Nociception: Difference between revisions

Nociception[edit | edit source]

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Definition/Descrition
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Nociception is the neural processes of encoding and processing noxious stimuli.^[1] In another ways, it refers to signal arriving in the central nervous system resulting from activation of specialized sensor receptors celled nociceptors (peripheral nerves endings) by adequate noxious stimuli. Nociception is physiological process that protects tissue against damage. This process is also known as nocioception or nociperception, but is not synonym of pain sense. Term ‘‘nociception” and ‘‘pain” should not be confused, because each can occur without the other.^[1] Pain arising from activation of nociceptors by actual or potentially harmful stimuli is called nociceptive pain. It is important to note that excitation of nociceptors does not always evoke pain.

Nociceptive pain can be classified by tissue origin:
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• Superficial somatic (e.g. skin)
• Deep somatic (e.g. ligaments, tendons, bones and muscles)
• Visceral (e.g. internal organs)
  

Noxious stimuli is divided by type:
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• Thermal
• Mechanical
• Chemical
  

Nociceptors
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Nociceptors (noci- is derived from the Latin for “hurt”) are sensory receptors capable of transducing and encoding noxious stimuli.^[1] The initial reception of noxious input occurs in functionally specialized free nerve endings of the skin, muscles, joints, viscera, dura, blood vessels and in fascia. The cell bodies of nociceptors are located in the dorsal root ganglia (DRG) for the periphery and the trigeminal ganglion for the face. However, not every nociceptor responds to each type of the noxious stimuli. The apparent lack of a response to a noxious stimulus may result because of different receptors located on membrane of 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, application of noxious stimulus of one modality may alter the response properties of the nociceptor to other modalities. Also application of particular stimulus for 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 are 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 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 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 tissue but has not been found in articular cartridge, synovial membranes, visceral pleura, lung parenhyma, pericardium, brain and spinal cord tissue.

Clasification of nociceptors.
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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 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 by classified by the conduction velocity of their axons^[3] or fibres diameter,^[4] this is group III or IV and Aδ or C respectively.

• Type Aδ medium diameter myelinated afferents that mediate acute, well-localized, sharp pricking type pain, known as group III afferent^[5]. Aδ aferent 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. Their 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). Activity of this afferent almost certainly mediates the “first” acute pain response to noxious heat.^[5] They have been reported in the knee joint (w195), viscera (w1990) and cornea (w1991).

C unmyelinated afferent fibres that convey poorly localized dull, burning, so called “second” or slow pain are known as group IV. Avarege fibre dimeter is 3mm and conductive velocity is 3 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) (AB). The response of CMHs is also strongly influenced by the stimulus history. Both fatigue and sensitization are observed (www3). 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 (www4). 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, histamin) and are often considered to be chemoreceptors. (sss)

In summury to the above, immediate, well localised, stingy pain sensation is mediated by small diameter mylinated nerve fibres, type Aδ. C fibres madate 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.

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References[edit | edit source]

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