Liam E. Browne scite author profile

P2X receptors are ATP-gated membrane ion channels with multifarious roles, including afferent sensation, autocrine feedback loops, and inflammation. Their molecular operation has been less well elucidated compared with other ligand-gated channels (nicotinic acetylcholine receptors, ionotropic glutamate receptors). This will change with the recent publication of the crystal structure of a closed P2X receptor. Here we re-interpret results from 15 years of experiments using site-directed mutagenesis with a model based on the new structure. Previous predictions of receptor stoichiometry, the extracellular ATP binding site, inter-subunit contacts, and many details of the permeation pathway fall into place in three dimensions. We can therefore quickly understand how the channel operates at the molecular level. This is important not only for ion- channel aficionados, but also those engaged in developing effective antagonists at P2X receptors for potential therapeutic use.

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Time-Resolved Fast Mammalian Behavior Reveals the Complexity of Protective Pain Responses

Browne

Latrémolière

Lehnert

et al. 2017

Cell Reports

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SUMMARY Potentially harmful stimuli are detected at the skin by nociceptor sensory neurons that drive rapid protective withdrawal reflexes and pain. We set out to define at a millisecond timescale the relationship between the activity of these sensory neurons and the resultant behavioral output. Brief optogenetic activation of cutaneous nociceptors was found to activate only a single action potential. This minimal input was used to determine high-speed behavioral responses in freely-behaving mice. The localised stimulus generated widespread dynamic repositioning and alerting sub-second behaviors whose nature and timing depended on the context of the animal, its position, activity and alertness. Our findings show that the primary response to injurious stimuli is not limited, fixed or localized, but is dynamic, and involves recruitment and gating of multiple circuits distributed throughout the central nervous system at a sub-second time scale to effectively both alert to the presence of danger and minimize risk of harm.

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Optical control of trimeric P2X receptors and acid-sensing ion channels

Browne¹,

Nunes

Sim

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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P2X receptors are trimeric membrane proteins that function as ion channels gated by extracellular ATP. We have engineered a P2X2 receptor that opens within milliseconds by irradiation at 440 nm, and rapidly closes at 360 nm. This requires bridging receptor subunits via covalent attachment of 4,4'-bis(maleimido)azobenzene to a cysteine residue (P329C) introduced into each second transmembrane domain. The cis-trans isomerization of the azobenzene pushes apart the outer ends of the transmembrane helices and opens the channel in a light-dependent manner. Lightactivated channels exhibited similar unitary currents, rectification, calcium permeability, and dye uptake as P2X2 receptors activated by ATP. P2X3 receptors with an equivalent mutation (P320C) were also light sensitive after chemical modification. They showed typical rapid desensitization, and they could coassemble with native P2X2 subunits in pheochromocytoma cells to form light-activated heteromeric P2X2/3 receptors. A similar approach was used to open and close human acid-sensing ion channels (ASICs), which are also trimers but are unrelated in sequence to P2X receptors. The experiments indicate that the opening of the permeation pathway requires similar and substantial movements of the transmembrane helices in both P2X receptors and ASICs, and the method will allow precise optical control of P2X receptors or ASICs in intact tissues. P 2X receptors and acid-sensing ion channels (ASICs) are trimeric membrane ion channels gated by binding extracellular ligands. P2X receptors are gated by extracellular ATP, and their physiological roles include neuroeffector transmission, primary afferent transmission (e.g., taste, hearing, chemoreception), central control of respiration, and neuroinflammation (1-3). ASICs are gated by protons and are involved in pain sensation (4, 5). The experimental study of ligand-gated channels in intact tissues is often hampered by difficulties in application of the appropriate ligand while recording ion channel activity in the millisecond time domain, and there are advantages to controlling channel activation by surrogate optical methods. The increase in our knowledge of molecular and atomic structure of ligand-gated channels over the past 10 years has allowed one such approach (photoswitchable tethered ligands) to become much more sophisticated, because cysteines can be introduced into the channel protein exactly where required to form an attachment point. The method has been applied to pentameric nicotinic receptors (6) and tetrameric glutamate receptors (7,8). Although attaching ligands through photoswitchable tethers is proving extremely valuable, an intimate structural knowledge of a closed and open state of a channel also allows for optical control of conformation at parts of the protein that are remote from the agonist binding site (9-11).High-resolution structures are available for P2X receptors (closed: ref. 12; open: ref. 13) and ASICs (closed: refs. 14 and 15; open: ref. 16). In both these trimeric channels the second of the...

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Epineural optogenetic activation of nociceptors initiates and amplifies inflammation

et al. 2020

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Activation of nociceptor sensory neurons by noxious stimuli both triggers pain and increases capillary permeability and blood flow to produce neurogenic inflammation 1 , 2 , but whether nociceptors also interact with the immune system remains poorly understood. Here we report a neurotechnology for selective epineural optogenetic neuromodulation of nociceptors and demonstrate that nociceptor activation drives both protective pain behavior and inflammation. The wireless optoelectronic system consists of sub-millimeter-scale light-emitting diodes embedded in a soft, circumneural sciatic nerve implant, powered and driven by a miniaturized head-mounted control unit. Photostimulation of axons in freely moving mice that express channelrhodopsin only in nociceptors resulted in behaviors characteristic of pain, reflecting orthodromic input to the spinal cord. It also led to immune reactions in the skin in the absence of inflammation and potentiation of established inflammation, a consequence of the antidromic activation of nociceptor peripheral terminals. These results reveal a link between nociceptors and immune cells, which may have implications for the treatment of inflammation.

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P2X Receptor Intermediate Activation States Have Altered Nucleotide Selectivity

Browne

North

2013

J. Neurosci.

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Optical cuff for optogenetic control of the peripheral nervous system

et al. 2018

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P2X receptor channels show threefold symmetry in ionic charge selectivity and unitary conductance

et al. 2010

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In the closed structure of the P2X cation channel, three α-helical transmembrane domains cross the membrane obliquely: in rat P2X2 receptors, these intersect at Thr339. Replacing Thr339 by lysine in one, two or three subunits progressively increased chloride permeability and reduced unitary conductance. This implies that the closed-open transition involves a symmetrical separation of the three subunits, and that Thr339 from each contributes symmetrically to the open channel permeation pathway.

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Liam E. Browne

P2X7 Receptor Channels Allow Direct Permeation of Nanometer-Sized Dyes

New structure enlivens interest in P2X receptors

Time-Resolved Fast Mammalian Behavior Reveals the Complexity of Protective Pain Responses

Optical control of trimeric P2X receptors and acid-sensing ion channels

Epineural optogenetic activation of nociceptors initiates and amplifies inflammation

P2X Receptor Intermediate Activation States Have Altered Nucleotide Selectivity

Optical cuff for optogenetic control of the peripheral nervous system

P2X receptor channels show threefold symmetry in ionic charge selectivity and unitary conductance

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