Molecular diagnostics in drug‐resistant focal epilepsy define new disease entities

Kobow, Katja; Baulac, Stéphanie; Deimling, Andreas von; Lee, Jehee

doi:10.1111/bpa.12963

Cited by 19 publications

(24 citation statements)

References 70 publications

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“…56 The dysregulation of the mTOR signaling pathway provides the rational mechanistic basis for a direct link between gene mutation and brain pathology involving dysmorphic neurons, balloon cells, oligodendrocytes, and astrocytes. 12,14,61 In contrast, a double hit with a germline and somatic lossof-function variant in repressors of the pathway (i.e., DEPDC5, NPRL2, NPRL3, TSC) is necessary for the expression of the brain lesion. Definite somatic second-hit events, either single nucleotide variants 19,60,62,63 or lossof-heterozygosity (LOH) 51,57 of the second allele leading to biallelic gene inactivation of DEPDC5 have now been reported, validating the two-hit model for mTORpathway repressor genes.…”

Section: Mild Malformations Of Cortical Development With Oligodendrog...mentioning

confidence: 99%

The ILAE consensus classification of focal cortical dysplasia: An update proposed by an ad hoc task force of the ILAE diagnostic methods commission

Najm¹,

et al. 2022

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Ongoing challenges in diagnosing focal cortical dysplasia (FCD) mandate continuous research and consensus agreement to improve disease definition and classification. An International League Against Epilepsy (ILAE) Task Force (TF) reviewed the FCD classification of 2011 to identify existing gaps and provide a timely update. The following methodology was applied to achieve this goal: a survey of published literature indexed with ((Focal Cortical Dysplasia) AND (epilepsy)) between 01/01/2012 and 06/30/2021 (n = 1349) in PubMed identified the knowledge gained since 2012 and new developments in the field. An online survey consulted the ILAE community about the current use of the FCD classification scheme with 367 people answering. The TF performed an iterative clinicopathological and genetic agreement study to objectively measure the diagnostic gap in blood/brain samples from 22 patients suspicious for FCD and submitted to epilepsy surgery. The literature confirmed new molecular-genetic characterizations involving the mechanistic Target Of Rapamycin (mTOR) pathway in FCD type II (FCDII), and SLC35A2 in mild malformations of cortical development (mMCDs) with oligodendroglial hyperplasia (MOGHE). The electro-clinicalimaging phenotypes and surgical outcomes were better defined and validated for FCDII. Little new information was acquired on clinical, histopathological, or genetic characteristics of FCD type I (FCDI) and FCD type III (FCDIII). The survey identified mMCDs, FCDI, and genetic characterization as fields for improvement in an updated classification. Our iterative clinico-pathological and genetic agreement study confirmed the importance of immunohistochemical staining, neuroimaging, and genetic tests to improve the diagnostic yield. The TF proposes to include mMCDs, MOGHE, and "no definite FCD on histopathology" as new categories in the updated FCD classification. The histopathological classification can be further augmented by advanced neuroimaging and genetic studies to comprehensively diagnose FCD subtypes; these different levels should then be integrated into a multi-layered diagnostic scheme. This update may help to foster multidisciplinary efforts toward a better understanding of FCD and the development of novel targeted treatment options.

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Section: Mild Malformations Of Cortical Development With Oligodendrog...mentioning

confidence: 99%

The ILAE consensus classification of focal cortical dysplasia: An update proposed by an ad hoc task force of the ILAE diagnostic methods commission

Najm¹,

et al. 2022

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“…Even in research, taking in account that individuals usually agree to share their whole data, access is usually a very limited process to ensure compliance. Strategies must be developed to capitalize on previous as well as future data and fully exploit the powerful collective data in order to assist the interpretation of genetic variation for patient care [76] . The balance between data sharing and maintaining confidentiality will ultimately impact our diagnostic capacity in the future.…”

Section: Limitations and Future Perspectivesmentioning

confidence: 99%

Developmental and epileptic encephalopathies after negative or inconclusive genetic testing: what is next?

Aledo‐Serrano¹,

Sánchez-Alcudia²,

Toledano³

et al. 2021

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The redefinition of classical electroclinical syndromes and the emergence of neurogenetics has led to a revolution in the field of developmental and epileptic encephalopathies (DEEs). In this context, advances in genetic techniques are leading to the final diagnosis of a large proportion of patients with DEE. However, up to 50% of patients with DEE remain undiagnosed. For patients with uncertain genetic etiology, there is a pressing need for the implementation of new targeted treatments and precision medicine. In some undiagnosed patients, genetic reanalysis with further in-depth or reverse phenotyping are valuable diagnostic tools to clarify new variants of uncertain significance. In other cases, the implementation of new bioinformatic algorithms is required for the update and reassessment of previously generated genetic data. Moreover, many other clinical tools have been developed for the management of patients of DEEs after a negative or inconclusive genetic testing. In this review, we highlight advances and limitations of new diagnostic strategies used in DEE patients without a known genetic etiology. Finally, we provide a wide perspective on aspects that will need further research, especially in non-Mendelian inheritance DEEs, such as those related to somatic mosaicism of the central nervous system or epigenetic and oligogenic mechanisms.

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“…Separately, ongoing studies of FCD surgical specimens are revealing a growing number of both germline and somatic mutations that appear to be pathogenic. 2 Based on the latter it may be time to update the classification of FCDs. The novel study by Blümcke et al 3 is a significant step forward in the diagnosis and classification of patients with FCDs who may undergo surgical resection to treat epilepsy because it combines standard histological findings with immunohistology and genetic features.…”

Section: Commentarymentioning

confidence: 99%

“… 8 Moreover, many Type IIb (especially bottom-of-the sulcus frontal lobe) lesions are found to contain germline and/or somatic gain-of-function mutations in the mTOR pathway. 1 , 2 , 8 A newer entity called mild malformation of cortical development with oligodendroglial hyperplasia (MOGHE) is often also located in the frontal lobe and is frequently associated with somatic mutations in the SLC35A2 gene affecting the glycosylation pathway. In contrast, genetic mutations have not commonly been seen thus far in FCD Type I lesions, but recent unpublished data, reviewed by Blümcke and colleagues, 1 suggest that DNA methylation patterns could distinguish Type Ia from other FCD types.…”

Section: Commentarymentioning

confidence: 99%

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Cutting-Edge Classification of Focal Cortical Dysplasia for Epilepsy Surgery

Vossler

2021

Epilepsy Curr

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Molecular diagnostics in drug‐resistant focal epilepsy define new disease entities

Cited by 19 publications

References 70 publications

The ILAE consensus classification of focal cortical dysplasia: An update proposed by an ad hoc task force of the ILAE diagnostic methods commission

The ILAE consensus classification of focal cortical dysplasia: An update proposed by an ad hoc task force of the ILAE diagnostic methods commission

Developmental and epileptic encephalopathies after negative or inconclusive genetic testing: what is next?

Cutting-Edge Classification of Focal Cortical Dysplasia for Epilepsy Surgery

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