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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
  25. Altmetric Badge
    Chapter 24 Erratum to: Drebrin - From Structure and Function to Physiological and Pathological Roles
Attention for Chapter 2: Molecular Cloning of Drebrin: Progress and Perspectives
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Chapter title
Molecular Cloning of Drebrin: Progress and Perspectives
Chapter number 2
Book title
Drebrin
Published in
Advances in experimental medicine and biology, January 2017
DOI 10.1007/978-4-431-56550-5_2
Pubmed ID
Book ISBNs
978-4-43-156548-2, 978-4-43-156550-5
Authors

Nobuhiko Kojima, Kojima, Nobuhiko

Abstract

Chicken drebrin isoforms were first identified in the optic tectum of developing brain. Although the time course of protein expression was different in each drebrin isoform, the similarity between their protein structures was suggested by biochemical analysis of purified protein. To determine their protein structures, the cloning of drebrin cDNAs was conducted. Comparison between the cDNA sequences shows that all drebrin cDNAs are identical except that the internal insertion sequences are present or absent in their sequences. Chicken drebrin are now classified into three isoforms, namely, drebrins E1, E2, and A. Genomic cloning demonstrated that the three isoforms are generated by an alternative splicing of individual exons encoding the insertion sequences from single drebrin gene. The mechanism should be precisely regulated in cell-type-specific and developmental stage-specific fashion. Drebrin protein, which is well conserved in various vertebrate species, although mammalian drebrin has only two isoforms, namely, drebrin E and drebrin A, is different from chicken drebrin that has three isoforms. Drebrin belongs to an actin-depolymerizing factor homology (ADF-H) domain protein family. Besides the ADF-H domain, drebrin has other domains, including the actin-binding domain and Homer-binding motifs. Diversity of protein isoform and multiple domains of drebrin could interact differentially with the actin cytoskeleton and other intracellular proteins and regulate diverse cellular processes.

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Geographical breakdown

Country Count As %
Unknown 3 100%

Demographic breakdown

Readers by professional status Count As %
Researcher 1 33%
Unknown 2 67%
Readers by discipline Count As %
Neuroscience 1 33%
Unknown 2 67%
Attention Score in Context

Attention Score in Context

This research output has an Altmetric Attention Score of 1. This is our high-level measure of the quality and quantity of online attention that it has received. This Attention Score, as well as the ranking and number of research outputs shown below, was calculated when the research output was last mentioned on 03 September 2017.
All research outputs
#20,446,373
of 23,001,641 outputs
Outputs from Advances in experimental medicine and biology
#3,985
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Outputs of similar age
#356,140
of 421,214 outputs
Outputs of similar age from Advances in experimental medicine and biology
#414
of 490 outputs
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