Kinetics of ATP release following compression injury of a peripheral nerve trunk

被引：17

作者：

Grafe P. ^{[1
]}

Schaffer V. ^{[1
]}

Rucker F. ^{[1
]}

机构：

[1] Department of Physiology, University of Munich, 80336 Munich

来源：

Purinergic Signalling | 2006年 / 2卷 / 3期

关键词：

Ectonucleotidase; Luciferase; Neuropathicpain; P1; receptor; P2;

D O I：

10.1007/s11302-006-9018-y

中图分类号：

学科分类号：

摘要：

Compression and/or contusion of a peripheral nerve trunk can result in painful sensations. It is possible that release of ATP into the extracellular space may contribute to this symptom. In the present study, we used real-time measurements of ATP-induced bioluminescence together with electrophysiological recordings of compound action potentials to follow changes in the extracellular ATP concentration of isolated rat spinal roots exposed to mechanical stimuli. Nerve compression for about 8 s resulted in an immediate release of ATP into the extracellular space and in a decrease in the amplitude of compound action potentials. On average, a rise in ATP to 60 nM was observed when nerve compression blocked 50% of the myelinated axons. After the compression, the extracellular concentration of ATP returned to the resting level within a few minutes. The importance of ecto-nucleotidases for the recovery period was determined by exposure of isolated spinal roots to high concentrations of ATP and by use of inhibitors of ecto-nucleotidases. It was observed that spinal roots have a high capacity for ATP hydrolysis which is only partially blocked by βγ-methylene ATP and ARL 67156. In conclusion, acute nerve compression produces an increase in the extracellular concentration of ATP and of its metabolites which may be sufficient for activation of purinergic P2 and/or P1 receptors on axons of nociceptive afferent neurons. © Springer Science + Business Media B.V. 2006.

引用

页码：527 / 536

页数：9

共 32 条

[1] Stewart J.D., Compression and entrapment neuropathies, Peripheral Neuropathy, pp. 961-979, (1993)
[2] Shi R., Blight A.R., Compression injury of mammalian spinal cord in vitro and the dynamics of action potential conduction failure, J Neurophysiol, 76, pp. 1572-1580, (1996)
[3] Maxwell W.L., Irvine A.G., Adams J.H., Gennarelli T.A., Tipperman R., Sturatis M., Focal axonal injury: The early axonal response to stretch, J Neurocytol, 20, pp. 157-164, (1991)
[4] Lazarowski E.R., Boucher R.C., Harden T.K., Mechanisms of release of nucleotides and integration of their action as P2X- and P2Y-receptor activating molecules, Mol Pharmacol, 64, pp. 785-795, (2003)
[5] Burnstock G., Wood J.N., Purinergic receptors: Their role in nociception and primary afferent neurotransmission, Curr Opin Neurobiol, 6, pp. 526-532, (1996)
[6] Chizh B.A., Illes P., P2X receptors and nociception, Pharmacol Rev, 53, pp. 553-568, (2001)
[7] Irnich D., Tracey D.J., Polten J., Burgstahler R., Grafe P., ATP stimulates peripheral axons in human, rat and mouse - Differential involvement of A 2B adenosine and P2X purinergic receptors, Neuroscience, 110, pp. 123-129, (2002)
[8] Labrakakis C., Tong C.K., Weissman T., Torsney C., MacDermott A.B., Localization and function of ATP and GABA A receptors expressed by nociceptors and other postnatal sensory neurons in rat, J Physiol (Lond), 549, pp. 131-142, (2003)
[9] Lyons S.A., Morell P., McCarthy K.D., Schwann cells exhibit P2Y purinergic receptors that regulate intracellular calcium and are up-regulated by cyclic AMP analogues, J Neurochem, 63, pp. 552-560, (1994)
[10] Mayer C., Quasthoff S., Grafe P., Differences in the sensitivity to purinergic stimulation of myelinating and non-myelinating Schwann cells in peripheral human and rat nerve, Glia, 23, pp. 374-382, (1998)

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