Temporal Lobe Epilepsy in the Elderly

Morillo, L. E.

doi:https://doi.org/10.1155/2012/641323

Epilepsy Research and Treatment

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Volume 2012 | Article ID 641323 | https://doi.org/10.1155/2012/641323

Temporal Lobe Epilepsy in the Elderly

L. E. Morillo^1,2

Academic Editor: Seyed M. Mirsattari

Received03 Aug 2011

Revised20 Sept 2011

Accepted09 Oct 2011

Published24 Nov 2011

Abstract

The incidence of epilepsy has bimodal distribution peaking at the extremes of life. Incidence is greater in younger and older age groups (Hauser et al., 1993, Sidenvall et al., 1993, Forsgren et al., 1996, and Olafsson et al., 2005). As the world population ages more elders with epilepsy will be identified. In the high-income countries with longer life expectancy, the number of elders with epilepsy will be even higher. CPSs account for 40% of all seizure types in the elderly (Hauser et al., 1992); however, the proportion with temporal lobe epilepsy (TLE) is uncertain.

1. Causes

The specific causes of TLE in the elderly have not been clearly disclosed. With advancing age underlying coexisting factors are more likely to be identified, and the proportion of people classified as idiopathic is less when compared to the younger age groups. Nonetheless, up to half of elderly patients with epilepsy go without an identified cause.

In the under 65-year age group, head trauma, brain tumors, and CNS infections are common associations. Etiology of seizures veers towards a cerebrovascular origin in the elderly [6]. Dementing illnesses have also taken their place as a significant etiology [7].

Idiopathic TLE has been reported in adults with familiar history of epilepsy (mean age of onset: 25.5; range: 11–45 years). This group was also found to have a better prognosis [8]. Similar reports in elderly patients are missing. There are however case reports of mesial temporal lobe sclerosis (MTS) in elderly persons with new onset seizures. These accounts highlight the challenging differential diagnosis overlap with primary cognitive disorders and nonparaneoplastic limbic encephalitis [9]. New onset TLE has also been reported without evidence of MTS [10].

The etiology of hippocampal damage is discussed in a retrospective study of 38 patients with adult onset TLE [11]. The median age at onset was 37.8 years (range: 21.0 to 78.7 years). A total of seven patients, 60 years and older, were included in this report. In all cases, the common features encompass frequent CPSs (range <1 to 600 seizures per month) developing over one year (defined as the median time from the initial onset of seizures to the time of assessment). Based on MRI evidence of hippocampal atrophy, history of causative events, concomitant disease, cerebrospinal fluid results, and autoantibodies patients were classified in one of four etiologic categories; secondary hippocampal sclerosis (HS); idiopathic HS; definite limbic encephalitis (LE) and MRI defined possible LE. Eleven patients met secondary HS criteria. Three had presented prolonged seizures and one nonprolonged repetitive seizures. In this subgroup, 36% showed bilateral MRI hippocampal abnormalities. Two patients had experienced a severe head trauma; two, old infarct; one a porencephalic cyst and one neurofibromatosis type I. Only two patients in this subgroup were 60 years and older. One showed bilateral hippocampal atrophy after head trauma and the other was unilateral. The latter reported 500 seizures per month. In the idiopathic HS group, all seven subjects had unilateral hippocampal abnormalities. Four underwent selective amygdalohippocampectomy and histopathology confirmed HS. In this subgroup of idiopathic HS, none of the seven patients were 60 years or older. Definite LE included nine patients with 5 (56%) showing bilateral hippocampal abnormalities on MRI. Six of the nine patients had sequential MRIs with initial hippocampal swelling, followed by normalization and ultimately atrophy and high-intensity signal. In addition to seizures, memory impairment was clinically significant. Four patients had positive voltage gated potassium channel antibodies (VGKC abs) and one anit-Hu antibodies. The remaining four patients were diagnosed with rectal, small cell lung cancer (SCLC), testicular tumor with Ma2 antibodies, and a uterine leiomyosarcoma, respectively. In this subgroup of definite LE, three patients were 60 years and older. All three showed bilateral MRI hippocampal abnormalities. VGKC abs, rectal cancer, and small cell lung cancer were documented in one patient each. Finally, 11 patients were classified as MRI defined possible LE based on repeated MRIs with initial hippocampal swelling, normalization and atrophy, and absence of malignancy or antibodies (one exception with atypical anti-Hu antibodies). Seven (63%) showed bilateral MRI changes. This subgroup also presents episodic memory impairment and affective disturbances. Two patients, 60 years and older, were included, both with unilateral hippocampal involvement. This report delineates idiopathic and secondary HS as well as paraneoplastic and non-paraneoplastic LE as causative factors of late onset TLE emphasizing bilateral HS in the latter two subgroups, however, not infrequent with secondary HS. Memory impairment was more common with bilateral HS and in all cases frequent CPSs developed over a relatively short period of time. The few elderly subjects included in this series appear to follow these general premises.

A potential etiologic factor of TLE in the elderly is represented in generalized convulsive status epilepticus (GCSE) recognized to occur more often in the elderly with an estimated incidence of 86 per 100000 [12, 13]. A complication of GCSE is subsequent damage to the hippocampus [14, 15]. Mortality after GCSE is significant. Survivors would be at risk of subsequent partial seizures originating after hippocampal damage [16].

2. Clinical Presentation

The clinical features of various partial seizure types have been recently reported comparing patients 55 years of age and older (mean ) to a group between 18 and 45 years of age (mean ); each group encompassed 55 consecutive subjects [17]. Diagnosis was based on clinical and/or EEG findings. Partial seizures with loss of awareness and lack of prominent automatisms were classified as dialeptic seizures and in the older group accounted for 60% of all focal seizures and 52% of the younger patients. Partial seizures with prominent mouth and/or hand automatisms happened in 18% of the older patients while in 14% of the younger group. These differences were not statistically significant. The authors did not specifically report on the localization of the origin of these seizures. In this series, baseline characteristics showed some relevant differences. Not surprisingly, the older group had a later age at seizure onset ( yrs versus yrs), seizure-free period greater than 1 year (20% versus 8%), and cerebral vascular disease as a risk factor (20% versus 6%). The younger group reported more than one seizure per month (54% versus 28%) and a history of febrile seizures (20% versus 6%). For the older and younger age groups, risk factors included trauma 30% in each group, CNS infection in 6% and 4% and CNS tumor in 8% and 6%. Among the 28 patients that had no recollection of their seizures, 17 (61%) were from the older age group. In total, 9 subjects (18%), all of the older age group, reported subtle perception of transient confusion (). The total number of subjects with aura (defined as partial seizures without loss of awareness) was less common in the older age group (54% versus 76% ). No significant differences could be demonstrated in the comparison of symptoms consisting of auras (psychic, autonomic, abdominal, visual, somatosensory or gustatory, auditory, olfactory, and vertigo) or generalized tonic clonic seizures (GTCSs) occurrence. Approximately one-third of patients in each group had a normal EEG, while 26% of the older group and 20% of the younger group had nonspecific finding. Focal epileptiform discharges were shown in 42% of the older and 23% of the younger subjects. Video-EEG monitoring was limited to a total of 9 patients yielding an additional 10% of older and 8% of younger patients with focal epileptiform and/or focal seizures.

In patients with epilepsy, memory dysfunction is not an unusual complaint. Transient epileptic amnesia is an emerging concept described in middle-aged and older people with an evident response to antiepileptic drug treatment (AED). Subjects with transient epileptic amnesia attacks may go unrecognized. A characteristic feature is prolonged periods of ante- and retrograde memory impairment with a mean duration between 30 and 60 minutes and subsequent amnesia that occurs upon awakening. The male population is more frequently affected. Transient amnesia may be the sole clinical manifestation in approximately one-third of patients. Attacks recur on the average 15 times per year. Hallucinations and automatisms have been frequently reported, while GTCSs are rare. Repetitive questioning is present in up to half of patients requiring differentiation from transient global amnesia. Interictal epileptiform abnormalities may be demonstrated in one-third of patients and ictal electrophysiological correlates have been recorded uni o bilaterally in the temporal lobes. Brain imaging is usually clear, or lesions involve the temporal lobe [18, 19].

Diagnosis is further challenged when symptoms of dementia compound the clinical picture. Alzheimer dementia may present with partial or generalized seizures and nonlocalizing EEG abnormalities. An overlap with memory complains is obviously expected in this group of cases [9].

The diagnosis of TLE in the elderly poses a challenge (see Table 1). The clinical features are subtle, and patients are unaware of seizures. Memory lapses, brief gaps in the flow of conversation, and blank stare and confusion may be the only clinical manifestations. Clinical features resemble TIA, delirium, congestive heart failure, cardiac arrhythmia, orthostatic hypotension, vasodepressor episodes, metabolic dysfunction with hypoglycemia, hyponatremia, sepsis, or drug toxicity [30].

3. Pharmacological Treatment

A small number of randomized controlled trials (RCTs) have been conducted in elderly patients testing the efficacy of AEDs. Studies do not specifically address TLE but serve to evaluate efficacy and safety issues of AEDs in the setting of epilepsy in the elderly.

Recently, a group of 77 people with a mean age of 68 years and partial onset seizures were randomized in a pilot study to topiramate (TPM) 50 mg or 200 mg doses as add-on or monotherapy. Etiology of seizures was identified in 52% of patients. Cerebrovascular causes and head trauma accounted for 40% and 33%, respectively. Seizure freedom was similar with the lower and higher doses (52% and 58%, resp.) as well as seizure frequency (0.26/month and 0.33/month, resp.). More than 60% in both study groups complained of adverse side effects with somnolence, dizziness, and headache being the most common. Overall 18% of patients had to discontinue TPM due to adverse effects [31].

One randomized controlled trial (RCT) tested carbamazepine (CBZ) versus lamotrigine (LMT) in a total of 64 subjects (mean age: 67 years) with partial seizures (simple or complex) with or without secondary generalization presenting on average between 8 and 12 months after stroke. Stroke was classified as cortical in 64% of patients allocated to LMT and 66.7% of the CBZ group. Subcortical strokes were diagnosed in 36% and 33.3%, respectively, in these study groups. Localization of the origin of the seizure was not reported. Subjects allocated to CBZ reported significantly more adverse effects than LMT leading to study withdrawal (31% versus 3%, ). On completion of the first year, 72% of patients on LMT and 44% on CBZ were seizure-free () [32].

A total of 590 elderly patients (mean age: 72 years) with newly diagnosed epilepsy with any seizure type were randomly allocated to gabapentin (GBP), LMT, or CBZ. In total, 42% of patients experienced CPSs. The etiology was similar among groups with an approximate one-third due to cerebral infarction. The localization of the origin of CPSs was not accounted for. A mild cognitive impairment or memory problems were present in 35% and 25% of patients, respectively. At 12 months, 46.7% had completed the study. LMT was significantly best retained than CBZ () or GBP (). At one year, seizure freedom was not significantly different between groups (LMT 51.4%, GBP 47.4%, and CBZ 64.3%). The time to first, second, fifth, and tenth seizure in the first year was also similar and no significant statistical differences were demonstrated between groups. Similarly, the overall seizure-free retention rate at one year was 24.9%. Severe adverse effects were reported in 8.1%. Weight gain was greatest with GBP, while hyponatremia and any rash with CBZ. Of the seven patients requiring hospital admission due to hypersensitivity reactions, one was due to LMT and six to CBZ. Thirty-nine subjects died during the study. In the one case, CBZ was stopped after a hypersensitivity reaction two weeks before death [33].

A total of 150 elderly people (mean age: 77 years) with any seizure type resulting from idiopathic, symptomatic, or cryptogenic epilepsies were included and randomized in a 2 : 1 ratio to either LMT or CBZ [34]. Cerebral infarction was disclosed in 30% of the LMT group and 38% in the CBZ group. In 79% the daily LMT median dose was 100 mg (range: 75–300 mg), and in 82% the daily CBZ median dose was 400 mg (range: 200–800 mg). Adverse effects forced 41% of dropouts with CBZ and 18% with LMT. Seizure freedom during the 16 weeks of the study period was significantly different favoring LMT over CBZ (39% versus 21%, ).

4. Surgery

Seizure outcome in 16 patients 50 years and older (mean 55.5 yrs, range 50–72) was compared to 184 younger patients (mean: 32.9 yrs, range: 16–49) undergoing anterior temporal lobectomy (ATL) [35]. All patients had pathologically confirmed unilateral HS and MRI lacked evidence of any other pathology. None of the variables showed to be predictors of the outcome. Following ATL older patients were less often seizure-free than the younger patients (56% versus 79%, ). Postsurgical complications were more frequent in the older patients (25% versus 4.4%, ).

Boling et al. reviewed 18 patients 50 years and older with 61% having MTS. The mean age at surgery was 54 years and followed for up to 64 months. Seizure freedom was reached by 61%, and 72% were able to reduce or stop their antiepileptic drugs. This older set of patients underwent multiple comparisons with subjects grouped in decades from ages 10 to 49 years. In the four resulting groups no significant differences could be demonstrated regarding proportions of seizure-free patients [36].

Sirven et al. reviewed a total of 30 patients aged 50 years and older (mean ) and compared them to 340 subjects younger than 50 years (mean ). These groups were followed for years and years, respectively. Seizure freedom was 52% in the older group and 75% in the younger group (). A discriminant function analysis disclosed that age at surgery and duration of epilepsy explained the largest fraction of variance. Younger age and shorter duration of epilepsy favored a seizure-freedom outcome. The authors consider that results could have been impacted by the fact that surgery in the older group was performed in their early 50’s with only 5 patients 59 years and older. In this retrospective analysis, MR images were not available for all patients [37].

5. Conclusions

As population grows, an increment is expected in the number of subjects 65 years and older identified with TLE. Countries with a longer life expectancy are going to be impacted to a greater extent. More often than not a coexisting significant medical condition may be revealed as well as acute or chronic brain involvement. Clinical diagnosis is elusive with subtle presenting features such as recurrent memory lapses or periods of confusion. Nevertheless, the typical signs of CPSs are likely. The undisputable advantage of video-EEG monitoring recognized in the investigation of people with epilepsy is clearly applicable to elderly populations [20–22, 38, 39]. AEDs continue to be the foundation of the medical pharmacological treatment.

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Copyright

Copyright © 2012 L. E. Morillo. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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