4.3 Review

Mechanisms of ATP release in pain: role of pannexin and connexin channels

Journal

PURINERGIC SIGNALLING
Volume 17, Issue 4, Pages 549-561

Publisher

SPRINGER
DOI: 10.1007/s11302-021-09822-6

Keywords

ATP release; Connexins; Pannexins; Acute pain; Chronic pain

Funding

  1. New Jersey Commission for Brain Injury Research [CBIR19IRG014]

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Pain serves as a physiological response to bodily damage and can progress into chronic conditions with emotional and psychological aspects. Understanding the mechanisms of ATP release and the role of connexin and pannexin channels in pain processing remains an unresolved question.
Pain is a physiological response to bodily damage and serves as a warning of potential threat. Pain can also transform from an acute response to noxious stimuli to a chronic condition with notable emotional and psychological components that requires treatment. Indeed, the management of chronic pain is currently an important unmet societal need. Several reports have implicated the release of the neurotransmitter adenosine triphosphate (ATP) and subsequent activation of purinergic receptors in distinct pain etiologies. Purinergic receptors are broadly expressed in peripheral neurons and the spinal cord; thus, purinergic signaling in sensory neurons or in spinal circuits may be critical for pain processing. Nevertheless, an outstanding question remains: what are the mechanisms of ATP release that initiate nociceptive signaling? Connexin and pannexin channels are established conduits of ATP release and have been suggested to play important roles in a variety of pathologies, including several models of pain. As such, these large-pore channels represent a new and exciting putative pharmacological target for pain treatment. Herein, we will review the current evidence for a role of connexin and pannexin channels in ATP release during nociceptive signaling, such as neuropathic and inflammatory pain. Collectively, these studies provide compelling evidence for an important role of connexins and pannexins in pain processing.

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