Buch, Englisch, Band 1135, 168 Seiten, HC runder Rücken kaschiert, Format (B × H): 160 mm x 241 mm, Gewicht: 442 g
Buch, Englisch, Band 1135, 168 Seiten, HC runder Rücken kaschiert, Format (B × H): 160 mm x 241 mm, Gewicht: 442 g
Reihe: Advances in Experimental Medicine and Biology
ISBN: 978-3-030-14264-3
Verlag: Springer International Publishing
Direct Mechanisms in Cholesterol Modulation of Protein Function offers comprehensive insights into the current understanding of cholesterol-driven modulation of protein function via direct sensing. Its nine chapters are organized into two distinct parts. In the first part, the chapters introduce the reader to the general characteristics of cholesterol binding sites in proteins. This part starts with a tour into common cholesterol recognition motifs, followed by an overview of the major classes of steroid-binding proteins. It then continues with two chapters that present a comprehensive analysis of molecular and structural characteristics of cholesterol binding sites in transmembrane and soluble protein domains. In the second part of the book, examples of cholesterol binding sites and consequences of specific cholesterol recognition for protein function are presented for G protein-coupled receptors, ion channels and cholesterol-transporting proteins.
The book is valuable for undergraduate and graduate students in biochemistry and nutrition, as well as basic science and medical researchers with a keen interest in the biophysical properties of cholesterol and physiological consequences of cholesterol presence in biological systems.
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Weitere Infos & Material
Introduction.- Direct binding of cholesterol to proteins.- Cholesterol-recognition motifs in membrane proteins.- Molecular determinants of cholesterol binding to proteins: overview of crystallographic studies.- Crystallographic studies of steroid-protein interactions.- Insights into cholesterol binding sites in proteins from computational studies.- Cholesterol binding to NPC1/NPC2.- I Biophysical elements of the interaction between cholesterol and the nicotinic acetylcholine receptor.- Modulation of TRPV1 channels by cholesterol.- Cholesterol binding sites in inwardly rectifying potassium channels.