Pathophysiology of pain in postherpetic neuralgia: A clinical and neurophysiological study

Truini, Andrea; Galeotti, F.; Haanpää, Maija; Zucchi, Riccardo; Albanesi, Ada; Biasiotta, A.; Gatti, Antonio; Cruccu, G.

doi:10.1016/j.pain.2008.08.018

Cited by 114 publications

(82 citation statements)

References 31 publications

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“…However, it is important to mention the possible contributions of C-low-threshold mechanoreceptors for tactile allodynia, reported in a recent publication (Seal et al, 2009). In addition, other sensory disturbances frequently associated with PHN are paresthesia, dysesthesia, hyperalgesia, and itching (Dworkin et al, 2008;Truini et al, 2008). Many hypotheses have been proposed to explain this diversity in symptomatology during PHN.…”

Section: Why Is There a Predilection For The Trigeminal Ophthalmic Brmentioning

confidence: 99%

“…Initially, it was proposed that there was a preferential destruction of larger myelinated fibers (Aβ fibers), leaving an excess of the small myelinated (Aδ) and unmyelinated (C) fibers interpreted as the cause of sensory dysfunction in PHN (Noordenbos, 1959;Watson et al, 1988). Recent studies have stated that all sets of sensory fibers may be affected in this condition (Truini et al, 2008;Delaney et al, 2009), and data from neurophysiological-clinical correlations suggest a relationship between constant pain and loss of Aδ and C fibers and between paroxysmal pain and Aβ fiber demyelinization (Truini et al, 2008). Furthermore, the density of epidermal innervation has been associated with the occurrence of PHN, since samples from skin biopsies, when immunolabeled with PGP 9.5 (an axonal marker), have shown a greater amount of neuritis/mm 2 in individuals without PHN than in those with PHN (Oaklander, 2001).…”

Section: Why Is There a Predilection For The Trigeminal Ophthalmic Brmentioning

confidence: 99%

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The Role of Sensory Fiber Demography in Trigeminal and Postherpetic Neuralgias

DaSilva

DosSantos

2011

J Dent Res

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A supplemental appendix to this article is published electronically only at http://jdr.sagepub.com/supplemental. AbstrActIn this study, we systematically investigated fiber demography, based on function and distribution, from the periphery to their destinations in the various central (sub) nuclei in the trigeminal brainstem nuclear sensory complex. Conventional and novel compelling information is provided, demonstrating that the ratio and somatotopy of types A and C sensory fibers at the site of a lesion can elucidate important puzzles in TNP disorders. For instance, we explain how of a major shift in the fibers' direction and ratio at the level of the trigeminal root entry zone (REZ) influences the pathophysiology of preand typical trigeminal neuralgia. As a result, there is a high A/C ratio of oral and peri-oral fibers in the supero-medial region of the REZ, which is mostly susceptible to vascular compression. However, this A/C ratio varies considerably at lower proportions in other areas along the peripheral trigeminal pathway, where an injury (viral, vessel compression, or trauma) can lead to a broader spectrum of fiber involvement and, consequently, pain outcome. In summary, we explain how fiber demography can influence pain quality, location, temporal features, progress, and treatment prognosis of TNP in those patients who develop it.

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Section: Why Is There a Predilection For The Trigeminal Ophthalmic Brmentioning

confidence: 99%

Section: Why Is There a Predilection For The Trigeminal Ophthalmic Brmentioning

confidence: 99%

The Role of Sensory Fiber Demography in Trigeminal and Postherpetic Neuralgias

DaSilva

DosSantos

2011

J Dent Res

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“…31,32 There is evidence that all sensory fiber types are affected in PHN, with constant pain possibly being associated with damage to nociceptive afferents and paroxysmal pain related to changes in A␤ fibers. 33 Quantitative thermal sensory testing showed greatly increased heat pain thresholds in the affected dermatome of some chronic PHN patients. 34 Thus, there is a subset of PHN patients with pain and loss of cutaneous C-nociceptor function in a region that is coextensive with allodynic skin.…”

Section: Postherpetic Neuralgiamentioning

confidence: 99%

Postherpetic Neuralgia: From Preclinical Models to the Clinic

et al. 2009

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Summary: Postherpetic neuralgia (PHN), a common complication of herpes zoster, which results from reactivation of varicella zoster virus, is a challenging neuropathic pain syndrome. The incidence and severity of herpes zoster and PHN increases with immune impairment or age and may become a greater burden both in terms of health economics and individual suffering. A clearer understanding of the underlying mechanisms of this disease and translation of preclinical outcomes to the clinic may lead to more efficacious treatment options. Here we give an overview of recent findings from preclinical models and clinical research on PHN.

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“…Sensory disturbances and pain were carefully assessed. Before testing, all patients were interviewed and asked to indicate the severity of their current pain, to rate the pain intensity on an 11-point NRS ranging from 0 (no pain) to 10 (worst possible pain) and to describe their predominant pain in one of the following categories: constant pain, deep pain, burning pain, paroxysmal pain, lancinating pain, allodynia, paresthesia, dysesthesia, hyperalgesia, and itching [12,24].…”

Section: Clinical Examinationmentioning

confidence: 99%