Lafora Disease

Overview

Journal Epileptic Disord

Publisher Wiley

Specialty Neurology

Date 2016 Oct 6

PMID 27702709

Citations 82

Authors

Julie Turnbull

Erica Tiberia

Pasquale Striano

Pierre Genton

Stirling Carpenter

Cameron A Ackerley

Berge A Minassian

Affiliations

Soon will be listed here.

Abstract

Lafora disease (LD) is an autosomal recessive progressive myoclonus epilepsy due to mutations in the EPM2A (laforin) and EPM2B (malin) genes, with no substantial genotype-phenotype differences between the two. Founder effects and recurrent mutations are common, and mostly isolated to specific ethnic groups and/or geographical locations. Pathologically, LD is characterized by distinctive polyglucosans, which are formations of abnormal glycogen. Polyglucosans, or Lafora bodies (LB) are typically found in the brain, periportal hepatocytes of the liver, skeletal and cardiac myocytes, and in the eccrine duct and apocrine myoepithelial cells of sweat glands. Mouse models of the disease and other naturally occurring animal models have similar pathology and phenotype. Hypotheses of LB formation remain controversial, with compelling evidence and caveats for each hypothesis. However, it is clear that the laforin and malin functions regulating glycogen structure are key. With the exception of a few missense mutations LD is clinically homogeneous, with onset in adolescence. Symptoms begin with seizures, and neurological decline follows soon after. The disease course is progressive and fatal, with death occurring within 10 years of onset. Antiepileptic drugs are mostly non-effective, with none having a major influence on the progression of cognitive and behavioral symptoms. Diagnosis and genetic counseling are important aspects of LD, and social support is essential in disease management. Future therapeutics for LD will revolve around the pathogenesics of the disease. Currently, efforts at identifying compounds or approaches to reduce brain glycogen synthesis appear to be highly promising.

Citing Articles

Brain Glycogen-Its Metabolic Role in Neuronal Health and Neurological Disorders-An Extensive Narrative Review.

Beltran-Velasco A Metabolites. 2025; 15(2).

PMID: 39997753 PMC: 11857135. DOI: 10.3390/metabo15020128.

Dapagliflozin ameliorates Lafora disease phenotype in a zebrafish model.

Della Vecchia S, Imbrici P, Liantonio A, Naef V, Damiani D, Licitra R Biomed Pharmacother. 2025; 183:117800.

PMID: 39753095 PMC: 11794196. DOI: 10.1016/j.biopha.2024.117800.

VAL-1221 for the treatment of patients with Lafora disease: study protocol for a single-arm, open-label clinical trial.

Muccioli L, Vignatelli L, Tappata M, Mazzone S, Zenesini C, Armstrong D BMJ Open. 2024; 14(10):e085062.

PMID: 39424378 PMC: 11492954. DOI: 10.1136/bmjopen-2024-085062.

Neuromuscular junction dysfunction in Lafora disease.

Shukla M, Chugh D, Ganesh S Dis Model Mech. 2024; 17(10).

PMID: 39301689 PMC: 11512103. DOI: 10.1242/dmm.050905.

Neurological glycogen storage diseases and emerging therapeutics.

Colpaert M, Singh P, Donohue K, Pires N, Fuller D, Corti M Neurotherapeutics. 2024; 21(5):e00446.

PMID: 39277505 PMC: 11581880. DOI: 10.1016/j.neurot.2024.e00446.

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