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1. Constitutive activation of PKA catalytic subunit in adrenal Cushing's syndrome

Author

Beuschlein, F., Fassnacht, M., Assié, G., Calebiro, D., Stratakis, C.A., Osswald, A., Ronchi, C.L., Wieland, T., Sbiera, S., Faucz, F.R., Schaak, K., Schmittfull, A., Schwarzmayr, T., Barreau, O., Vezzosi, D., Rizk-Rabin, M., Zabel, U., Szarek, E., Salpea, P., Forlino, A., Vetro, A., Zuffardi, O., Kisker, C., Diener, S., Meitinger, T., Lohse, M.J., Reincke, M., Bertherat, J., Strom, T.M., and Allolio, B.

Abstract

Background Corticotropin-independent Cushing's syndrome is caused by tumors or hyperplasia of the adrenal cortex. The molecular pathogenesis of cortisol-producing adrenal adenomas is not well understood. Methods We performed exome sequencing of tumor-tissue specimens from 10 patients with cortisol-producing adrenal adenomas and evaluated recurrent mutations in candidate genes in an additional 171 patients with adrenocortical tumors. We also performed genomewide copy-number analysis in 35 patients with cortisol-secreting bilateral adrenal hyperplasias. We studied the effects of these genetic defects both clinically and in vitro. Results Exome sequencing revealed somatic mutations in PRKACA, which encodes the catalytic subunit of cyclic AMP-dependent protein kinase (protein kinase A [PKA]), in 8 of 10 adenomas (c.617A→C in 7 and c.595_596insCAC in 1). Overall, PRKACA somatic mutations were identified in 22 of 59 unilateral adenomas (37%) from patients with overt Cushing's syndrome; these mutations were not detectable in 40 patients with subclinical hypercortisolism or in 82 patients with other adrenal tumors. Among 35 patients with cortisol-producing hyperplasias, 5 (including 2 first-degree relatives) carried a germline copy-number gain (duplication) of the genomic region on chromosome 19 that includes PRKACA. In vitro studies showed impaired inhibition of both PKA catalytic subunit mutants by the PKA regulatory subunit, whereas cells from patients with germline chromosomal gains showed increased protein levels of the PKA catalytic subunit; in both instances, basal PKA activity was increased. Conclusions Genetic alterations of the catalytic subunit of PKA were found to be associated with human disease. Germline duplications of this gene resulted in bilateral adrenal hyperplasias, whereas somatic PRKACA mutations resulted in unilateral cortisol-producing adrenal adenomas. (Funded by the European Commission Seventh Framework Program and others.).

Published
2014

14. Fluorescence Resonance Energy Transfer Analysis of α2a-Adrenergic Receptor Activation Reveals Distinct Agonist-Specific Conformational Changes

Author

Zürn, A., Zabel, U., Vilardaga, J.-P., Schindelin, H., Lohse, M. J., and Hoffmann, C.

Abstract

Several lines of evidence suggest that G-protein-coupled receptors can adopt different active conformations, but their direct demonstration in intact cells is still missing. Using a fluorescence resonance energy transfer (FRET)-based approach we studied conformational changes in α2A-adrenergic receptors in intact cells. The receptors were C-terminally labeled with cyan fluorescent protein and with fluorescein arsenical hairpin binder at different sites in the third intracellular loop: N-terminally close to transmembrane domain V (I3-N), in the middle of the loop (I3-M), or C-terminally close to transmembrane domain VI (I3-C). All constructs retained normal ligand binding and signaling properties. Changes in FRET between the labels were determined in intact cells in response to different agonists. The full agonist norepinephrine evoked similar FRET changes for all three constructs. The strong partial agonists clonidine and dopamine induced partial FRET changes for all constructs. However, the weak partial agonists octopamine and norphenephrine only induced detectable changes in the construct I3-C but no change in I3-M and I3-N. Dopamine-induced FRET-signals were 1.5-fold slower than those for norepinephrine in I3-C and I3-M but >3-fold slower in I3-N. Our data indicate that the different ligands induced conformational changes in the receptor that were sensed differently in different positions of the third intracellular loop. This agrees with X-ray receptor structures indicating larger agonist-induced movements at the cytoplasmic ends of transmembrane domain VI than V and suggests that partial agonism is linked to distinct conformational changes within a G-protein-coupled receptor.

Published
2009

15. Homodimerization of soluble guanylyl cyclase subunits. Dimerization analysis using a glutathione s-transferase affinity tag.

Author

Zabel, U, Häusler, C, Weeger, M, and Schmidt, H H

Abstract

Soluble guanylyl cyclase (sGC) is an alpha/beta-heterodimeric hemoprotein that, upon interaction with the intercellular messenger molecule NO, generates cGMP. Although the related family of particulate guanylyl cyclases (pGCs) forms active homodimeric complexes, it is not known whether homodimerization of sGC subunits occurs. We report here the expression in Sf9 cells of glutathione S-transferase-tagged recombinant human sGCalpha1 and beta1 subunits, applying a novel and rapid purification method based on GSH-Sepharose affinity chromatography. Surprisingly, in intact Sf9 cells, both homodimeric GSTalpha/alpha and GSTbeta/beta complexes were formed that were catalytically inactive. Upon coexpression of the respective complementary subunits, GSTalpha/beta or GSTbeta/alpha heterodimers were preferentially formed, whereas homodimers were still detectable. When subunits were mixed after expression, e.g. GSTbeta and beta or GSTalpha and beta, no dimerization was observed. In conclusion, our data suggest the previously unrecognized possibility of a physiological equilibrium between homo- and heterodimeric sGC complexes.

Published
1999

19. The C-terminus of the prototypical M2 muscarinic receptor localizes to the mitochondria and regulates cell respiration under stress conditions.

Author

Fasciani I, Petragnano F, Wang Z, Edwards R, Telugu N, Pietrantoni I, Zabel U, Zauber H, Grieben M, Terzenidou ME, Di Gregorio J, Pellegrini C, Santini S Jr, Taddei AR, Pohl B, Aringhieri S, Carli M, Aloisi G, Marampon F, Charlesworth E, Roman A, Diecke S, Flati V, Giorgi F, Amicarelli F, Tobin AB, Scarselli M, Tokatlidis K, Rossi M, Lohse MJ, Annibale P, and Maggio R

Subjects
Animals, Humans, Mice, Cell Proliferation, HEK293 Cells, Induced Pluripotent Stem Cells metabolism, Oxidative Phosphorylation, Oxygen Consumption, Reactive Oxygen Species metabolism, Stress, Physiological, Cell Respiration, Mitochondria metabolism, Receptor, Muscarinic M2 metabolism, Receptor, Muscarinic M2 genetics
Abstract

Muscarinic acetylcholine receptors are prototypical G protein-coupled receptors (GPCRs), members of a large family of 7 transmembrane receptors mediating a wide variety of extracellular signals. We show here, in cultured cells and in a murine model, that the carboxyl terminal fragment of the muscarinic M2 receptor, comprising the transmembrane regions 6 and 7 (M2tail), is expressed by virtue of an internal ribosome entry site localized in the third intracellular loop. Single-cell imaging and import in isolated yeast mitochondria reveals that M2tail, whose expression is up-regulated in cells undergoing integrated stress response, does not follow the normal route to the plasma membrane, but is almost exclusively sorted to the mitochondria inner membrane: here, it controls oxygen consumption, cell proliferation, and the formation of reactive oxygen species (ROS) by reducing oxidative phosphorylation. Crispr/Cas9 editing of the key methionine where cap-independent translation begins in human-induced pluripotent stem cells (hiPSCs), reveals the physiological role of this process in influencing cell proliferation and oxygen consumption at the endogenous level. The expression of the C-terminal domain of a GPCR, capable of regulating mitochondrial function, constitutes a hitherto unknown mechanism notably unrelated to its canonical signaling function as a GPCR at the plasma membrane. This work thus highlights a potential novel mechanism that cells may use for controlling their metabolism under variable environmental conditions, notably as a negative regulator of cell respiration., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2024 Fasciani et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published
2024
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20. β-arrestin1 and 2 exhibit distinct phosphorylation-dependent conformations when coupling to the same GPCR in living cells.

Author

Haider RS, Matthees ESF, Drube J, Reichel M, Zabel U, Inoue A, Chevigné A, Krasel C, Deupi X, and Hoffmann C

Subjects
G-Protein-Coupled Receptor Kinases metabolism, Luciferases, Parathyroid Hormone metabolism, Phosphorylation physiology, Protein Isoforms metabolism, Receptors, G-Protein-Coupled metabolism, beta-Arrestin 1 genetics, beta-Arrestin 1 metabolism, beta-Arrestin 2 genetics, beta-Arrestin 2 metabolism, beta-Arrestins metabolism, Arrestins metabolism, Signal Transduction physiology
Abstract

β-arrestins mediate regulatory processes for over 800 different G protein-coupled receptors (GPCRs) by adopting specific conformations that result from the geometry of the GPCR-β-arrestin complex. However, whether β-arrestin1 and 2 respond differently for binding to the same GPCR is still unknown. Employing GRK knockout cells and β-arrestins lacking the finger-loop-region, we show that the two isoforms prefer to associate with the active parathyroid hormone 1 receptor (PTH1R) in different complex configurations ("hanging" and "core"). Furthermore, the utilisation of advanced NanoLuc/FlAsH-based biosensors reveals distinct conformational signatures of β-arrestin1 and 2 when bound to active PTH1R (P-R*). Moreover, we assess β-arrestin conformational changes that are induced specifically by proximal and distal C-terminal phosphorylation and in the absence of GPCR kinases (GRKs) (R*). Here, we show differences between conformational changes that are induced by P-R* or R* receptor states and further disclose the impact of site-specific GPCR phosphorylation on arrestin-coupling and function., (© 2022. The Author(s).)

Published
2022
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21. Functional modulation of PTH1R activation and signaling by RAMP2.

Author

Nemec K, Schihada H, Kleinau G, Zabel U, Grushevskyi EO, Scheerer P, Lohse MJ, and Maiellaro I

Subjects
Biosensing Techniques, Ligands, Parathyroid Hormone metabolism, Receptors, G-Protein-Coupled metabolism, beta-Arrestin 2 metabolism, Receptor Activity-Modifying Protein 2 genetics, Receptor Activity-Modifying Protein 2 metabolism, Receptor, Parathyroid Hormone, Type 1 genetics, Receptor, Parathyroid Hormone, Type 1 metabolism, Signal Transduction
Abstract

Receptor-activity-modifying proteins (RAMPs) are ubiquitously expressed membrane proteins that associate with different G protein-coupled receptors (GPCRs), including the parathyroid hormone 1 receptor (PTH1R), a class B GPCR and an important modulator of mineral ion homeostasis and bone metabolism. However, it is unknown whether and how RAMP proteins may affect PTH1R function. Using different optical biosensors to measure the activation of PTH1R and its downstream signaling, we describe here that RAMP2 acts as a specific allosteric modulator of PTH1R, shifting PTH1R to a unique preactivated state that permits faster activation in a ligand-specific manner. Moreover, RAMP2 modulates PTH1R downstream signaling in an agonist-dependent manner, most notably increasing the PTH-mediated Gi3 signaling sensitivity. Additionally, RAMP2 increases both PTH- and PTHrP-triggered β-arrestin2 recruitment to PTH1R. Employing homology modeling, we describe the putative structural molecular basis underlying our functional findings. These data uncover a critical role of RAMPs in the activation and signaling of a GPCR that may provide a new venue for highly specific modulation of GPCR function and advanced drug design.

Published
2022
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23. Determination of G-protein-coupled receptor oligomerization by molecular brightness analyses in single cells.

Author

Işbilir A, Serfling R, Möller J, Thomas R, De Faveri C, Zabel U, Scarselli M, Beck-Sickinger AG, Bock A, Coin I, Lohse MJ, and Annibale P

Subjects
Fluorescence, HEK293 Cells, Humans, Membrane Proteins metabolism, Microscopy, Confocal methods, Microscopy, Fluorescence methods, Protein Multimerization physiology, Signal Transduction physiology, Spectrometry, Fluorescence methods, Optical Imaging methods, Receptors, G-Protein-Coupled metabolism, Single-Cell Analysis methods
Abstract

Oligomerization of membrane proteins has received intense research interest because of their importance in cellular signaling and the large pharmacological and clinical potential this offers. Fluorescence imaging methods are emerging as a valid tool to quantify membrane protein oligomerization at high spatial and temporal resolution. Here, we provide a detailed protocol for an image-based method to determine the number and oligomerization state of fluorescently labeled prototypical G-protein-coupled receptors (GPCRs) on the basis of small out-of-equilibrium fluctuations in fluorescence (i.e., molecular brightness) in single cells. The protocol provides a step-by-step procedure that includes instructions for (i) a flexible labeling strategy for the protein of interest (using fluorescent proteins, small self-labeling tags or bio-orthogonal labeling) and the appropriate controls, (ii) performing temporal and spatial brightness image acquisition on a confocal microscope and (iii) analyzing and interpreting the data, excluding clusters and intensity hot-spots commonly observed in receptor distributions. Although specifically tailored for GPCRs, this protocol can be applied to diverse classes of membrane proteins of interest. The complete protocol can be implemented in 1 month.

Published
2021
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24. Optical Mapping of cAMP Signaling at the Nanometer Scale.

Author

Bock A, Annibale P, Konrad C, Hannawacker A, Anton SE, Maiellaro I, Zabel U, Sivaramakrishnan S, Falcke M, and Lohse MJ

Subjects
Computer Simulation, Cyclic AMP chemistry, Cyclic AMP-Dependent Protein Kinases chemistry, Cytoplasm metabolism, Fluorescence Resonance Energy Transfer, HEK293 Cells, Humans, Models, Molecular, Phosphoric Diester Hydrolases chemistry, Protein Binding, Protein Domains, Recombinant Proteins, Spatio-Temporal Analysis, Spectrometry, Fluorescence, Cyclic AMP metabolism, Cyclic AMP-Dependent Protein Kinases metabolism, Phosphoric Diester Hydrolases metabolism, Signal Transduction, Single-Cell Analysis methods
Abstract

Cells relay a plethora of extracellular signals to specific cellular responses by using only a few second messengers, such as cAMP. To explain signaling specificity, cAMP-degrading phosphodiesterases (PDEs) have been suggested to confine cAMP to distinct cellular compartments. However, measured rates of fast cAMP diffusion and slow PDE activity render cAMP compartmentalization essentially impossible. Using fluorescence spectroscopy, we show that, contrary to earlier data, cAMP at physiological concentrations is predominantly bound to cAMP binding sites and, thus, immobile. Binding and unbinding results in largely reduced cAMP dynamics, which we term "buffered diffusion." With a large fraction of cAMP being buffered, PDEs can create nanometer-size domains of low cAMP concentrations. Using FRET-cAMP nanorulers, we directly map cAMP gradients at the nanoscale around PDE molecules and the areas of resulting downstream activation of cAMP-dependent protein kinase (PKA). Our study reveals that spatiotemporal cAMP signaling is under precise control of nanometer-size domains shaped by PDEs that gate activation of downstream effectors., Competing Interests: Declaration of Interests The authors declare no competing interests., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published
2020
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25. Development of a Conformational Histamine H 3 Receptor Biosensor for the Synchronous Screening of Agonists and Inverse Agonists.

Author

Schihada H, Ma X, Zabel U, Vischer HF, Schulte G, Leurs R, Pockes S, and Lohse MJ

Subjects
Histamine, Ligands, Protein Binding, Biosensing Techniques, Receptors, Histamine H3 metabolism
Abstract

The histamine H 3 receptor (H 3 R) represents a highly attractive drug target for the treatment of various central nervous system disorders, but the discovery of novel H 3 R targeting compounds relies on the assessment of highly amplified intracellular signaling events that do not only reflect H 3 R modulation and carry the risk of high false-positive and -negative screening rates. To address these limitations, we designed an intramolecular H 3 R biosensor based on the principle of bioluminescence resonance energy transfer (BRET) that reports the receptor's real-time conformational dynamics and provides an advanced tool to screen for both H 3 R agonists and inverse agonists in a live cell screening-compatible assay format. This conformational G-protein-coupled receptor (GPCR) sensor allowed us to characterize the pharmacological properties of known and new H 3 receptor ligands with unprecedented accuracy. Interestingly, we found that one newly developed H 3 receptor ligand possesses even stronger inverse agonistic activity than reference H 3 R inverse agonists including the current gold standard pitolisant. Taken together, we describe here the design and validation of the first screening-compatible H 3 R conformational biosensor that will aid in the discovery of novel H 3 R ligands and can be employed to gain deeper insights into the (in-)activation mechanism of this highly attractive drug target.

Published
2020
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26. Stepwise activation of a class C GPCR begins with millisecond dimer rearrangement.

Author

Grushevskyi EO, Kukaj T, Schmauder R, Bock A, Zabel U, Schwabe T, Benndorf K, and Lohse MJ

Subjects
Dimerization, HEK293 Cells, Humans, Kinetics, Receptors, G-Protein-Coupled radiation effects, Receptors, G-Protein-Coupled metabolism
Abstract

G protein-coupled receptors (GPCRs) are key biological switches that transmit both internal and external stimuli into the cell interior. Among the GPCRs, the "light receptor" rhodopsin has been shown to activate with a rearrangement of the transmembrane (TM) helix bundle within ∼1 ms, while all other receptors are thought to become activated within ∼50 ms to seconds at saturating concentrations. Here, we investigate synchronous stimulation of a dimeric GPCR, the metabotropic glutamate receptor type 1 (mGluR1), by two entirely different methods: ( i ) UV light-triggered uncaging of glutamate in intact cells or ( ii ) piezo-driven solution exchange in outside-out patches. Submillisecond FRET recordings between labels at intracellular receptor sites were used to record conformational changes in the mGluR1. At millimolar ligand concentrations, the initial rearrangement between the mGluR1 subunits occurs at a speed of τ 1 ∼ 1-2 ms and requires the occupancy of both binding sites in the mGluR1 dimer. These rapid changes were followed by significantly slower conformational changes in the TM domain ( τ 2 ∼ 20 ms). Receptor deactivation occurred with time constants of ∼40 and ∼900 ms for the inter- and intrasubunit conformational changes, respectively. Together, these data show that, at high glutamate concentrations, the initial intersubunit activation of mGluR1 proceeds with millisecond speed, that there is loose coupling between this initial step and activation of the TM domain, and that activation and deactivation follow a cyclic pathway, including-in addition to the inactive and active states-at least two metastable intermediate states., Competing Interests: The authors declare no conflict of interest., (Copyright © 2019 the Author(s). Published by PNAS.)

Published
2019
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27. A universal bioluminescence resonance energy transfer sensor design enables high-sensitivity screening of GPCR activation dynamics.

Author

Schihada H, Vandenabeele S, Zabel U, Frank M, Lohse MJ, and Maiellaro I

Abstract

G-protein-coupled receptors (GPCRs) represent one of the most important classes of drug targets. The discovery of new GCPR therapeutics would greatly benefit from the development of a generalizable high-throughput assay to directly monitor their activation or de-activation. Here we screened a variety of labels inserted into the third intracellular loop and the C-terminus of the α 2A -adrenergic receptor and used fluorescence (FRET) and bioluminescence resonance energy transfer (BRET) to monitor ligand-binding and activation dynamics. We then developed a universal intramolecular BRET receptor sensor design to quantify efficacy and potency of GPCR ligands in intact cells and real time. We demonstrate the transferability of the sensor design by cloning β 2 -adrenergic and PTH1-receptor BRET sensors and monitored their efficacy and potency. For all biosensors, the Z factors were well above 0.5 showing the suitability of such design for microtiter plate assays. This technology will aid the identification of novel types of GPCR ligands., Competing Interests: The authors declare that The University of Würzburg holds a patent on this technology: WO2004057333 A1.

Published
2018
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28. Single-Molecule Microscopy Reveals Dynamic FLNA Interactions Governing SSTR2 Clustering and Internalization.

Author

Treppiedi D, Jobin ML, Peverelli E, Giardino E, Sungkaworn T, Zabel U, Arosio M, Spada A, Mantovani G, and Calebiro D

Subjects
Actin Cytoskeleton metabolism, Adenoma drug therapy, Adenoma genetics, Adenoma metabolism, Animals, CHO Cells, Coated Pits, Cell-Membrane metabolism, Cricetulus, Filamins ultrastructure, Growth Hormone-Secreting Pituitary Adenoma drug therapy, Growth Hormone-Secreting Pituitary Adenoma genetics, Growth Hormone-Secreting Pituitary Adenoma metabolism, HEK293 Cells, Humans, Protein Binding, Protein Transport, Receptors, Somatostatin agonists, Receptors, Somatostatin ultrastructure, Single Molecule Imaging, Filamins metabolism, Gene Expression Regulation, Neoplastic, Receptors, Somatostatin metabolism, Somatostatin analogs & derivatives
Abstract

The cytoskeletal protein filamin A (FLNA) has been suggested to play an important role in the responsiveness of GH-secreting pituitary tumors to somatostatin receptor subtype 2 (SSTR2) agonists by regulating SSTR2 expression and signaling. However, the underlying mechanisms are unknown. In this study, we use fast multicolor single-molecule microscopy to image individual SSTR2 and FLNA molecules at the surface of living cells with unprecedented spatiotemporal resolution. We find that SSTR2 and FLNA undergo transient interactions, which occur preferentially along actin fibers and contribute to restraining SSTR2 diffusion. Agonist stimulation increases the localization of SSTR2 along actin fibers and, subsequently, SSTR2 clustering and recruitment to clathrin-coated pits (CCPs). Interfering with FLNA-SSTR2 binding with a dominant-negative FLNA fragment increases SSTR2 mobility, hampers the formation and alignment of SSTR2 clusters along actin fibers, and impairs both SSTR2 recruitment to CCPs and SSTR2 internalization. These findings indicate that dynamic SSTR2-FLNA interactions critically control the nanoscale localization of SSTR2 at the plasma membrane and are required for coupling SSTR2 clustering to internalization. These mechanisms explain the critical role of FLNA in the control of SSTR2 expression and signaling and suggest the possibility of targeting SSTR2-FLNA interactions for the therapy of pharmacologically resistant GH-secreting pituitary tumors.

Published
2018
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29. FRET Studies of Quinolone-Based Bitopic Ligands and Their Structural Analogues at the Muscarinic M 1 Receptor.

Author

Messerer R, Kauk M, Volpato D, Alonso Canizal MC, Klöckner J, Zabel U, Nuber S, Hoffmann C, and Holzgrabe U

Subjects
Fluorescence Resonance Energy Transfer, Ligands, Quinolones chemistry, Receptor, Muscarinic M1 chemistry
Abstract

Aiming to design partial agonists as well as allosteric modulators for the M 1 muscarinic acetylcholine (M 1 AChR) receptor, two different series of bipharmacophoric ligands and their structural analogues were designed and synthesized. The hybrids were composed of the benzyl quinolone carboxylic acid (BQCA)-derived subtype selective allosteric modulator 3 and the orthosteric building block 4-((4,5-dihydroisoxazol-3-yl)oxy)-N,N-dimethylbut-2-yn-1-amine (base of iperoxo) 1 or the endogenous ligand 2-(dimethylamino)ethyl acetate (base of acetylcholine) 2, respectively. The two pharmacophores were linked via alkylene chains of different lengths (C4, C6, C8, and C10). Furthermore, the corresponding structural analogues of 1 and 2 and of modified BQCA 3 with varying alkyl chain length between C2 and C10 were investigated. Fluorescence resonance energy transfer (FRET) measurements in a living single cell system were investigated in order to understand how these compounds interact with a G protein-coupled receptor (GPCR) on a molecular level and how the single moieties contribute to ligand receptor interaction. The characterization of the modified orthosteric ligands indicated that a linker attached to an orthoster rapidly attenuates the receptor response. Linker length elongation increases the receptor response of bitopic ligands, until reaching a maximum, followed by a gradual decrease. The optimal linker length was found to be six methylene groups at the M 1 AChR. A new conformational change is described that is not of inverse agonistic origin for long linker bitopic ligands and was further investigated by exceptional fragment-based screening approaches.

Published
2017
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30. β-Arrestin biosensors reveal a rapid, receptor-dependent activation/deactivation cycle.

Author

Nuber S, Zabel U, Lorenz K, Nuber A, Milligan G, Tobin AB, Lohse MJ, and Hoffmann C

Subjects
Animals, Arrestins chemistry, Biosensing Techniques, Cattle, Cell Line, Cell Membrane metabolism, Cell Survival, Crystallography, X-Ray, Fluorescence Resonance Energy Transfer, Humans, Kinetics, Models, Molecular, Protein Binding, Protein Conformation, Receptors, G-Protein-Coupled chemistry, Signal Transduction, Substrate Specificity, Time Factors, beta-Arrestins, Arrestins metabolism, Receptors, G-Protein-Coupled metabolism
Abstract

(β-)Arrestins are important regulators of G-protein-coupled receptors (GPCRs). They bind to active, phosphorylated GPCRs and thereby shut off 'classical' signalling to G proteins, trigger internalization of GPCRs via interaction with the clathrin machinery and mediate signalling via 'non-classical' pathways. In addition to two visual arrestins that bind to rod and cone photoreceptors (termed arrestin1 and arrestin4), there are only two (non-visual) β-arrestin proteins (β-arrestin1 and β-arrestin2, also termed arrestin2 and arrestin3), which regulate hundreds of different (non-visual) GPCRs. Binding of these proteins to GPCRs usually requires the active form of the receptors plus their phosphorylation by G-protein-coupled receptor kinases (GRKs). The binding of receptors or their carboxy terminus as well as certain truncations induce active conformations of (β-)arrestins that have recently been solved by X-ray crystallography. Here we investigate both the interaction of β-arrestin with GPCRs, and the β-arrestin conformational changes in real time and in living human cells, using a series of fluorescence resonance energy transfer (FRET)-based β-arrestin2 biosensors. We observe receptor-specific patterns of conformational changes in β-arrestin2 that occur rapidly after the receptor-β-arrestin2 interaction. After agonist removal, these changes persist for longer than the direct receptor interaction. Our data indicate a rapid, receptor-type-specific, two-step binding and activation process between GPCRs and β-arrestins. They further indicate that β-arrestins remain active after dissociation from receptors, allowing them to remain at the cell surface and presumably signal independently. Thus, GPCRs trigger a rapid, receptor-specific activation/deactivation cycle of β-arrestins, which permits their active signalling.

Published
2016
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31. PKA catalytic subunit mutations in adrenocortical Cushing's adenoma impair association with the regulatory subunit.

Author

Calebiro D, Hannawacker A, Lyga S, Bathon K, Zabel U, Ronchi C, Beuschlein F, Reincke M, Lorenz K, Allolio B, Kisker C, Fassnacht M, and Lohse MJ

Subjects
Adrenal Cortex Neoplasms genetics, Adrenal Cortex Neoplasms pathology, Adrenocortical Adenoma genetics, Adrenocortical Adenoma pathology, Catalytic Domain, Cell Line, Tumor, Cushing Syndrome genetics, Cushing Syndrome pathology, Cyclic AMP metabolism, Cyclic AMP-Dependent Protein Kinase Catalytic Subunits chemistry, Cyclic AMP-Dependent Protein Kinase RIIbeta Subunit chemistry, Cyclic AMP-Dependent Protein Kinase RIIbeta Subunit genetics, Cyclic AMP-Dependent Protein Kinase RIalpha Subunit chemistry, Cyclic AMP-Dependent Protein Kinase RIalpha Subunit genetics, Cyclic AMP-Dependent Protein Kinases chemistry, Cyclic AMP-Dependent Protein Kinases genetics, Cyclic AMP-Dependent Protein Kinases metabolism, Humans, Mutation, Protein Binding, Protein Stability, Adrenal Cortex Neoplasms enzymology, Adrenocortical Adenoma enzymology, Cushing Syndrome enzymology, Cyclic AMP-Dependent Protein Kinase Catalytic Subunits genetics, Cyclic AMP-Dependent Protein Kinase Catalytic Subunits metabolism, Cyclic AMP-Dependent Protein Kinase RIIbeta Subunit metabolism, Cyclic AMP-Dependent Protein Kinase RIalpha Subunit metabolism
Abstract

We recently identified a high prevalence of mutations affecting the catalytic (Cα) subunit of protein kinase A (PKA) in cortisol-secreting adrenocortical adenomas. The two identified mutations (Leu206Arg and Leu199_Cys200insTrp) are associated with increased PKA catalytic activity, but the underlying mechanisms are highly controversial. Here we utilize a combination of biochemical and optical assays, including fluorescence resonance energy transfer in living cells, to analyze the consequences of the two mutations with respect to the formation of the PKA holoenzyme and its regulation by cAMP. Our results indicate that neither mutant can form a stable PKA complex, due to the location of the mutations at the interface between the catalytic and the regulatory subunits. We conclude that the two mutations cause high basal catalytic activity and lack of regulation by cAMP through interference of complex formation between the regulatory and the catalytic subunits of PKA.

Published
2014
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32. Constitutive activation of PKA catalytic subunit in adrenal Cushing's syndrome.

Author

Beuschlein F, Fassnacht M, Assié G, Calebiro D, Stratakis CA, Osswald A, Ronchi CL, Wieland T, Sbiera S, Faucz FR, Schaak K, Schmittfull A, Schwarzmayr T, Barreau O, Vezzosi D, Rizk-Rabin M, Zabel U, Szarek E, Salpea P, Forlino A, Vetro A, Zuffardi O, Kisker C, Diener S, Meitinger T, Lohse MJ, Reincke M, Bertherat J, Strom TM, and Allolio B

Subjects
Adenoma complications, Adenoma enzymology, Adrenal Gland Neoplasms complications, Adrenal Gland Neoplasms enzymology, Adult, Catalytic Domain, Cushing Syndrome enzymology, Cyclic AMP-Dependent Protein Kinases chemistry, Cyclic AMP-Dependent Protein Kinases metabolism, Exome, Humans, Hydrocortisone biosynthesis, Middle Aged, Mutation, Protein Conformation, Sequence Analysis, DNA, Adenoma genetics, Adrenal Gland Neoplasms genetics, Adrenal Hyperplasia, Congenital genetics, Cushing Syndrome etiology, Cyclic AMP-Dependent Protein Kinases genetics, Germ-Line Mutation
Abstract

Background: Corticotropin-independent Cushing's syndrome is caused by tumors or hyperplasia of the adrenal cortex. The molecular pathogenesis of cortisol-producing adrenal adenomas is not well understood., Methods: We performed exome sequencing of tumor-tissue specimens from 10 patients with cortisol-producing adrenal adenomas and evaluated recurrent mutations in candidate genes in an additional 171 patients with adrenocortical tumors. We also performed genomewide copy-number analysis in 35 patients with cortisol-secreting bilateral adrenal hyperplasias. We studied the effects of these genetic defects both clinically and in vitro., Results: Exome sequencing revealed somatic mutations in PRKACA, which encodes the catalytic subunit of cyclic AMP-dependent protein kinase (protein kinase A [PKA]), in 8 of 10 adenomas (c.617A→C in 7 and c.595_596insCAC in 1). Overall, PRKACA somatic mutations were identified in 22 of 59 unilateral adenomas (37%) from patients with overt Cushing's syndrome; these mutations were not detectable in 40 patients with subclinical hypercortisolism or in 82 patients with other adrenal tumors. Among 35 patients with cortisol-producing hyperplasias, 5 (including 2 first-degree relatives) carried a germline copy-number gain (duplication) of the genomic region on chromosome 19 that includes PRKACA. In vitro studies showed impaired inhibition of both PKA catalytic subunit mutants by the PKA regulatory subunit, whereas cells from patients with germline chromosomal gains showed increased protein levels of the PKA catalytic subunit; in both instances, basal PKA activity was increased., Conclusions: Genetic alterations of the catalytic subunit of PKA were found to be associated with human disease. Germline duplications of this gene resulted in bilateral adrenal hyperplasias, whereas somatic PRKACA mutations resulted in unilateral cortisol-producing adrenal adenomas. (Funded by the European Commission Seventh Framework Program and others.).

Published
2014
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33. Single-molecule analysis of fluorescently labeled G-protein-coupled receptors reveals complexes with distinct dynamics and organization.

Author

Calebiro D, Rieken F, Wagner J, Sungkaworn T, Zabel U, Borzi A, Cocucci E, Zürn A, and Lohse MJ

Subjects
Animals, Bridged Bicyclo Compounds, Heterocyclic, CHO Cells, Carbocyanines, Cricetinae, Cricetulus, Cyclic AMP metabolism, HEK293 Cells, Humans, Lipids, Microscopy, Fluorescence, Molecular Dynamics Simulation, Plasmids genetics, Radioligand Assay, Thiazolidines, Algorithms, Models, Chemical, Multiprotein Complexes chemistry, Receptors, Adrenergic, beta-1 chemistry, Receptors, Adrenergic, beta-2 chemistry, Receptors, GABA chemistry
Abstract

G-protein-coupled receptors (GPCRs) constitute the largest family of receptors and major pharmacological targets. Whereas many GPCRs have been shown to form di-/oligomers, the size and stability of such complexes under physiological conditions are largely unknown. Here, we used direct receptor labeling with SNAP-tags and total internal reflection fluorescence microscopy to dynamically monitor single receptors on intact cells and thus compare the spatial arrangement, mobility, and supramolecular organization of three prototypical GPCRs: the β(1)-adrenergic receptor (β(1)AR), the β(2)-adrenergic receptor (β(2)AR), and the γ-aminobutyric acid (GABA(B)) receptor. These GPCRs showed very different degrees of di-/oligomerization, lowest for β(1)ARs (monomers/dimers) and highest for GABA(B) receptors (prevalently dimers/tetramers of heterodimers). The size of receptor complexes increased with receptor density as a result of transient receptor-receptor interactions. Whereas β(1)-/β(2)ARs were apparently freely diffusing on the cell surface, GABA(B) receptors were prevalently organized into ordered arrays, via interaction with the actin cytoskeleton. Agonist stimulation did not alter receptor di-/oligomerization, but increased the mobility of GABA(B) receptor complexes. These data provide a spatiotemporal characterization of β(1)-/β(2)ARs and GABA(B) receptors at single-molecule resolution. The results suggest that GPCRs are present on the cell surface in a dynamic equilibrium, with constant formation and dissociation of new receptor complexes that can be targeted, in a ligand-regulated manner, to different cell-surface microdomains.

Published
2013
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34. Sequential inter- and intrasubunit rearrangements during activation of dimeric metabotropic glutamate receptor 1.

Author

Hlavackova V, Zabel U, Frankova D, Bätz J, Hoffmann C, Prezeau L, Pin JP, Blahos J, and Lohse MJ

Subjects
Animals, Bacterial Proteins metabolism, COS Cells, Calcium metabolism, Chlorocebus aethiops, DNA Primers genetics, Dimerization, Fluorescence Resonance Energy Transfer, Green Fluorescent Proteins metabolism, HEK293 Cells, Humans, Kinetics, Luminescent Proteins metabolism, Microscopy, Confocal, Mutation, Missense genetics, Polymerase Chain Reaction, Receptors, Metabotropic Glutamate metabolism, Protein Conformation, Protein Subunits chemistry, Receptors, Metabotropic Glutamate chemistry, Synaptic Transmission physiology
Abstract

The metabotropic glutamate receptor 1 (mGluR1), a class C member of the heterotrimeric guanine nucleotide-binding protein (G protein)-coupled receptor family, is a constitutive dimer that regulates excitatory neurotransmission. We investigated the role of homodimer formation in mGluR1 activation by examining activation-dependent inter- and intrasubunit conformational changes by fluorescence resonance energy transfer (FRET). We inserted yellow and cyan fluorescent proteins in the second intracellular loop and at the carboxyl terminus of mGluR1 to act as FRET sensors and expressed these proteins in human embryonic kidney 293 cells. Agonist-dependent activation of these mGluR1 chimeras rapidly increased the intersubunit FRET, suggesting rapid movement of the subunits relative to each other. After intersubunit movement, the intrasubunit FRET decreased, reflecting conformational changes within a subunit. Cotransfection of chimeric receptor subunits that were capable or incapable of G protein coupling revealed that only a single subunit assumes an active state in an mGluR1 receptor dimer.

Published
2012
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35. [Appreciating the multiplicity of residents].

Author

Zabel U

Subjects
Aged, Cultural Diversity, Germany, Humans, Professional-Family Relations, Professional-Patient Relations, Cultural Competency, Emigrants and Immigrants, Geriatric Nursing organization & administration, Homes for the Aged, Nursing Homes, Transcultural Nursing organization & administration
Published
2012

36. FRET-based sensors for the human M1-, M3-, and M5-acetylcholine receptors.

Author

Ziegler N, Bätz J, Zabel U, Lohse MJ, and Hoffmann C

Subjects
HEK293 Cells, Humans, Kinetics, Ligands, Microscopy, Confocal, Muscarinic Agonists metabolism, Muscarinic Agonists pharmacology, Oxotremorine analogs & derivatives, Oxotremorine metabolism, Oxotremorine pharmacology, Protein Conformation, Receptor, Muscarinic M1 chemistry, Receptor, Muscarinic M3 chemistry, Receptor, Muscarinic M5 chemistry, Signal Transduction, Stereoisomerism, Fluorescence Resonance Energy Transfer methods, Fluorescent Dyes, Green Fluorescent Proteins, Receptor, Muscarinic M1 metabolism, Receptor, Muscarinic M3 metabolism, Receptor, Muscarinic M5 metabolism
Abstract

Based on the recently developed approach to generate fluorescence resonance energy transfer (FRET)-based sensors to measure GPCR activation, we generated sensor constructs for the human M(1)-, M(3)-, and M(5)-acetylcholine receptor. The receptors were labeled with cyan fluorescent protein (CFP) at their C-terminus, and with fluorescein arsenical hairpin binder (FlAsH) via tetra-cysteine tags inserted in the third intracellular loop. We then measured FRET between the donor CFP and the acceptor FlAsH in living cells and real time. Agonists like acetylcholine, carbachol, or muscarine activate each receptor construct with half-maximal activation times between 60 and 70ms. Removal of the agonist caused the reversal of the signal. Compared with all other agonists, oxotremorine M differed in two major aspects: it caused significantly slower signals at M(1)- and M(5)-acetylcholine receptors and the amplitude of these signals was larger at the M(1)-acetylcholine receptor. Concentration-response curves for the agonists reveal that all agonists tested, with the mentioned exception of oxotremorine M, caused similar maximal FRET-changes as acetylcholine for the M(1)-, M(3)- and M(5)-acetylcholine receptor constructs. Taken together our data support the notion that orthosteric agonists behave similar at different muscarinic receptor subtypes but that kinetic differences can be observed for receptor activation., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published
2011
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37. Site-specific, orthogonal labeling of proteins in intact cells with two small biarsenical fluorophores.

Author

Zürn A, Klenk C, Zabel U, Reiner S, Lohse MJ, and Hoffmann C

Subjects
Amino Acid Sequence, Arrestins analysis, Arrestins chemistry, Arrestins metabolism, Cell Line, Fluorescent Dyes metabolism, Humans, Molecular Sequence Data, Protein Binding, Proteins chemistry, Receptor, Parathyroid Hormone, Type 1 analysis, Receptor, Parathyroid Hormone, Type 1 chemistry, Receptor, Parathyroid Hormone, Type 1 metabolism, beta-Arrestins, Fluorescence Resonance Energy Transfer methods, Fluorescent Dyes chemistry, Proteins analysis, Proteins metabolism
Abstract

The fusion of fluorescent proteins to proteins of interest has greatly advanced fluorescence microscopy, but is often limited by their large size. Here, we report site-specific, orthogonal labeling of two cellular proteins in intact cells with two small fluorescent dyes: fluorescein arsenical hairpin binder, FlAsH, and its red analogue, ReAsH, which bind to tetracysteine motifs. Development of a sequential labeling method to two different motifs, CCPGCC and FLNCCPGCCMEP, allowed site-specific labeling with FlAsH and ReAsH, respectively. Using the cell surface receptor for parathyroid hormone and its cytosolic binding protein, beta-arrestin2, we show their selective visualization in intact cells and analyze their interaction by colocalization and fluorescence resonance energy transfer (FRET). We propose that this method may be widely applied to label intracellular proteins and to study their interactions in intact cells with minimal disturbance of their function.

Published
2010
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38. Fluorescence resonance energy transfer analysis of alpha 2a-adrenergic receptor activation reveals distinct agonist-specific conformational changes.

Author

Zürn A, Zabel U, Vilardaga JP, Schindelin H, Lohse MJ, and Hoffmann C

Subjects
Adrenergic Agonists metabolism, Animals, Cell Line, Clonidine metabolism, Dopamine metabolism, Fluorescence Resonance Energy Transfer methods, Humans, Ligands, Mice, Norepinephrine metabolism, Octopamine metabolism, Protein Binding drug effects, Protein Binding physiology, Protein Conformation drug effects, Receptors, Adrenergic, alpha-2 metabolism, Adrenergic Agonists pharmacology, Adrenergic alpha-2 Receptor Agonists, Receptors, Adrenergic, alpha-2 chemistry
Abstract

Several lines of evidence suggest that G-protein-coupled receptors can adopt different active conformations, but their direct demonstration in intact cells is still missing. Using a fluorescence resonance energy transfer (FRET)-based approach we studied conformational changes in alpha(2A)-adrenergic receptors in intact cells. The receptors were C-terminally labeled with cyan fluorescent protein and with fluorescein arsenical hairpin binder at different sites in the third intracellular loop: N-terminally close to transmembrane domain V (I3-N), in the middle of the loop (I3-M), or C-terminally close to transmembrane domain VI (I3-C). All constructs retained normal ligand binding and signaling properties. Changes in FRET between the labels were determined in intact cells in response to different agonists. The full agonist norepinephrine evoked similar FRET changes for all three constructs. The strong partial agonists clonidine and dopamine induced partial FRET changes for all constructs. However, the weak partial agonists octopamine and norphenephrine only induced detectable changes in the construct I3-C but no change in I3-M and I3-N. Dopamine-induced FRET-signals were approximately 1.5-fold slower than those for norepinephrine in I3-C and I3-M but >3-fold slower in I3-N. Our data indicate that the different ligands induced conformational changes in the receptor that were sensed differently in different positions of the third intracellular loop. This agrees with X-ray receptor structures indicating larger agonist-induced movements at the cytoplasmic ends of transmembrane domain VI than V and suggests that partial agonism is linked to distinct conformational changes within a G-protein-coupled receptor.

Published
2009
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39. Dual role of the beta2-adrenergic receptor C terminus for the binding of beta-arrestin and receptor internalization.

Author

Krasel C, Zabel U, Lorenz K, Reiner S, Al-Sabah S, and Lohse MJ

Subjects
Amino Acid Sequence, Cell Line, Humans, Kinetics, Ligands, Molecular Sequence Data, Mutation genetics, Phosphorylation, Protein Binding, Protein Transport, Receptors, Adrenergic, beta-2 chemistry, Receptors, Adrenergic, beta-2 genetics, Sequence Alignment, beta-Arrestins, Arrestins metabolism, Receptors, Adrenergic, beta-2 metabolism
Abstract

Homologous desensitization of beta2-adrenergic and other G-protein-coupled receptors is a two-step process. After phosphorylation of agonist-occupied receptors by G-protein-coupled receptor kinases, they bind beta-arrestins, which triggers desensitization and internalization of the receptors. Because it is not known which regions of the receptor are recognized by beta-arrestins, we have investigated beta-arrestin interaction and internalization of a set of mutants of the human beta2-adrenergic receptor. Mutation of the four serine/threonine residues between residues 355 and 364 led to the loss of agonist-induced receptor-beta-arrestin2 interaction as revealed by fluorescence resonance energy transfer (FRET), translocation of beta-arrestin2 to the plasma membrane, and receptor internalization. Mutation of all seven serine/threonine residues distal to residue 381 did not affect agonist-induced receptor internalization and beta-arrestin2 translocation. A beta2-adrenergic receptor truncated distal to residue 381 interacted normally with beta-arrestin2, whereas its ability to internalize in an agonist-dependent manner was compromised. A similar impairment of internalization was observed when only the last eight residues of the C terminus were deleted. Our experiments show that the C terminus distal to residue 381 does not affect the initial interaction between receptor and beta-arrestin, but its last eight amino acids facilitate receptor internalization in concert with beta-arrestin2.

Published
2008
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40. Reduced cGMP signaling associated with neointimal proliferation and vascular dysfunction in late-stage atherosclerosis.

Author

Melichar VO, Behr-Roussel D, Zabel U, Uttenthal LO, Rodrigo J, Rupin A, Verbeuren TJ, Kumar H S A, and Schmidt HH

Subjects
Animals, Aorta, Thoracic pathology, Aorta, Thoracic physiopathology, Cell Adhesion Molecules chemistry, Cell Adhesion Molecules physiology, Cyclic GMP-Dependent Protein Kinases metabolism, Guanylate Cyclase metabolism, Lipids blood, Microfilament Proteins, Nitric Oxide physiology, Nitric Oxide Synthase metabolism, Nitric Oxide Synthase Type II, Peroxynitrous Acid metabolism, Phosphoproteins chemistry, Phosphoproteins physiology, Phosphoric Diester Hydrolases metabolism, Phosphorylation, Rabbits, Signal Transduction, Superoxide Dismutase metabolism, Arteriosclerosis pathology, Arteriosclerosis physiopathology, Cyclic GMP physiology
Abstract

Atherosclerosis is associated with alterations in nitric oxide (NO)/cGMP signaling. In early stages of the disease, inflammatory and possibly other cells produce reactive oxygen species that scavenge vasoprotective NO. In addition to the oxidative stress, expression and activity of enzymes downstream to NO formation may also be affected. Here, we show in the aortas of chronically hypercholesterolemic rabbits (a model of late-stage atherosclerosis), both subunits and specific activity of the NO receptor soluble guanylyl cyclase (sGC) were significantly reduced, whereas overall NO synthase activity was unaffected. These changes were most prominent in the neointimal layer, wherein cGMP-dependent protein kinase I (cGK) levels also were reduced. Additionally, a protein (p38(nt)) that was constitutively tyrosine-nitrated was detected, and its expression was significantly reduced in atherosclerotic aorta. Phosphorylation of the cGK substrate vasodilator-stimulated phosphoprotein (VASP) at Ser-239, an established biochemical endpoint of NO/cGMP signaling, also was reduced. Thus, late-stage atherosclerosis is associated not only with enhanced NO breakdown but also with altered NO reception and cGMP signaling. Preferential down-regulation in neointima suggests a direct connection of these changes to neointimal proliferation and vascular dysfunction and provides a rationale for future pharmacotherapy using classical and novel sGC activators.

Published
2004
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41. Synaptic localization of nitric oxide synthase and soluble guanylyl cyclase in the hippocampus.

Author

Burette A, Zabel U, Weinberg RJ, Schmidt HH, and Valtschanoff JG

Subjects
Animals, Antibody Specificity, Cell Count, Dendrites metabolism, Dendrites ultrastructure, Guanylate Cyclase, Hippocampus cytology, Immunohistochemistry, Isoenzymes biosynthesis, Long-Term Potentiation physiology, Male, Mice, Mice, Knockout, Nerve Tissue Proteins metabolism, Nitric Oxide Synthase Type I, Protein Isoforms biosynthesis, Pyramidal Cells cytology, Pyramidal Cells metabolism, Rats, Rats, Sprague-Dawley, Receptors, N-Methyl-D-Aspartate biosynthesis, Soluble Guanylyl Cyclase, Synapses ultrastructure, Tissue Fixation methods, Hippocampus metabolism, Nitric Oxide Synthase biosynthesis, Receptors, Cytoplasmic and Nuclear biosynthesis, Synapses metabolism
Abstract

Functional evidence suggests that nitric oxide released from CA1 pyramidal cells can act as a retrograde messenger to mediate hippocampal long-term potentiation, but the failure to find neuronal nitric oxide synthase (NOS-I) in the dendritic spines of these cells has cast doubt on this suggestion. We hypothesized that NOS-I may be in spines but in a form inaccessible to antibody when using standard histological fixation procedures. Supporting this hypothesis, we found that after a weak fixation protocol shown previously to enhance staining of synaptic proteins, CA1 pyramidal cells exhibit clear immunoreactivity for NOS-I. Confocal microscopy revealed that numerous dendritic spines in the stratum radiatum contained the NR2 subunit of the NMDA receptor and the adaptor protein postsynaptic density-95, and a subset of these spines also contained NOS-I. Quantitative studies showed that only approximately 8% of synaptic puncta (identified by synaptophysin staining) were associated with NOS-I, and approximately 9% contained the beta subunit of soluble guanylyl cyclase (sGC), a major target of NO. However, the majority of NOS-I-positive synaptic puncta was associated with sGC and vice versa. Postembedding immunogold electron microscopy showed that NOS-I concentrates just inside the postsynaptic plasma membrane of asymmetric axospinous synapses in the stratum radiatum of CA1, whereas sGCbeta concentrates just inside the presynaptic membrane. Together, these findings support the possibility that NO may act as a retrograde messenger to help mediate homosynaptic plasticity in a subpopulation of synapses in the stratum radiatum of CA1.

Published
2002

43. Calcium-dependent membrane association sensitizes soluble guanylyl cyclase to nitric oxide.

Author

Zabel U, Kleinschnitz C, Oh P, Nedvetsky P, Smolenski A, Müller H, Kronich P, Kugler P, Walter U, Schnitzer JE, and Schmidt HH

Subjects
Animals, Binding Sites, Blood Platelets metabolism, Blotting, Western, Cell Membrane metabolism, Cytosol metabolism, Dose-Response Relationship, Drug, Endothelial Growth Factors metabolism, Endothelium pathology, Humans, Immunohistochemistry, Lung pathology, Lymphokines metabolism, Myocardium metabolism, Protein Binding, Protein Transport, Rats, Signal Transduction, Subcellular Fractions metabolism, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Calcium metabolism, Guanylate Cyclase metabolism, Nitric Oxide metabolism
Abstract

Nitric oxide (NO) is a ubiquitous, cell-permeable intercellular messenger. The current concept assumes that NO diffuses freely through the plasma membrane into the cytoplasm of a target cell, where it activates its cytosolic receptor enzyme, soluble guanylyl cyclase (sGC). Recent evidence, however, suggests that cellular membranes are not only the predominant site of calcium-dependent NO synthesis, but also the site of its distribution and binding. Here we extend this concept to NO signalling to show that active sGC is partially associated with the plasma membrane in a state of enhanced NO sensitivity. After cellular activation, sGC further translocates to the membrane fraction in human platelets and associates with the NO-synthase-containing caveolar fraction in rat lung endothelial cells, in a manner that is dependent on the concentration of intracellular calcium. Our data suggest that the entire NO signalling pathway is more spatially confined than previously assumed and that sGC dynamically translocates to the plasma membrane, where it is sensitized to NO.

Published
2002
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44. Downregulation of soluble guanylyl cyclase in young and aging spontaneously hypertensive rats.

Author

Ruetten H, Zabel U, Linz W, and Schmidt HH

Subjects
Animals, Animals, Newborn growth & development, Animals, Newborn physiology, Aorta physiology, Aorta, Thoracic enzymology, Cyclic GMP metabolism, Cyclic GMP-Dependent Protein Kinases genetics, Endothelium, Vascular physiopathology, Hypertension physiopathology, In Vitro Techniques, Isoenzymes metabolism, Male, Myocardium enzymology, RNA, Messenger metabolism, Rats, Rats, Inbred SHR physiology, Rats, Inbred WKY, Solubility, Tissue Distribution, Vasodilation, Aging metabolism, Animals, Newborn metabolism, Guanylate Cyclase metabolism, Hypertension metabolism, Rats, Inbred SHR metabolism
Abstract

Endothelial dysfunction, as observed in hypertension and atherosclerosis, is associated with a reduction in the bioavailability of endothelium-derived nitric oxide (NO). We tested the hypothesis that alterations in the soluble guanylyl cyclase (sGC) pathway may also contribute to the pathogenesis of hypertension. Therefore, we investigated the expression and activity of sGC in young (6 weeks) and aging (17 months) spontaneously hypertensive (SHR) and normotensive Wistar-Kyoto rats (WKY). Endothelium-independent relaxation of aortic rings in response to the sGC activator YC-1 was attenuated in SHR, and expression of both alpha(1) and beta(1) subunits of heterodimeric sGC and the basal contents of cGMP were reduced specifically in SHR aorta. Moreover, mRNA expression of the cGMP receptor and effector protein cGMP-dependent protein kinase type Ialpha (cGKIalpha) was also reduced. Interestingly, downregulation of both sGC and cGKIalpha expression was observed in young, ie, normotensive SHR, whereas impairment of the endothelium-independent relaxation was found only in aging SHR. Accordingly, similar cGMP levels were reached in response to YC-1 in young SHR and young WKY, suggesting a compensatory increased sensitivity or effectiveness of the sGC pathway in young SHR. In aging SHR, however, increased sensitivity to YC-1 no longer compensated for the impairment of endothelium-independent relaxation, suggesting that other mechanisms were involved. In fact, endothelium-independent relaxations were partially restored by superoxide dismutase, suggesting a pathophysiological role of superoxide production, particularly at later disease stages. Thus, tissue-specific downregulation of components of the sGC/cGMP pathway is an early event in the pathogenesis of hypertension.

Published
1999
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45. Effects of the soluble guanylyl cyclase activator, YC-1, on vascular tone, cyclic GMP levels and phosphodiesterase activity.

Author

Galle J, Zabel U, Hübner U, Hatzelmann A, Wagner B, Wanner C, and Schmidt HH

Subjects
Animals, Aorta, Thoracic drug effects, Aorta, Thoracic enzymology, Enzyme Activation, Enzyme Inhibitors pharmacology, In Vitro Techniques, Isoenzymes metabolism, Kinetics, Muscle Contraction drug effects, Muscle Relaxation drug effects, Muscle Tonus drug effects, Muscle, Smooth, Vascular drug effects, Nitric Oxide Donors pharmacology, Nitroprusside pharmacology, Nitroso Compounds pharmacology, Oxadiazoles pharmacology, Quinoxalines pharmacology, Rabbits, Vasodilator Agents pharmacology, Cyclic GMP metabolism, Guanylate Cyclase metabolism, Indazoles pharmacology, Muscle, Smooth, Vascular enzymology, Phosphoric Diester Hydrolases metabolism
Abstract

The vasomotor and cyclic GMP-elevating activity of YC-1, a novel NO-independent activator of soluble guanylyl cyclase (sGC), was studied in isolated rabbit aortic rings and compared to that of the NO donor compounds sodium nitroprusside (SNP) and NOC 18. Similarly to SNP and NOC 18, YC-1 (0.3-300 microM) caused a concentration-dependent, endothelium-independent relaxation that was greatly reduced by the sGC inhibitor 1-H-[1,2,4]oxadiazole[4,3-a]quinoxalin-1-one (ODQ 10 microM; 59% inhibition of dilation induced by 100 microM YC-1) suggesting the activation of sGC as one mechanism of action. Preincubation with YC-1 (3 and 30 microM) significantly increased the maximal dilator responses mediated by endogenous NO in aortic rings that was released upon exposure to acetylcholine, and enhanced the dilator response to the exogenous NO-donors, SNP and NOC 18, by almost two orders of magnitude. Vasoactivity induced by SNP and YC-1 displayed different kinetics as evidenced by a longlasting inhibition by YC-1 (300 microM) on the phenylephrine (PE)-induced contractile response, which was not fully reversible even after extensive washout (150 min) of YC-1, and was accompanied by a long-lasting elevation of intracellular cyclic GMP content. In contrast, SNP (30 microM) had no effect on the vasoconstrictor potency of PE, and increases in intravascular cyclic GMP levels were readily reversed after washout of this NO donor compound. Surprisingly, YC-1 not only activated sGC, but also affected cyclic GMP metabolism, as it inhibited both cyclic GMP break down in aortic extracts and the activity of phosphodiesterase isoforms 1-5 in vitro. In conclusion, YC-1 caused persistent elevation of intravascular cyclic GMP levels in vivo by activating sGC and inhibiting cyclic GMP break down. Thus, YC-1 is a highly effective vasodilator compound with a prolonged duration of action, and mechanisms that are unprecedented for any previously known sGC activator.

Published
1999
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46. Human soluble guanylate cyclase: functional expression and revised isoenzyme family.

Author

Zabel U, Weeger M, La M, and Schmidt HH

Subjects
Amino Acid Sequence, Animals, Cattle, Cyclic GMP metabolism, Guanosine Triphosphate metabolism, Guanylate Cyclase metabolism, Humans, Indazoles pharmacology, Isoenzymes metabolism, Molecular Sequence Data, Nitric Oxide metabolism, Nitroprusside pharmacology, Platelet Aggregation Inhibitors pharmacology, Protein Conformation, Rats, Recombinant Proteins biosynthesis, Solubility, Spodoptera, Vasodilator Agents pharmacology, Guanylate Cyclase biosynthesis, Isoenzymes biosynthesis
Abstract

Soluble guanylate cyclase (sGC), a heterodimeric (alpha/beta) haem protein that converts GTP to the second messenger cGMP, functions as the receptor for nitric oxide (NO) and nitrovasodilator drugs. Three distinct cDNA species of each subunit (alpha1-alpha3, beta1-beta3) have been reported from various species. From human sources, none of these have been expressed as functionally active enzyme. Here we describe the expression of human alpha/beta heterodimeric sGC in Sf9 cells yielding active recombinant enzyme that was stimulated by the nitrovasodilator sodium nitroprusside or the NO-independent activator 3-(5'-hydroxymethyl-2'-furyl)-1-benzylindazole (YC-1). At the protein level, both alpha and beta subunits were detected in human tissues, suggesting co-expression also in vivo. Moreover, resequencing of the human cDNA clones [originally termed alpha3 and beta3; Giuili, Scholl, Bulle and Guellaen (1992) FEBS Lett. 304, 83-88] revealed several sequencing errors in human alpha3; correction of these eliminated major regions of divergence from rat and bovine alpha1. As human beta3 also displays more than 98% similarity to rat and bovine beta1 at the amino acid level, alpha3 and beta3 represent the human homologues of rat and bovine alpha1 and beta1, and the isoenzyme family is decreased to two isoforms for each subunit (alpha1, alpha2; beta1, beta2). Having access to the human key enzyme of NO signalling will now permit the study of novel sGC-modulating compounds with therapeutic potential.

Published
1998
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47. Intramolecular masking of the nuclear location signal and dimerization domain in the precursor for the p50 NF-kappa B subunit.

Author

Henkel T, Zabel U, van Zee K, Müller JM, Fanning E, and Baeuerle PA

Subjects
Amino Acid Sequence, Animals, Base Sequence, Cell Line, Chlorocebus aethiops, DNA-Binding Proteins chemistry, Models, Molecular, Molecular Sequence Data, Molecular Structure, NF-kappa B metabolism, NF-kappa B p50 Subunit, Nuclear Proteins chemistry, Protein Conformation, Protein Precursors metabolism, NF-kappa B chemistry, Protein Precursors chemistry
Abstract

We show that the non-DNA-binding precursor for the p50 subunit (p110), like NF-kappa B, is subject to control of nuclear uptake. In contrast to p50, p110 was excluded from nuclei and unable to associate detectably with p50 or p65 NF-kappa B subunits. The nuclear location signal in the N-terminal half of p110 was not accessible for monospecific antibodies. Removal of only 191 amino acids from the C-terminus of p110 restored antibody accessibility as well as nuclear uptake. The C-terminal half of p110, which is linked to the p50 portion via a glycine-rich hinge, could also noncovalently bind to p50. This helps to explain why p50, after cleavage of the precursor in intact cells, was still retained in an inactive form in the cytoplasm. Our study describes a novel mechanism of nuclear uptake control by masking of a nuclear location signal through a remote domain within a precursor molecule.

Published
1992
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48. [Premature return of the drivers' license--temporal limits according to section 69 a Abs. 7 StGB].

Author

Zabel GE and Zabel U

Subjects
Germany, Humans, Time Factors, Alcohol Drinking legislation & jurisprudence, Alcoholic Intoxication prevention & control, Alcoholism rehabilitation, Automobile Driving legislation & jurisprudence
Abstract

1) Text of law and kind of crime (driving under the influence of alcohol) don't allow a reduction of the minimal period of revocation. 2) A new definition of section 69 a Abs. 7 StGB and a reduction respectively a renunciation of minimal period of revocation should give possibility to courts and reprieval authorities to ensure the inclusion of a large number of persons suitable for additional training and in cases of total abstinence traffic authority should regard the aptitude for participation in traffic as regranted.

Published
1992

49. [Reducing the duration of revoked driving permit penalty in alcoholic drivers following psychological remedial traffic education].

Author

Zabel GE and Zabel U

Subjects
Accidents, Traffic prevention & control, Alcohol Drinking prevention & control, Germany, Humans, Accidents, Traffic legislation & jurisprudence, Alcohol Drinking legislation & jurisprudence, Alcoholism rehabilitation, Automobile Driving education, Automobile Driving legislation & jurisprudence, Licensure legislation & jurisprudence
Abstract

1) Also new facts--driver improvement, longstanding good reputation in road traffic (minimum 25 years)--are only conditionally acceptable to substantiate a reduction in the blocking period in terms of section 69 a section 7 StGB. 2) A high blood alcohol level (as from 0.2 g %) precludes the reduction in the blocking period for obtaining a driving licence of drunken drivers. 3) Attending a post-schooling course may, in individual cases, as a new fact able to justify a reduction of blocking period. 4) In many cases the court is insisting behind own behaviour prognosis on a specialist for psychological selection tests.

Published
1991

50. [Driving fitness of apprehended alcoholics--fitness test and remedial psychological traffic education].

Author

Zabel G and Zabel U

Subjects
Accidents, Traffic prevention & control, Aged, Alcohol Drinking adverse effects, Alcohol Drinking legislation & jurisprudence, Alcoholism psychology, Automobile Driving legislation & jurisprudence, Follow-Up Studies, Germany, Humans, Male, Middle Aged, Accidents, Traffic legislation & jurisprudence, Alcoholism rehabilitation, Automobile Driver Examination legislation & jurisprudence, Automobile Driving education
Abstract

1) No Therapy Without Screening: According to the prevailing opinion of jurists and psychologists) who are occupied with problems concerning post-schooling and of the traffic authorities in charge of issuing driving licences screening is absolutely necessary with regard to traffic-psychological post-schoolings as characteristical maladjustments of either reparable or irreparable nature can only be detected at such screening). Only medical and psychological screening can help to achieve the necessary clarification.) Screening is frequently connected with counselling for therapy, as it is for example stressed in the names of the institutions concerned in the länder of Rhineland-Palatine, North Rhine-Westphalia and Lower Saxony). 2) Exclusion of Drink-Drivers: Screening is particularly essential to exclude the so called drink-drivers who are alcoholics from post-schooling. The necessity of such an exclusion is stressed by Müller's) latest investigation of traffic--accident data in correlation to the blood-alcohol concentration, and it must be assumed that the percentage of undetected drink-drivers with a medium blood-alcohol concentration is extremely high. One has to agree with Himmelreich) that models for post-schooling must not exclude alcoholics and criminal offenders. In this case one has to differentiate between the problem drinker) who can be post-schooled and the drink-driver described by Winkler.) Bode) and Scherer) with rigid drinking habits, a raised disposition for risk) and a reduced responsibility according to sections 20, 21 of the German Criminal Law (StGB) to such an extend that a consciousness of guilt can be ruled out). Already after the preliminary examination of such alcoholics) it has to be assumed that an immediate traffic-psychological post-schooling will hardly be successful because of the lack or considerably reduced ability of responsibility. Post-schoolings do not have compensatory effects when regular alcohol abuse (drink-driver) is concerned. In extreme cases a detoxication and the attendance of sessions of a self-help group would have to take place first. Only afterwards a traffic-psychological post-schooling can be carried out as a long term therapy. 3) Models for the Post-schooling of Individuals Tested: The "Saarbrücken model" of a collaboration of the medical-psychological institutes of the technical supervision union (TUV) and independent psychologists allows a culmination of different post-schooling and control measures with drink-drivers after negative examinations: medical tests, laboratory, chemical checks of the liver data, traffic-psychological post-schoolings of individuals and the attendance of sessions of self-help groups.(ABSTRACT TRUNCATED AT 400 WORDS)

Published
1991

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