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High Pressure Bioscience : Basic Concepts, Applications and Frontiers

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Cover of 'High Pressure Bioscience : Basic Concepts, Applications and Frontiers'

Table of Contents

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    Book Overview
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    Chapter 1 Early Days of Pressure Denaturation Studies of Proteins
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    Chapter 2 Protein Denaturation on p - T Axes – Thermodynamics and Analysis
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    Chapter 3 Driving Forces in Pressure-Induced Protein Transitions
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    Chapter 4 Why and How Does Pressure Unfold Proteins?
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    Chapter 5 Volume and Compressibility of Proteins
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    Chapter 6 High Pressure Bioscience
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    Chapter 7 Water Turns the “Non-biological” Fluctuation of Protein into “Biological” One
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    Chapter 8 Pressure Effects on the Intermolecular Interaction Potential of Condensed Protein Solutions
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    Chapter 9 High Pressure NMR Methods for Characterizing Functional Substates of Proteins
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    Chapter 10 High-Pressure NMR Spectroscopy Reveals Functional Sub-states of Ubiquitin and Ubiquitin-Like Proteins
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    Chapter 11 Functional Sub-states by High-pressure Macromolecular Crystallography
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    Chapter 12 Cavities and Excited States in Proteins
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    Chapter 13 Exploring the Protein Folding Pathway with High-Pressure NMR: Steady-State and Kinetics Studies
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    Chapter 14 Basic Equations in Statics and Kinetics of Protein Polymerization and the Mechanism of the Formation and Dissociation of Amyloid Fibrils Revealed by Pressure Perturbation
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    Chapter 15 Pressure-Inactivated Virus: A Promising Alternative for Vaccine Production
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    Chapter 16 How Do Membranes Respond to Pressure?
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    Chapter 17 Pressure Effects on Artificial and Cellular Membranes
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    Chapter 18 Effects of High Hydrostatic Pressure on Microbial Cell Membranes: Structural and Functional Perspectives.
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    Chapter 19 Homeoviscous Adaptation of Membranes in Archaea.
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    Chapter 20 Pressure-Dependent Gene Activation in Yeast Cells.
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    Chapter 21 Environmental Adaptation of Dihydrofolate Reductase from Deep-Sea Bacteria.
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    Chapter 22 Moss Spores Can Tolerate Ultra-high Pressure.
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    Chapter 23 Pressure-Based Strategy for the Inactivation of Spores
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    Chapter 24 Use of Pressure Activation in Food Quality Improvement
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    Chapter 25 Use of Pressure for Improving Storage Quality of Fresh-Cut Produce.
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    Chapter 26 Application of High-Pressure Treatment to Enhancement of Functional Components in Agricultural Products and Development of Sterilized Foods
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    Chapter 27 High-Pressure Microscopy for Studying Molecular Motors.
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    Chapter 28 Ion Channels Activated by Mechanical Forces in Bacterial and Eukaryotic Cells
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    Chapter 29 Gravitational Effects on Human Physiology.
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    Chapter 30 High Pressure Small-Angle X-Ray Scattering
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    Chapter 31 High Pressure Macromolecular Crystallography
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    Chapter 32 High-Pressure Fluorescence Spectroscopy.
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    Chapter 33 High Pressure NMR Spectroscopy
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    Chapter 34 Erratum
Attention for Chapter 28: Ion Channels Activated by Mechanical Forces in Bacterial and Eukaryotic Cells
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Chapter title
Ion Channels Activated by Mechanical Forces in Bacterial and Eukaryotic Cells
Chapter number 28
Book title
High Pressure Bioscience
Published in
Sub cellular biochemistry, January 2015
DOI 10.1007/978-94-017-9918-8_28
Pubmed ID
Book ISBNs
978-9-40-179917-1, 978-9-40-179918-8
Authors

Masahiro Sokabe, Yasuyuki Sawada, Takeshi Kobayashi, Sokabe, Masahiro, Sawada, Yasuyuki, Kobayashi, Takeshi

Abstract

Since the first discovery of mechanosensitive ion channel (MSC) in non-sensory cells in 1984, a variety of MSCs has been identified both in prokaryotic and eukaryotic cells. One of the central issues concerning MSCs is to understand the molecular and biophysical mechanisms of how mechanical forces activate/open MSCs. It has been well established that prokaryotic (mostly bacterial) MSCs are activated exclusively by membrane tension. Thus the problem to be solved with prokaryotic MSCs is the mechanisms how the MSC proteins receive tensile forces from the lipid bilayer and utilize them for channel opening. On the other hand, the activation of many eukaryotic MSCs crucially depends on tension in the actin cytoskeleton. By using the actin cytoskeleton as a force sensing antenna, eukaryotic MSCs have obtained sophisticated functions such as remote force sensing and force-direction sensing, which bacterial MSCs do not have. Actin cytoskeletons also give eukaryotic MSCs an interesting and important function called "active touch sensing", by which cells can sense rigidity of their substrates. The contractile actin cytoskeleton stress fiber (SF) anchors its each end to a focal adhesion (FA) and pulls the substrate to generate substrate-rigidity-dependent stresses in the FA. It has been found that those stresses are sensed by some Ca(2+)-permeable MSCs existing in the vicinity of FAs, thus the MSCs work as a substrate rigidity sensor that can transduce the rigidity into intracellular Ca(2+) levels. This short review, roughly constituting of two parts, deals with molecular and biophysical mechanisms underlying the MSC activation process mostly based on our recent studies; (1) structure-function in bacterial MSCs activation at the atomic level, and (2) roles of actin cytoskeletons in the activation of eukaryotic MSCs.

Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 8 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
United Kingdom 1 13%
Unknown 7 88%

Demographic breakdown

Readers by professional status Count As %
Professor 4 50%
Student > Ph. D. Student 2 25%
Researcher 1 13%
Unknown 1 13%
Readers by discipline Count As %
Biochemistry, Genetics and Molecular Biology 4 50%
Agricultural and Biological Sciences 1 13%
Immunology and Microbiology 1 13%
Physics and Astronomy 1 13%
Unknown 1 13%