Resumen
Multiple sclerosis (MS) is a progressive neurologic disorder that disrupts axonal myelin in the central nervous system. Demyelination produces alterations in saltatory conduction, slowed conduction velocity, and a predisposition to conduction block. An estimated 60–80% of MS patients experience temporary worsening of clinical signs and neurologic symptoms with heat exposure (Uhthoff's phenomenon). This heat intolerance in MS is related to the detrimental effects of increased temperature on action potential propagation in demyelinated axons, resulting in conduction slowing and/or block. Additionally, MS may produce impaired neural control of autonomic and endocrine functions. Isolating and interpreting mechanisms responsible for autonomic dysfunction due to MS can be difficult as it may involve sensory impairments, altered neural integration within the central nervous system, impaired effector responses, or combinations of all of these factors. MS lesions occur in areas of the brain responsible for the control and regulation of body temperature and thermoregulatory effector responses, resulting in impaired neural control of sudomotor pathways or neural-induced changes in eccrine sweat glands, as evidenced by observations of reduced sweating responses in MS patients. Although not comprehensive, some evidence exists concerning treatments (cooling, precooling, and pharmacologic) for the MS patient to preserve function and decrease symptom worsening during heat stress. This review focuses on four main themes influencing current understanding of thermoregulatory dysfunction in MS: (1) heat intolerance; (2) central regulation of body temperature; (3) thermoregulatory effector responses; and (4) countermeasures to improve or maintain function during thermal stress.
| Idioma original | English |
|---|---|
| Título de la publicación alojada | Handbook of Clinical Neurology |
| Páginas | 701-714 |
| Número de páginas | 14 |
| DOI | |
| Estado | Published - ene 1 2018 |
Serie de la publicación
| Nombre | Handbook of Clinical Neurology |
|---|---|
| Volumen | 157 |
| ISSN (versión impresa) | 0072-9752 |
| ISSN (versión digital) | 2212-4152 |
Nota bibliográfica
Publisher Copyright:© 2018 Elsevier B.V.
Financiación
The authors would like to express their gratitude to the following collaborators who assisted with the authors’ studies contained herein: Elliot M. Frohman, MD, PhD; Craig G. Crandall, PhD; Andrea T. White, PhD; Teresa C. Frohman, PA; David M. Keller, PhD; Paul J. Fadel, PhD; Jamie M. Vener, PhD; Mu Huang, PhD; Dustin R. Allen, PhD; and Jack H. Petajan MD, PhD. Presented work conducted by the authors was funded by grants from the National Multiple Sclerosis Society grants RG2922B1/1, PP0887, PP1040, RG4043A1/1 (S.L. Davis), National Heart, Lung, and Blood Institute grant R15-HL-117224 (S.L. Davis), the Kuzell Institute (S. L. Davis and O. Jay), and MS Research Australia Incubator grant 14-009 (O. Jay and S. L. Davis).
| Financiadores | Número del financiador |
|---|---|
| Kuzell Institute | |
| MS Research Australia Incubator | 14-009 |
| National Heart, Lung, and Blood Institute (NHLBI) | R15-HL-117224 |
| National Heart, Lung, and Blood Institute (NHLBI) | |
| National Multiple Sclerosis Society | RG4043A1/1, PP0887, PP1040, RG2922B1/1 |
| National Multiple Sclerosis Society |
ASJC Scopus subject areas
- Neurology
- Clinical Neurology
Huella
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