88 research outputs found
Monitoring Ion Channel Function In Real Time Through Quantum Decoherence
In drug discovery research there is a clear and urgent need for non-invasive
detection of cell membrane ion channel operation with wide-field capability.
Existing techniques are generally invasive, require specialized nano
structures, or are only applicable to certain ion channel species. We show that
quantum nanotechnology has enormous potential to provide a novel solution to
this problem. The nitrogen-vacancy (NV) centre in nano-diamond is currently of
great interest as a novel single atom quantum probe for nanoscale processes.
However, until now, beyond the use of diamond nanocrystals as fluorescence
markers, nothing was known about the quantum behaviour of a NV probe in the
complex room temperature extra-cellular environment. For the first time we
explore in detail the quantum dynamics of a NV probe in proximity to the ion
channel, lipid bilayer and surrounding aqueous environment. Our theoretical
results indicate that real-time detection of ion channel operation at
millisecond resolution is possible by directly monitoring the quantum
decoherence of the NV probe. With the potential to scan and scale-up to an
array-based system this conclusion may have wide ranging implications for
nanoscale biology and drug discovery.Comment: 7 pages, 6 figure
Ion Channel Density Regulates Switches between Regular and Fast Spiking in Soma but Not in Axons
The threshold firing frequency of a neuron is a characterizing feature of its dynamical behaviour, in turn determining its role in the oscillatory activity of the brain. Two main types of dynamics have been identified in brain neurons. Type 1 dynamics (regular spiking) shows a continuous relationship between frequency and stimulation current (f-Istim) and, thus, an arbitrarily low frequency at threshold current; Type 2 (fast spiking) shows a discontinuous f-Istim relationship and a minimum threshold frequency. In a previous study of a hippocampal neuron model, we demonstrated that its dynamics could be of both Type 1 and Type 2, depending on ion channel density. In the present study we analyse the effect of varying channel density on threshold firing frequency on two well-studied axon membranes, namely the frog myelinated axon and the squid giant axon. Moreover, we analyse the hippocampal neuron model in more detail. The models are all based on voltage-clamp studies, thus comprising experimentally measurable parameters. The choice of analysing effects of channel density modifications is due to their physiological and pharmacological relevance. We show, using bifurcation analysis, that both axon models display exclusively Type 2 dynamics, independently of ion channel density. Nevertheless, both models have a region in the channel-density plane characterized by an N-shaped steady-state current-voltage relationship (a prerequisite for Type 1 dynamics and associated with this type of dynamics in the hippocampal model). In summary, our results suggest that the hippocampal soma and the two axon membranes represent two distinct kinds of membranes; membranes with a channel-density dependent switching between Type 1 and 2 dynamics, and membranes with a channel-density independent dynamics. The difference between the two membrane types suggests functional differences, compatible with a more flexible role of the soma membrane than that of the axon membrane
Anaesthesia and PET of the Brain
Although drugs have been used to administer general anaesthesia for more than a century and a half, relatively little was known until recently about the molecular and cellular effects of the anaesthetic agents and the neurobiology of anaesthesia. Positron emission tomography (PET) and single-photon emission computed tomography (SPECT) studies have played a valuable role in improving this knowledge. PET studies using 11C-flumazenil binding have been used to demonstrate that the molecular action of some, but not all, of the current anaesthetic agents is mediated via the GABAA receptor. Using different tracers labelled with 18F, 11C and 15O, PET studies have shown the patterns of changes in cerebral metabolism and blood flow associated with different intravenous and volatile anaesthetic agents. Within classes of volatile agents, there are minor variations in patterns. More profound differences are found between classes of agents. Interestingly, all agents cause alterations in the blood flow and metabolism of the thalamus, providing strong support for the hypothesis that the anaesthetic agents interfere with consciousness by interfering with thalamocortical communication.</p
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Population based models of cortical drug response: insights from anaesthesia
A great explanatory gap lies between the molecular pharmacology of psychoactive agents and the neurophysiological changes they induce, as recorded by neuroimaging modalities. Causally relating the cellular actions of psychoactive compounds to their influence on population activity is experimentally challenging. Recent developments in the dynamical modelling of neural tissue have attempted to span this explanatory gap between microscopic targets and their macroscopic neurophysiological effects via a range of biologically plausible dynamical models of cortical tissue. Such theoretical models allow exploration of neural dynamics, in particular their modification by drug action. The ability to theoretically bridge scales is due to a biologically plausible averaging of cortical tissue properties. In the resulting macroscopic neural field, individual neurons need not be explicitly represented (as in neural networks). The following paper aims to provide a non-technical introduction to the mean field population modelling of drug action and its recent successes in modelling anaesthesia
[The Lasker Prize 1999. Molecular structure of ion channels as a theme of awarded research]
Ion channel density and threshold dynamics of repetitive firing in a cortical neuron model
Spontaneous signalling in small central neurons: Mechanisms and roles of spike-amplitude and spike-interval fluctuations
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