PAP and NT5E Inhibit Nociceptive Neurotransmission by Rapidly Hydrolyzing Nucleotides to Adenosine

Author:

Street Sarah E1,Walsh Paul L2,Sowa Nathaniel A3,Taylor-Blake Bonnie1,Guillot Thomas S2,Vihko Pirkko4,Wightman R Mark23,Zylka Mark J13

Affiliation:

1. Department of Cell and Molecular Physiology, University of North Carolina, CB #7545, Chapel Hill, North Carolina, 27599, USA

2. Department of Chemistry, University of North Carolina, CB #3290, Chapel Hill, North Carolina, 27599, USA

3. UNC Neuroscience Center, University of North Carolina, CB #7250, Chapel Hill, North Carolina, 27599, USA

4. Department of Clinical Medicine, Division of Clinical Chemistry, HUSLAB, P.O. Box 62, FI-00014, University of Helsinki, Finland

Abstract

Background: Prostatic acid phosphatase (PAP) and ecto-5'-nucleotidase (NT5E, CD73) produce extracellular adenosine from the nucleotide AMP in spinal nociceptive (pain-sensing) circuits; however, it is currently unknown if these are the main ectonucleotidases that generate adenosine or how rapidly they generate adenosine. Results: We found that AMP hydrolysis, when measured histochemically, was nearly abolished in dorsal root ganglia (DRG) neurons and lamina II of spinal cord from Pap/Nt5e double knockout (dKO) mice. Likewise, the antinociceptive effects of AMP, when combined with nucleoside transport inhibitors (dipyridamole or 5-iodotubericidin), were reduced by 80-100% in dKO mice. In addition, we used fast scan cyclic voltammetry (FSCV) to measure adenosine production at subsecond resolution within lamina II. Adenosine was maximally produced within seconds from AMP in wild-type (WT) mice but production was reduced >50% in dKO mice, indicating PAP and NT5E rapidly generate adenosine in lamina II. Unexpectedly, we also detected spontaneous low frequency adenosine transients in lamina II with FSCV. Adenosine transients were of short duration (<2 s) and were reduced (>60%) in frequency in Pap−/−, Nt5e−/− and dKO mice, suggesting these ectonucleotidases rapidly hydrolyze endogenously released nucleotides to adenosine. Field potential recordings in lamina II and behavioral studies indicate that adenosine made by these enzymes acts through the adenosine A1 receptor to inhibit excitatory neurotransmission and nociception. Conclusions: Collectively, our experiments indicate that PAP and NT5E are the main ectonucleotidases that generate adenosine in nociceptive circuits and indicate these enzymes transform pulsatile or sustained nucleotide release into an inhibitory adenosinergic signal.

Publisher

SAGE Publications

Subject

Anesthesiology and Pain Medicine,Cellular and Molecular Neuroscience,Molecular Medicine

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