Acquired Epileptic Aphasia

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Acquired epileptic aphasia (AEA) typically develops in healthy children who acutely or progressively lose receptive and expressive language ability coincident with the appearance of paroxysmal electroencephalographic (EEG) changes. In 1957, Landau and Kleffner initially described acquired epileptic aphasia and subsequently reluctantly agreed to the attachment of their names to the syndrome. In this article, acquired epileptic aphasia is used as a synonym for Landau-Kleffner syndrome (LKS).

In most cases described in detail, a clearly normal period of motor and language development occurs before acquired epileptic aphasia symptoms appear. However, in the last 2-3 decades, several reported cases have been difficult to classify, because the patients’ presenting symptoms appear to have been variants of those originally described. In one case, expressive language deteriorated instead of receptive language, whereas in another case, a brief period of normal language development (single words) was followed by language regression with abnormal EEG findings.

Acquired epileptic aphasia must be differentiated from autism with minimal language regression, especially when it is associated with isolated EEG abnormalities. Many current researchers classify acquired epileptic aphasia as part of the syndrome of electrical status epilepticus of sleep (ESES), which is also known as continuous spike and wave of slow-wave sleep (CSWS) as initially described by Patry et al 1971. ^[1]

See also the following:

Benign Neonatal Convulsions

Epilepsy and Seizures

Epileptic and Epileptiform Encephalopathies

Autism

PET Scanning in Autism Spectrum Disorders

Benign Childhood Epilepsy

Epilepsy Surgery

Epileptiform Normal Variants on EEG

First Pediatric Seizure

Neuroimaging Epilepsy

Outcome of Epilepsy Surgery

Whether seizures and epileptiform discharges cause language dysfunction in acquired epileptic aphasia (AEA) is disputed. Aphasia and electroencephalographic (EEG) abnormalities might have a common cause (eg, a left temporal brain astrocytoma or head injury). Some authors speculate that reinforcement of synaptogenesis mediates the neurologic deficits in acquired epileptic aphasia and that epileptiform discharges during a critical period of synaptic reinforcement or pruning in turn mediate the reinforcement of synaptogenesis.

Concrete substantiation of this hypothesis is the existence of poor speech in patients who are affected early and whose condition does not respond to anticonvulsant measures. Other patients with acquired epileptic aphasia appear to have worsened language skills during periods of increased epileptiform activity. However, some reports describe no correlation between EEG abnormality and language dysfunction.

Most cases of acquired epileptic aphasia are spontaneous, although familial clustering has been reported. Descriptions of monozygotic twins include cases in which acquired epileptic aphasia affects only one sibling, cases in which this condition affects both siblings, and cases in which it affects one twin and developmental dysphasia affects the other. ^[2] These cases cast serious doubt on the role of epilepsy in speech dysfunction.

Most cases of acquired epileptic aphasia (AEA) do not have a well-defined cause. However, a few cases of secondary acquired epileptic aphasia have been described. ^[3]

Low-grade brain tumors, ^[4] closed-head injury, neurocysticercosis, ^[5] and demyelinating disease ^{[6, 7]} have been associated with the clinical picture of acquired epileptic aphasia. Central nervous system (CNS) vasculitis may also be associated with this condition. One case of otherwise typical acquired epileptic aphasia has been described in association with mitochondrial respiratory chain complex I deficiency. ^[8] Bilateral perisylvian polymicrogyria may also present with new onset of speech disturbance after a 2-year period of normal language and electroencephalographic (EEG) findings typical of acquired epileptic aphasia. ^[9] Other diagnostic considerations might be warranted when evaluated a case of suspected acquired epileptic aphasia.

Population-based epidemiologic data related to acquired epileptic aphasia (AEA) in the United States are limited. The Children’s Hospital and Medical Center (Seattle, Wash) treats 1-2 new cases of acquired epileptic aphasia each year.

Globally, more than 200 cases have been described in the literature. Between 1957 and 1980, 81 cases of acquired epileptic aphasia were reported; more than 100 cases are documented every 10 years. Detailed numbers are difficult to report, because patients may be repeated in various series, as switching professional care is common due to the patient’s and family’s frustration with aggressive treatment that does not improve the patient’s speech. An urban Israeli pediatric neurology clinic reported a 0.2% rate of acquired epileptic aphasia.

The first study of AEA in Japan concluded that the incidence in children aged 5-14 years was about 1 in a million; the prevalence of AEA in children aged 5-19 and under medical care was 1 in about 300,000-410,000. ^[10]

In affected children, aphasia usually appears at age 4-7 years, and there is a slight male predominance (male-to-female ratio, 1.7:1). However, symptom onset has been described in patients as young as 18 months and in those as old as 13 years. This discussion excludes the congenital cases with typical electroencephalographic (EEG) patterns and little or no language development; in such cases, the precise age of onset can never be determined.

In the early descriptions of the syndrome, language dysfunction was not recognized in the early acquisition phase in the first 18 months of life. In the last 2 decades, scrutiny of the language development has revealed some minor abnormalities. Soprano et al found signs of developmental dysphasia in 9 of 12 cases, ^[11] and Robinson et al reported language delay in 4 of 18 cases. ^[12]

Long-term outcome studies of patients with acquired epileptic aphasia (AEA) are limited by the lack of uniformity in diagnostic criteria. About half the patients have some fluctuation in aphasia, and the fluctuations usually occur over several months. On occasion, aphasia may worsen for as long as 7 years after the disease onset.

Worsened outcome has been noted in patients with an onset of language regression before age 5 years. Morrell found that symptoms persisting for longer than 1 year are predictive of poor language recovery, ^[13] and Robinson et al found that poor language recovery was correlated with electrical status epilepticus of sleep (ESES) for longer than 36 months. ^[12] Impaired short-term memory was universal on long-term follow-up of all of their patients with acquired epileptic aphasia. ^[12]

Short-term remissions pose a challenge in evaluating responses to various therapeutic modalities. One should be mindful that fluctuations are not unusual on the course of this disease. Both the clinical course and the electroencephalographic (EEG) changes may get worse, better, and even return to the baseline. ^[13] In many studies, these fluctuations did not always occur simultaneously (see History under the Clinical section for the explanation).

Lower rates of good outcomes have been reported, ranging from 14% to 50%, with a combined rate of 28.6% (see Table 1, below). Duran et al completed a transversal study of 7 patients (all males, aged 8-27 y) with Landau-Kleffner syndrome (acquired epileptic aphasia). ^[14] On long-term follow-up, most patients did not experience total epilepsy remission and language disturbances persisted. One patient had a normal quality of life and 6 patients reported agnosia/aphasia to be their biggest difficulty. ^[14]

Beaumanoir analyzed cases with follow-up of more than 10 years, which included those published in peer-reviewed journals and those from other sources, such as a doctoral thesis reported before 1992. ^[15]

Table 1. Long-Term Follow-up of Acquired Epileptic Aphasia (Open Table in a new window)

Study

Number of Patients

Mean Follow-up, y

Number of Patients with Normal or Mild Language Problems

Soprano et al ^[11] (1994)

12

8

3

Mantovani and Landau ^[16] (1980)

9

22

6

Paquier ^[17] (1992)

6

8.1

3

Rossi ^[18] (1999)

11

9.7

2

Robinson et al ^[12] (2001)

18

5.6

3

Duran et al ^[14] (2009)

7

9.5

1

Total

63

18 (28.6%)

Patients with acquired epileptic aphasia (AEA) have special educational needs. Teaching them sign language when they are aphasic may be helpful in maintaining a useful communication channel. Learning sign language does not prevent or delay the recovery of aphasia. These patients may be able to read and write; therefore, these skills should be used for teaching whenever doing so is possible.

It is important to educate patients and their parents regarding acquired epileptic aphasia and realistic outcomes. A potential cause of litigation in acquired epileptic aphasia is the high parental expectations for a complete and quick recovery of language and speech functions. These unrealistic expectations often come from information in the lay press and from television shows that mention isolated miracle cures in cases of acquired epileptic aphasia after treatment with steroids or other measures. These cases do not represent the usual course of most children with this condition but make up good cases for television or newspaper stories.

Patry G, Lyagoubi S, Tassinari CA. Subclinical “electrical status epilepticus” induced by sleep in children. A clinical and electroencephalographic study of six cases. Arch Neurol. 1971 Mar. 24(3):242-52. [Medline].

Feekery CJ, Parry-Fielder B, Hopkins IJ. Landau-Kleffner syndrome: six patients including discordant monozygotic twins. Pediatr Neurol. 1993 Jan-Feb. 9(1):49-53. [Medline].

Kotagal P. Secondary epileptogenesis [editorial]. J Clin Neurophysiol. 1997 Mar. 14(2):89. [Medline].

Solomon GE, Carson D, Pavlakis S, et al. Intracranial EEG monitoring in Landau-Kleffner syndrome associated with left temporal lobe astrocytoma. Epilepsia. 1993 May-Jun. 34(3):557-60. [Medline].

Otero E, Cordova S, Diaz F, et al. Acquired epileptic aphasia (the Landau-Kleffner syndrome) due to neurocysticercosis. Epilepsia. 1989 Sep-Oct. 30(5):569-72. [Medline].

Perniola T, Margari L, Buttiglione M, et al. A case of Landau-Kleffner syndrome secondary to inflammatory demyelinating disease. Epilepsia. 1993 May-Jun. 34(3):551-6. [Medline].

Primavera A, Gianelli MV, Bandini F. Aphasic status epilepticus in multiple sclerosis. Eur Neurol. 1996. 36(6):374-7. [Medline].

Kang HC, Kim HD, Lee YM. Landau-Kleffner syndrome with mitochondrial respiratory chain-complex I deficiency. Pediatr Neurol. 2006 Aug. 35(2):158-61. [Medline].

Huppke P, Kallenberg K, Gartner J. Perisylvian polymicrogyria in Landau-Kleffner syndrome. Neurology. 2005 May 10. 64(9):1660. [Medline].

Kaga M, Inagaki M, Ohta R. Epidemiological study of Landau-Kleffner syndrome (LKS) in Japan. Brain Dev. 2013 May 21. [Medline].

Soprano AM, Garcia EF, Caraballo R, Fejerman N. Acquired epileptic aphasia: neuropsychologic follow-up of 12 patients. Pediatr Neurol. 1994 Oct. 11(3):230-5. [Medline].

Robinson RO, Baird G, Robinson G, Simonoff E. Landau-Kleffner syndrome: course and correlates with outcome. Dev Med Child Neurol. 2001 Apr. 43(4):243-7. [Medline].

Morrell F. Electrophysiology of CSWS in Landau-Kleffner syndrome. In: Beaumanoir A, Bureau M, Deona T, Mira L, Tassinari CA, eds. Continuous Spikes and Waves During Slow Sleep Electrical Status Epilepticus During Slow Wave Sleep. London, England: John Libbey; 1995. 77-90.

Duran MH, Guimaraes CA, Medeiros LL, Guerreiro MM. Landau-Kleffner syndrome: long-term follow-up. Brain Dev. 2009 Jan. 31(1):58-63. [Medline].

Beaumanoir A. The Landau-Kleffner syndrome. In: Roger J, Dravet C, Bureau M, Dreifuss FE, Perret A, Wolf P, eds. Epileptic Syndromes in Infancy, Childhood, and Adolescence. 2nd ed. London, England: John Libbey Eurotext Ltd. 1992:181-91, 231-43.

Mantovani JF, Landau WM. Acquired aphasia with convulsive disorder: course and prognosis. Neurology. 1980 May. 30(5):524-9. [Medline].

Paquier PF, Van Dongen HR, Loonen CB. The Landau-Kleffner syndrome or acquired aphasia with convulsive disorder: long-term follow-up of six children and a review of the recent literature. Arch Neurol. 1992 Apr. 49(4):354-9. [Medline].

Rossi PG, Parmeggiani A, Posar A, et al. Landau-Kleffner syndrome (LKS): long-term follow-up and links with electrical status epilepticus during sleep (ESES). Brain Dev. 1999 Mar. 21(2):90-8. [Medline].

Rousselle C, Revol M. Relationship between cognitive function and CSWS. In: Beaumanoir A, Bureau M, Deona T, Dreifuss FE, Perret A, Wolf P, eds. Epileptic Syndromes in Infancy, Childhood, and Adolescence. 2nd ed. London, England: John Libbey Eurotext Ltd; 1995: 123-33.

Caraballo RH, Astorino F, Cersosimo R, et al. Atypical evolution in childhood epilepsy with occipital paroxysms (Panayiotopoulos type). Epileptic Disord. 2001 Sep. 3(3):157-62. [Medline].

Ferrie CD, Koutroumanidis M, Rowlinson S, et al. Atypical evolution of Panayiotopoulos syndrome: a case report. Epileptic Disord. 2002 Mar. 4(1):35-42. [Medline].

Scheffer IE, Jones L, Pozzebon M, et al. Autosomal dominant rolandic epilepsy and speech dyspraxia: a new syndrome with anticipation. Ann Neurol. 1995 Oct. 38(4):633-42. [Medline].

Tuchman RF, Rapin I. Regression in pervasive developmental disorders: seizures and epileptiform electroencephalogram correlates. Pediatrics. 1997 Apr. 99(4):560-6. [Medline]. [Full Text].

Lesca G, Rudolf G, Bruneau N, Lozovaya N, Labalme A, Boutry-Kryza N, et al. GRIN2A mutations in acquired epileptic aphasia and related childhood focal epilepsies and encephalopathies with speech and language dysfunction. Nat Genet. 2013 Aug 28. 45(9):1061-6. [Medline].

Carvill GL, Regan BM, Yendle SC, O’Roak BJ, Lozovaya N, Bruneau N. GRIN2A mutations cause epilepsy-aphasia spectrum disorders. Nat Genet. 2013 Aug 28. 45(9):1073-6. [Medline].

Rapin I. Acquired aphasia in children [editorial]. J Child Neurol. 1995 Jul. 10(4):267-70. [Medline].

Rapin I. Autistic regression and disintegrative disorder: how important the role of epilepsy?. Semin Pediatr Neurol. 1995 Dec. 2(4):278-85. [Medline].

Luat AF, Chugani HT, Asano E. Episodic receptive aphasia in a child with Landau-Kleffner Syndrome: PET correlates. Brain Dev. 2006 Oct. 28(9):592-6. [Medline].

Nickels K, Wirrell E. Electrical status epilepticus in sleep. Semin Pediatr Neurol. 2008 Jun. 15(2):50-60. [Medline].

Tassinari CA, Cantalupo G, Rios-Pohl L, Giustina ED, Rubboli G. Encephalopathy with status epilepticus during slow sleep: “the Penelope syndrome”. Epilepsia. 2009 Aug. 50 Suppl 7:4-8. [Medline].

Paetau R, Kajola M, Korkman M, et al. Landau-Kleffner syndrome: epileptic activity in the auditory cortex. Neuroreport. 1991 Apr. 2(4):201-4. [Medline].

Paetau R. Magnetoencephalography in Landau-Kleffner syndrome. Epilepsia. 2009 Aug. 50 Suppl 7:51-4. [Medline].

Pascual-Castroviejo I, Lopez Martin V, Martinez Bermejo A, Perez Higueras A. Is cerebral arteritis the cause of the Landau-Kleffner syndrome? Four cases in childhood with angiographic study. Can J Neurol Sci. 1992 Feb. 19(1):46-52. [Medline].

Arts WF, Aarsen FK, Scheltens-de Boer M, Catsman-Berrevoets CE. Landau-Kleffner syndrome and CSWS syndrome: treatment with intravenous immunoglobulins. Epilepsia. 2009 Aug. 50 Suppl 7:55-8. [Medline].

Riviello JJ. The Boston Children’s Hospital experience with ESES and LKS course. Paper presented at: Annual Meeting of the American Epilepsy Society; December 2006; San Diego, California.

Kossoff EH, Boatman D, Freeman JM. Landau-Kleffner syndrome responsive to levetiracetam. Epilepsy Behav. 2003 Oct. 4(5):571-5. [Medline].

von Stülpnagel C, Kluger G, Leiz S, Holthausen H. Levetiracetam as add-on therapy in different subgroups of “benign” idiopathic focal epilepsies in childhood. Epilepsy Behav. 2010 Feb. 17(2):193-198. [Medline].

Van Bogaert P. Epileptic encephalopathy with continuous spike-waves during slow-wave sleep including Landau-Kleffner syndrome. Handb Clin Neurol. 2013. 111:635-40. [Medline].

Kramer U, Sagi L, Goldberg-Stern H, Zelnik N, Nissenkorn A, Ben-Zeev B. Clinical spectrum and medical treatment of children with electrical status epilepticus in sleep (ESES). Epilepsia. 2009 Jun. 50(6):1517-24. [Medline].

Glauser TA, Olberding LS, Titanic MK, Piccirillo DM. Felbamate in the treatment of acquired epileptic aphasia. Epilepsy Res. 1995 Jan. 20(1):85-9. [Medline].

Buzatu M, Bulteau C, Altuzarra C, Dulac O, Van Bogaert P. Corticosteroids as treatment of epileptic syndromes with continuous spike-waves during slow-wave sleep. Epilepsia. 2009 Aug. 50 Suppl 7:68-72. [Medline].

Morrell F, Whisler WW, Smith MC, et al. Landau-Kleffner syndrome. Treatment with subpial intracortical transection. Brain. 1995 Dec. 118 ( Pt 6):1529-46. [Medline].

Sawhney IM, Robertson IJ, Polkey CE, et al. Multiple subpial transection: a review of 21 cases. J Neurol Neurosurg Psychiatry. 1995 Mar. 58(3):344-9. [Medline].

Bergqvist AG, Chee CM, Lutchka LM, Brooks-Kayal AR. Treatment of acquired epileptic aphasia with the ketogenic diet. J Child Neurol. 1999 Nov. 14(11):696-701. [Medline].

Nikanorova M, Miranda MJ, Atkins M, Sahlholdt L. Ketogenic diet in the treatment of refractory continuous spikes and waves during slow sleep. Epilepsia. 2009 May. 50(5):1127-31. [Medline].

Arslan N, Guzel O, Kose E, Yılmaz U, Kuyum P, Aksoy B, et al. Is ketogenic diet treatment hepatotoxic for children with intractable epilepsy?. Seizure. 2016 Dec. 43:32-38. [Medline].

Chermak G. and Musiek F. Handbook of (Central) Auditory Processing Disorder, Volume II: Comprehensive Intervention. Second Edition. San Diego, CA: Plural Publishing; 2007.

Hurley, A. Auditory Remediation for Patients With Landau-Kleffner Syndrome. The ASHS Leader. Available at http://leader.pubs.asha.org/article.aspx?articleid=2279034. April 2011; Accessed: October 19, 2017.

Marescaux C, Hirsch E, Finck S, et al. Landau-Kleffner syndrome: a pharmacologic study of five cases. Epilepsia. 1990 Nov-Dec. 31(6):768-77. [Medline].

Okuyaz C, Aydin K, Gucuyener K, Serdaroglu A. Treatment of electrical status epilepticus during slow-wave sleep with high-dose corticosteroid. Pediatr Neurol. 2005 Jan. 32(1):64-7. [Medline].

Van Hirtum-Das M, Licht EA, Koh S. Children with ESES: variability in the syndrome. Epilepsy Res. 2006 Aug. 70 Suppl 1:S248-58. [Medline].

Study

Number of Patients

Mean Follow-up, y

Number of Patients with Normal or Mild Language Problems

Soprano et al ^[11] (1994)

12

8

3

Mantovani and Landau ^[16] (1980)

9

22

6

Paquier ^[17] (1992)

6

8.1

3

Rossi ^[18] (1999)

11

9.7

2

Robinson et al ^[12] (2001)

18

5.6

3

Duran et al ^[14] (2009)

7

9.5

1

Total

63

18 (28.6%)

Source

Diagnosis

Number of Patients

Number of Patients with EEGs

Patients with Abnormal EEGs (%)

Tuchman et al (1991)

Autism with epilepsy

42

40

75

Autism without epilepsy

160

139

8

Dysphasia with epilepsy

19

19

58

Dysphasia without epilepsy

218

66

9

Tuchman and Rapin ^[23] (1997)

PDD or autism

585

392^*

NA

With epilepsy

NA

66

59

Without epilepsy

NA

66

59

Without epilepsy but with history of regression

NA

155

14

Without epilepsy and without history of regression

NA

364

6

EEG(s) = electroencephalogram(s); NA = not applicable; PDD = personality developmental disorder.

^* Sleep EEGs.

Diagnosis

Deterioration

EEG Patterns

Autistic epileptiform regression

Expressive language, RL, S, verbal and nonverbal communication

Centrotemporal spikes

Autistic regression

Expressive language, RL, S, verbal and nonverbal communication

Normal

Acquired epileptic aphasia

RL, possibly behavioral

Left or right temporal or parietal spikes, possibly ESES

Acquired expressive epileptic aphasia

Expressive language, oromotor apraxia

Centrotemporal spikes

ESES

Expressive language, RL, possibly behavioral

ESES

Developmental dysphasia (developmental expressive language disease)

No; lack of expressive language acquisition

Temporal or parietal spikes

Disintegrative epileptiform disorder

Expressive language, RL, S, verbal and nonverbal communication, possibly behavioral

ESES

EEG = electroencephalographic; ESES = electrical status epilepticus of sleep; RL = receptive language; S = sociability.

^* Continuous spike and wave of slow-wave sleep (>85% of slow-wave sleep).

Eli S Neiman, DO, FACN Clinical Associate Professor of Neurology, Department of Neurology, Kansas City University of Medicine and Biosciences College of Osteopathic Medicine; Clinical Assistant Professor, Robert C Byrd Health Science Center, West Virginia University School of Medicine; Assistant Professor of Neurology, Hackensack Meridian School of Medicine at Seton Hall University; Neurologist and Clinical Neurophysiologist, National Neuromonitoring Services, LLC; Neurologist, Advanced Neurology Center

Eli S Neiman, DO, FACN is a member of the following medical societies: American Academy of Neurology, American Epilepsy Society, American Osteopathic Association

Disclosure: Nothing to disclose.

Zev Kizelnik Touro College of Dental Medicine

Zev Kizelnik is a member of the following medical societies: American Heart Association, American Student Dental Association

Disclosure: Nothing to disclose.

Michael Seyffert, MD Resident Physician, Department of Psychiatry, University of Michigan Medical School

Michael Seyffert, MD is a member of the following medical societies: American Academy of Neurology, American Academy of Psychiatry and the Law, Child Neurology Society, American Academy of Sleep Medicine, Society for the Study of Psychiatry and Culture

Disclosure: Nothing to disclose.

Francisco Talavera, PharmD, PhD Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Received salary from Medscape for employment. for: Medscape.

Amy Kao, MD Attending Neurologist, Children’s National Medical Center

Amy Kao, MD is a member of the following medical societies: American Academy of Neurology, American Epilepsy Society, Child Neurology Society

Disclosure: Have stock (managed by a financial services company) in healthcare companies including AbbVie, Allergan, Celgene, Cellectar Biosciences, Danaher Corp, Mckesson.

Robert Stanley Rust, Jr, MD, MA Thomas E Worrell Jr Professor of Epileptology and Neurology, Co-Director of FE Dreifuss Child Neurology and Epilepsy Clinics, Director, Child Neurology, University of Virginia School of Medicine; Chair-Elect, Child Neurology Section, American Academy of Neurology

Robert Stanley Rust, Jr, MD, MA is a member of the following medical societies: Child Neurology Society, Society for Pediatric Research, American Headache Society, International Child Neurology Association, American Academy of Neurology, American Epilepsy Society, American Neurological Association

Disclosure: Nothing to disclose.

The authors and editors of Medscape Reference gratefully acknowledge the contributions of previous author Marcio Sotero de Menezes, MD, to the development and writing of the source article.

Acquired Epileptic Aphasia

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