Perceiving pain is essential to survival of an organism. One definition of pain is the perception of harmful stimuli. This may be from an internal (inflammation, bowel distention, etc.) or external stimulus (for example, mechanical or thermal), and these types of pain are perceived by nociceptive pain receptors. The current view is that external harmful (noxious) stimuli directly activate unmyelinated nerve endings in the skin. These nerve endings are associated with Remak glial cells that protect and metabolically support the unmyelinated nerves. These Remak glial cells are Schwann cells that do not myelinate the axons. Recently Hind Abdo, Laura Calvo-Enrique, Patrik Ernfors, and others investigated how these cutaneous Remak Schwann cells are distributed and interact with receptors (nociceptive nerve terminals) for detection of noxious stimuli [Reference Abdo1]. What they found is described as a distinct type of Schwann cell and a new organ for feeling pain.
Abdo et al. used genetic labeling to identify these cutaneous Schwann cells. Recombination of specifically tagged cells revealed their location in the dermis near the border with the epidermis (Figure 1). Combining this with specific stains for neurons demonstrated that epidermal Schwann cell processes attached to the nerves. Transmission electron microscopy showed that nerve terminals emerged from the soma of Schwann cells located a few micrometers from the border of the epidermis and that the glial cell was the only source of cytoplasmic sheaths for the nerve terminals. These morphologically distinct glia also had other vital characterisitics such as a high expression of aquaporin, a protein that functions in water balance of cells. Nerve and Schwann cell processes were surrounded by a thick layer of fibrillar collagen that was distinct from the rest of the collagen in the dermis. Immunoelectron microscopy further confirmed the existence of a morphologically and molecularly specialized type of Schwann cell that formed a mesh-like network in the subepidermal border. This constituted a glial-neural complex with an intimate association with nociceptive nerves, which is insulated by a structural support of collagen fibers. Abdo et al. called these specialized glial cells nociceptive Schwann cells. These nociceptive cells were found to be a population distinct from other cutaneous Schwann cells.
After the nociceptive Schwann cells were clearly identified, Abdo et al. used a technique called optogenetics to determine if these cells could be stimulated by painful stimuli. Since these cells are located superficially, intense light stimulation was used and was found to elicit limb withdrawal in certain strains of mice. This withdrawal also elicited shaking and licking of the paw, which are considered to be pain-specific behaviors, and was associated with increased electrical activity in nerves from the paw.
Electrical properties of nociceptive Schwann cells in response to mechanical stimuli were also examined in cultured cells by whole-cell current-clamp electrophysiological recordings. It was found that nociceptive Schwann cells responded to both positive and negative changes in force but much less to sustained force. This and other evidence suggests a very fast response of these cells to mechanical stimuli, similar to what has been described in sensory neurons.
Abdo et al. provide strong evidence for a specialized glial cell type that forms a newly described sensory organ in the skin, responsible for initiating the sensation of pain. The nociceptive Schwann cells and nociceptive nerves form a pain-detecting glial-neural complex with two sensor-receptor cell types: the glia and the nerve. The functional implications of these findings are immense, presenting a new way that animals perceive pain. This is not only important for a better understanding of how the body performs this essential perception of pain, but it could play a key role in developing future therapies for dealing with pain, including treatment of debilitating clinical conditions such as chronic pain syndromes.