Klein-Seetharaman / Vaidehi | Membrane Protein Structure and Dynamics | Buch | 978-1-4939-6233-4 | www.sack.de

Buch, Englisch, Band 914, 357 Seiten, Previously published in hardcover, Format (B × H): 178 mm x 254 mm, Gewicht: 699 g

Reihe: Methods in Molecular Biology

Klein-Seetharaman / Vaidehi

Membrane Protein Structure and Dynamics

Methods and Protocols
Softcover Nachdruck of the original 1. Auflage 2012
ISBN: 978-1-4939-6233-4
Verlag: Humana Press

Methods and Protocols

Buch, Englisch, Band 914, 357 Seiten, Previously published in hardcover, Format (B × H): 178 mm x 254 mm, Gewicht: 699 g

Reihe: Methods in Molecular Biology

ISBN: 978-1-4939-6233-4
Verlag: Humana Press


Membrane proteins play key roles in numerous cellular processes, in particular mediating cell-to-cell communication and signaling events that lead to a multitude of biological effects. Membrane proteins have also been implicated in many critical diseases such as atherosclerosis, hypertension, diabetes and cancer. In Membrane Protein Structure Predictions Methods: Methods and Protocols, expert researcher in the field detail the advances in both experimental and computational approaches of the structure, dynamics and interactions of membrane proteins dividing the volume into two sections. The first section details the procedures used for measurements of structure and dynamics of membrane proteins. While the second section contains a survey of the computational methods that have played a critical role in membrane protein structure prediction as well as in providing atomic level insight into the mechanism of the dynamics of membrane receptors. Written in the highly successful Methods in Molecular Biology™ series format, the chapters include the kind of detailed description and implementation advice that is crucial for getting optimal results in the laboratory.

Thorough and intuitive, Membrane Protein Structure Predicitons: Methods and Protocols seeks to aid scientists in the further study of membrane protein structure and function.

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Weitere Infos & Material


Crystallization of Membrane Proteins in Bicelles.-Vapor Diffusion Controlled  meso Crystallization of Membrane Proteins.-Solution NMR Studies of Integral Polytopic -helical Membrane Proteins: The Structure Determination of the Seven-helix Transmembrane Receptor Sensory Rhodopsin II, pSRII.-Use of NMR Saturation Transfer Difference Spectroscopy to Study Ligand Binding to Membrane Proteins.-How to Investigate Interactions Between Membrane Proteins and Ligands by Solid-state NMR.-Identifying and Measuring Transmembrane Helix-helix Interactions by FRET.-Studying Substrate Binding to Reconstituted Secondary Transporters by Attenuated Total Reflection Infrared Difference Spectroscopy.-UV-Visible and Infrared Methods for Investigating Lipid-Rhodopsin Membrane Interactions.-Proteomic Characterization of Integral Membrane Proteins Using Thermostatted Liquid Chromatography Coupled with Tandem Mass Spectrometry.-LITiCon: A Discrete Conformational Sampling Computational Method for Mapping Various Functionally Selective Conformational States of Transmembrane Helical Proteins.-Homology Model-assisted Elucidation of Binding Sites in GPCRs.-Comparative Modeling of Lipid Receptors.-Quantification of Structural Distortions in the Transmembrane Helices of GPCRs.-Structure Prediction of G Protein-Coupled Receptors and Their Ensemble of Functionally Important Conformations.-Target Based Virtual Screening by Docking into Automatically Generated GPCR Models.-Predicting the Biological Activities through QSAR Analysis and Docking-based Scoring.-Identification of Motions in Membrane Proteins by Elastic Network Models and Their Experimental Validation.-Modeling theStructural Communication in Supramolecular Complexes Involving GPCRs.-Exploring Substrate Diffusion in Channels using Biased Molecular Dynamics Simulations.



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