Multilobar unilateral hypoplasia with emphasis on the posterior quadrant and severe epilepsy in children with FCD ILAE Type 1A

Holthausen, Hans; Coras, Roland; Tang, Yingying; Bai, Lily; Wang, Irène; Pieper, Tom; Kudernatsch, Manfred; Hartlieb, Till; Staudt, Martin; Winkler, Peter; Höfer, W; Jabari, Samir; Kobow, Katja; Blümcke, Ingmar

doi:10.1111/epi.17114

Cited by 17 publications

(35 citation statements)

References 73 publications

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“…Excellent seizure outcomes were associated with surgical resections involving FCDII 5 . But nonfavorable outcomes have been reported following resections of FCDI 41 with the outcomes of FCDIII depending mainly on the principal lesion associated with FCD 46 …”

Section: Resultsmentioning

confidence: 99%

“…Nine genes have been reported to cause canonical FCDII: AKT3, DEPDC5, MTOR, NPRL2, NPRL3, PIK3CA, RHEB, TSC1, and TSC2 . SLC35A2 should be included in the panel in order to differentiate MOGHE 13,17,61 from its most common differential diagnosis: FCDIa 41 . The diagnostic yield using such gene panel sequencing from routine FFPE or frozen tissue ranges from 32% when assessing various epilepsy‐related lesions 13,60 to 45% in patients selected for MOGHE, 19 and 63% in patients with hemimegalencephaly or FCDII 60 .…”

Section: Resultsmentioning

confidence: 99%

“…14 Methodological approaches aside, due consideration of clinically significant thresholds for methylation is warranted. 3.1.7 | Challenges identified in the first ILAE classification scheme Whereas FCDIa is hitherto confirmed in a series of 19 children with early seizure onset, subtle unilateral hemispheric hypoplasia, global developmental delay, and drug resistance from seizure onset, 41 a consistent clinico-pathological characterization of the patient cohort with FCDIb and FCDIc is still lacking and convincing examples are scarce in the current literature. [36][37][38][39] In addition, Figure 2C from the original ILAE publication in 2011 showed loss of layer 4 neurons in a young boy with focal epilepsy as an example of FCDIb with horizontal dyslamination 10 ; however, upon review, this should be classified as FCDIIId, since there is evidence that loss of layer 4 neurons results from early (perinatal) hypoxicischemic injury in the occipital lobe, predominantly in boys (Figure 1H).…”

Section: Emerging Role Of Epigenetics In Epilepsymentioning

confidence: 99%

“…[36][37][38][39] In addition, Figure 2C from the original ILAE publication in 2011 showed loss of layer 4 neurons in a young boy with focal epilepsy as an example of FCDIb with horizontal dyslamination 10 ; however, upon review, this should be classified as FCDIIId, since there is evidence that loss of layer 4 neurons results from early (perinatal) hypoxicischemic injury in the occipital lobe, predominantly in boys (Figure 1H). 76 This kind of confusion raises the issue of whether cortical architectural abnormalities other than the bona fide dyslamination of FCDIa in patients with diffuse unilateral lesions mentioned above 41 truly represents "dysplastic" abnormalities or simply variable architectural changes. Furthermore, histopathology of FCDIc was never described before the ILAE classification in 2011, and it quickly developed into a "wastebasket" of cases clinically suspected as FCD with no or very subtle MRI findings.…”

Section: Emerging Role Of Epigenetics In Epilepsymentioning

confidence: 99%

“…5 DNA methylation array analysis from routine FFPE tissue may increase the diagnostic yield in the near future. 41 Building on the most recent scientific advances, the TF proposes to include lesions compromising the white matter as new F I G U R E 3 Histopathological hallmarks of FCDIa. An 18-year-old female patient.…”

Section: Consensus Proposal For a Pathology Update And The Creation O...mentioning

confidence: 99%

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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: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Emerging Role Of Epigenetics In Epilepsymentioning

confidence: 99%

Section: Emerging Role Of Epigenetics In Epilepsymentioning

confidence: 99%

Section: Consensus Proposal For a Pathology Update And The Creation O...mentioning

confidence: 99%

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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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Multiparametric Characterization of Focal Cortical Dysplasia Using 3D MR Fingerprinting

Su,

Choi,

et al. 2024

Annals of Neurology

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ObjectivesTo develop a multiparametric machine‐learning (ML) framework using high‐resolution 3 dimensional (3D) magnetic resonance (MR) fingerprinting (MRF) data for quantitative characterization of focal cortical dysplasia (FCD).MaterialsWe included 119 subjects, 33 patients with focal epilepsy and histopathologically confirmed FCD, 60 age‐ and gender‐matched healthy controls (HCs), and 26 disease controls (DCs). Subjects underwent whole‐brain 3 Tesla MRF acquisition, the reconstruction of which generated T1 and T2 relaxometry maps. A 3D region of interest was manually created for each lesion, and z‐score normalization using HC data was performed. We conducted 2D classification with ensemble models using MRF T1 and T2 mean and standard deviation from gray matter and white matter for FCD versus controls. Subtype classification additionally incorporated entropy and uniformity of MRF metrics, as well as morphometric features from the morphometric analysis program (MAP). We translated 2D results to individual probabilities using the percentage of slices above an adaptive threshold. These probabilities and clinical variables were input into a support vector machine for individual‐level classification. Fivefold cross‐validation was performed and performance metrics were reported using receiver‐operating‐characteristic‐curve analyses.ResultsFCD versus HC classification yielded mean sensitivity, specificity, and accuracy of 0.945, 0.980, and 0.962, respectively; FCD versus DC classification achieved 0.918, 0.965, and 0.939. In comparison, visual review of the clinical magnetic resonance imaging (MRI) detected 48% (16/33) of the lesions by official radiology report. In the subgroup where both clinical MRI and MAP were negative, the MRF‐ML models correctly distinguished FCD patients from HCs and DCs in 98.3% of cross‐validation trials for the magnetic resonance imaging negative group and MAP negative group. Type II versus non‐type‐II classification exhibited mean sensitivity, specificity, and accuracy of 0.835, 0.823, and 0.83, respectively; type IIa versus IIb classification showed 0.85, 0.9, and 0.87. In comparison, the transmantle sign was present in 58% (7/12) of the IIb cases.InterpretationThe MRF‐ML framework presented in this study demonstrated strong efficacy in noninvasively classifying FCD from normal cortex and distinguishing FCD subtypes. ANN NEUROL 2024

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Focal epilepsies: Update on diagnosis and classification

Nascimento

Friedman

Peters

et al. 2023

Epileptic Disorders

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Correctly diagnosing and classifying seizures and epilepsies is paramount to ensure the delivery of optimal care to patients with epilepsy. Focal seizures, defined as those that originate within networks limited to one hemisphere, are primarily subdivided into focal aware, focal impaired awareness, and focal to bilateral tonic-clonic seizures. Focal epilepsies account for most epilepsy cases both in children and adults. In children, focal epilepsies are typically subdivided in three groups: self-limited focal epilepsy syndromes (e.g., self-limited epilepsy with centrotemporal spikes), focal epilepsy of unknown cause but which do not meet criteria for a self-limited focal epilepsy syndrome, and focal epilepsy of known cause (e.g., structural lesions-developmental or acquired). In adults, focal epilepsies are often acquired and may be caused by a structural lesion such as stroke, infection and traumatic brain injury, or brain tumors, vascular malformations, metabolic disorders, autoimmune, and/or genetic causes. In addition to seizure semiology, neuroimaging, neurophysiology, and neuropathology constitute the cornerstones of a diagnostic evaluation. Patients with focal epilepsy who become drug-resistant should promptly undergo assessment in an epilepsy center. After excluding pseudo-resistance, these patients should be considered for presurgical evaluation as a means to identify the location and extent of the epileptogenic zone and assess their candidacy for a surgical procedure. The goal of this seminar in epileptology is to summarize clinically relevant information concerning focal epilepsies. This contributes to the ILAE's mission to ensure that worldwide healthcare professionals, patients, and caregivers continue to have access to highquality educational resources concerning epilepsy.

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Multilobar unilateral hypoplasia with emphasis on the posterior quadrant and severe epilepsy in children with FCD ILAE Type 1A

Cited by 17 publications

References 73 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

Multiparametric Characterization of Focal Cortical Dysplasia Using 3D MR Fingerprinting

Focal epilepsies: Update on diagnosis and classification

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