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Citation |
Hung A, Kuyucak S, Schroeder CI, Kaas Q. Neuropharmacology 2017; 127: 20-31. |
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Affiliation |
Institute for Molecular Bioscience, The University of Queensland, Brisbane 4072, Australia. Electronic address: q.kaas@imb.uq.edu.au. |
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Copyright |
(Copyright © 2017, Elsevier Publishing) |
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DOI |
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PMID |
28778835 |
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Abstract |
The active components of animal venoms are mostly peptide toxins, which typically target ion channels and receptors of both the central and peripheral nervous system, interfering with action potential conduction and/or synaptic transmission. The high degree of sequence conservation of their molecular targets makes a range of these toxins active at human receptors. The high selectivity and potency displayed by some of these toxins have prompted their use as pharmacological tools as well as drugs or drug leads. Molecular modelling has played an essential role in increasing our molecular-level understanding of the activity and specificity of animal toxins, as well as engineering them for biotechnological and pharmaceutical applications. This review focuses on the biological insights gained from computational and experimental studies of animal venom toxins interacting with membranes and ion channels. A host of recent X-ray crystallography and electron-microscopy structures of the toxin targets has contributed to a dramatic increase in the accuracy of the molecular models of toxin binding modes greatly advancing this exciting field of study. Language: en |
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Keywords |
Animal toxins; Ion channels; Molecular dynamics; Molecular modelling; Nicotinic acetylcholine receptors; Voltage-gated ion channels |