บทคัดย่อ
Pain and headache are common problems in clinical practice. In general, pain
can be classified as nociceptive or neuropathic pain. In nociceptive pain, the unpleasant
symptom is caused by noxious stimulation leading to tissue injuries. Various chemical
mediators are involved in the process of inflammation occurred in the injured tissue.
These chemicals induce significant changes in neurons in several levels of neural
pathways involving in the nociceptive processing. Increased excitability of neurons
known as ‘peripheral and central sensitization’ is now believed to be the utmost
important mechanisms in development of chronic pain. In neuropathic pain, the pain is
caused by alteration of neuronal excitability which results in the increase neural firing in
the nociceptive pathway. This type of pain can be secondary to the structural change in
neural pathway such as nerve injuries, ischemia in path processing are such as thalamus,
etc. It can also occur after prolonged exposure to noxious stimulation which induces
secondary change in the neuronal pathway.
Similar to pain, headache can be classifies as primary and secondary headaches.
In the recent years, several remarkable discoveries have been reported which can
increase our understanding in the pathogenesis of primary headache. Our
Chulalongkorn Headache Research Group has shown that the excitability of cortical
neurons is increased in animal model of medication-overuse headache. Cortical
hyperexcitability may facilitate the development of cortical spreading depression, while
increased excitability of trigeminal neurons may facilitate the process of peripheral and
central sensitization. These changes may be secondary to the derangement of central,
probably serotonin (5-HT)-, and perhaps endocannabinoid-dependent or other,
modulating systems. Increased expression of excitatory cortical 5-HT2A receptors may
increase the susceptibility to developing cortical spreading depression, an analog of
migraine aura. A reduction of diffuse noxious inhibitory controls may facilitate the
process of central sensitization, activate the nociceptive facilitating system, or promote
similar molecular mechanisms to those involved in kindling. Low 5-HT levels also
increase the expression and release of calcitonin gene-related peptide from the
trigeminal ganglion and sensitize trigeminal nociceptors. Thus, derangement of central
modulation of the trigeminal system as a result of chronic medication use may increase
sensitivity to pain perception and foster or reinforce medication overuse headache.
