| Literature DB >> 29241414 |
Damian Bartuzi1, Agnieszka A Kaczor1,2, Dariusz Matosiuk1.
Abstract
Allostery is one of the most important features of proteins. It greatly contributes to the complexity of life, since it enables possibility of precise tuning of protein function, as well as performing more than one function per protein. Probe dependence is one of the unique features of allostery. It allows a protein to respond differently to the same allosteric modulator when different drugs or transmitters are bound. Unfortunately, allosteric mechanisms are difficult to investigate experimentally. Instead, they can be reproduced artificially in simulations. We simulated in silico a native-like cell membrane fragment with an active-state human μ opioid receptor (MOR) in order to investigate diverse effects of a receptor's positive allosteric modulator on various agonists. Particular emphasis on native-likeness of the environment was put. We managed to reproduce the experimentally observed effects, which allowed us to take deeper insight into their underlying mechanisms. We found an allosteric pathway in the receptor, leading from the ligand binding site to the intracellular, effector site. We observed that the modulator affected the pathway, inducing different resultant responses for full and partial agonists.Entities:
Keywords: GPCRs; allosterism; molecular dynamics; probe dependence; μ opioid receptor
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Year: 2017 PMID: 29241414 DOI: 10.1080/07391102.2017.1417914
Source DB: PubMed Journal: J Biomol Struct Dyn ISSN: 0739-1102