Nociception


Overview [edit | edit source]

Nociception is a subcategory of somatosensation. Nociception is the neural processes of encoding and processing noxious stimuli.[1] Nociception refers to a signal arriving at the central nervous system as a result of the stimulation of specialised sensory receptors in the peripheral nervous system called nociceptors. Nociceptors are activated by potentially noxious stimuli, as such nociception is the physiological process by which body tissues are protected from damage. Nociception is important for the "fight or flight response" of the body and protects us from harm in our surrounding environment.

Nociceptors can be activated by three types of stimulus within the target tissue - temperature (thermal), mechanical (e.g stretch/strain) and chemical (e.g. pH change as a result of local inflammatory process). Thus, a noxious stimulus can be categorised into one of these three groups. 

The terms nociception and pain should not be used synonymously, because each can occur without the other.[1]. Pain arising from activation of the nociceptors is called nociceptive pain. Nociceptive pain can be classified according to the tissue in which the nociceptor activation occurred: superficial somatic ( e.g. skin), deep somatic (e.g. ligaments/tendons/bones/muscles) or visceral ( internal organs).

Nociception pathway[edit | edit source]

Not every nociceptor responds to each type of noxious stimuli. The apparent lack of a response to a noxious stimulus may result because of different receptors located on the membrane of the end terminal (free nerve ending) or the stimulus intensity is insufficient.[2] Usually, the stimulation threshold of a nociceptor is below tissue-damaging intensity. Nociceptors have heterogeneous properties, responding to multiple stimulus modalities (polymodal). However, the application of noxious stimulus of one modality may alter the response properties of the nociceptor to other modalities. Also, the application of a particular stimulus for a given length of time may induce long-term changes in the response properties of the nociceptor.[3] Injury and inflammation decrease the threshold and increase the magnitude of the response for a given stimulus, a phenomenon known as peripheral sensitization. Of particular interest is the heat responsive, but mechanically insensitive unmyelinated afferents that develop mechanical sensitivity only in the setting of injury.


Nociceptors have the morphological appearance of free nerve endings. The term “free nerve ending” indicates that in the light microscope no (corpuscular) receptive structure can be recognized. At present, there are no clear ultrastructural differences between non-nociceptive free nerve endings (e.g., sensitive mechanoreceptors and thermoreceptors) and nociceptive ones. Functionally, different free nerve endings

Schematic drawing of nociceptor showing the four regions of the cell.

are assumed to possess different sets of receptor molecules in their axonal membrane. Receptor molecules that are particularly important for the function of muscle nociceptors are acid-sensing ion channels (ASICs) that open at a low tissue pH, P2X3 receptors that are activated by binding adenosine triphosphate (ATP), and the transient receptor potential receptor subtype 1 (TRPV1) that is sensitive to high temperatures, capsaicin chemical, and low pH. The neuropeptide substance P has been reported to be present predominantly in nociceptive afferent fibres. While there are numerous neurotransmitters within the nervous system, the three most common participating in nociceptive transmission are peptides, purines, and excitatory amino acids (EAA). The EAA, particularly glutamate, produce the initial excitatory response on the postsynaptic, second-order, neuron, followed by the release of peptides, including substance P, causing a more prolonged depolarization and sustained nociceptive transmission


Nociceptors are present in many body tissues but have not been found in articular cartilage, visceral pleura, lung parenchyma, pericardium, brain, and cord tissue.

Types of nociceptors[edit | edit source]

Several classes of nociceptors have been described. Some nociceptors respond to noxious cold, noxious heat and high threshold mechanical stimuli as well as a variety of chemical mediators. Nociceptors, although polymodal, can be further divided into two main classes on the basis of response to mechanical stimuli, leading to a distinction between mechanically sensitive afferents (MSA) and mechanically insensitive afferents (MIA) defined as afferents that have very high mechanical thresholds or are unresponsive to mechanical stimuli.

Nociceptors can be classified by the conduction velocity of their axons[3] or fibres diameter,[4] this is group III and IV ord Aδ and C respectively.

Type Aδ medium diameter myelinated afferents that mediate acute, well-localized, sharp pricking type pain, known as group III afferent. Aδ afferent fibres have average fibre diameter 2-5mm and conductive velocity 5-30 m/s. Aδ nociceptors can be further divided into two types (it appears to exist proximately 50% of each type)

  • Type I Aδ are mechanically sensitive afferents (MSA) that respond with a slowly adapting discharge to strong punctuate pressure. They also respond to heat and chemical stimuli and have relatively high heat thresholds (>50C).
  • Type II Aδ nociceptors have lower heat threshold than Type I units but have very high mechanical thresholds (called mechanically insensitive afferents - MIAs). The activity of this afferent almost certainly mediates the “first” acute pain response to noxious heat. They have been reported in the knee joint,[5] viscera[6] and cornea.[7]

Type C unmyelinated afferent fibres that convey poorly localized dull, burning, so called “second” or slow pain are known as group IV. Average fibre diameter is below 2mm and conductive velocity is 2 m/s or less. The unmyelinated C fibres are also heterogeneous. C fiber afferents can be divided into two classes based on their response to mechanical stimuli. Like the myelinated Aδ afferent fibres, most C fibres are polymodal, that is, they include a population that is both mechanically and heat sensitive (CMHs). The response of CMHs is also strongly influenced by the stimulus history. Both fatigue and sensitization are observed.[8] A decrease in the response to heat is also observed following mechanical stimuli applied to the receptive field or electrical stimuli applied to the nerve trunk.[9] This suggests that fatigue in response to a given stimulus modality can be induced by heterologous stimulation, that is, by excitation with a stimulus of a different modality. These are the predominant type of C-fibre nociceptors in mammalian skin. Mechanically insensitive C-fibers (C-MIAs) are either unresponsive to mechanical stimuli or have a very high mechanical threshold. These afferents respond to heat and various noxious chemical stimuli (e.g., capsaicin, histamine) and are often considered to be chemoreceptors.

In summary to the above, immediate, well localised, stingy pain sensation is mediated by small diameter myelinated nerve fibres, type Aδ. C fibres mediate poorly localized anatomically type of pain, it has an aching and burning character, comes later than the initial first sensation and it is difficult to estimate its strength.

TRP Channels[edit | edit source]

Nociceptors respond to certain temperature range and mechanical stimulus.

The peripheral end of the axon contains encapsulated proteins called transduction proteins (TRP), which can be activated by a specific stimulus. The transient receptor potential (TRP) multigene superfamily encodes integral membrane proteins that function as ion channels. The TRP channel family is of interest because several members have been implicated in nociceptor signal transduction.
Noxious cold and noxious heat stimuli are detected by Aδ and C fiber nociceptors. The TRP channel family provides a group of molecules equipped to detect thermal changes. The full range of temperatures, from noxious cold to noxious heat, appears to be transduced by the activity in these ion channels. TRPM8 and TRPV3/4 encode cool and warm, respectively, TRPA1 transduces noxious cold and TRPV1/2 sense noxious heat. Some of the thermosensitive TRP channels respond to chemical and mechanical stimuli as well.[10]
For example, TRPV1 is essential for transducing the nociceptive by inflammatory, and hypothermic effects of vanilloid compounds and contributes to acute thermal nociception and thermal hyperalgesia following tissue injury. TRPV1 current is potentiated by bradykinin and nerve growth factor via several possible mechanisms and is also activated by protons and capsaicin, the ‘‘hot’’ compound in chili peppers.[11] In contrast to the hyperalgesia following intense noxious stimuli, prolonged exposure to capsaicin can result in subsequent desensitization.
While the discovery of thermosensitive TRP channels has greatly enhanced our understanding of transduction mechanisms of thermal stimuli, findings in animals with selective gene deletions clearly indicate that multiple and yet unknown transduction mechanisms are engaged by thermal stimuli.

Chemical mediators[edit | edit source]

Injury results in the local release of numerous chemicals from non-neuronal cells (e.g., fibroblasts, mast cells, neutrophils, monocytes, and platelets), as well as from the sensory terminals of primary afferent fibers that mediate or facilitate the inflammatory process. Inflammatory mediators include prostaglandins, leukotrienes, bradykinin, serotonin, histamine, SP, thromboxanes, platelet-activating factor, purines such as adenosine and ATP, protons, and free radicals. Cytokines, such as interleukins and tumor necrosis factor, and neurotrophins, especially NGF, are also generated during inflammation. It is worth to note that most of those chemicals (mainly substances such as bradykinin and prostaglandin E2) are generally considered to not activate nociceptors directly but rather enhance the sensation of pain in response to natural stimuli and other endogenous chemicals by increasing the frequency of action potential firing.[3]

Membrane chemical receptors of a nociceptive nerve ending.


Activation of nociceptors not only transmits afferent messages to the dorsal horn of the spinal cord but also initiates the process of neurogenic inflammation. Neurogenic inflammation causes a release of neurotransmitters, notably substance P and calcitonin gene-related peptide (CGRP), which leads to severe vasodilation, as well as plasma leakage of proteins and fluid from post capillary venules.[3]


Two chemicals are of particular interest:

  • Adenosine triphosphate (ATP)

ATP is the energy-carrying molecule in all cells of the body. It is released from all tissues during trauma and other pathologic changes that are associated with cell death. For this reason, ATP has been considered a general signal substance for tissue trauma and pain. In human microneurographic studies, injection of ATP activated 60% of mechano-responsive and mechano-insensitive C-nociceptive fibers without sensitizing these fibers to mechanical or heat stimuli. ATP activates purinergic P2X3 receptors in nociceptors causing a discharge. ATP is particularly important for muscle pain because it is present in muscle cells in high concentration.

  • Protons alteration in tissue pH

Acid-sensing ion channels (ASICs) constitute a family of receptor molecules that are sensitive to a drop in pH and open at various pH values. The channel proteins react already too small pH changes. This receptor family (for instance ASIC1 and ASIC3) is particularly important for muscle pain because almost all pathologic changes in muscle are accompanied by a drop in tissue pH, e.g., exhausting exercise, ischemia, and inflammation.

Location of Nociceptors[edit | edit source]

The cell bodies of nociceptors are located in the dorsal root ganglia (DRG) for the periphery and the trigeminal ganglion for the face. Their axons extend into the peripheral nervous system and terminate in branches creating receptive fields.

  • Skin

Free nerve endings terminating in the skin are the machinery for signaling local mechanical, thermal, and chemical changes.[3] The large majority of free nerve endings in the skin are called polymodal nociceptors because they contain multiple receptors and thus respond to various combinations of the above mentioned stimulus.[3] Type I Aδ high-threshold mechanoreceptors units are densely distributed in hairy and glabrous skin.

Receptor molecules that are particularly important for the function of muscle nociceptors are acid-sensing ion channels (ASICs) that open at a low tissue pH, P2X3 receptors that are activated by binding adenosine triphosphate (ATP), and the transient receptor potential receptor subtype 1 (TRPV1) that is sensitive to high temperatures and low pH.
In skeletal muscle, the free nerve endings appear to be distributed quite evenly. No difference between the proximal and distal portions of the rat gastrocnemius–soleus muscle was found. However, in the same study, the nerve fiber density in the peritendineum of the rat calcaneal tendon was found to be several times higher than that in the GS muscle. In contrast, the collagen fiber bundles of the tendon tissue proper were almost free of free nerve endings.

Innervation of Achilles tendons human is provided by nerves from the surrounding muscles and by small fasciculi from cutaneous nerves but this involves all nerve ending.[12] Free nerve endings are represented inside the tendons, but mainly in peritendinous tissue, are pain receptors. The number and location of all nerve fibers and nerve endings vary according to the function of the tendon, being more represented in the smaller tendons involved in fine movements.

Nociceptors in joints are located within the joint capsule, ligaments and proximal tendons, bone, periosteum, articular fat pad and around blood vessels but not in the joint cartilage. High threshold nociceptive afferents terminate primarily in the synovium and periosteum and normally respond only to the movement of the joint beyond the working limits. Following joint damage, two factors combine to alter the mechanical sensitivity of articular nociceptors. First, physical changes (joint effusion and tissue edema) alter the resting and movement-induced forces exerted on the joint tissues, and second, inflammatory mediators released within the damaged tissue sensitize articular nociceptive afferents by binding to receptors on the nerve endings. Many nociceptors of the joint respond to innocuous movements but are increasingly activated when movements exceed the physiological working range, whereas other nociceptors are active exclusively during noxious movements.[5] The third group of so-called silent nociceptors are normally inactive and respond only under pathological circumstances such as inflammation.[5]


The lumbar facet joint capsule has been demonstrated to be richly innervated by nociceptors and proprioceptive fibers.[13] In a normal state, nociceptors such as those seen in the facet joint capsule have a high threshold and would not be expected to discharge unless loads are supraphysiologic. However, in the presence of pathologic joint inflammation, synovitis chemical mediators may sensitize these nociceptors and supraphysiologic levels of stress may no longer be required to stimulate pain. Such inflammatory mediators (substance P, bradykinin, phospholipase A2) have been detected in the facet joint capsule.[13]


Nociceptors in intervertebral discs are normally limited to the outer third of the annulus, could be the substrate for discogenic pain when they are expanded over the larger annular area and penetrate further into the degenerated disk along the vasculature and fissures. Those C- and A δ fibers are likely responsible for transmitting pain responses. The posterior longitudinal ligament and the outer annulus fibrosus layers of intervertebral disc contain plenty of nociceptive fibers. Nerve fibres and nerve endings also occur in the subchondral bone of the zygapophysial joints. They occur in erosion channels extending from the subchondral bone to the articular cartilage.
A human study by (Kiter et al., 2010)[14] showed both free and encapsulated nerve endings in the human iliolumbar ligament. Studie by (Hirsch et al., 1963)[15] suggested the presence of fine nerve fibers and complex unencapsulated endings in the supraspinous and intraspinous ligaments.

  • Viscera

Visceral nociceptors do not respond to cutting or burning injuries like their counterparts in the peripheral cutaneous tissue. Instead, they are activated in response to pathological change. Pain producing stimuli in the viscera including traction on the mesentery, inflammation, distension of hollow muscular-walled organs such as gastrointestinal, urinary tract, gall bladder and strong contractions of muscle layers surrounding such hollow organs, chemicals irritants or ischaemia in organs such as the heart. The distribution of these fibers varies among organs. High-threshold receptors exclusively innervate organs from which pain is the only conscious sensation (i.e., ureter, kidney, lungs, heart), but are relatively few in organs that provide innocuous and noxious sensations (e.g., colon, stomach, and bladder), innervated mostly by low-threshold receptors. Organs, such as the liver, lungs, kidneys, and the pancreas, have few receptors, but the pain from these organs comes mostly from the activation of receptors in the capsules of these organs. Nociceptive stimulation of viscera leads to diffuse pain that is difficult to localize. Afferent nociceptive fibres in viscera are found in association with sympathetic and parasympathetic nerves. Majority of visceral organs are innervated by vagal nerve, but studies do not show clearly whether or not this nerve is capable to carry nociceptive afferent input. However, some studies clearly demonstrate that vagal afferents convey information about high intensity mechanical stimuli to the central nervous system. A number of studies involving humans or animals have shown that subjects with spinal cor lesion are able to report pain likely originating from visceral organs area.[16]

References[edit | edit source]

  1. 1.0 1.1 Loeser JD, Treede RD. The Kyoto protocol of IASP Basic Pain Terminology. Pain. 2008; 137(3): 473–7. doi:10.1016/j.pain.2008.04.025. PMID 18583048
  2. Basbaum AI, Jessell T. The Perception of Pain. In: Kandel ER, Schwartz J, Jessell T. editors. Principles of Neuroscience. New York: Appleton and Lange; 2000. p472-491
  3. 3.0 3.1 3.2 3.3 3.4 3.5 Meyer RA, Ringkamp M, Campbell JN, Raja SN. Peripheral mechanisms of cutaneous nociception. In: McMahon SB, Koltzenburg M, editors. Wall and Melzack’s Textbook of Pain. London: Elsevier; 2006. p3–34.
  4. Lloyd DPC. Neuron patterns controlling transmission of ipsilateral hindlimb reflexes in cat. J Neurophysiol. 1943;6:293–315
  5. 5.0 5.1 5.2 Schaible HG, Schmidt RF. Effects of an experimental arthritis on the sensory properties of fine articular afferent units. Journal of Neurophysiology. 1985; 54:1109-1122
  6. Häbler HJ, Jänig W, Koltzenburg M. A novel type of unmyelinated chemosensitive nociceptor in the acutely inflamed urinary bladder. Agents and Actions. 1988;25:219-221
  7. Tanelian DL. Cholinergic activation of a population of corneal afferent nerves. Experimental Brain Research. 1991;86:414-420
  8. LaMotte RH, Campbell JN. Comparison of responses of warm and nociceptive C-fiber afferents in monkey with human judgements of thermal pain. Journal of Neurophysiology. 1978;41:509-528
  9. Treede RD, Meyer RA, Raja SN, Campbell JN. Evidence for two different heat transduction mechanisms in nociceptive primary afferents innervating monkey skin. Journal of Physiology. 1995;483:747-758
  10. Schepers RJ, Ringkamp M. Thermoreceptors and thermosensitive afferents. Neuroscience & Biobehavioral Reviews. 2010; 34(2):177-184
  11. Caterina MJ, Schumacher MA, Tominaga M, Rosen TA, Levine JD, Julius D. The capsaicin receptor: a heat-activated ion channel in the pain pathway. Nature 1997; 389:816–824
  12. Bjur D, Alfredson H, Forsgren S. The innervation pattern of the human Achilles tendon: studies of the normal and tendinosis tendon with markers for general and sensory innervation. Cell Tissue Res. 2005; 320:201-206
  13. 13.0 13.1 Ashton IK, Ashton BA, Gibson SJ,  Polak JM, Jaffray DC, Eisenstein SM. Morphological basis for back pain: the demonstration of nerve fibers and neuropeptides in the lumbar facet joint capsule but not in ligamentum flavum. J Orthop Res. 1992;10(1):72-78
  14. Kiter E, Karaboyun T, Tufan AC, Acar K. ImmunohistochemicalfckLRdemonstration of free nerve endings in iliolumbar ligament. Spine. 2010; 35(4):E101-4. doi: 10.1097/BRS.0b013e3181ae561d.
  15. Hirsch C, Ingelmark BE, Miller M. The anatomical basis for lowfckLRback pain. Studies on the presence of sensory nerve endings infckLRligamentous, capsular and intervertebral disc structures in thefckLRhuman lumbar spine. Acta Orthop Scand. 1963; 33:1–17.
  16. Moller, Aage (2014-04-22). Pain, Its Anatomy, Physiology and Treatment. Kindle Edition.