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27 results on '"Scriven, David R. L."'

1. Phosphorylation of RyR2 simultaneously expands the dyad and rearranges the tetramers.

Author

Asghari, Parisa, Scriven, David R. L., Shahrasebi, Saba, Valdivia, Hector H., Alsina, Katherina M., Valdivia, Carmen R., Navarro-Garcia, J. Alberto, Wehrens, Xander H. T., and Moore, Edwin D. W.

Subjects
*RYANODINE receptors, *DYADS, *PHOSPHORYLATION, *TRANSMISSION electron microscopy
Abstract

We have previously demonstrated that type II ryanodine receptors (RyR2) tetramers can be rapidly rearranged in response to a phosphorylation cocktail. The cocktail modified downstream targets indiscriminately, making it impossible to determine whether phosphorylation of RyR2 was an essential element of the response. Here, we used the ß-agonist isoproterenol and mice homozygous for one of the following clinically relevant mutations: S2030A, S2808A, S2814A, or S2814D. We measured the length of the dyad using transmission electron microscopy (TEM) and directly visualized RyR2 distribution using dual-tilt electron tomography. We found that the S2814D mutation, by itself, significantly expanded the dyad and reorganized the tetramers, suggesting a direct link between the phosphorylation state of the tetramer and its microarchitecture. S2808A and S2814A mutant mice, as well as wild types, had significant expansions of their dyads in response to isoproterenol, while S2030A mutants did not. In agreement with functional data from these mutants, S2030 and S2808 were necessary for a complete ß-adrenergic response, unlike S2814 mutants. Additionally, all mutants had unique effects on the organization of their tetramer arrays. Lastly, the correlation of structural with functional changes suggests that tetramer-tetramer contacts play an important functional role. We thus conclude that both the size of the dyad and the arrangement of the tetramers are linked to the state of the channel tetramer and can be dynamically altered by a ß-adrenergic receptor agonist. [ABSTRACT FROM AUTHOR]

Published
2024
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4. Cardiomyocyte ryanodine receptor clusters expand and coalesce after application of isoproterenol.

Author

Scriven, David R. L., Johnsen, Anne Berit, Asghari, Parisa, Chou, Keng C., and Moore, Edwin D. W.

Subjects
*RYANODINE receptors, *ISOPROTERENOL, *SARCOPLASMIC reticulum, *SURFACE area, *PHOSPHORYLATION
Abstract

Earlier work has shown that ventricular ryanodine receptors (RyR2) within a cluster rearrange on phosphorylation as well as with a number of other stimuli. Using dSTORM, we investigated the effects of 300 nmol/liter isoproterenol on RyR2 clusters. In rat ventricular cardiomyocytes, there was a symmetrical enlargement of RyR2 cluster areas, a decrease in the edge-to-edge nearest neighbor distance, and distribution changes that suggested movement to increase the cluster areas by coalescence. The surface area covered by the phosphorylated clusters was significantly greater than in the control cells, as was the cluster density. This latter change was accompanied by a decreased cluster fragmentation, implying that new tetramers were brought into the sarcoplasmic reticulum. We propose a possible mechanism to explain these changes. We also visualized individual RyR2 tetramers and confirmed our earlier electron-tomographic finding that the tetramers are in a disorganized but non-random array occupying about half of the cluster area. Multiclusters, cluster groups defined by the maximum distance between their members, were analyzed for various distances. At 100 nm, the areas occupied by the multiclusters just exceeded those of the single clusters, and more than half of the multiclusters had only a single subcluster that could initiate a spark. Phosphorylation increased the size of the multiclusters, markedly so for distances >100 nm. There was no relationship between the number of subclusters in a group and the area covered by it. We conclude that isoproterenol induces rapid, significant, changes in the molecular architecture of excitation--contraction coupling. [ABSTRACT FROM AUTHOR]

Published
2023
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7. Cardiac ryanodine receptor distribution is dynamic and changed by auxiliary proteins and post-translational modification.

Author

Asghari, Parisa, Scriven, David R. L., Ng, Myles, Panwar, Pankaj, Chou, Keng C., van Petegem, Filip, and Moore, Edwin D. W.

Abstract

The effects of the immunophilins, FKBP12 and FKBP12.6, and phosphorylation on type II ryanodine receptor (RyR2) arrangement and function were examined using correlation microscopy (line scan confocal imaging of Ca2+ sparks and dual-tilt electron tomography) and dSTORM imaging of permeabilized Wistar rat ventricular myocytes. Saturating concentrations (10 mmol/L) of either FKBP12 or 12.6 significantly reduced the frequency, spread, amplitude and Ca2+ spark mass relative to control, while the tomograms revealed both proteins shifted the tetramers into a largely side-by-side configuration. Phosphorylation of immunophilin-saturated RyR2 resulted in structural and functional changes largely comparable to phosphorylation alone. dSTORM images of myocyte surfaces demonstrated that both FKBP12 and 12.6 significantly reduced RyR2 cluster sizes, while phosphorylation, even of immunophilin-saturated RyR2, increased them. We conclude that both RyR2 cluster size and the arrangement of tetramers within clusters is dynamic and respond to changes in the cellular environment. Further, these changes affect Ca2+ spark formation. [ABSTRACT FROM AUTHOR]

Published
2020
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10. Single molecule localization deep within thick cells; a novel super-resolution microscope.

Author

Tafteh, Reza, Scriven, David R. L., Moore, Edwin D. W., and Chou, Keng C.

Abstract

A novel 3D imaging system based on single-molecule localization microscopy is presented to allow high-accuracy drift-free (<0.7 nm lateral; 2.5 nm axial) imaging many microns deep into a cell. When imaging deep within the cell, distortions of the point-spread function result in an inaccurate and very compressed Z distribution. For the system to accurately represent the position of each blink, a series of depth-dependent calibrations are required. The system and its allied methodology are applied to image the ryanodine receptor in the cardiac myocyte. Using the depth-dependent calibration, the receptors deep within the cell are spread over a Z range that is many hundreds of nanometers greater than implied by conventional analysis. We implemented a time domain filter to detect overlapping blinks that were not filtered by a stringent goodness of fit criterion. This filter enabled us to resolve the structure of the individual (30 nm square) receptors giving a result similar to that obtained with electron tomography. [ABSTRACT FROM AUTHOR]

Published
2016
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18. PHOSPHORYLATION OF RyR2 SIMULTANEOUSLY EXPANDS THE DYAD AND REARRANGES THE TETRAMERS.

Author

Asghari P, Scriven DRL, Shahrasebi S, Valdivia HH, Wehrens XHT, and Moore EDW

Abstract

We have previously demonstrated that type II ryanodine receptors (RyR2) tetramers can be rapidly rearranged in response to a phosphorylation cocktail. The cocktail modified downstream targets indiscriminately making it impossible to determine whether phosphorylation of RyR2 was an essential element of the response. We therefore used the β-agonist isoproterenol and mice with one of the homozygous mutations, S2030A +/+ , S2808A +/+ , S2814A +/+ , or S2814D +/+ , to address this question and to elucidate the role of these clinically relevant mutations. We measured the length of the dyad using transmission electron microscopy (TEM) and directly visualized RyR2 distribution using dual-tilt electron tomography. We found that: 1) The S2814D mutation, by itself, significantly expanded the dyad and reorganized the tetramers suggesting a direct link between the phosphorylation state of the tetramer and the microarchitecture. 2) All of the wild-type, as well as the S2808A and S2814A mice, had significant expansions of their dyads in response to ISO, while S2030A did not. 3) In agreement with functional data from the same mutants, S2030 and S2808 were necessary for a complete β-adrenergic response, whereas S2814 was not. 4) All the mutated residues had unique effects on the organization of their tetramer arrays. 5) The correlation of structure with function suggests that tetramer-tetramer contacts play an important functional role. We conclude that both the size of the dyad and the arrangement of the tetramers are linked to the state of the channel tetramer and can be dynamically altered by a β-adrenergic receptor agonist., Summary: Analysis of RyR2 mutants suggests a direct link between the phosphorylation state of the channel tetramer and the microarchitecture of the dyad. All phosphorylation site mutations produced significant and unique effects on the structure of the dyad and its response to isoproterenol.

Published
2023
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19. Nonuniform and variable arrangements of ryanodine receptors within mammalian ventricular couplons.

Author

Asghari P, Scriven DR, Sanatani S, Gandhi SK, Campbell AI, and Moore ED

Subjects
Animals, Calcium Signaling drug effects, Electron Microscope Tomography, Enzyme Activation drug effects, Heart Ventricles cytology, Heart Ventricles ultrastructure, Humans, Magnesium pharmacology, Male, Myocytes, Cardiac drug effects, Myocytes, Cardiac ultrastructure, Phosphorylation, Protein Kinases physiology, Protein Processing, Post-Translational, Rats, Rats, Wistar, Ryanodine Receptor Calcium Release Channel metabolism, Sarcoplasmic Reticulum physiology, Excitation Contraction Coupling, Heart Ventricles chemistry, Myocytes, Cardiac chemistry, Ryanodine Receptor Calcium Release Channel analysis
Abstract

Rationale: Single-tilt tomograms of the dyads in rat ventricular myocytes indicated that type 2 ryanodine receptors (RYR2s) were not positioned in a well-ordered array. Furthermore, the orientation and packing strategy of purified type 1 ryanodine receptors in lipid bilayers is determined by the free Mg2+ concentration. These observations led us to test the hypothesis that RYR2s within the mammalian dyad have multiple and complex arrangements., Objectives: To determine the arrangement of RYR2 tetramers in the dyads of mammalian cardiomyocytes and the effects of physiologically and pathologically relevant factors on this arrangement., Methods and Results: We used dual-tilt electron tomography to produce en-face views of dyads, enabling a direct examination of RYR2 distribution and arrangement. Rat hearts fixed in situ; isolated rat cardiomyocytes permeabilized, incubated with 1 mmol/L Mg2+, and then fixed; and sections of human ventricle, all showed that the tetramer packing within a dyad was nonuniform containing a mix of checkerboard and side-by-side arrangements, as well as isolated tetramers. Both phosphorylation and 0.1 mmol/L Mg2+ moved the tetramers into a predominantly checkerboard configuration, whereas the 4 mmol/L Mg2+ induced a dense side-by-side arrangement. These changes occurred within 10 minutes of application of the stimuli., Conclusions: The arrangement of RYR2 tetramers within the mammalian dyad is neither uniform nor static. We hypothesize that this is characteristic of the dyad in vivo and may provide a mechanism for modulating the open probabilities of the individual tetramers., (© 2014 American Heart Association, Inc.)

Published
2014
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20. Microarchitecture of the dyad.

Author

Scriven DR, Asghari P, and Moore ED

Subjects
Animals, Calcium metabolism, Calcium Channels, L-Type physiology, Calsequestrin physiology, Excitation Contraction Coupling, Humans, Membrane Proteins physiology, Ryanodine Receptor Calcium Release Channel physiology, Sodium-Calcium Exchanger physiology, Myocytes, Cardiac ultrastructure, Sarcolemma ultrastructure, Sarcoplasmic Reticulum ultrastructure
Abstract

This review highlights recent and ongoing discoveries that are transforming the previously held view of dyad structure and function. New data show that dyads vary greatly in both structure and in their associated molecules. Dyads can contain varying numbers of type 2 ryanodine receptor (RYR2) clusters that range in size from one to hundreds of tetramers and they can adopt numerous orientations other than the expected checkerboard. The association of Ca(v)1.2 with RYR2, which defines the couplon, is not absolute, leading to a number of scenarios such as dyads without couplons and those in which only a fraction of the clusters are in couplons. Different dyads also vary in the transporters and exchangers with which they are associated producing functional differences that amplify their structural diversity. The essential role of proteins, such as junctophilin-2, calsequestrin, triadin, and junctin that maintain both the functional and structural integrity of the dyad have recently been elucidated giving a new mechanistic understanding of heart diseases, such as arrhythmias, hypertension, failure, and sudden cardiac death.

Published
2013
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21. Ca²⁺ channel and Na⁺/Ca²⁺ exchange localization in cardiac myocytes.

Author

Scriven DR and Moore ED

Subjects
Animals, Calcium Channels, L-Type genetics, Humans, Protein Binding genetics, Ryanodine Receptor Calcium Release Channel genetics, Sarcolemma metabolism, Sodium Channels genetics, Sodium-Calcium Exchanger genetics, Sodium-Calcium Exchanger metabolism, Sodium-Potassium-Exchanging ATPase genetics, Sodium-Potassium-Exchanging ATPase metabolism, Calcium Channels, L-Type metabolism, Myocytes, Cardiac metabolism, Ryanodine Receptor Calcium Release Channel metabolism, Sodium Channels metabolism
Abstract

L-type Ca(2+) channels and the Na(+)/Ca(2+) exchanger are the main pathways for Ca(2+) influx and efflux across the sarcolemma. The majority of Ca(2+) channels are found in couplons adjacent to ryanodine receptors, but there are at least two smaller, physically and functionally distinct, extradyadic populations. NCX is more widely dispersed in the membrane although a subpopulation is closely associated with the alpha-2 isoform of the Na(+)/K(+) ATPase and has a direct effect on ECC. In addition to Ca(2+) channels and ryanodine receptors, couplons in adult animals contain a variety of other occupants that modulate their function. These modulators can vary from one couplon to another creating a variety of molecular architectures. In this review we examine our current understanding of the molecular composition, binding partners and determinants of the localization of these proteins., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published
2013
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22. Analysis of Cav1.2 and ryanodine receptor clusters in rat ventricular myocytes.

Author

Scriven DR, Asghari P, Schulson MN, and Moore ED

Subjects
Animals, Cluster Analysis, Heart Ventricles, Male, Myocytes, Cardiac cytology, Rats, Rats, Wistar, Staining and Labeling, Calcium Channels, L-Type metabolism, Myocytes, Cardiac metabolism, Ryanodine Receptor Calcium Release Channel metabolism
Abstract

We analyzed the distribution of ryanodine receptor (RyR) and Cav1.2 clusters in adult rat ventricular myocytes using three-dimensional object-based colocalization metrics. We found that ∼75% of the Cav1.2 clusters and 65% of the RyR clusters were within couplons, and both were roughly two and a half times larger than their extradyadic counterparts. Within a couplon, Cav1.2 was concentrated near the center of the underlying RyR cluster and accounted for ∼67% of its size. These data, together with previous findings from binding studies, enable us to estimate that a couplon contains 74 RyR tetramers and 10 copies of the α-subunit of Cav1.2. Extradyadic clusters of RyR contained ∼30 tetramers, whereas the extradyadic Cav1.2 clusters contained, on average, only four channels. Between 80% and 85% of both RyR and Cav1.2 molecules are within couplons. RyR clusters were in the closest proximity, with a median nearest-neighbor distance of 552 nm; comparable values for Cav1.2 clusters and couplons were 619 nm and 735 nm, respectively. Extradyadic RyR clusters were significantly closer together (624 nm) and closer to the couplons (674 nm) than the couplons were to each other. In contrast, the extradyadic clusters of Cav1.2 showed no preferential localization and were broadly distributed. These results provide a wealth of morphometric data that are essential for understanding intracellular Ca2+ regulation and modeling Ca2+ dynamics., (Copyright © 2010 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published
2010
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23. Multi-image colocalization and its statistical significance.

Author

Fletcher PA, Scriven DR, Schulson MN, and Moore ED

Subjects
Animals, Calcium Channels, L-Type metabolism, Heart Atria cytology, Monte Carlo Method, Muscle Cells cytology, Muscle Cells metabolism, Rats, Rats, Wistar, Ryanodine Receptor Calcium Release Channel metabolism, Molecular Imaging methods, Molecular Imaging statistics & numerical data
Abstract

Accurately localizing molecules within the cell is one of main tasks of modern biology, and colocalization analysis is one of its principal and most often used tools. Despite this popularity, interpretation is often uncertain because colocalization between two or more images is rarely analyzed to determine whether the observed values could have occurred by chance. To address this, we have developed a robust methodology, based on Monte Carlo randomization, to measure the statistical significance of a colocalization. The method works with voxel-based, intensity-based, object-based, and nearest-neighbor metrics. We extend all of these to measure colocalization in images with three colors. We also introduce three new metrics; blob colocalization, where the blob consists of a local maximum surrounded by a three-dimensional group of voxels; cluster diameter, to measure the clustering of fluorophores in three or more images; and the intercluster distance to measure the distance between these clusters. The robustness of these metrics was tested by varying the image thresholds over a broad range, which produced no change in the statistical significance of the colocalizations. A comparison of blob colocalization with voxel and Manders colocalization metrics shows that the different measures produce consistent results with similar values for significance and nonsignificance. Using our methodology, we are able to determine not only whether the labeled molecules colocalize with a probability greater than chance, but also whether they are sequestrated into different compartments. The program, written in C++, is freely available as source, as well as in a Linux version., (Copyright © 2010 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published
2010
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24. Axial tubules of rat ventricular myocytes form multiple junctions with the sarcoplasmic reticulum.

Author

Asghari P, Schulson M, Scriven DR, Martens G, and Moore ED

Subjects
Animals, Calcium Channels, L-Type metabolism, Calcium Channels, L-Type ultrastructure, Fluorescent Antibody Technique, Heart Atria metabolism, Heart Atria ultrastructure, Heart Ventricles ultrastructure, Imaging, Three-Dimensional, Male, Microscopy, Electron, Transmission, Microscopy, Fluorescence, Rats, Rats, Wistar, Sarcomeres metabolism, Sarcomeres ultrastructure, Tomography, Monocytes metabolism, Monocytes ultrastructure, Ryanodine Receptor Calcium Release Channel metabolism, Ryanodine Receptor Calcium Release Channel ultrastructure, Sarcoplasmic Reticulum metabolism, Sarcoplasmic Reticulum ultrastructure
Abstract

Ryanodine receptors (RyRs) are located primarily on the junctional sarcoplasmic reticulum (SR), adjacent to the transverse tubules and on the cell surface near the Z-lines, but some RyRs are on junctional SR adjacent to axial tubules. Neither the size of the axial junctions nor the numbers of RyRs that they contain have been determined. RyRs may also be located on the corbular SR and on the free or network SR. Because determining and quantifying the distribution of RyRs is critical for both understanding and modeling calcium dynamics, we investigated the distribution of RyRs in healthy adult rat ventricular myocytes, using electron microscopy, electron tomography, and immunofluorescence. We found RyRs in only three regions: in couplons on the surface and on transverse tubules, both of which are near the Z-line, and in junctions on most of the axial tubules--axial junctions. The axial junctions averaged 510 nm in length, but they occasionally spanned an entire sarcomere. Numerical analysis showed that they contain as much as 19% of a cell's RyRs. Tomographic analysis confirmed the axial junction's architecture, which is indistinguishable from junctions on transverse tubules or on the surface, and revealed a complexly structured tubule whose lumen was only 26 nm at its narrowest point. RyRs on axial junctions colocalize with Ca(v)1.2, suggesting that they play a role in excitation-contraction coupling.

Published
2009
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25. Image acquisition for colocalization using optical microscopy.

Author

Scriven DR, Lynch RM, and Moore ED

Subjects
Algorithms, Image Interpretation, Computer-Assisted, Microscopy, Electron, Refractometry, Sensitivity and Specificity, Microscopy, Microscopy, Fluorescence
Abstract

Colocalization, in which images of two or more fluorescent markers are overlaid, and coincidence between the probes is measured or displayed, is a common analytical tool in cell biology. Interpreting the images and the meaning of this identified coincidence is difficult in the absence of basic information about the acquisition parameters. In this commentary, we highlight important factors in the acquisition of images used to demonstrate colocalization, and we discuss the minimum information that authors should include in a manuscript so that a reader can interpret both the fluorescent images and any observed colocalization.

Published
2008
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26. Caveolin-3 is adjacent to a group of extradyadic ryanodine receptors.

Author

Scriven DR, Klimek A, Asghari P, Bellve K, and Moore ED

Subjects
Algorithms, Animals, Arabidopsis Proteins, Calcium Channels, L-Type chemistry, Caveolin 3 chemistry, Caveolin 3 metabolism, Caveolins chemistry, Cell Membrane metabolism, Cells, Cultured, Heart Ventricles cytology, Image Processing, Computer-Assisted, Ions chemistry, Male, Microscopy, Fluorescence, Monte Carlo Method, Muscle Cells metabolism, Myocardial Contraction, Myocytes, Cardiac cytology, Protein Binding, Protein Isoforms, Rats, Rats, Wistar, Signal Transduction, Sodium-Calcium Exchanger metabolism, Caveolin 3 physiology, Ryanodine Receptor Calcium Release Channel chemistry, Sodium-Calcium Exchanger chemistry
Abstract

Caveolae are present in almost all cells and concentrate a wide variety of signaling molecules, receptors, transporters, and ion pumps. We have investigated the distribution of the ryanodine receptor, the Na(+)/Ca(2+) exchanger, the predominant Na(+) channel isoform rH1, and the L-type calcium channel, Ca(v)1.2, relative to the muscle-specific caveolin isoform, caveolin-3, in adult rat ventricular myocytes. Three-dimensional immunofluorescence images were deconvolved and analyzed. Caveolin-3 colocalizes with all of these molecules at the surface of the cell, but there is no significant colocalization between caveolin-3 and either the Na(+)/Ca(2+) exchanger or the Na(+) channel in the cell interior. The distribution of the surface colocalization indicates that the caveolae that colocalize with each molecule form distinct populations. This organization indicates that there are multiple populations of caveolae separable by location and occupants. In the interior of the cell, caveolin-3 shows a marked colocalization with a population of ryanodine receptors that are separate from those within the dyad. Because of their location, the signaling molecules contained within these caveolae may have preferred access to the neighboring nondyadic ryanodine receptors.

Published
2005
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27. Epitope-dependent localization of estrogen receptor-alpha, but not -beta, in en face arterial endothelium.

Author

Dan P, Cheung JC, Scriven DR, and Moore ED

Subjects
Animals, Antibodies, Antibody Specificity, Basilar Artery chemistry, Basilar Artery ultrastructure, Blotting, Western, Caveolin 1, Caveolins analysis, Cell Line, Cell Line, Transformed, Cell Membrane chemistry, Cell Nucleus chemistry, Cerebral Arteries chemistry, Cerebral Arteries ultrastructure, Coronary Vessels chemistry, Coronary Vessels ultrastructure, Epithelial Cells, Estradiol blood, Estradiol pharmacology, Estrogen Receptor alpha, Estrogen Receptor beta, Female, Fluorescent Antibody Technique, Lipoproteins, LDL metabolism, Ovariectomy, Ovary, Protein Conformation, Rats, Rats, Sprague-Dawley, Receptors, Estrogen chemistry, Receptors, Estrogen immunology, Endothelium, Vascular chemistry, Epitopes analysis, Receptors, Estrogen analysis
Abstract

Rapid, nongenomic effects of 17 beta-estradiol (E(2)) in endothelial cells are postulated to arise from membrane-associated estrogen receptors (ERs), which have not been visualized in vascular tissue. To identify membrane ERs, we used multiple site-directed ER alpha or ER beta antibodies to label en face rat cerebral and coronary arterial endothelia. Western blots revealed a novel 55-kDa ER alpha isoform. Three-dimensional images of cells labeled with these antibodies and markers for the nucleus and caveolin-1 were acquired with a wide-field microscope, deconvolved, and numerically analyzed. We found ER alpha in the nucleus and cell periphery, where one-third colocalized with caveolin-1. The receptor location was dependent on the epitope of the antibody. Human ovarian surface epithelium produced similar results; but in rat myometrium, the distribution was epitope independent and nuclear. ER beta distribution was predominantly intranuclear and epitope independent. A small amount of ER alpha colocalized with ER beta within the nucleus. The results were identical in both arterial preparations and insensitive to E(2). We postulate that the different ER alpha conformations at the membrane, in the nucleus, and between different cell types allow E(2) to trigger cell- and location-specific signaling cascades.

Published
2003
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