptimierung, Heizbedarf, Kühlbedarf, Erneuerbare Energien, GIS, RESRO
Abstract

In vorliegender Arbeit werden die Auswirkungen des Klimawandels auf regionale Energiesysteme untersucht. Auf Basis räumlich hochaufgelöster Klima- und Gebäudedaten werden hierzu der Wärme- und Kältebedarf für drei ländlich geprägte Regionen in Österreich bis zum Jahr 2050 modelliert. Die Ergebnisse finden Eingang in eine Energiesystemoptimierung, bei der die kostenoptimale Energiebereitstellung unter Berücksichtigung regional verfügbarer Potenziale erneuerbarer Energien berechnet wird. Neben den Erkenntnissen zur klimabedingten Verschiebung zwischen Wärme- und Kältebedarf in Gebäuden zeigt die Arbeit somit Konzepte zur zukünftigen Zusammensetzung regionaler Energiesysteme auf. In the following thesis effects of climate change on regional energy systems are examined. Heating and cooling demand for three rural regions in Austria are modelled until the year 2050 using climate and building data with high spatial resolution. The outcomes are then fed into an energy system optimisation, where the cost-optimum energy supply considering regionally available renewable energy potentials is calculated. The thesis provides findings about the climate-induced shift between heating and cooling demand in buildings, and shows concepts concerning the future composition of regional energy systems.

Published
2019

26. A background Ca2+entry pathway mediated by TRPC1/TRPC4 is critical for development of pathological cardiac remodelling

Author

Veit Flockerzi, Frank Schweda, Ulrich Laufs, Laura Schröder, Tao He, Juan E. Camacho Londoño, Marc Freichel, Stefanie Mannebach, Ilka Mathar, Martin Oberhofer, Lars Kaestner, Peter Lipp, Stephan Philipp, Wiebke Tabellion, Karin P. Hammer, Jan Christian Reil, Alexander Dietrich, Lutz Birnbaumer, Julia Camacho Londoño, and Qinghai Tian

Subjects
medicine.medical_specialty, Otras Ciencias Biológicas, Angiotensinogen, Cardiomegaly, Muscle hypertrophy, Ciencias Biológicas, purl.org/becyt/ford/1 [https], TRPC3, Basic Science, Internal medicine, Cardiac remodelling, medicine, Animals, Homeostasis, Myocytes, Cardiac, Calcium Signaling, purl.org/becyt/ford/1.6 [https], Ventricular remodeling, TRPC, TRPC Cation Channels, Mice, Knockout, Ventricular Remodeling, business.industry, Angiotensin II, Cardiac myocyte, Hemodynamics, TRPC1/TRPC4, medicine.disease, Endocrinology, Ion channels, Knockout mouse, cardiovascular system, Background Ca2+ entry, Calcium, Calcium Channels, Cardiology and Cardiovascular Medicine, business, CIENCIAS NATURALES Y EXACTAS
Abstract

Aims: Pathological cardiac hypertrophy is a major predictor for the development of cardiac diseases. It is associated with chronic neurohumoral stimulation and with altered cardiac Ca2+ signalling in cardiomyocytes. TRPC proteins form agonist-induced cation channels, but their functional role for Ca2+ homeostasis in cardiomyocytes during fast cytosolic Ca2+ cycling and neurohumoral stimulation leading to hypertrophy is unknown. Methods and results: In a systematic analysis of multiple knockout mice using fluorescence imaging of electrically paced adult ventricular cardiomyocytes and Mn2+-quench microfluorimetry, we identified a background Ca2+ entry (BGCE) pathway that critically depends on TRPC1/C4 proteins but not others such as TRPC3/C6. Reduction of BGCE in TRPC1/C4-deficient cardiomyocytes lowers diastolic and systolic Ca2+ concentrations both, under basal conditions and under neurohumoral stimulation without affecting cardiac contractility measured in isolated hearts and in vivo. Neurohumoral-induced cardiac hypertrophy as well as the expression of foetal genes (ANP, BNP) and genes regulated by Ca2+-dependent signalling (RCAN1-4, myomaxin) was reduced in TRPC1/C4 knockout (DKO), but not in TRPC1- or TRPC4-single knockout mice. Pressure overload-induced hypertrophy and interstitial fibrosis were both ameliorated in TRPC1/C4-DKO mice, whereas they did not show alterations in other cardiovascular parameters contributing to systemic neurohumoral-induced hypertrophy such as renin secretion and blood pressure. Conclusions: The constitutively active TRPC1/C4-dependent BGCE fine-tunes Ca2+ cycling in beating adult cardiomyocytes. TRPC1/C4-gene inactivation protects against development of maladaptive cardiac remodelling without altering cardiac or extracardiac functions contributing to this pathogenesis. Fil: Camacho Londoño, Juan E.. Pharmakologisches Institut; Alemania. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania. German Centre for Cardiovascular Research; Alemania Fil: Tian, Qinghai. Institut fur Molekulare Zellbiologie; Alemania Fil: Hammer, Karin. Institut fur Molekulare Zellbiologie; Alemania Fil: Schröder, Laura. Institut fur Molekulare Zellbiologie; Alemania Fil: Camacho Londoño, Julia. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania Fil: Reil, Jan C.. Universitat des Saarlandes; Alemania Fil: He, Tao. German Centre for Cardiovascular Research; Alemania. Research Unit Cardiac Epigenetics; Alemania. Tongji Hospital; China Fil: Oberhofer, Martin. Institut fur Molekulare Zellbiologie; Alemania Fil: Mannebach, Stefanie. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania Fil: Mathar, Ilka. Pharmakologisches Institut; Alemania. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania Fil: Philipp, Stephan E.. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania Fil: Tabellion, Wiebke. Institut fur Molekulare Zellbiologie; Alemania Fil: Schweda, Frank. Universitat Regensburg; Alemania Fil: Dietrich, Alexander. Walther-Straub-Institut fur Pharmakologie und Toxikologie; Alemania Fil: Kaestner, Lars. Institut fur Molekulare Zellbiologie; Alemania Fil: Laufs, Ulrich. Universitat des Saarlandes; Alemania Fil: Birnbaumer, Lutz. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Transmembrane Signaling Group; Alemania Fil: Flockerzi, Veit. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania Fil: Freichel, Marc. Pharmakologisches Institut; Alemania. Experimentelle und Klinische Pharmakologie und Toxikologie; Alemania. German Centre for Cardiovascular Research; Alemania Fil: Lipp, Peter. Institut fur Molekulare Zellbiologie; Alemania

Published
2015
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27. Auswirkungen des Klimawandels auf regionale Energiesysteme

Author

Hamacher, Thomas (Prof. Dr.), Streicher, Wolfgang (Prof. Dr.), Hausl, Stephan Philipp, Hamacher, Thomas (Prof. Dr.), Streicher, Wolfgang (Prof. Dr.), and Hausl, Stephan Philipp

Abstract

In vorliegender Arbeit werden die Auswirkungen des Klimawandels auf regionale Energiesysteme untersucht. Auf Basis räumlich hochaufgelöster Klima- und Gebäudedaten werden hierzu der Wärme- und Kältebedarf für drei ländlich geprägte Regionen in Österreich bis zum Jahr 2050 modelliert. Die Ergebnisse finden Eingang in eine Energiesystemoptimierung, bei der die kostenoptimale Energiebereitstellung unter Berücksichtigung regional verfügbarer Potenziale erneuerbarer Energien berechnet wird. Neben den Erkenntnissen zur klimabedingten Verschiebung zwischen Wärme- und Kältebedarf in Gebäuden zeigt die Arbeit somit Konzepte zur zukünftigen Zusammensetzung regionaler Energiesysteme auf., In the following thesis effects of climate change on regional energy systems are examined. Heating and cooling demand for three rural regions in Austria are modelled until the year 2050 using climate and building data with high spatial resolution. The outcomes are then fed into an energy system optimisation, where the cost-optimum energy supply considering regionally available renewable energy potentials is calculated. The thesis provides findings about the climate-induced shift between heating and cooling demand in buildings, and shows concepts concerning the future composition of regional energy systems.

Published
2019

28. Common fibrillar spines of amyloid-β and human islet amyloid polypeptide revealed by microelectron diffraction and structure-based inhibitors

Author

Michael R. Sawaya, Pascal Krotee, Paul M. Seidler, Dan Shi, Charles G. Glabe, Sarah Griner, Lorena Saelices, David Eisenberg, Kevin A. Murray, Duilio Cascio, Ji Lee, Stephan Philipp, Tamir Gonen, Lin Jiang, and Jose Rodriguez

Subjects
Models, Molecular, 0301 basic medicine, Aging, Molecular model, Amyloid β, Neurodegenerative, Crystallography, X-Ray, Alzheimer's Disease, Biochemistry, Medical and Health Sciences, Mice, 0302 clinical medicine, Models, Insulin-Secreting Cells, 2.1 Biological and endogenous factors, Aetiology, Cytotoxicity, Nootropic Agents, Neurons, Microscopy, geography.geographical_feature_category, Tumor, Crystallography, Chemistry, Diabetes, amyloid, Molecular Bases of Disease, Neurofibrillary Tangles, Biological Sciences, Islet, Recombinant Proteins, Islet Amyloid Polypeptide, inhibitor, Neurological, electron diffraction, crystal structure, Biochemistry & Molecular Biology, Amyloid, human islet amyloid polypeptide, Structural similarity, amyloid-β, Fibril, Protein Aggregation, Pathological, Electron, peptide interaction, Cell Line, 03 medical and health sciences, Microscopy, Electron, Transmission, Pathological, Cell Line, Tumor, Acquired Cognitive Impairment, Animals, Humans, Hypoglycemic Agents, Transmission, Molecular Biology, Metabolic and endocrine, geography, Amyloid beta-Peptides, Computational Biology, Molecular, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Cell Biology, Protein Aggregation, Peptide Fragments, Rats, Brain Disorders, 030104 developmental biology, HEK293 Cells, Amino Acid Substitution, Drug Design, Mutation, Chemical Sciences, Biophysics, X-Ray, Structure based, Dementia, 030217 neurology & neurosurgery
Abstract

Amyloid-β (Aβ) and human islet amyloid polypeptide (hIAPP) aggregate to form amyloid fibrils that deposit in tissues and are associated with Alzheimer's disease (AD) and type II diabetes (T2D), respectively. Individuals with T2D have an increased risk of developing AD, and conversely, AD patients have an increased risk of developing T2D. Evidence suggests that this link between AD and T2D might originate from a structural similarity between aggregates of Aβ and hIAPP. Using the cryoEM method microelectron diffraction, we determined the atomic structures of 11-residue segments from both Aβ and hIAPP, termed Aβ(24–34) WT and hIAPP(19–29) S20G, with 64% sequence similarity. We observed a high degree of structural similarity between their backbone atoms (0.96-Å root mean square deviation). Moreover, fibrils of these segments induced amyloid formation through self- and cross-seeding. Furthermore, inhibitors designed for one segment showed cross-efficacy for full-length Aβ and hIAPP and reduced cytotoxicity of both proteins, although by apparently blocking different cytotoxic mechanisms. The similarity of the atomic structures of Aβ(24–34) WT and hIAPP(19–29) S20G offers a molecular model for cross-seeding between Aβ and hIAPP.

Published
2018

29. Early long-term administration of the CSF1R inhibitor PLX3397 ablates microglia and reduces accumulation of intraneuronal amyloid, neuritic plaque deposition and pre-fibrillar oligomers in 5XFAD mouse model of Alzheimer's disease

Author

Ricardo Albay, Frank M. LaFerla, Charles G. Glabe, Jorge Mauricio Reyes-Ruiz, David Baglietto-Vargas, Justyna Sosna, and Stephan Philipp

Subjects
0301 basic medicine, Amyloid, Amyloid beta, Aminopyridines, Amyloidogenic Proteins, Mice, Transgenic, Plaque, Amyloid, lcsh:Geriatrics, lcsh:RC346-429, 03 medical and health sciences, Cellular and Molecular Neuroscience, Mice, 0302 clinical medicine, Neuroinflammation, Alzheimer Disease, medicine, Animals, Pyrroles, Senile plaques, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, Neurons, biology, Microglia, Chemistry, Neurodegeneration, Neurotoxicity, Brain, Neurofibrillary tangle, Alzheimer's disease, medicine.disease, 3. Good health, Cell biology, lcsh:RC952-954.6, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Plaques, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, biology.protein, Intraneuronal amyloid, Neurology (clinical), Alzheimer’s disease, 030217 neurology & neurosurgery, Research Article
Abstract

Background Besides the two main classical features of amyloid beta aggregation and tau-containing neurofibrillary tangle deposition, neuroinflammation plays an important yet unclear role in the pathophysiology of Alzheimer’s disease (AD). Microglia are believed to be key mediators of neuroinflammation during AD and responsible for the regulation of brain homeostasis by balancing neurotoxicity and neuroprotective events. We have previously reported evidence that neuritic plaques are derived from dead neurons that have accumulated intraneuronal amyloid and further recruit Iba1-positive cells, which play a role in either neuronal demise or neuritic plaque maturation or both. Methods To study the impact of microglia on neuritic plaque development, we treated two-month-old 5XFAD mice with a selective colony stimulation factor 1 receptor (CSF1R) inhibitor, PLX3397, for a period of 3 months, resulting in a significant ablation of microglia. Directly after this treatment, we analyzed the amount of intraneuronal amyloid and neuritic plaques and performed behavioral studies including Y-maze, fear conditioning and elevated plus maze. Results We found that early long-term PLX3397 administration results in a dramatic reduction of both intraneuronal amyloid as well as neuritic plaque deposition. PLX3397 treated young 5XFAD mice also displayed a significant decrease of soluble fibrillar amyloid oligomers in brain lysates, a depletion of soluble pre-fibrillar oligomers in plasma and an improvement in cognitive function measured by fear conditioning tests. Conclusions Our findings demonstrate that CSF1R signaling, either directly on neurons or mediated by microglia, is crucial for the accumulation of intraneuronal amyloid and formation of neuritic plaques, suggesting that these two events are serially linked in a causal pathway leading to neurodegeneration and neuritic plaque formation. CSF1R inhibitors represent potential preventative or therapeutic approach that target the very earliest stages of the formation of intraneuronal amyloid and neuritic plaques.

Published
2017
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32. The development of an authentic Mexican Food concept in Europe

Author

Grafl, Stephan Philipp and Duarte, Miguel Munoz

Subjects
Food concept, Authentic mexican cuisine, Development, Ciências Sociais::Economia e Gestão [Domínio/Área Científica], Casual dining
Abstract

Mexican food is on-trend. Top chefs around the world appreciate the variety of the cuisine and see a tremendous potential in it. In Europe, people are lacking knowledge of Mexican cuisine, because Mexican food services are rare in terms of authenticity and an adapted version of it is prevalent. Therefore, this work project focuses on the development of authentic Mexican food concept in Europe. Based on actual findings as well as primary and secondary research, four potential concepts are elaborated and evaluated in order to come up with a top concept – “Mercado Auténtico” with its mission, target markets, positioning and marketing-mix.

Published
2017

33. Atomic structures of fibrillar segments of hIAPP suggest tightly mated beta-sheets are important or cytotoxicity

Author

David Eisenberg, Pascal Krotee, Stephan Philipp, Michael R. Sawaya, Jose A. Rodriguez, Tamir Gonen, Marie E. Oskarsson, Gunilla T. Westermark, Duilio Cascio, Sarah Griner, Dan Shi, Charles G. Glabe, Brent L. Nannenga, Francis E. Reyes, Johan Hattne, and Lin Jiang

Subjects
0301 basic medicine, Protein Conformation, Cell- och molekylärbiologi, Biochemistry, Type ii diabetes, Insulin-Secreting Cells, biophysics, amyloid fibril, Cytotoxic T cell, structural biology, Biology (General), Cytotoxicity, Cells, Cultured, Cultured, Chemistry, General Neuroscience, General Medicine, Biophysics and Structural Biology, Islet Amyloid Polypeptide, Cell and molecular biology, Endokrinologi och diabetes, Medicine, cytotoxicity, MicroED, Research Article, Human, Programmed cell death, Amyloid, QH301-705.5, Cell Survival, Science, Cells, Endocrinology and Diabetes, Fibril, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Type-II Diabetes, Humans, biochemistry, human, 030102 biochemistry & molecular biology, General Immunology and Microbiology, Cryoelectron Microscopy, 030104 developmental biology, Structural biology, Biophysics, Protein Conformation, beta-Strand, beta-Strand, Generic health relevance, Biochemistry and Cell Biology, Cell and Molecular Biology
Abstract

hIAPP fibrils are associated with Type-II Diabetes, but the link of hIAPP structure to islet cell death remains elusive. Here we observe that hIAPP fibrils are cytotoxic to cultured pancreatic β-cells, leading us to determine the structure and cytotoxicity of protein segments composing the amyloid spine of hIAPP. Using the cryoEM method MicroED, we discover that one segment, 19–29 S20G, forms pairs of β-sheets mated by a dry interface that share structural features with and are similarly cytotoxic to full-length hIAPP fibrils. In contrast, a second segment, 15–25 WT, forms non-toxic labile β-sheets. These segments possess different structures and cytotoxic effects, however, both can seed full-length hIAPP, and cause hIAPP to take on the cytotoxic and structural features of that segment. These results suggest that protein segment structures represent polymorphs of their parent protein and that segment 19–29 S20G may serve as a model for the toxic spine of hIAPP. DOI: http://dx.doi.org/10.7554/eLife.19273.001, eLife digest In Type-II Diabetes, an individual’s cells fail to respond correctly to the hormone insulin, leaving them unable to counteract high levels of sugar in the blood. Another hormone, human islet amyloid polypeptide (hIAPP), works with insulin to regulate blood sugar levels. hIAPP is an amyloid protein, which means that it can lose its normal structure and form fibrils. Fibrils are difficult for cells to break down and are often associated with disease. Indeed, fibrils of hIAPP often form in the pancreas as part of Type-II Diabetes. Some studies have shown that hIAPP fibrils are toxic to pancreatic cells and worsen the symptoms of Type-II Diabetes. Others suggest that it is the process of fibril formation that is toxic, not the fibrils themselves. Although the structures of the fibrils have been described, whether these structures cause cell toxicity has not been investigated. Krotee et al. have now explored the structures of two overlapping segments of hIAPP using a new cryo electron microscopy method called MicroED that is ideal for studying such segments. One segment, called 19-29 S20G, forms a standard amyloid fibril structure that is similar to the structure of full-length hIAPP fibrils. Adding these segments to human cells causes similar levels of toxicity as the full-length hIAPP fibrils. The second segment, called 15-25 WT, forms a non-toxic structure that is less stable than standard amyloid fibrils. The results presented by Krotee et al. support the view that standard amyloid fibril structures are toxic to cells and suggest that 19-29 S20G may be a good model to use when studying how full-length hIAPP fibrils behave. The structure of 19-29 S20G may also be useful as a template for designing molecules that block amyloid fibril growth. If amyloid fibrils cause cell toxicity in the pancreas, then these molecules could be used to treat Type-II Diabetes. DOI: http://dx.doi.org/10.7554/eLife.19273.002

Published
2017

35. Differences and Similarities in TRAIL- and Tumor Necrosis Factor-Mediated Necroptotic Signaling in Cancer Cells

Author

Carina Saggau, Christoph Arenz, Justyna Sosna, Thomas Pinkert, Anna Trauzold, Johannes Plenge, Alexandra Föll, Stefan Schütze, Dieter Adam, Johaiber Fuchslocher Chico, Stephan Philipp, Ingo Schmitz, Holger Kalthoff, Jürgen Fritsch, and Helmholtz Centre for infection research

Subjects
0301 basic medicine, Programmed cell death, Necroptosis, ATG5, Apoptosis, Mitochondrion, Biology, Jurkat cells, TNF-Related Apoptosis-Inducing Ligand, 03 medical and health sciences, Jurkat Cells, Mice, Necrosis, Cell Line, Tumor, Neoplasms, Animals, Humans, Molecular Biology, Cell Biology, Articles, Mitochondria, 030104 developmental biology, Cancer cell, Immunology, Tumor Necrosis Factors, Cancer research, Tumor necrosis factor alpha, Signal transduction, HT29 Cells, Signal Transduction
Abstract

Recently, a type of regulated necrosis (RN) called necroptosis was identified to be involved in many pathophysiological processes and emerged as an alternative method to eliminate cancer cells. However, only a few studies have elucidated components of TRAIL-mediated necroptosis useful for anticancer therapy. Therefore, we have compared this type of cell death to tumor necrosis factor (TNF)-mediated necroptosis and found similar signaling through acid and neutral sphingomyelinases, the mitochondrial serine protease HtrA2/Omi, Atg5, and vacuolar H(+)-ATPase. Notably, executive mechanisms of both TRAIL- and TNF-mediated necroptosis are independent of poly(ADP-ribose) polymerase 1 (PARP-1), and depletion of p38α increases the levels of both types of cell death. Moreover, we found differences in signaling between TNF- and TRAIL-mediated necroptosis, e.g., a lack of involvement of ubiquitin carboxyl hydrolase L1 (UCH-L1) and Atg16L1 in executive mechanisms of TRAIL-mediated necroptosis. Furthermore, we discovered indications of an altered involvement of mitochondrial components, since overexpression of the mitochondrial protein Bcl-2 protected Jurkat cells from TRAIL- and TNF-mediated necroptosis, and overexpression of Bcl-XL diminished only TRAIL-induced necroptosis in Colo357 cells. Furthermore, TRAIL does not require receptor internalization and endosome-lysosome acidification to mediate necroptosis. Taken together, pathways described for TRAIL-mediated necroptosis and differences from those for TNF-mediated necroptosis might be unique targets to increase or modify necroptotic signaling and eliminate tumor cells more specifically in future anticancer approaches.

Published
2016

36. Cancer and necroptosis: friend or foe?

Author

Dieter Adam, Justyna Sosna, and Stephan Philipp

Subjects
0301 basic medicine, Cell signaling, Necrosis, Necroptosis, Context (language use), Apoptosis, Biology, Metastasis, TNF-Related Apoptosis-Inducing Ligand, 03 medical and health sciences, Cellular and Molecular Neuroscience, Neoplasms, medicine, Humans, Molecular Biology, Pharmacology, Tumor Necrosis Factor-alpha, Cancer, Cell Biology, medicine.disease, Cell biology, 030104 developmental biology, Molecular Medicine, Tumor necrosis factor alpha, Signal transduction, medicine.symptom, Neuroscience, Signal Transduction
Abstract

Regulated cell death is one major factor to ensure homoeostasis in multicellular organisms. For decades, apoptosis was considered as the sole form of regulated cell death, whereas necrosis was believed to be accidental and unregulated. Due to this view, research on necrosis was somewhat neglected, especially in the field of anti-cancer treatment. However, new interest in necrosis has been sparked by the recent discovery of different forms of necrosis that show indeed regulated pathways. More and more studies now address the molecular pathways of regulated necrosis and its connections within the cellular signaling networks. Necroptosis, a subform of regulated necrosis, has so far hardly been focused on with regard to a future treatment of cancer patients and may emerge as a novel and effective approach to eliminate tumor cells. However, and similar to apoptosis, tumor cells can develop resistances against necroptosis to ensure their own survival. In this context, new molecules that enhance necroptosis are currently being identified to overcome such resistances. This review discusses cancer and necroptosis as friends or foes, i.e. the options to exploit necroptosis in anti-cancer therapies ("foes"), but also potential limitations that may block or actually cause necroptosis to act in a protumoral manner ("friends"). The balance between these two possible roles will determine whether necroptosis can indeed be used as a promising tool for early diagnosis of tumors, prevention of metastasis and anti-cancer treatment.

Published
2016

37. Isolation of erythrocytes infected with viable early stages ofPlasmodium falciparumby flow cytometry

Author

Stephan Philipp, Hans-Heinrich Oberg, Matthias Leippe, Christoph Gelhaus, and Ottmar Janssen

Subjects
Erythrocytes, Time Factors, Histology, Plasmodium falciparum, Schizonts, Diamines, Parasitemia, Azure Stains, Plasmodium, Pathology and Forensic Medicine, Flow cytometry, parasitic diseases, medicine, Humans, Parasite hosting, Benzothiazoles, Organic Chemicals, Fluorescent Dyes, Staining and Labeling, biology, medicine.diagnostic_test, Cell Biology, Flow Cytometry, biology.organism_classification, medicine.disease, Virology, Malaria, Staining, Red blood cell, medicine.anatomical_structure, Quinolines, Cytometry
Abstract

The erythrocytic life cycle of Plasmodium falciparum is highly associated with severe clinical symptoms of malaria that causes hundreds of thousands of death each year. The parasite develops within human erythrocytes leading to the disruption of the infected red blood cell (iRBC) prior to the start of a new cycle of erythrocyte infection. Emerging mechanisms of resistance against antimalarial drugs require improved knowledge about parasite's blood stages to facilitate new alternative antimalarial strategies. For the analysis of young blood stages of Plasmodium at the molecular level, the isolation of ring stages is essential. However, early stages can hardly be separated from both, late stages and non-infected red blood cells using conventional methods. Here, iRBCs were stained with the DNA-binding dyes Vybrant® DyeCycle™ Violet and SYBR® Green I. Subsequently, cells were subjected to flow-cytometric analysis. This enabled the discrimination of early stage iRBCs as well as late-stage iRBCs from non-infected erythrocytes and the properties of the used dyes were evaluated. Moreover, early stage iRBCs were isolated with high purity (>98%) by FACS. Subsequently, development of sorted early stages of the parasite was monitored over time and compared with control cultures. The described flow cytometry method, based on staining with Vybrant DyeCycle Violet, allows the isolation of viable ring stages of the malarial agent P. falciparum, and thereby provides the basis for new, broad-range molecular investigations of the parasite. © 2012 International Society for Advancement of Cytometry

Published
2012
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38. The Polycomb group protein EED couples TNF receptor 1 to neutral sphingomyelinase

Author

Malte Puchert, Sabine Mathieu, Stephan Philipp, Yusuf A. Hannun, Norma Marchesini, Ljudmila Kolker, Stefan Schütze, Vladimir Tchikov, Dieter Adam, Sabine Adam-Klages, Dieter Kabelitz, Andrea Deerberg, and Supandi Winoto-Morbach

Subjects
Multidisciplinary, Polycomb Repressive Complex 2, Inflammation, Biological Sciences, Biology, Receptors, Tumor Necrosis Factor, Proinflammatory cytokine, Enzyme Activation, Repressor Proteins, Enzyme activator, Sphingomyelin Phosphodiesterase, Mediator, RNA interference, Cancer research, medicine, Humans, Tumor necrosis factor alpha, Signal transduction, medicine.symptom, Protein FAN, HeLa Cells
Abstract

The phospholipase neutral sphingomyelinase (N-SMase) has been recognized as a major mediator of processes such as inflammation, development and growth, differentiation and death of cells, as well as in diseases such as Alzheimer’s, atherosclerosis, heart failure, ischemia/reperfusion damage, or combined pituitary hormone deficiency. Although activation of N-SMase by the proinflammatory cytokine TNF was described almost two decades ago, the underlying signaling pathway is unresolved. Here, we identify the Polycomb group protein EED (embryonic ectodermal development) as an interaction partner of nSMase2. In yeast, the N terminus of EED binds to the catalytic domain of nSMase2 as well as to RACK1, a protein that modulates the activation of nSMase2 by TNF in concert with the TNF receptor 1 (TNF-R1)-associated protein FAN. In mammalian cells, TNF causes endogenous EED to translocate from the nucleus and to colocalize and physically interact with both endogenous nSMase2 and RACK1. As a consequence, EED and nSMase2 are recruited to the TNF-R1•FAN•RACK1-complex in a timeframe concurrent with activation of nSMase2. After knockdown of EED by RNA interference, the TNF-dependent activation of nSMase2 is completely abrogated, identifying EED as a protein that both physically and functionally couples TNF-R1 to nSMase2, and which therefore represents the “missing link” that completes one of the last unresolved signaling pathways of TNF-R1.

Published
2009
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39. Aluminiumschaum zur Verbesserung der Akustik und des Crashverhaltens

Author

Steffen Klan, Dirk Weid, Stephan Philipp, and Leopold Kniewallner

Subjects
Gynecology, medicine.medical_specialty, media_common.quotation_subject, Automotive Engineering, medicine, Art, Humanities, media_common
Abstract

Bis heute ist es nicht gelungen, Aluminiumschaume in der Grosserienfertigung des Fahrzeugbaus anzuwenden. Dies liegt unter anderem daran, dass fur die Automobilindustrie die Wirtschaftlichkeit der Anwendung noch nicht gegeben ist und noch keine Werkstoffmodelle vorliegen, um das Verhalten von Aluminiumschaum durch Simulation hinreichend genau vorherzusagen. Georg Fischer Automotive hat zusammen mit dem kanadischen Unternehmen Cymat ein Verfahren weiterentwickelt, das vor allem bezuglich Wirtschaftlichkeit und Flexibilitat bei der Formgebung uberzeugt.

Published
2007
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40. Homoharringtonine, a clinically approved anti-leukemia drug, sensitizes tumor cells for TRAIL-induced necroptosis

Author

Holger Kalthoff, Johannes Plenge, Dieter Adam, Justyna Sosna, and Stephan Philipp

Subjects
Regulated necrosis, Harringtonines, Myeloid, Necroptosis, Antineoplastic Agents, TRAIL, Pharmacology, Biology, Biochemistry, TNF-Related Apoptosis-Inducing Ligand, Necrosis, RIPK1, Cell Line, Tumor, Neoplasms, medicine, Humans, Cytotoxic T cell, Cycloheximide, Molecular Biology, Protein Synthesis Inhibitors, Research, Cancer, Cell Biology, medicine.disease, Receptors, TNF-Related Apoptosis-Inducing Ligand, medicine.anatomical_structure, Apoptosis, Homoharringtonine, Cancer cell, Signal Transduction
Abstract

Background One hallmark of cancer cells is their ability to evade physiologic signals causing regulated cell death (RCD). Correspondingly, TRAIL-based therapies to eliminate human cancer cells via enforced induction of apoptosis have been established and represent a promising approach in anti-cancer research. However, due to frequently appearing intrinsic or acquired resistances of tumor cells against apoptosis, TRAIL-based apoptotic strategies for the treatment of cancer patients have shown limited efficacy. As a potential alternative, regulated necrosis (and necroptosis triggered e.g. by TRAIL receptors 1/2) has recently gained considerable attention. Regulated necrosis represents a mode of RCD molecularly distinct from apoptosis whose potential in anti-cancer therapy is almost uncharacterized. Since in most cancer cells survival pathways counteract the effects of TRAIL-induced RCD, sensitizers such as cycloheximide (CHX) are frequently added in cell culture to overcome this problem. Unfortunately, those sensitizers are cytotoxic and therefore not suitable for the treatment of cancer patients. Here, we have alternatively employed homoharringtonine (HHT), a plant alkaloid which was recently approved by the U. S. Food and Drug Administration to treat patients with chronic myeloid lymphoma. Results We show that HHT is an efficient sensitizer for TRAIL-induced necroptosis in multiple human cancer cell lines. In addition, HHT-enhanced TRAIL-mediated necroptosis occurs via the same signaling pathways (involving RIPK1/RIPK3/MLKL) as CHX-enhanced necroptosis. Importantly, consecutive treatment schedules of necroptosis and apoptosis in either combination revealed remarkable additive effects not reached by repetitive apoptotic treatments alone. Conclusions Taken together, our data demonstrate that HHT can replace harmful substances such as CHX to sensitize human cancer cells to TRAIL-induced necroptosis. Thus, HHT represents a promising enhancer in TRAIL-based necroptotic anti-cancer therapies also in patients.

Published
2015
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41. TRPV6 potentiates calcium-dependent cell proliferation

Author

Stephan Philipp, Barbara A. Niemeyer, Markus Hoth, Veit Flockerzi, Eva C. Schwarz, Ulrich Wissenbach, and Bettina Strauss

Subjects
Male, Programmed cell death, TRPV6, Cell Survival, Physiology, Gene Expression, TRPV Cation Channels, Biology, Transfection, Cell Line, Thiadiazoles, Humans, Anilides, Calcium Signaling, Molecular Biology, Cell Proliferation, Cell growth, Calcium channel, Prostatic Neoplasms, Cell Biology, Molecular biology, Recombinant Proteins, Cell biology, Cell culture, Apoptosis, Calcium Channels, Econazole, Homeostasis
Abstract

The Ca(2+) homeostasis within cells controls a diversity of cellular processes including gene transcription, proliferation and apoptosis. Perturbance of Ca(2+) signaling may induce deregulation of cell proliferation and suppression of cell death providing the basis for cancer development. In human prostate cancer, a correlation between the mRNA expression of the Ca(2+) channel TRPV6 and the staging of the cancer has been described. We have analyzed the influence of TRPV6 on cell proliferation within HEK-293 cells. We show that TRPV6 increases cell proliferation of HEK-293 cells in a Ca(2+) dependent manner. The increased proliferation correlates with slightly increased intracellular Ca(2+) levels without interfering with the intrinsic Ca(2+) dependence of HEK-293 cell proliferation. Low doses of econazole inhibit both, TRPV6 dependent Ca(2+) signals and cell proliferation while BTP2, a potent inhibitor of Ca(2+) signals and cell proliferation in T-cells, neither influences TRPV6 dependent Ca(2+) signals nor cell proliferation of HEK-293 cells. Our data demonstrate that TRPV6 increases the rate of Ca(2+) dependent cell proliferation which is a prerequisite for its potential role in tumor progression.

Published
2006
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42. Ipsilesional motor area size correlates with functional recovery after stroke: a 6-month follow-up longitudinal TMS motor mapping study

Author

Christian Gerloff, Anna Drabik, Friedhelm C. Hummel, Stephan Philipp, Nils Freundlieb, and Nils D. Forkert

Subjects
Adult, Male, medicine.medical_specialty, Neuronavigation, medicine.medical_treatment, Functional Laterality, Physical medicine and rehabilitation, Developmental Neuroscience, medicine, Humans, Longitudinal Studies, Stroke, Aged, Aged, 80 and over, Brain Mapping, Motor area, business.industry, Motor Cortex, Organ Size, Recovery of Function, Middle Aged, Functional recovery, medicine.disease, Transcranial Magnetic Stimulation, body regions, Transcranial magnetic stimulation, medicine.anatomical_structure, Neurology, Acute Disease, Chronic Disease, Upper limb, Female, Neurology (clinical), Motor mapping, business, Month follow up, Follow-Up Studies
Abstract

Transcranial magnetic stimulation (TMS) and measurements of upper limb function were longitudinally applied to gain further insights into processes involved in functional recovery from the acute to the chronic stage after stroke.10 acute stroke patients were monitored over 6 months behaviourally and with established TMS protocols. By using neuronavigated motor mapping, behavioural parameters, and a mixed model analysis, the role of the frontal and parietal part of the motor area of both hemispheres for functional recovery was determined.Size and volume of the ipsilesional motor area (MAipsi) were significantly decreased in the acute phase compared to the contralesional motor area (MAcontra). Size of MAipsi, especially its frontal part, changed over time and was positively correlated with functional recovery, whereas resting motor threshold, volume of both MA or the shift of its center of gravity did not show any association with recovery.The present data suggests the presence of a positive correlation between changes of the motor representation of the lesioned hemisphere and functional recovery after stroke. A possible interpretation is that rather (re-)activated corticomotor outputs are substrates of functional recovery after stroke than increased efficacy of residual, non-lesioned pathways.

Published
2014

43. Molecular analysis of regulation of gene expression of the human erythroid anion exchanger (AE) 1

Author

Matthias Kneussel, Heribert Appelhans, Jörg König, and Stephan Philipp

Subjects
Transcription, Genetic, Recombinant Fusion Proteins, Molecular Sequence Data, Biophysics, Erythroid specific expression, Biology, Transfection, Biochemistry, Antiporters, Hemoglobins, Genes, Reporter, Structural Biology, Transcription (biology), Gene expression, Genetics, Humans, Chloride-Bicarbonate Antiporters, Luciferases, Molecular Biology, Gene, Band 3, Anion exchanger 1, Regulation of gene expression, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, CT-rich region, Promoter, Cell Biology, Molecular biology, Gene Expression Regulation, Liposomes, Red blood cell maturation, biology.protein, K562 Cells, K562 cells
Abstract

The anion exchange protein AE1 is the most abundant membrane protein in human erythrocytes mediating the electroneutral chloride/bicarbonate exchange. We identified a promoter region in the 5′ flanking region of the human AE1 gene which controls transcription in a cell type independent manner. In addition a second, distal promoter element mediates gene expression only in erythroid cells and in dependence upon differentiation. Within this distal promoter region we defined a 44 bp sequence containing a novel CT-rich motif with very strong promoter activity whereas a second 28 bp segment suppresses gene expression.

Published
1998
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45. Cationic detergents enable the separation of membrane proteins of Plasmodium falciparum-infected erythrocytes by 2D gel electrophoresis

Author

Stephan, Philipp, Thomas, Jakoby, Andreas, Tholey, Ottmar, Janssen, Matthias, Leippe, and Christoph, Gelhaus

Subjects
Proteomics, Cetrimonium, Detergents, Erythrocyte Membrane, Plasmodium falciparum, Protozoan Proteins, Membrane Proteins, Host-Parasite Interactions, Quaternary Ammonium Compounds, Cetrimonium Compounds, Humans, Electrophoresis, Gel, Two-Dimensional, Fatty Alcohols, Malaria, Falciparum
Abstract

The intraerythrocytic stage of Plasmodium falciparum alters the characteristics of its host cell by exporting selected plasmodial proteins. Although it is clear that the physicochemical and immunobiological properties of the host cell are modulated during parasite development, the involved plasmodial proteins and their mode of action are not completely known. Using cetyltrimethylammonium bromide (CTAB) or benzyldimethyl-n-hexadecylammonium chloride (16-BAC) for the first dimension and SDS for the second dimension, we separated proteins from membranes of human erythrocytes and of erythrocytes infected with the malaria parasite P. falciparum. Protein spots were analyzed by MALDI-TOF/TOF MS and annotated in respective 2D master gels. By using the alternative 2D approach, characteristic host cell membrane proteins and, more importantly, membrane-associated and exported plasmodial proteins were identified that might play a role in parasite-induced host cell modulation.

Published
2012

46. No association of the BDNF val66met polymorphism with implicit associative vocabulary and motor learning

Author

Susanne A. Schneider, Christian Gerloff, Christine Klein, Norbert Brüggemann, Nils Freundlieb, Friedhelm C. Hummel, and Stephan Philipp

Subjects
Central Nervous System, Adult, Male, Serial reaction time, Genotype, Cognitive Neuroscience, Science, education, Neurophysiology, Biology, Verbal learning, Motor Reactions, Young Adult, Cognition, Learning and Memory, Genetic, Neuropsychology, Neurorehabilitation and Trauma, Reaction Time, Humans, Learning, Polymorphism, Motor Systems, Brain-derived neurotrophic factor, Polymorphism, Genetic, Multidisciplinary, Cognitive Neurology, Brain-Derived Neurotrophic Factor, Verbal Learning, Implicit learning, Associative learning, Neurology, Amino Acid Substitution, Medicine, Female, Motor learning, Psychomotor Performance, Research Article, Neuroscience, Cognitive psychology
Abstract

Brain-derived neurotrophic factor (BDNF) has been suggested to play a major role in plasticity, neurogenesis and learning in the adult brain. The BDNF gene contains a common val66met polymorphism associated with decreased activity-dependent excretion of BDNF and a potential influence on behaviour, more specifically, on motor learning. The objective of this study was to determine the influence of the BDNF val66met polymorphism on short-term implicit associative learning and whether its influence is cognitive domain-specific (motor vs. language). A sample of 38 young healthy participants was genotyped, screened for background and neuropsychological differences, and tested with two associative implicit learning paradigms in two different cognitive domains, i.e., motor and vocabulary learning. Subjects performed the serial reaction time task (SRTT) to determine implicit motor learning and a recently established associative vocabulary learning task (AVL) for implicit learning of action and object words. To determine the influence of the BDNF polymorphism on domain-specific implicit learning, behavioural improvements in the two tasks were compared between val/val (n = 22) and met carriers (val/met: n = 15 and met/met: n = 1). There was no evidence for an impact of the BDNF val66met polymorphism on the behavioural outcome in implicit short-term learning paradigms in young healthy subjects. Whether this polymorphism plays a relevant role in long-term training paradigms or in subjects with impaired neuronal plasticity or reduced learning capacity, such as aged individuals, demented patients or patients with brain lesions, has to be determined in future studies.

Published
2012

47. Thapsigargin induces expression of activating transcription factor 3 in human keratinocytes involving Ca2+ ions and c-Jun N-terminal protein kinase

Author

Shigetaka Kitajima, Stephan Philipp, Michael Raubuch, Markus Hoth, Gerald Thiel, Oliver G. Rössler, Daniel Spohn, and Désirée Griesemer

Subjects
Keratinocytes, Thapsigargin, Cations, Divalent, p38 mitogen-activated protein kinases, Activating transcription factor, Apoptosis, Calcium-Transporting ATPases, Biology, p38 Mitogen-Activated Protein Kinases, Cell Line, chemistry.chemical_compound, Humans, Protein kinase A, Pharmacology, Activating Transcription Factor 1, Caspase 7, Caspase 3, Endoplasmic reticulum, c-jun, JNK Mitogen-Activated Protein Kinases, Dual Specificity Phosphatase 1, Molecular biology, Cell biology, Up-Regulation, Enzyme Activation, HaCaT, chemistry, Molecular Medicine, Dual-Specificity Phosphatases, Mitogen-Activated Protein Kinase Phosphatases, Calcium, Signal transduction, Anisomycin, Signal Transduction
Abstract

Thapsigargin is a specific inhibitor of the sarco/endoplasmic reticulum Ca(2+) ATPase of the endoplasmic reticulum. Here, we show that stimulation of human HaCaT keratinocytes with nanomolar concentrations of thapsigargin triggers expression of activating transcription factor (ATF) 3, a basic-region leucin zipper transcription factor. ATF3 expression was also up-regulated in thapsigargin-stimulated glioma cells, hepatoma cells, retinal pigment epithelial cells, and airway epithelial cells. Thapsigargin-induced up-regulation of ATF3 expression in keratinocytes was attenuated by BAPTA-acetoxymethyl ester or by expression of the Ca(2+)-binding protein parvalbumin in the cytosol of HaCaT cells but not by a panel of pharmacological agents that chelate extracellular Ca(2+) (EGTA) or inhibit either ryanodine receptors (dantrolene) or voltage-gated Ca(2+) channels (nifedipine). Hence, elevated levels of intracellular Ca(2+), released from intracellular stores, are essential for the effect of thapsigargin on the biosynthesis of ATF3. The thapsigargin-induced signaling pathway was blocked by expression of either mitogen-activated protein kinase phosphatase-1 or -5. Experiments involving pharmacological and genetic tools revealed the importance of c-Jun N-terminal protein kinase (JNK) within the signaling cascade, whereas inhibition of extracellular signal-regulated protein kinase or p38 protein kinase did not attenuate thapsigargin-induced expression of ATF3. Functional studies showed that treatment of HaCaT keratinocytes with thapsigargin led to a 2-fold induction of caspase-3/7 activity. The up-regulation of caspase-3/7 activity in thapsigargin-stimulated HaCaT cells was attenuated by inhibition of JNK. Together, these data show that stimulation of HaCaT cells with thapsigargin induces a specific signaling pathway in keratinocytes involving activation of JNK, biosynthesis of ATF3, and up-regulation of caspase-3/7 activity.

Published
2010

48. TRPM3 channels provide a regulated influx pathway for zinc in pancreatic beta cells

Author

Anna Drews, Sabine Loch, Stephan Philipp, Sachar Lambert, Johannes Oberwinkler, Florian Mohr, and Thomas Wagner

Subjects
Patch-Clamp Techniques, Voltage-dependent calcium channel, Physiology, Chemistry, Clinical Biochemistry, Cell Membrane, T-type calcium channel, chemistry.chemical_element, TRPM Cation Channels, Zinc, Calcium, Transfection, Exocytosis, Cell Line, Transient receptor potential channel, Biochemistry, Physiology (medical), Insulin-Secreting Cells, Biophysics, TRPM3, Humans, Patch clamp
Abstract

Zinc is stored in insulin-containing dense core vesicles of pancreatic beta-cells where it forms crystals together with insulin and calcium ions. Zinc ions are therefore released together with insulin upon exocytosis of these vesicles. Consequently, pancreatic beta-cells need to take up large amounts of zinc from the extracellular space across their plasma membrane. The pathways for zinc uptake are only partially understood. TRPM3 channels are present in pancreatic beta-cells and can be activated by the endogenous steroid pregnenolone sulfate. We demonstrate here that recombinant TRPM3 channels are highly permeable for many divalent cations, in particular also for zinc ions. Importantly, TRPM3 channels endogenously expressed in pancreatic beta-cells are also highly permeable for zinc ions. Using FluoZin3 to image changes of the intracellular zinc concentration, we show that pancreatic beta-cells take up zinc through TRPM3 channels even when extracellular zinc concentrations are low and physiological levels of calcium and magnesium are present. Activation of TRPM3 channels also leads to depolarization of beta-cells and to additional zinc influx through voltage-gated calcium channels. Our data establish that TRPM3 channels constitute a regulated entry pathway for zinc ions in pancreatic beta-cells.

Published
2010

49. Purification and characterization of the tyrosinase ofStreptomyces michiganensis DSM 40015

Author

Stephan Philipp, Thomas Held, and Hans J. Kutzner

Subjects
Chromatography, Isoelectric point, biology, Sephadex, Tyrosinase, Hydrophilic interaction chromatography, biology.protein, Substrate (chemistry), General Medicine, Streptomyces michiganensis, Applied Microbiology and Biotechnology, Ammonium sulfate precipitation, Enzyme assay
Abstract

Tyrosinase of Streptomyces michiganensis DSM 40015 was purified 61-fold from the culture broth: After a fractionated ammonium sulfate precipitation the enzyme was separated by hydrophobic interaction chromatography with Phenyl-Sepharose and ionic interaction chromatography with CM-Cellulose; finally a gel filtration with Sephadex G-75 yielded 1.7% of the originally existent enzyme. SDS gel-electrophoresis of the purified enzyme showed two bands representing a size of 34500 and 32000 dalton, respectively. However, by isoelectric focussing only one band could be found exhibiting an isoelectric point of approximately 9.0. Temperature and pH-optimum of the enzyme activity were 33°C and pH 7.0, respectively. Whereas the enzyme is specific in regard to the aromatic part of its substrate variations of the aliphatic rest are tolerated.

Published
1991
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