Qian Zhao1, Lichao Sun2, Boqi Hu3, Weihong Lin1. 1. Department of Neurology, Neuroscience Center. 2. Department of Emergency, The First Hospital of Jilin University. 3. Department of Radiology, China-Japan Friendship Hospital of Jilin University, Changchun, Jilin, China.
Abstract
RATIONALE: Nonconvulsive status epilepticus (NCSE) is a heterogeneous disease with multiple subtypes. NCSE poses great diagnostic and therapeutic challenges due to the lack of typical symptoms. Here, we report a case of NCSE manifesting as rapidly progressive dementia (RPD) and infarction in the splenium of the corpus callosum. Additionally, the relevant literature was reviewed. PATIENT CONCERNS: A 63-year-old man presented with RPD. Electroencephalogram (EEG) revealed NCSE, and brain magnetic resonance imaging (MRI) showed an isolated infarction in the splenium of the corpus callosum. Mini-mental state examination showed moderate cognitive impairment (14/30 points). DIAGNOSIS: A diagnosis of NCSE with RPD and infarction in the splenium of the corpus callosum was made. INTERVENTIONS: The patient was treated with intravenous diazepam (10 mg), oral levetiracetam (1.0g twice daily), oral sodium valproate (0.2g twice daily), and intramuscular phenobarbital sodium (0.2g once daily). OUTCOMES: After the treatment, the symptoms were improved. The patient could answer questions. Repeated EEG showed that the background a rhythm was slightly overdeveloped, and no clinical or electrical seizures were observed. After discharge, the patient was treated with oral levetiracetam (1.0g twice daily) and oral sodium valproate (0.2g twice daily) for 6 months. At the last follow-up, the patient had clear consciousness, sensitive response, and fluent answering ability. Repeated mini-mental state examination showed that his cognitive function was significantly improved (28/30 points); nevertheless, the lesion in the splenium of corpus callosum remained unchanged on MRI. LESSONS: NCSE manifesting as RPD and infarction in the splenium of the corpus callosum is extremely rare. Epileptic events and focal infarction are usually overlooked in patients with dementia, and the diagnostic value of MRI and EEG should be highlighted.
RATIONALE: Nonconvulsive status epilepticus (NCSE) is a heterogeneous disease with multiple subtypes. NCSE poses great diagnostic and therapeutic challenges due to the lack of typical symptoms. Here, we report a case of NCSE manifesting as rapidly progressive dementia (RPD) and infarction in the splenium of the corpus callosum. Additionally, the relevant literature was reviewed. PATIENT CONCERNS: A 63-year-old man presented with RPD. Electroencephalogram (EEG) revealed NCSE, and brain magnetic resonance imaging (MRI) showed an isolated infarction in the splenium of the corpus callosum. Mini-mental state examination showed moderate cognitive impairment (14/30 points). DIAGNOSIS: A diagnosis of NCSE with RPD and infarction in the splenium of the corpus callosum was made. INTERVENTIONS: The patient was treated with intravenous diazepam (10 mg), oral levetiracetam (1.0g twice daily), oral sodium valproate (0.2g twice daily), and intramuscular phenobarbital sodium (0.2g once daily). OUTCOMES: After the treatment, the symptoms were improved. The patient could answer questions. Repeated EEG showed that the background a rhythm was slightly overdeveloped, and no clinical or electrical seizures were observed. After discharge, the patient was treated with oral levetiracetam (1.0g twice daily) and oral sodium valproate (0.2g twice daily) for 6 months. At the last follow-up, the patient had clear consciousness, sensitive response, and fluent answering ability. Repeated mini-mental state examination showed that his cognitive function was significantly improved (28/30 points); nevertheless, the lesion in the splenium of corpus callosum remained unchanged on MRI. LESSONS: NCSE manifesting as RPD and infarction in the splenium of the corpus callosum is extremely rare. Epileptic events and focal infarction are usually overlooked in patients with dementia, and the diagnostic value of MRI and EEG should be highlighted.
Nonconvulsive status epilepticus (NCSE) refers to a distinct subtype of status epilepticus with no obvious tonic-clonic activity.[ This condition is clinically latent, and there are no typical onset symptoms. NCSE often occurs following a coma or post-epileptic state, and it is usually underdiagnosed.[ Although there have been numerous reports of NCSE secondary to stroke, NCSE complicated with infarction in the splenium of the corpus callosum is exceedingly rare because of the rich blood supply of the corpus callosum.[ Rapidly progressive dementia (RPD) refers to dementia that progresses subacutely, typically over the course of weeks to months. RPD is caused by vascular occlusion in the corpus callosum or thalamus or multiple cerebral infarctions, and some of RPD cases are reversible and curable.[ According to the literature, epilepsy with higher brain dysfunction is associated with dementia; for example, temporal lobe epilepsy can lead to memory loss or behavioral abnormalities, which is similar to Alzheimer disease or frontotemporal dementia. Epilepsy with higher brain dysfunction can be classified into a transient subtype and a persistent subtype, and the latter form is caused by NCSE or antiepileptic drug-responsive neurofunctional impairment.[ Currently, NCSE poses great diagnostic and therapeutic challenges due to the lack of typical symptoms. In the present report, we present a case of NCSE manifesting as RPD and irreversible infarction in the splenium of the corpus callosum and review the relevant literature.
Case report
A 63-year-old man presented to us with RPD. Twenty days previously, the patient developed lags in response. However, other behaviors were normal, and he was able to take care of himself. Five days before admission, the symptom was aggravated, and the intermittent attacks were frequent (4–5 episodes per day; each episode lasted for approximately 5 minutes). The patient could not recognize common objects or answer questions accurately. He was completely normal during the interictal period. Brain computed tomography showed no remarkable abnormalities. During the previous 5 days, the patient developed severe paroxysmal headache (7–8 episodes per day). Physical examination revealed fuzzy consciousness and slow response. There was no dysarthria, cranial nerve paresis, or motor function disturbance, and bilateral pathological signs were negative. Cerebrospinal fluid examination after lumbar puncture showed a slightly increased protein level (0.93 g/dL; normal range, 0.15–0.45 g/dL), an increased glucose level (4.8 mmol/L; normal range, 2.3–4.1 mmol/L), and an elevated leukocyte count (9 × 106/L; normal range, (0–8) × 106/L). Antibodies against autoimmune encephalitis and 1433 protein and paraneoplastic antibodies were negative. Mini-mental state examination showed moderate cognitive impairment (14/30 points). Electroencephalogram (EEG) monitored spike and spike-slow waves (4–6 Hz) originating from the left temporal area (F7/T3/T1) during the ictal period (lasting for 6–30 seconds; Fig. 1). Brain magnetic resonance imaging (MRI) showed an isolated lesion in the splenium of the corpus callosum with hyperintensity on diffusion-weighted imaging and hypointensity on the apparent diffusion coefficient map (Fig. 2). A diagnosis of NCSE with RPD and infarction in the splenium of the corpus callosum was made. The patient was treated with intravenous diazepam (10 mg), oral levetiracetam (1.0 g twice daily), oral sodium valproate (0.2 g twice daily), and intramuscular phenobarbital sodium (0.2 g once daily). After the treatment, the symptoms were improved. The patient could answer questions. Repeated EEG showed that the background α rhythm was slightly overdeveloped, and no clinical or electrical seizures were observed (Fig. 3). After discharge, the patient was treated with oral levetiracetam (1.0 g twice daily) and oral sodium valproate (0.2 g twice daily) for 6 months. At the last follow-up, the patient had clear consciousness, sensitive response, and fluent answering ability. Repeated mini-mental state examination showed that his cognitive function was significantly improved (28/30 points); nevertheless, the lesion in the splenium of corpus callosum remained unchanged on MRI (Fig. 4).
Figure 1
Electroencephalogram on admission. Electroencephalogram monitored spike and spike-slow waves (4–6 Hz) originating from the left temporal area (F7/T3/T1) during the ictal period (lasting for 6–30 s).
Figure 2
Brain magnetic resonance imaging on admission. Brain magnetic resonance imaging showed an isolated lesion in the splenium of the corpus callosum with hypointensity on T1-weighted imaging (A) and the apparent diffusion coefficient map (F) and hyperintensity on T2-weighted imaging (B), and diffusion-weighted imaging (C).
Figure 3
Electroencephalogram after treatment. Electroencephalogram after treatment showed the background α rhythm was slightly overdeveloped, but no clinical or electrical seizures were observed.
Figure 4
Brain magnetic resonance imaging after a 6-mo follow-up. Brain magnetic resonance imaging showed an isolated lesion in the splenium of the corpus callosum with hypointensity on T1-weighted imaging (A) and the apparent diffusion coefficient map (D) and hyperintensity on T2-weighted imaging (B), diffusion-weighted imaging (C).
Electroencephalogram on admission. Electroencephalogram monitored spike and spike-slow waves (4–6 Hz) originating from the left temporal area (F7/T3/T1) during the ictal period (lasting for 6–30 s).Brain magnetic resonance imaging on admission. Brain magnetic resonance imaging showed an isolated lesion in the splenium of the corpus callosum with hypointensity on T1-weighted imaging (A) and the apparent diffusion coefficient map (F) and hyperintensity on T2-weighted imaging (B), and diffusion-weighted imaging (C).Electroencephalogram after treatment. Electroencephalogram after treatment showed the background α rhythm was slightly overdeveloped, but no clinical or electrical seizures were observed.Brain magnetic resonance imaging after a 6-mo follow-up. Brain magnetic resonance imaging showed an isolated lesion in the splenium of the corpus callosum with hypointensity on T1-weighted imaging (A) and the apparent diffusion coefficient map (D) and hyperintensity on T2-weighted imaging (B), diffusion-weighted imaging (C).Reporting of this case was approved by the Ethics Committee of The First Hospital of Jilin University. Written informed consent was obtained from the patient's relatives.
Discussion
Clinical manifestations of NCSE are variable, with consciousness changes being the most common, and other symptoms include speech disturbances, myoclonic, behavioral abnormalities, anxiety, delirium, extrapyramidal symptoms, and hallucinations. In 2007, Kaplan proposed the EEG diagnostic criteria for adult NCSE.[ In addition to repeated extensive or focal spike waves, polyspike waves, sharp waves, spike-slow waves, and sharp-slow waves, EEG characteristics of NCSE should include:rhythmic (θ-δ) waves with a frequency ≥0.50 Hz and alterations in amplitude and/or frequency,a pattern change with a frequency change >1 Hz or position change, andbackground waves with a decreased amplitude and/or frequency following periodic discharges.[EEG monitoring is the gold standard for the diagnosis of NCSE.[Status epilepticus is usually underdiagnosed, especially in patients without convulsive episodes. When patients with NCSE are admitted to the emergency room, EEG is usually not available. For these cases, experimental usage of intravenous benzodiazepines may facilitate the diagnosis. Notably, the cognitive symptoms of NCSE may be improved several months after the administration of benzodiazepines.[ In the current case, the patient developed lags in response 20 days before admission, and then the symptom was aggravated. The clinical manifestation and EEG evidence supported a diagnosis of NCSE.NCSE can be associated with stroke in the acute and chronic stages. However, the infarction in the splenium of the corpus callosum is uncommon in patients with NCSE. MRI is the optimal modality for the diagnosis of corpus callosum infarction. As previously reported, the incidence of acute corpus callosum infarction is 2.3%, and the negative rate of computed tomography examination was 76.4% even 24 hours after onset.[ The corpus callosum, located at the base of the longitudinal fissure of the brain, is the largest connective fibers in the central nervous system and connects the neocortex in the bilateral hemispheres. The splenium of the corpus callosum is the posterior part of the corpus callosum, which connects the temporal and occipital lobes. In the previous literature, the infarction often occurs in the genu or body of the corpus callosum.[ David et al reported 5 patients with corpus callosum infarction. They found the infarction only involved the genu or body of the corpus callosum; none involved the splenium of the corpus callosum. They hypothesized that this phenomenon might be due to the difference in the patient population.[ Corpus callosum infarction is caused by hemodynamic changes secondary to cerebral arteriosclerosis, and clinical manifestations mainly include speech disorders and cognitive impairment. The subcallosal artery supplies the beak and genu of the corpus callosum as well as the anterior fornix, and its occlusion causes acute loss of short-term memory, which is known as “amnestic syndrome of the subcallosal artery” and appear “cup sign” on MRI.[ Rabinstein et al reported a case of RPD caused by bilateral internal carotid artery occlusion with infarction of the whole corpus callosum.[ These findings support that RPD may be caused by occlusion of large vessels in the thalamus and corpus callosum. Zhang et al reported 2 cases of infarction in the splenium of the corpus callosum; both patients presented with sudden cognitive impairment and sensorimotor dysfunctions in the right limb.[ Notably, in the above studies, no NCSE was observed, and the reversibility of the infarction in the splenium of the corpus callosum was not reported. In the current case, the splenium infarction was irreversible.At present, there is no consensus on the definition and diagnostic criteria of RPD. Kelley et al believed that RPD progresses from clinical onset to severe dementia or death within 18 months.[ Geschwind et al proposed that RPD progresses to dementia within 1 to 2 years after clinical onset, typically over the course of weeks to months.[ Papageorgiou et al considered that RPD is a subtype of dementia with obvious cognitive impairment within a few months, and RPD cases with a clinical course of <3 years were included in their study.[ Meanwhile, Josephs et al found that the survival time of RPD is less than 4 years, generally 0.2 to 3.5 years.[ Geschwind et al investigated the etiology of RPD and found that 62% of all RPDs were prion diseases, 15% were neurodegenerative diseases, 8% were autoimmune diseases, 4% were infectious diseases, and 2% were other diseases (such as neoplastic, metabolic, psychiatric, and vascular diseases).[NCSE with concomitant RPD is rarely reported. NCSE is most commonly associated with focal epileptic seizures with impaired consciousness, and one of the main clinical manifestations is an acute confusional state.[ As a potential cause of consciousness changes in the elderly, NCSE should be included in the differential diagnoses for patients with rapid cognitive decline.[ Cordonnier and Reuck hypothesized that epilepsy and new-onset dementia may be caused by changes in white matter, asymptomatic infarcts, and microbleeds, and that poststroke seizures are independent predictors of new-onset dementia.[ Epileptic seizures can occur in 3.6% of individuals with dementia, and it is often difficult to recognize when the clinical manifestations are only slight behavioral changes.[ In the previous literature, some epileptic patients developed reversible splenial lesion syndrome.[ However, in the current case, the infarction in the splenium of the corpus callosum was irreversible, which is different from reversible splenial lesion syndrome.
Conclusion
NCSE manifesting as RPD and infarction in the splenium of the corpus callosum is extremely rare. Clinicians should be aware of this distinct condition. Epileptic events and focal infarction are commonly overlooked in patients with dementia, and the diagnostic value of MRI and EEG should be highlighted.
Authors: Lara Pardina-Vilella; Ana Pinedo-Brochado; Iñigo Vicente; Jone Bocos-Portillo; Amaia Martínez-Arroyo; Jose Maria Ontañon; Marian Gómez-Beldarrain; Juan Carlos García-Moncó Journal: Neurol Sci Date: 2018-05-01 Impact factor: 3.307
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