cover image European Journal of Neurology

European Journal of Neurology

2020 - Volume 27
Issue 4 | April 2020
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Original Article

Background and purpose

The efficacy of galcanezumab, a monoclonal antibody for migraine prevention, has been demonstrated in two pivotal trials in patients with episodic migraine.

Methods

EVOLVE‐1 and EVOLVE‐2 were identical phase 3, randomized, double‐blind, placebo‐controlled studies in patients with episodic migraine. Mean migraine headache days per month at baseline was 9. Patients were randomized 2:1:1 to monthly injections of placebo, galcanezumab 120 mg/240 mg during the 6‐month double‐blind treatment period. Key efficacy outcomes were assessed in subgroups amongst patients for whom, previously, for efficacy and/or safety/tolerability reasons (i) one or more (≥1) preventives failed, (ii) two or more (≥2) preventives failed and (iii) preventives were never used, or used but not failed (no prior failure).

Results

In an integrated analysis of EVOLVE studies, galcanezumab 120 mg/240 mg versus placebo led to larger overall mean (SE) reductions in monthly migraine headache days across 6 months in patients with prior preventive failures ( < 0.001): ≥1 failure: 120 mg: −4.0 (0.4); 240 mg: −4.2 (0.5); placebo: −1.3 (0.4); ≥2 failures: 120 mg: −3.1 (0.7); 240 mg: −3.8 (0.8); placebo: −0.5 (0.6). Similar results were observed amongst patients with no prior failure, but the placebo response was larger: 120 mg: −4.7 (0.2); 240 mg: −4.5 (0.2); placebo: −3.0 (0.2) ( < 0.001 versus placebo). Significant improvements were observed with galcanezumab versus placebo for ≥50% and ≥75% reduction in monthly migraine headache days.

Conclusion

In patients with episodic migraine treated with galcanezumab, those with ≥1 or ≥2 prior preventive failures had significantly larger improvements, versus placebo, in efficacy outcomes. Similar results were observed in patients with no prior failure, with a larger placebo response.

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Authors:
D. D. Ruff, J. H. Ford, A. Tockhorn‐Heidenreich, V. L. Stauffer, S. Govindan, S. K. Aurora, G. M. Terwindt and P. J. Goadsby
Article first published online:
02 Dec 2019 | DOI: 10.1111/ene.14114

Original Article

Background and purpose

Cholinergic dysfunction appears to play a role in the cognitive impairment observed in Parkinson’s disease and dementia with Lewy bodies. The occurrence of cholinergic dysfunction in the early stages of these conditions, however, has not been investigated. The objective of this study was to investigate cholinergic function in patients with idiopathic rapid eye movement sleep behaviour disorder (iRBD), a disorder recognized to be an early stage of both Parkinson’s disease and dementia with Lewy bodies.

Methods

A total of 21 patients with polysomnography‐confirmed iRBD with no evidence of parkinsonism and cognitive impairment and 10 controls underwent positron emission tomography (PET) to assess brain acetylcholinesterase levels (C‐donepezil PET) and nigrostriatal dopaminergic function (F‐DOPA PET). Clinical examination included the Movement Disorder Society–Unified Parkinson’s Disease Rating Scale part III, Mini Mental State Examination and Montreal Cognitive Assessment.

Results

The C‐donepezil PET was successfully performed in 17 patients with iRBD and nine controls. Compared with controls, patients with iRBD showed a mean 7.65% reduction in neocortical C‐donepezil levels ( = 0.005). Bilateral superior temporal cortex, occipital cortex, cingulate cortex and dorsolateral prefrontal cortex showed the most significant reductions at voxel level.

Conclusion

Reduced neocortical C‐donepezil binding in our patients indicates cholinergic denervation and suggests that the projections from the nucleus basalis of Meynert, which supplies cholinergic innervation to the neocortex, are dysfunctional in iRBD. Longitudinal studies will clarify if these changes are predictive of future cognitive impairment in these patients.

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Authors:
M. Gersel Stokholm, A. Iranzo, K. Østergaard, M. Serradell, M. Otto, K. Bacher Svendsen, A. Garrido, D. Vilas, T.D. Fedorova, J. Santamaria, A. Møller, C. Gaig, K. Hiraoka, D.J. Brooks, N. Okamura, P. Borghammer, E. Tolosa and N. Pavese
Article first published online:
22 Dec 2019 | DOI: 10.1111/ene.14127

Original Article

Background and purpose

Increasing evidence has demonstrated that aquaporin‐4 (AQP4) immunoglobulin G causes damage to the kidney in neuromyelitis optica spectrum disorder (NMOSD). However, changes in urinalysis in NMOSD have not been investigated thus far. Our objective was to evaluate the changes in urinalysis in NMOSD patients.

Methods

Case data were collected from 44 patients with AQP4 antibody‐positive NMOSD, 53 patients with multiple sclerosis (MS) and 79 age‐ and sex‐matched healthy controls. Analyses of early morning urine and 24‐h urine samples comparing NMOSD with MS patients were conducted.

Results

In the acute phase, urine pH levels ( < 0.001) and urine specific gravity levels ( < 0.001) from NMOSD patients were significantly higher and lower, respectively, than for MS patients. 24‐h urine sodium and 24‐h urine volume from NMOSD patients were significantly higher than for MS patients (both  = 0.001). A 24‐h urine volume higher than 2500 ml (odds ratio 11.7, 95% confidence interval 1.863–73.066) and a 24‐h urine sodium higher than 200 mmol (odds ratio 16.0, 95% confidence interval 2.122–120.648) are more likely to occur in NMOSD patients in the acute phase than in MS patients.

Conclusions

The urinalysis results were significantly different between NMOSD patients and MS patients. The pathophysiological changes in AQP4 antibody‐positive NMOSD patients were not limited to the central nervous system.

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Authors:
Z. G. Chen, J. Huang, R. Fan, R. H. Weng, R. T. Shinohara, J. R. Landis, Y. Chen and Y. Jiang
Article first published online:
02 Dec 2019 | DOI: 10.1111/ene.14128

Original Article

Background and purpose

Genetic generalized epilepsies (GGEs) encompass a group of syndromes of mainly genetic causes, characterized by the involvement of both hemispheres. MicroRNAs (miRNAs) are small non‐coding RNAs with a critical role in the regulation of neuronal biological processes through gene expression modulation. Dysregulated miRNA expression has been shown in epilepsy. Due to their stability in biological fluids like serum, miRNAs have assumed a prominent role in biomarker research. Our aim was to evaluate circulating levels of three miRNAs in GGE patients and assess their putative diagnostic value.

Methods

MiR‐146a, miR‐155 and miR‐132 were quantified by real‐time polymerase chain reaction in the serum of 79 GGE patients (47 women, 32 men, 35.1 ± 12.4 years) and 67 healthy individuals (41 women, 26 men, 42.4 ± 10.1 years). Relative expression values were calculated using the 2 method. Receiver operating characteristic curve analysis was performed to assess diagnostic value. MiRNA expression was correlated with clinicopathological features.

Results

Serum levels of miR‐146a and miR‐155 were significantly upregulated in GGE patients relative to controls (3.13 and 6.05, respectively). Combined miR‐146a, miR‐155 and miR‐132 serum levels performed well as a diagnostic biomarker, discriminating GGE patients from controls with an area under the curve of 0.85, 80% specificity and 73% sensitivity.

Conclusions

Our results indicate that miR‐146a, miR‐155 and miR‐132 may partake in GGE epileptogenesis. A panel of three circulating miRNAs with potential value as a GGE biomarker is reported for the first time. Novel biomarkers may help to identify new treatment targets and contribute to improved patients’ quality of life through earlier diagnosis and a more precise prognosis.

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Authors:
R. Martins‐Ferreira, J. Chaves, C. Carvalho, A. Bettencourt, R. Chorão, J. Freitas, R. Samões, D. Boleixa, J. Lopes, J. Ramalheira, B. M. da Silva, A. Martins da Silva, P. P. Costa and B. Leal
Article first published online:
15 Dec 2019 | DOI: 10.1111/ene.14129

Original Article

Background and purpose

Amyotrophic lateral sclerosis (ALS) is increasingly recognized as a multisystem disorder with 30%–50% of patients exhibiting cognitive impairment. The pathophysiological mechanisms of cognitive dysfunction are probably multifactorial although hypoventilation secondary to respiratory dysfunction may contribute to cognitive decline. The current study aimed to identify the relationship between respiratory function in ALS patients and the presence and degree of cognitive impairment.

Methods

Amyotrophic lateral sclerosis patients were prospectively recruited from a multidisciplinary ALS clinic. Baseline clinical assessments including respiratory function as assessed by spirometry were recorded with forced vital capacity (FVC) ≤ 75% considered to be reduced respiratory function. Cognitive testing was performed utilizing the Addenbrooke’s Cognitive Examination (ACE) and the Mini‐Mental State Examination (MMSE).

Results

From a cohort of 100 ALS patients, 48% were categorized as having impaired respiratory function (FVC = 58.24% ± 2.15%) whilst 52% had normal function (88.65% ± 1.27%). Compared to the group with normal respiratory function (ACE 90.68 ± 0.89, MMSE 28.22 ± 0.21), patients with respiratory dysfunction had significantly reduced cognitive function (ACE 86.83 ± 1.5,  = 0.025; MMSE 26.29 ± 0.45,  = 0.029). Furthermore, subscores demonstrated significant differences between the groups with respect to domains in memory ( = 0.003) and attention ( = 0.05) with a trend observed in fluency ( = 0.082). There was a significant correlation between patient baseline FVC and ACE scores as well as between FVC and memory and fluency subscores ( < 0.01).

Conclusion

Amyotrophic lateral sclerosis patients with respiratory compromise were more likely to develop reduced cognitive function. In addition to improving physical function, it remains plausible that non‐invasive ventilation may alter the progression of cognitive impairment in ALS patients and potentially improve overall quality of life and carer burden.

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Authors:
W. Huynh, L. E. Sharplin, J. Caga, E. Highton‐Williamson and M. C. Kiernan
Article first published online:
11 Dec 2019 | DOI: 10.1111/ene.14130

Original Article

Background and purpose

The aim was to assess the value of insoluble PABPN1 muscle fibre nuclei accumulation in the diagnosis of atypical cases of oculopharyngeal muscular dystrophy (OPMD).

Methods

Muscle biopsies from a selected cohort of 423 adult patients from several Italian neuromuscular centres were analysed by immunofluorescence: 30 muscle biopsies of genetically proven OPMD, 30 biopsies from patients not affected by neuromuscular disorders, 220 from genetically undiagnosed patients presenting ptosis or swallowing disturbances, progressive lower proximal weakness and/or isolated rimmed vacuoles at muscle biopsy and 143 muscle biopsies of patients affected by other neuromuscular diseases.

Results

The detection of insoluble nuclear PABPN1 accumulation is rapid, sensitive (100%) and specific (96%). The revision of our cohort allowed us to discover 23 new OPMD cases out of 220 patients affected with nonspecific muscle diseases.

Conclusions

Oculopharyngeal muscular dystrophy is often misdiagnosed leading to diagnosis delay, causing waste of time and resources. A great number of these cases present symptoms and histological findings frequently overlapping with other muscle diseases, i.e. inclusion body myositis and progressive external ophthalmoplegia. PABPN1 nuclear accumulation is a reliable method for diagnostic purposes and it is safe and useful in helping pathologists and clinicians to direct genetic analysis in the case of suspected OPMD, even when clinical and histological clues are deceptive.

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Authors:
V. Galimberti, R. Tironi, A. Lerario, M. Scali, R. Del Bo, C. Rodolico, T. Brizzi, S. Gibertini, L. Maggi, M. Mora, A. Toscano, G. P. Comi, M. Sciacco, M. Moggio and L. Peverelli
Article first published online:
15 Dec 2019 | DOI: 10.1111/ene.14131

Original Article

Background and purpose

The pathophysiology of Parkinson’s disease (PD) remains unclear. Voxel‐based morphometry (VBM) detects local structural differences in brain tissue such as grey matter volume (GMV) between groups, which is helpful in understanding the pathophysiology of PD. Published VBM studies of GMV changes in PD have shown inconsistent results. Therefore, a voxel‐wise meta‐analysis of VBM studies was conducted to detect consistent GMV changes in PD.

Methods

The published literature was searched comparing whole‐brain GMV between PD patients and healthy controls (HCs) using VBM. Coordinates were extracted for the clusters of significant GMV differences between PD patients and HCs. The meta‐analysis was performed by seed‐based mapping software.

Results

A total of 63 studies with 2867 PD patients and 1990 HCs were included. Significant GMV reductions in some brain regions were detected in PD patients, which were involved in the basal ganglia, theory of mind, vocal and visual networks. These findings remained largely unchanged in the jackknife sensitivity analysis, and no significant heterogeneity or publication bias was detected.

Conclusions

Parkinson’s disease patients have GMV reductions in a number of brain regions involved in specific networks. These findings provide morphological evidence for the pathophysiology of PD.

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Authors:
X. Xu, Q. Han, J. lin, L. Wang, F. Wu and H. Shang
Article first published online:
23 Dec 2019 | DOI: 10.1111/ene.14132

Original Article

Background and purpose

Chronic inflammatory demyelinating polyradiculoneuropathy (CIDP) is a heterogeneous autoimmune disorder critically lacking diagnostic biomarkers. Autoantibodies to nodal and paranodal components have recently been described in a small subset of patients. Here, the diagnostic value of immune reactivity toward the myelin compartment was investigated.

Methods

Ninety‐four French CIDP patients were retrospectively studied. The reactivity toward the peripheral nerve was investigated. Sural nerve biopsies were examined by electron microscopy and immunofluorescence.

Results

Twenty‐one patients (22%) and three patients (3%) presented with a strong immunoglobulin G or immunoglobulin M reactivity respectively against the myelin compartment. The clinical, electrophysiological and morphological features were examined in nine of these patients for whom sural nerve biopsies were available. Seven patients were electrodiagnosed with definite CIDP, one with possible CIDP and one was unclassifiable but sural nerve biopsy argued for CIDP diagnosis. Electron microscopy of sural nerve biopsies demonstrated the presence of macrophage‐mediated demyelination restricted to the internode in all nine patients. Immunolabelling for voltage‐gated sodium channels, myelin and axonal markers confirmed the presence of segmental demyelination and of remyelination. The nodal and paranodal regions, however, were unaffected in these patients. Nerve conduction studies corroborated the multifocal and segmental profile, and seven patients showed increased duration of proximal (1.5–5.1 times) and/or distal (1.2–3.4 times) compound muscle action potential in at least two nerves.

Conclusion

Antibody‐ and macrophage‐mediated demyelination appears responsible for conduction alterations in CIDP patients and nerve immunostaining assays may serve as a supportive diagnostic biomarker.

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Authors:
J.‐M. Vallat, S. Mathis, E. Vegezzi, L. Richard, M. Duchesne, G. Gallouedec, P. Corcia, L. Magy, A. Uncini and J. Devaux
Article first published online:
22 Dec 2019 | DOI: 10.1111/ene.14133

Original Article

Background and purpose

Previous investigations show that bilinguals exhibit the first symptoms of dementia 4–5 years later than monolinguals. Therefore, bilingualism has been proposed as a cognitive reserve mechanism. Recent studies have advanced towards an understanding of the brain mechanisms underlying bilingualism’s protection against dementia, but none of them deals with white matter (WM) diffusion.

Methods

In this study, the topic was investigated by measuring WM integrity in a sample of 35 bilinguals and 53 passive bilinguals with mild cognitive impairment.

Results

No significant differences were found between the groups in cognitive level, education, age or sex. However, bilinguals showed higher mean diffusivity in the fornix, but higher fractional anisotropy, lower mean diffusivity, axial diffusivity and radial diffusivity in the parahippocampal cingulum, and lower radial diffusivity in the right uncinate fasciculus. Significant correlations were also found between WM integrity in the left parahippocampal cingulum and the Boston Naming Test in passive bilinguals.

Conclusions

These results suggest that bilingualism contributes to a differential pattern of WM disintegration due to mild cognitive impairment in fibers related to bilingualism and memory.

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Authors:
L. Marin‐Marin, V. Costumero, V. Belloch, J. Escudero, M. Baquero, M.‐A. Parcet and C. Ávila
Article first published online:
03 Jan 2020 | DOI: 10.1111/ene.14135

Original Article

Background and purpose

Little is known about the long‐term association between transient ischaemic attack (TIA) and stroke. Therefore, the goal of this study was to analyze the long‐term risk of stroke and associated predictors in a large cohort of TIA patients followed in general practices in Germany.

Methods

This study included patients with an initial TIA diagnosis and subsequently followed up in one of 1262 general practices in Germany between January 2007 and December 2016 ( = 19 824 patients). The primary outcome of the study was the risk of ischaemic stroke within 10 years of the initial diagnosis of TIA. The secondary outcome was the identification of demographic, clinical and pharmaceutical variables significantly associated with stroke in TIA patients.

Results

Within 10 years of the initial TIA diagnosis, 18.3% of individuals were diagnosed with stroke. Age was positively associated with stroke, with hazard ratios ranging from 1.88 in patients aged 51–60 years to 4.00 in those aged >80 years (reference group: patients aged ≤50 years). Furthermore, male sex, hypertension, diabetes mellitus, atrial fibrillation and ischaemic heart diseases had an additional impact on the risk of stroke. Finally, new oral anticoagulants, heparins, diuretics, angiotensin II receptor blockers and platelet aggregation inhibitors were identified as protective factors.

Conclusions

In a cohort of almost 20 000 TIA patients, 18.3% were diagnosed with stroke within 10 years after the TIA index event. Several demographic, clinical and pharmaceutical variables significantly predicted the long‐term risk of stroke in TIA patients.

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Authors:
L. Jacob, C. Tanislav and K. Kostev
Article first published online:
26 Dec 2019 | DOI: 10.1111/ene.14136

Original Article

Background and purpose

Transorbital sonography (TOS) has emerged as promising imaging method for the diagnosis and follow‐up of acute optic neuritis (ON). Available studies report an increase in the optic nerve diameter (OND) and the optic nerve sheath diameter (ONSD) in the case of a first episode of ON in the affected eye compared to either the contralateral unaffected eye or controls. However, the utility of TOS in the case of recurrent episodes of ON has never been assessed.

Methods

In our prospective cohort study, the diagnostic utility of TOS in patients with demyelinating diseases of the central nervous system was assessed, and the association between TOS, optical coherence tomography (OCT) and visual evoked potentials was examined further.

Results

Seventy‐eight patients with a history of demyelinating disorders of the central nervous system (mean age 38.2 ± 14.2 years; 24% with acute ON) were included. No differences in the OND (3.2 ± 0.5 mm vs. 3.2 ± 0.4 mm) and ONSD (5.1 ± 0.8 mm vs. 5.1 ± 0.7 mm) measurements were found between patients with and without acute ON. Papillary swelling was more frequent in patients with acute ON (14.2% vs. 1.5%,  = 0.002). Patients with a history of previous ON were found to have lower OND ( < 0.001) and ONSD ( = 0.007) compared to patients without a history of previous ON. TOS measurements were inversely associated with disease duration and positively correlated with OCT findings. No association with visual evoked potential measurements was found.

Conclusion

No evidence was found for TOS‐sensitive differences in the OND and ONSD of patients with demyelinating diseases, according to the presence of acute ON. The association between TOS and OCT measurements deserves further investigation.

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Authors:
C. Schroeder, A. H. Katsanos, I. Ayzenberg, C. Schwake, A. Gahlen, G. Tsivgoulis, K. Voumvourakis, R. Gold and C. Krogias
Article first published online:
26 Dec 2019 | DOI: 10.1111/ene.14137

Original Article

Background and purpose

Previous studies have reported conflicting results regarding possible anticipation in familial E200K Creutzfeldt–Jakob disease (fCJD). Our objective was to use a large database to assess the age of disease onset (AODO) in CJD.

Methods

The study population included 477 CJD patients [266 with fCJD, 145 with sporadic CJD (sCJD) and 66 patients of Libyan origin but negative family history] from the Israeli registry of CJD conducted since 1954. In all patients, AODO in relatives and family trees was documented. Comparison of AODO was done using a paired test and regression using Pearson correlation for birth and year of onset.

Results

The initial analysis in 52/73 families in which more than one generation was affected revealed an AODO of 63.30 ± 9.44 in the first generation compared to 56.96 ± 8.99 in the second generation ( < 0.001). However, inspection of individual AODO values plotted by year of birth showed a clear rhomboid methodological artifact generated by missing data of many young onset CJD patients who died before the database began to function in 1954 and of many late onset CJD patients missing at the present time since they will only develop the disease in the future. The ‘generation’ effect completely disappears if analysis is performed by year of disease onset or for the periods in which complete data are available.

Conclusions

In this very large dataset, true anticipation in fCJD patients was not detected. It is plausible that previous reports supporting the presence of anticipation are biased by a rhomboid‐shaped data availability artifact.

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Authors:
O. S. Cohen, E. Kahana, A. D. Korczyn, T. Ziv‐Baran, Z. Nitsan, S. Appel, H. Rosenmann and J. Chapman
Article first published online:
03 Feb 2020 | DOI: 10.1111/ene.14138

Original Article

Background and purpose

Autoimmune encephalitides (AE) include a spectrum of neurological disorders whose diagnosis revolves around the detection of neuronal antibodies (Abs). Consensus‐based diagnostic criteria (AE‐DC) allow clinic‐serological subgrouping of AE, with unclear prognostic implications. The impact of AE‐DC on patients’ management was studied, focusing on the subgroup of Ab‐negative‐AE.

Methods

This was a retrospective multicenter study on patients fulfilling AE‐DC. All patients underwent Ab testing with commercial cell‐based assays (CBAs) and, when available, in‐house assays (immunohistochemistry, live/fixed CBAs, neuronal cultures) that contributed to defining final categories. Patients were classified as Ab‐positive‐AE [‐methyl‐‐aspartate‐receptor encephalitis (NMDAR‐E), Ab‐positive limbic encephalitis (LE), definite‐AE] or Ab‐negative‐AE (Ab‐negative‐LE, probable‐AE, possible‐AE).

Results

Commercial CBAs detected neuronal Abs in 70/118 (59.3%) patients. Testing 37/48 Ab‐negative cases, in‐house assays identified Abs in 11 patients (29.7%). A hundred and eighteen patients fulfilled the AE‐DC, 81 (68.6%) with Ab‐positive‐AE (Ab‐positive‐LE, 40; NMDAR‐E, 32; definite‐AE, nine) and 37 (31.4%) with Ab‐negative‐AE (Ab‐negative‐LE, 17; probable/possible‐AE, 20). Clinical phenotypes were similar in Ab‐positive‐LE versus Ab‐negative‐LE. Twenty‐four/118 (20.3%) patients had tumors, and 19/118 (16.1%) relapsed, regardless of being Ab‐positive or Ab‐negative. Ab‐positive‐AE patients were treated earlier than Ab‐negative‐AE patients ( = 0.045), responded more frequently to treatments (92.3% vs. 65.6%,  < 0.001) and received second‐line therapies more often (33.3% vs. 10.8%,  = 0.01). Delays in first‐line therapy initiation were associated with poor response ( = 0.022; odds ratio 1.02; confidence interval 1.00–1.04).

Conclusions

In‐house diagnostics improved Ab detection allowing better patient management but was available in a patient subgroup only, implying possible Ab‐positive‐AE underestimation. Notwithstanding this limitation, our findings suggest that Ab‐negative‐AE and Ab‐positive‐AE patients share similar oncological profiles, warranting appropriate tumor screening. Ab‐negative‐AE patients risk worse responses due to delayed and less aggressive treatments.

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Authors:
M. Gastaldi, S. Mariotto, M. P. Giannoccaro, R. Iorio, M. Zoccarato, M. Nosadini, L. Benedetti, S. Casagrande, M. Di Filippo, M. Valeriani, S. Ricci, S. Bova, C. Arbasino, M. Mauri, M. Versino, F. Vigevano, L. Papetti, M. Romoli, C. Lapucci, F. Massa, S. Sartori, L. Zuliani, A. Barilaro, P. De Gaspari, G. Spagni, A. Evoli, R. Liguori, S. Ferrari, E. Marchioni, B. Giometto, L. Massacesi and D. Franciotta
Article first published online:
14 Jan 2020 | DOI: 10.1111/ene.14139

Original Article

Background and purpose

The purpose was to examine the consequences of antiepileptic drug (AED) exposure during pregnancy on language abilities in children aged 5 and 8 years of mothers with epilepsy.

Methods

The study population included children of mothers with and without epilepsy enrolled in the Norwegian Mother and Child Cohort Study 1999–2008. Mothers prospectively provided information on epilepsy diagnosis, AED use during pregnancy and the child’s language abilities at age 5 and 8 years, in questionnaires with validated language screening tools. AED concentrations in gestation week 17–19 and in the umbilical cord were measured.

Results

The study population included 346 AED‐exposed and 388 AED‐unexposed children of mothers with epilepsy, and 113 674 children of mothers without epilepsy. Mothers of 117 and 121 AED‐exposed children responded to the questionnaires at age 5 and 8 years, respectively. For AED‐exposed children, the adjusted odds ratio for language impairment was 1.6 [confidence interval (CI) 1.1–2.5,  = 0.03] at age 5 years and 2.0 (CI 1.4–3.0,  < 0.001) at age 8 years, compared to children of mothers without epilepsy. Children exposed to carbamazepine monotherapy had a significantly increased risk of language impairment compared to control children at age 8 years (adjusted odds ratio 3.8, CI 1.6–9.0,  = 0.002). Higher maternal valproate concentrations correlated with language impairment at age 5 years. Periconceptional folic acid supplement use protected against AED‐associated language impairment.

Conclusion

Foetal AED exposure is associated with an increased risk of language impairment in children aged 5 and 8 years of mothers with epilepsy. Periconceptional folic acid use had a protective effect on AED‐associated language impairment.

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Authors:
E. S. N. Husebye, N. E. Gilhus, O. Spigset, A. K. Daltveit and M. H. Bjørk
Article first published online:
30 Dec 2019 | DOI: 10.1111/ene.14140

Original Article

Background and purpose

Drug‐resistant idiopathic generalized epilepsy (IGE) remains challenging despite a favourable overall prognosis of IGE, and little is known about basic epidemiology and long‐term outcome of drug‐resistant IGE. The aim of the study was to describe the incidence, prevalence and outcome of IGE in an unbiased, population‐based cohort.

Methods

In 2014–2018, all patients (≥17 years) with IGE inhabiting the island of Funen (496 000 inhabitants) were recruited. The socioeconomic and clinical information available for 406 individuals was assessed. Median follow‐up was 15 years.

Results

The average IGE incidence (2008–2017) was 2.9/100 000 inhabitants/year. The point prevalence of identifiable IGE patients was 1.0/1000 adults (juvenile myoclonic epilepsy 0.4/1000; absence epilepsy 0.3/1000, epilepsy with generalized tonic–clonic seizures alone 0.3/1000); 92.1% of the patients were diagnosed before 25 years of age. When correcting for unequal age distribution in the cohort, 1102 people on the island of Funen fulfilled the diagnostic criteria for IGE at the age of 25 (estimated prevalence 2.7/1000 adults). In the year before data closure, 121 patients reported seizures. Fifty patients met the definition of drug‐resistant IGE (12.1% of the cohort, 4.5% of the estimated 1102 IGE patients). The average seizure burden of all patients with drug‐resistant IGE was 2.2 generalized tonic–clonic seizures per year; only 14 patients suffered more than two generalized tonic–clonic seizures per year. Drug‐resistant IGE was associated with an increased risk of requiring treatment for affective disorders and a reduced probability of working full time.

Conclusion

Idiopathic generalized epilepsy was associated with a low risk of persistent drug‐resistant seizures requiring specialist medical attention. Drug resistance was associated with a negative socioeconomic outcome.

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Authors:
J. Gesche, J. Christensen, H. Hjalgrim, G. Rubboli and C. P. Beier
Article first published online:
03 Jan 2020 | DOI: 10.1111/ene.14142

Letter to the Editor

Do different treatment strategies of galcanezumab have a similar effect on migraine?

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Authors:
I.‐H. Huang, P.‐C. Wu, Y.‐H. Lee and Y.‐N. Kang
Article first published online:
03 Jan 2020 | DOI: 10.1111/ene.14143

Original Article

Background and purpose

This study was to investigate the prevalence and cardiovascular risk factors (CRFs) of asymptomatic intracranial atherosclerotic stenosis (aICAS) amongst middle‐aged and older adults living in rural communities in China.

Methods

This population‐based study included 2019 subjects (aged ≥40 years, 52.3% women) who were free of stroke and living in rural communities in China. From October 2017 to May 2018, data on demographics, CRFs and health conditions were collected through face‐to‐face interviews, physical examination and laboratory tests. Asymptomatic ICAS was detected through a two‐phase procedure: a screening phase with transcranial Doppler ultrasound, followed by a diagnostic phase with magnetic resonance angiography examination. Multivariable logistic regression models were used to analyse CRFs associated with aICAS.

Results

Of the 2019 participants, aICAS was detected in 153 persons. The overall prevalence of aICAS was 7.6%, and the prevalence of moderate‐to‐severe aICAS was 5.0%. The multi‐adjusted odds ratio (95% confidence interval) of aICAS associated with CRFs was 2.40 (1.56–3.69) for hypertension, 1.91 (1.32–2.76) for high hypersensitive C‐reactive protein, 1.68 (1.14–2.49) for diabetes and 1.61 (1.08–2.41) for overweight or obesity. When these four CRFs were aggregated, compared with participants without any of these factors, the multi‐adjusted odds ratios (95% confidence interval) of aICAS for persons concurrently having one, two and three or more of these factors were 1.14 (0.52–2.48), 2.91 (1.42–5.99) and 5.51 (2.64–11.50), respectively ( for linear trend <0.001).

Conclusions

Asymptomatic ICAS is common amongst rural‐dwelling middle‐aged and older Chinese people. Hypertension, diabetes, overweight or obesity and high hypersensitive C‐reactive protein, especially when coexisting, are strongly associated with aICAS.

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Authors:
Q. Sun, Q. Wang, X. Wang, X. Ji, S. Sang, S. Shao, Y. Zhao, Y. Xiang, Y. Xue, J. Li, G. Wang, M. Lv, F. Xue, C. Qiu and Y. Du
Article first published online:
26 Jan 2020 | DOI: 10.1111/ene.14144

Original Article

Background and purpose

Anaemia is associated with poor clinical outcome after ischaemic and haemorrhagic stroke. The association between anaemia and outcome in patients with cerebral venous thrombosis (CVT) was examined.

Methods

Consecutive adult patients with CVT were included from seven centres. Anaemia at admission was scored according to World Health Organization definitions. Poor clinical outcome was defined as a modified Rankin Scale score 3–6 at last follow‐up. A multiple imputation procedure was applied for handling missing data in the multivariable analysis. Using binary logistic regression analysis, adjustments were made for age, sex, cancer and centre of recruitment (model 1). In a secondary analysis, adjustments were additionally made for coma, intracerebral haemorrhage, non‐haemorrhagic lesion and deep venous system thrombosis (model 2). In a sensitivity analysis, patients with cancer were excluded.

Results

Data for 952 patients with CVT were included, 22% of whom had anaemia at admission. Patients with anaemia more often had a history of cancer (17% vs. 7%,  < 0.001) than patients without anaemia. Poor clinical outcome (21% vs. 11%,  < 0.001) and mortality (11% vs. 6%,  = 0.07) were more common amongst patients with anaemia. After adjustment, anaemia at admission increased the risk of poor outcome [adjusted odds ratio (aOR) 2.4, 95% confidence interval (CI) 1.5–3.7, model 1]. Model 2 revealed comparable results (aOR 1.9, 95% CI 1.2–3.2), as did the sensitivity analysis excluding patients with cancer (aOR 2.3, 95% CI 1.3–3.8, model 1).

Conclusion

The risk of poor clinical outcome is doubled in CVT patients presenting with anaemia at admission.

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Authors:
S. M. Silvis, E. Reinstra, S. Hiltunen, E. Lindgren, M. R. Heldner, M. Mansour, M. Ghiasian, K. Jood, S. M. Zuurbier, A. E. Groot, M. Arnold, M. A. Barboza, A. Arauz, J. Putaala, T. Tatlisumak and J. M. Coutinho
Article first published online:
24 Jan 2020 | DOI: 10.1111/ene.14148

Original Article

Background and purpose

To characterize the frequency and risk of serious infections in patients with myasthenia gravis (MG) relative to age/sex/area‐matched comparators.

Methods

This was a population‐based cohort study in Ontario, Canada of patients with newly‐diagnosed MG and 1:4 age/sex/area‐matched general population comparators accrued from 1 April 2002 to 31 December 2015. The main outcome was a serious infection, defined by a primary diagnosis code on a hospitalization or emergency department record. We computed crude overall and sex‐specific rates of infection among patients with MG and comparators, and the frequency of specific types of infection. Adjusted hazard ratios and 95% confidence intervals were estimated using Cox regression.

Results

Among 3823 patients with MG, 1275 (33.4%) experienced a serious infection compared with 2973/15 292 (19.4%) of comparators over a mean follow‐up of over 5 years. Crude infection rates among patients with MG were twice those in comparators (72.5 vs. 35.0 per 1000 person‐years, respectively). The most common infection types were respiratory infections, particularly bacterial pneumonia. After adjustment for potential confounders, MG was associated with a 39% increased infection risk (adjusted hazard ratio, 1.39; 95% confidence intervals, 1.28–1.51).

Conclusions

Patients with MG are at a significantly higher absolute and relative risk of serious infections compared with age/sex/area‐matched comparators. This needs to be considered when selecting MG treatments and when planning vaccination/prophylaxis. Determining whether this risk is due to the use of immunosuppressive medications (vs. MG itself) is an important area for future research.

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Authors:
C. D. Kassardjian, J. Widdifield, J. M. Paterson, A. Kopp, C. Nagamuthu, C. Barnett, K. Tu and A. Breiner
Article first published online:
17 Feb 2020 | DOI: 10.1111/ene.14153

Editorial

How can neurology be affected by the ‘100 Radical Innovation Breakthroughs for the Future’ report of the European Commission?

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Authors:
D. Leys
Article first published online:
26 Feb 2020 | DOI: 10.1111/ene.14166

Issue Information

Issue Information

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Authors:
Article first published online:
18 Mar 2020 | DOI: 10.1111/ene.14205