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Inicio Neurología (English Edition) Non-motor neurological symptoms in patients with amyotrophic lateral sclerosis
Información de la revista
Vol. 33. Núm. 7.
Páginas 474-476 (septiembre 2018)
Vol. 33. Núm. 7.
Páginas 474-476 (septiembre 2018)
Letter to the Editor
Open Access
Non-motor neurological symptoms in patients with amyotrophic lateral sclerosis
Síntomas neurológicos extra-motores en pacientes con esclerosis lateral amiotrófica
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3188
H.R. Martíneza,c,
Autor para correspondencia
, C.E. Escamilla-Ocañasa, M. Hernández-Torreb
a Instituto de Neurología y Neurocirugía, Hospital Zambrano-Hellion, Tecnológico de Monterrey, San Pedro Garza García, Mexico
b Instituto de Medicina Interna, Hospital Zambrano-Hellion, Tecnológico de Monterrey, San Pedro Garza García, Mexico
c Servicio de Neurología, Hospital Universitario UANL, Monterrey, Mexico
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Tablas (1)
Table 1. Non-motor symptoms of ALS, classified by domain, frequency, and ratio.
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Dear Editor:

Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease traditionally defined as clinical symptoms involving the upper motor neuron, in the motor homunculus, and the lower motor neuron, in the spinal cord.1,2 However, recent publications have described non-motor signs and symptoms in patients with definite ALS, including impaired higher cerebral functions, signs of dysautonomia, metabolic disorders,3,4 and cognitive alterations linked to frontotemporal dementia.5 Post mortem histopathological studies of patients with definite sporadic ALS have identified protein inclusions of transactive response DNA binding protein 43kDa (TDP-43) in non-motor areas of the central nervous system (CNS), including the nigrostriatal system, cerebellum, forebrain, hypothalamus, and neocortical and allocortical areas.6,7 ALS and frontotemporal dementia are currently considered to be TDP-43 proteinopathies.

We performed a retrospective study of the medical records of 112 patients diagnosed with definite sporadic ALS according to the El Escorial clinical and neurophysiological criteria.8 We analysed the non-motor neurological signs and symptoms reported at the time of diagnosis and those manifesting in the first year of clinical follow-up. All patients with diagnosis of definite ALS were assessed with the revised ALS functional rating scale (ALSFRS-r), the Mini-Mental State Examination, a neuropsychological test, a genetic test, and the Hamilton Anxiety and Depression Scale during the baseline consultation, and underwent at least one additional evaluation during the one-year follow-up period. In our sample, we identified 25 non-motor symptoms, with the most prevalent being: depression (in 47% of patients), pain (26%), fatigue (24%), anxiety (18%), pseudobulbar symptoms (13%), and paraesthesias (13%) (Table 1). No diagnosis of frontotemporal dementia was established in any of our patients; curiously, all cases with pseudobulbar symptoms, depression, or anxiety were negative for the chromosome 9 hexanucleotide repeat expansion normally associated with pseudobulbar symptoms (C9Orf72 gene). We identified an average of 4.2±2.03 non-motor symptoms per patient. Patients with bulbar ALS presented a higher number of non-motor symptoms than patients with spinal ALS (5.41±1.61 and 3.85±2.01 non-motor symptoms per patient, respectively). Furthermore, we observed correlations between symptom pairs which may have similar pathophysiological mechanisms, including: anxiety and depression (χ2; P=.025), bladder incontinence and constipation (χ2; P=.017), and pain and paraesthesias (χ2; P=.027).

Table 1.

Non-motor symptoms of ALS, classified by domain, frequency, and ratio.

Symptom  Frequencya  Ratiob 
Cardiovascular
Oedema 
Orthostatic hypotension 
Somnolence/fatigue
Fatigue  27  24 
Restless legs 
Insomnia 
Daytime somnolence 
Mood/cognition
Depression  53  47 
Anxiety  20  18 
Anhedonia 
Cognitive impairment 
Perceptual alterations/hallucinations
Pseudobulbar symptoms  14  13 
Blurred vision 
Gastrointestinal tract
Nausea 
Vomiting 
Bowel incontinence 
Constipation 
Urinary
Urinary problems 
Miscellaneous
Pain  29  26 
Paraesthesias  14  13 
Diaphoresis 
Seborrhoea 
Weight gain 
a

Frequency of symptom in the ALS patient total.

b

Ratio: percentage of symptom in patient total.

A recent study by Cykowski et al.7 detected TDP-43 inclusions in the forebrain and hypothalamus, reporting a significant correlation between this histopathological finding and predominantly bulbar ALS. In our sample, patients with predominantly bulbar ALS presented more non-motor symptoms than patients with spinal ALS.

Clinical heterogeneity of ALS is characteristic9; the presence of pathological inclusions in non-motor areas of the CNS in cases of definite sporadic ALS may explain the presence of atypical symptoms, which are frequently omitted and therefore are not approached or treated adequately, limiting quality of life. In our sample, the non-motor symptoms observed in patients with ALS may be incidental manifestations due to disability, or clinical manifestations due to the progression of the neurodegenerative process. Timely identification of non-motor manifestations in patients with classic motor symptoms may facilitate medical treatment and improve the clinical condition of these patients. The wide variety of clinical phenotypes, the recent histopathological findings in the CNS, and the presence of non-motor symptoms suggest that ALS is a multisystemic disease which is not restricted to the motor system.

References
[1]
M.H. Toft, O. Gredal, B. Pakkenberg.
The size distribution of neurons in the motor cortex in amyotrophic lateral sclerosis.
[2]
J.M. Ravits, A.R. la Spada.
ALS motor phenotype heterogeneity, focality, and spread. Deconstructing motor neuron degeneration.
Neurology, 73 (2009), pp. 805-811
[3]
S. Pinto, A. Pinto, M. de Carvahlo.
Decreased heart rate variability predicts death in amyotrophic lateral sclerosis.
Muscle Nerve, 46 (2012), pp. 341-345
[4]
L. Jelsone-Swain, C. Persad, K.L. Votruba, S.L. Weisenbach, T. Johnson, K.L. Gruis, et al.
The relationship between depressive symptoms, disease state, and cognition in amyotrophic lateral sclerosis.
Front Psychol, 3 (2012), pp. 1-10
[5]
S. Lattamte, S. Ciura, G.A. Rouleau, E. Kabashi.
Defining the genetic connection linking amyotrophic lateral sclerosis (ALS) with frontotemporal dementia (FTD).
Trends Genet, 31 (2015), pp. 263-273
[6]
J. Brettschneider, K.D. Tredici, J.B. Toledo, J.L. Robinson, D.J. Irwin, M. Grossman, et al.
Stages of pTDP-43 pathology in amyotrophic lateral sclerosis.
Ann Neurol, 74 (2013), pp. 20-38
[7]
M.D. Cykowski, H. Takei, P.E. Schultz, S.H. Appel, S.Z. Powell.
TDP-43 pathology in the basal forebrain and hypothalamus of patients with amyotrophic lateral sclerosis.
Acta Neuropathol Commun, 2 (2014), pp. 171
[8]
B.R. Brooks, R.G. Miller, M. Swash, T.L. Munsat, World Federation of Neurology Research Group on Motor Neuron Disease.
El Escorial revisited: revised criteria for the diagnosis of amyotrophic lateral sclerosis.
Amyotroph Lateral Scler Other Motor Neuron Disord, 1 (2000), pp. 293-299
[9]
J. Ravits, S. Appel, R.H. Baloh, R. Barohn, B.R. Brooks, L. Elman, et al.
Deciphering amyotrophic lateral sclerosis: what phenotype, neuropathology and genetics are telling us about pathogenesis.
Amyotroph Lateral Scler Frontotemporal Degener, 14 (2013), pp. 5-18

Please cite this article as: Martínez HR, Escamilla-Ocañas CE, Hernández-Torre M. Síntomas neurológicos extra-motores en pacientes con esclerosis lateral amiotrófica. Neurología. 2018;33:474–476.

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