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Drebrin

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Cover of 'Drebrin'

Table of Contents

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    Book Overview
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    Chapter 1 General Introduction to Drebrin
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    Chapter 2 Molecular Cloning of Drebrin: Progress and Perspectives
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    Chapter 3 Biochemistry of Drebrin and Its Binding to Actin Filaments
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    Chapter 4 Phosphorylation of Drebrin and Its Role in Neuritogenesis
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    Chapter 5 Remodeling of Actin Filaments by Drebrin A and Its Implications
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    Chapter 6 Cell Shape Change by Drebrin
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    Chapter 7 Localization of Drebrin: Light Microscopy Study
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    Chapter 8 Making of a Synapse: Recurrent Roles of Drebrin A at Excitatory Synapses Throughout Life
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    Chapter 9 Drebrin in Neuronal Migration and Axonal Growth
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    Chapter 10 Drebrin and Spine Formation
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    Chapter 11 Role of Drebrin in Synaptic Plasticity
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    Chapter 12 Drebrin in Alzheimer’s Disease
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    Chapter 13 Drebrins and Connexins: A Biomedical Perspective
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    Chapter 14 Homer, Spikar, and Other Drebrin-Binding Proteins in the Brain
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    Chapter 15 Role of Drebrin at the Immunological Synapse
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    Chapter 16 Drebrin Regulation of Calcium Signaling in Immune Cells
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    Chapter 17 Drebrin and Spermatogenesis
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    Chapter 18 Drebrin at Junctional Plaques
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    Chapter 19 Juxtanuclear Drebrin-Enriched Zone
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    Chapter 20 Drebrin in Renal Glomeruli
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    Chapter 21 Drebrin’s Role in the Maintenance of Endothelial Integrity
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    Chapter 22 Regulation of Skeletal Myoblast Differentiation by Drebrin
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    Chapter 23 The Role of Drebrin in Cancer Cell Invasion
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    Chapter 24 Erratum to: Drebrin - From Structure and Function to Physiological and Pathological Roles
Attention for Chapter 19: Juxtanuclear Drebrin-Enriched Zone
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Chapter title
Juxtanuclear Drebrin-Enriched Zone
Chapter number 19
Book title
Drebrin
Published in
Advances in experimental medicine and biology, January 2017
DOI 10.1007/978-4-431-56550-5_19
Pubmed ID
Book ISBNs
978-4-43-156548-2, 978-4-43-156550-5
Authors

Wiebke K. Ludwig-Peitsch, Ludwig-Peitsch, Wiebke K.

Abstract

Drebrin E contributes to remodeling of the actin cytoskeleton and formation of cell processes. Therefore, its role in cell migration was studied in prototypes of motile cells with prominent lamellipodia such as murine B16F1 melanoma and Swiss 3T3 cells and in human SV80 fibroblasts. Confocal microscopy revealed absence of drebrin from the tips of lamellipodia but enrichment in the tail of the cells, in retraction zones and in a specific juxtanuclear actin filament compartment, named "drebrin-enriched zone." A similar subset of juxtanuclear actin filaments is characterized by the actin-binding protein SWAP-70, but drebrin and SWAP-70 localized to different compartments, suggesting the existence of novel distinct subdomains within the actin filament system. In cells overexpressing drebrin-EGFP, numerous long, branched cell processes were formed which slowly retracted and extended. However, in stable transfectants containing lower amounts of the fusion protein, drebrin-EGFP was recruited to the same sites as the endogenous protein during cell migration, i.e., to retracting membrane domains and into the juxtanuclear drebrin-enriched zone. In the leading edges of SV80 cells, characterized by pronounced actin microspikes, drebrin was concentrated along posterior portions of the microspikes, together with tropomyosin, with which it competes for actin binding. Drebrin knockdown by siRNA did not impact forward migration or ruffling. Taken together, these findings suggest that during cell migration drebrin is involved in retraction processes but not in lamellipodia formation. The novel, sizable juxtanuclear drebrin-enriched zone remains to be characterized in detail with respect to its molecular assembly and functions.

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