Chapter 17 Principles of Pain Management

Pain is ubiquitous in daily life, and multiple treatment modalities are available under normal circumstances. However, the wilderness setting presents significant challenges when available treatments are limited to those that are included with medical supplies for travel into remote locations. Many travelers have medical conditions that may restrict or limit the use of certain therapies. Some travelers may suffer chronic pain and are already receiving treatment with medications or implanted devices. The treatment of pain in remote and extreme environments is guided by patient characteristics, type of injury, and available therapies. Optimal treatment reduces the chances of further injury, decreases suffering, and improves the likelihood of successful rescue.

The International Association for the Study of Pain ⁴ defines pain as “an unpleasant sensory and emotional experience associated with actual or potential tissue damage or described in terms of such damage.” This definition indicates that pain is not simply sensory input from tissue damage; rather, it is a complex experience that depends in varying degrees on an emotional component. The emotional component can vary markedly among individuals and circumstances; however, these factors may significantly affect physiology and dramatically alter the impact of pain on an individual patient. For example, fear and anxiety associated with injury in remote areas can exacerbate the situation.

The optimal management of pain often requires a multimodal approach. This approach includes treatment of ongoing tissue damage, which may include interventions locally and systemically, non-narcotic medications, opioid and adjuvant medications, and awareness and management of psychological factors that affect an individual’s perception of pain.

Anatomy and Physiology of Acute Nociceptive Pain

The early understanding of the transmission of sensation was that pain perception followed nerves that were simple conduits to the brain. As a greater understanding of pain has developed, it is clear that nociceptive pain, which is defined as the pain of tissue injury or potential tissue injury, is initiated by nociceptor activation in the periphery and modulated at multiple levels in the nervous system, thereby allowing for multiple targets for therapy. This sequence of events is categorized into four processes:

1 Transduction: Chemical, thermal, or mechanical energy is converted into an electrochemical signal.

2 Transmission: The signal is conducted to the central nervous system via Aδ and C fibers.

3 Modulation: The signal is altered by both positive and negative feedback loops in the spinal cord and the brain.

4 Perception: The signal is finally appreciated as pain.

The skin, the periosteum, and the joint surfaces are abundantly populated with nociceptors that are activated by potential or actual tissue damage. Thinly myelinated Aδ and unmyelinated C fibers terminate in the skin as nociceptors and transmit nociception to the spinal cord. Fast-conducting Aδ fibers respond to mechanical stimuli and transmit sharp sensations. Slow-conducting C fibers respond to chemical, thermal, and mechanical stimuli and transmit burning sensations. Acute injury of the skin results in simultaneous transmission through Aδ and C fibers. Cell bodies of the Aδ and C fibers are located in the dorsal root ganglion, and they project fibers to the posterior horn of the spinal cord. Aδ and C fibers synapse with second-order neurons in the dorsal horn of lamina I to lamina V. These second-order neurons cross to the contralateral side of the spinal cord and ascend in the anterolateral spinal tracts to the thalamic nuclei, brainstem, and midbrain, where they synapse with third-order neurons and project to the cerebral cortex.

The simple stimulation of nociceptors without tissue damage may result in transmission of an action potential to the spinal cord and higher levels of the nervous system, and this may eventually result in a perception. However, if stimulation results in tissue damage, a host of changes can occur; these include the local release of many chemicals near the site of the injury as well as chemical changes at the spinal cord and higher levels of the central nervous system.

Locally released chemicals may be excitatory or inhibitory. Substance P and neurokinin A are excitatory neuropeptides that are released locally during tissue damage that may facilitate nociceptive transmission. Release of calcitonin gene-related peptide and substance P results in tissue edema and erythema by increasing vascular permeability in peripheral vasculature, thereby contributing to inflammation. There are proinflammatory substances released during tissue damage, including bradykinin, which can initiate pain transmission and sensitize nociceptors. Glutamate, nerve growth factor, serotonin, and histamine also potentiate the response of nociceptors. In addition, low pH may reduce the threshold of nociceptors. There are many additional sensitizing chemicals that act locally at the site of tissue injury as well as at the spinal cord level. The opposing system includes release of pain-inhibitory substances such as endogenous opioids, β-endorphins, acetylcholine, γ-aminobutyric acid, and somatostatin; these substances impede nociceptive transmission. Modulating nociceptive input can inhibit or facilitate the transmission of signals.

In addition to local and spinal cord effects of these chemicals, transmission of action potentials to the spinal cord may be modulated by the transmission of signals by other fiber types. A landmark publication by Melzack and Wall ³ described the gate control theory, which operates at the spinal cord level. The authors described input from Aβ fibers, which transmit light touch and pressure and have an inhibitory modulation effect on transmission of nociception to the spinal cord. This description of the gate control theory may explain the mechanism for modulating nociception at the spinal cord level when transcutaneous electrical nerve stimulation (TENS) is applied.

At the level of the spinal cord, nociception and the autonomic nervous system are under descending inhibitory control from supraspinal levels. A familiar example of descending inhibitory control is found in our normal disregard for the sounds of our heartbeat and respirations. Normally these signals are suppressed, but they are easily called into consciousness by cortical mechanisms. Similarly, the nociceptive system is also under descending inhibition from supraspinal systems, allowing us to ignore our pain at times during stressful situations. Serotonin and norepinephrine appear to be the primary neurotransmitters that regulate descending inhibitory control; however, others (e.g., α2 agonists, cannabinoids) may be involved.

Thus the perception of pain involves not simply the transmission of signals from peripheral sensors to the brain. It is in fact a complex system that is initiated by stimulating peripheral nociceptors in the presence of a milieu of local mediators that facilitate or inhibit signal transmission. As transmission of the signal moves centrally, modulating influences exert their influence before the perception of the sensation occurs.