Postinjury Sensitization

Sensitization can occur in both the peripheral and central nervous systems (CNS) following a surgical injury. The relative contribution of each component is a matter of debate. However, following tissue injury, gene expression is altered and mediators are released to activate the peripheral nociceptive afferent. The continued activation of these afferents enhances the patient’s response to further stimuli. The inflammatory mediators can activate and increase the sensitivity of the nociceptors, thereby changing the nociceptive threshold of the afferent. Persistent activation can also lead to alterations in the neurophysiological properties of the primary afferent itself. Peripheral sensitization refers to the summation of these processes.

There are a number of events that occur on the cellular level that are responsible for peripheral sensitization. Transient receptor potential vanilloid (TRPV) receptors on small C fibers are nonselective cation channels. TRPV receptors are known to play an important role in peripheral sensitization and, thus, are prime targets for novel analgesics. They are activated by repeated heat stimulation, acidic environments, and a wide variety of mediators found in postoperative healing tissues (prostaglandin E2, serotonin, bradykinin, epinephrine, adenosine triphosphate, interleukin-1a, interleukin-6, tumor necrosis factor, chemokines, and nerve growth factor). Activation of TRPV channels results in a painful burning sensation. The release of these mediators also increases the magnitude of Na ⁺ current in sensory neuron voltage-gated sodium channels. The activation of TRPV and these Na ⁺ channels begin a vicious circle that culminates in increased pain. Both sensory neuron-specific sodium channels and TRPV receptors can be phosphorylated by intracellular kinases (protein kinase C or tyrosine kinase), thereby potentiating the release of excitatory amino acids and peptides from sensory afferents and accentuating the pain. The inflammatory activation of TRPV receptors and sensory neuron-specific sodium channels results in vasodilatation and edema. The neurogenic inflammation is mediated by a calcitonin gene-related peptide, substance P, and neurokinin A, and can further sensitize the nociceptive afferents, leading to allodynia or hyperalgesia.

Hypersensitivity and alterations also take place in the CNS, the spinal cord, and supraspinal structures as a result of a surgical injury. Following a tissue injury, such as an incision through the skin, fascia, and muscle, a subset of A-delta and C fibers become spontaneously active and barrage the second-order neurons in the spinal cord. In turn, these neurons release excitatory neurotransmitters, which increase the amplitude of the spinal cord neuron response and lower the response threshold for further stimuli. Therefore the response of the dorsal horn neurons to a particular stimulus—be it noxious (hyperalgesia) and/or innocuous (allodynia)—is altered, and perception of the painful stimulus is increased in intensity as well as duration. The injury also results in alterations of dorsal horn neurons. These neurons react to nonnoxious stimuli as if they were noxious (allodynia) and to noxious stimuli (hyperalgesia) with an exaggerated response, but they also begin to respond to stimuli outside their original receptive field (secondary sites). There is evidence that C fiber input from an injury also causes formation of anatomic connections at the spinal cord level between neurons that respond to A-beta fiber transmission and neurons that respond to A-delta and C fiber transmission. Animal studies have shown that A-beta fibers from injured tissue begin to produce and release substance P, normally found in C fibers, and contribute to pain sensitivity. Central sensitization has two temporally distinct phases. An early phase of hypersensitivity is triggered by changes in glutamate receptor phosphorylation and ion channel properties. The second phase (longer lasting) involves transcriptional changes that result in the formation of new proteins responsible for prolonged pain hypersensitivity.

The development of central and/or peripheral sensitization after traumatic injury or surgical incision can result in amplification of pain, or pain greater than the magnitude anticipated postoperatively. Therefore preventing the establishment of altered central processing by analgesic treatment may, in the short term, reduce postprocedural or traumatic pain and accelerate recovery. In the long term, the benefits may include a reduction in chronic pain and improvement in the patient’s quality of recovery and overall function. Theoretically, providing analgesia to block the initial barrage of afferent produced by the surgical incision can result in a reduction of pain from minor or short-duration surgical procedures. However, surgical procedures that produce substantial tissue injury, resulting in the release of inflammatory mediators and peripheral or central sensitization, will require analgesic techniques that are in effect throughout the period of injury and recovery. Crile first discussed this concept at the turn of the century. Woolf established the neurophysiological basis of central sensitization after injury in a series of animal experiments, and Wall, in an editorial, suggested preinjury analgesia for the reduction of postinjury pain.