No evidence of a role for cystatin <scp>B</scp> gene in juvenile myoclonic epilepsy

Mumoli, Laura; Tarantino, Patrizia; Michelucci, Roberto; Bianchi, Amedeo; Labate, Angelo; Franceschetti, Silvana; Marini, Carla; Striano, Pasquale; Gagliardi, Monica; Ferlazzo, Edoardo; Sofia, Vito; Pennese, Loredana; Annesi, Grazia; Aguglia, Umberto; Guerrini, Renzo; Zara, Federico; Gambardella, Antonio

doi:10.1111/epi.12944

Cited by 7 publications

(8 citation statements)

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“…They described a case of a compound heterozygous female patient affected by a mild phenotype that was mistaken for juvenile myoclonic epilepsy (genotype screening was performed for a distant family history of EPM1). It is worth noting that CSTB mutations were never found in juvenile myoclonic epilepsy . On these data we speculate that in heterozygous compound patients an association of genetic and gender‐specific factors can reduce the efficacy of residual Cystatin B (to counteract damages resulting from endogenous protease activity).…”

Section: Discussionmentioning

confidence: 80%

“…It is worth noting that CSTB mutations were never found in juvenile myoclonic epilepsy. 8 On these data we speculate that in heterozygous compound patients an association of genetic and gender-specific factors can reduce the efficacy of residual Cystatin B (to counteract damages resulting from endogenous protease activity). Even if a haploinsufficiency of CSTB seems to not affect heterozygous compound patients, 5 a functional deficit of mutated protein cannot be excluded.…”

Section: Discussionmentioning

confidence: 85%

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A novel c132‐134del mutation in Unverricht‐Lundborg disease and the review of literature of heterozygous compound patients

et al. 2016

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Unverricht-Lundborg disease or progressive myoclonic epilepsy type 1 (EPM1) is an autosomal recessive disease caused by mutation of the cystatin B gene (CSTB), located on chromosome 21q22.3. The most common mutation is an expansion of unstable dodecamer repetition (CCCCGCCCCGCG), whereas other types of mutations are rare. Among these, heterozygous compound mutations are described to induce a more severe phenotype than that of homozygous dodecameric repetition. We report two siblings affected by heterozygous compound mutations carrying a novel mutation of the deletion of three nucleotides in exon 2 of the gene in position 132-134 of the coding sequence (c.132-134del) in the allele not including the dodecamer repetition. This mutation results in the loss of two amino acid residues and insertion of an asparagine in position 44 (p.Lys44_Ser45delinsAsn). Our patients presented a very different clinical picture. The male patient had a severe myoclonus, drug-resistant epilepsy and psychiatric comorbidity, while his affected sister had only very rare seizures and sporadic myoclonic jerks at awakening. The revision of literature about heterozygous compound EPM1 patients confirms this gender phenotypic expressivity, with female patients carrying less severe symptoms than male patients. These data lead to the hypothesis of complex gender-specific factors interacting with CSTB expressivity in EPM1 patients.

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Section: Discussionmentioning

confidence: 80%

Section: Discussionmentioning

confidence: 85%

A novel c132‐134del mutation in Unverricht‐Lundborg disease and the review of literature of heterozygous compound patients

et al. 2016

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“…This clinical presentation could be more frequent in Tunisia than in European countries since it was shown that the course of the disease is more severe in Northern Europe than in Maghreb (Gargouri-Berrechid et al, 2016). In addition, Laura Mumoli and colleagues showed an absence of mutation associated with ULD in 33 unrelated patients with JME from Italy (Mumoli et al, 2015). The size of repeats in Family 1 was within the classic range and even larger than that of Family 2, which does not account for the very mild phenotype.…”

Section: Discussionmentioning

confidence: 99%

Juvenile myoclonic epilepsy phenotype in a family with Unverricht‐Lundborg disease

Berrechid

Bendjebara

Bouteiller

et al. 2019

Epileptic Disorders

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Aims . Unverricht‐Lundborg disease (ULD), an autosomal recessive progressive myoclonus epilepsy, is due to an expansion, or less commonly a mutation, of the cystatin B ( CSTB ) gene. We report a clinical and molecular study of a Tunisian ULD family with five affected members presenting with a juvenile myoclonic epilepsy (JME)‐like phenotype. Methods . The expansion of dodecamers was detected by a deamination/PCR assay. The expression profiles of CSTB and other candidate modifying genes, cathepsin B and cystatin C, were established by quantitative RT‐PCR, and their respective transcription levels were compared with those from patients with a classic picture of ULD. Results . Three patients had a fixed phenotype mimicking JME after 29 years of evolution. Only a discrete dysarthria was noticed in the two other patients. No correlation was observed between transcription level and severity of disease. Conclusion . Genetic screening should be performed in patients with a JME‐like phenotype, when careful examination reveals discrete atypical signs of JME. This particular phenotype may be due to modifying genes and/or gene‐environment interactions which require further clarification.

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“…Although ULD remains uncommon, it has been increasingly diagnosed among patients with drug-resistant myoclonic epilepsy, as shown, for instance, in Holland (de Haan et al, 2004). However, whereas the most common mutation in ULD affects the cystatin B gene (CSTB), no evidence for a role of this gene was found in sporadic or familial cases of juvenile myoclonic epilepsy (JME) (Mumoli et al, 2015). The availability of molecular genetic diagnostic techniques in developed countries has certainly helped.…”

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confidence: 99%

Unverricht‐Lundborg disease

Crespel¹,

Ferlazzo²,

Franceschetti³

et al. 2016

Epileptic Disorders

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We first review the clinical presentation and current therapeutic approaches available for treating Unverricht‐Lundborg disease (ULD), a progressive myoclonus epilepsy. Next, we describe the identification of disease causing mutations in the gene encoding cystatin B (CSTB). A Cstb‐deficient mouse model, which recapitulates the key features of ULD including myoclonic seizures, ataxia, and neuronal loss, was generated to shed light on the mechanisms contributing to disease pathophysiology. Studies with this model have elucidated the diverse biological roles for Cstb from functioning as a protease inhibitor, to regulating glial activation, oxidative stress, serotonergic neurotransmission, and hyperexcitability. These findings set the stage for future studies that may open avenues to improved therapeutic approaches.

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No evidence of a role for cystatin B gene in juvenile myoclonic epilepsy

Cited by 7 publications

References 15 publications

A novel c132‐134del mutation in Unverricht‐Lundborg disease and the review of literature of heterozygous compound patients

A novel c132‐134del mutation in Unverricht‐Lundborg disease and the review of literature of heterozygous compound patients

Juvenile myoclonic epilepsy phenotype in a family with Unverricht‐Lundborg disease

Unverricht‐Lundborg disease

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