Article
Clinical Neurology
Shehrazade Dahimene, Leonie von Elsner, Tess Holling, Lauren S. Mattas, Jess Pickard, Davor Lessel, Kjara S. Pilch, Ivan Kadurin, Wendy S. Pratt, Igor B. Zhulin, Hongzheng Dai, Maja Hempel, Maura R. Z. Ruzhnikov, Kerstin Kutsche, Annette C. Dolphin
Summary: This study reports biallelic variants in CACNA2D1 causing developmental and epileptic encephalopathy in two unrelated individuals. Patient 1 showed a frameshift variant leading to nonsense-mediated mRNA decay and absence of alpha(2)delta-1 protein. Patient 2 exhibited a compound heterozygous with a frameshift variant likely representing a null allele and a missense variant severely impairing the function of alpha(2)delta-1 as a calcium channel subunit.
Review
Biochemistry & Molecular Biology
Carlotta Spagnoli, Carlo Fusco, Antonio Percesepe, Vincenzo Leuzzi, Francesco Pisani
Summary: Despite advancements in next generation sequencing technologies and increased clinical interest in complex neurological phenotypes associating epilepsies and developmental/epileptic encephalopathies (DE/EE) with movement disorders (MD), monogenic conditions characterized by neonatal onset epilepsy and/or DE/EE with development of an MD have been less extensively studied in the neonatal period compared to infancy. High genetic heterogeneity and low numbers of described patients were found in this review, with complex neurological phenotypes reflecting the involvement of genes crucial for early brain development. Future studies should focus on accurate neonatal epileptic phenotyping and detailed description of semiology and time-course of the associated movement disorders, especially for the rarest conditions.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2021)
Article
Clinical Neurology
Stephanie Efthymiou, Marina Dutra-Clarke, Reza Maroofian, Rauan Kaiyrzhanov, Marcello Scala, Javeria Reza Alvi, Tipu Sultan, Marilena Christoforou, Thi Tuyet Mai Nguyen, Kshitij Mankad, Barbara Vona, Aboulfazl Rad, Pasquale Striano, Vincenzo Salpietro, Maria J. Guillen Sacoto, Maha S. Zaki, Joseph G. Gleeson, Philippe M. Campeau, Bianca E. Russell, Henry Houlden
Summary: The study identified previously unreported variants in the PIGS gene that cause a novel congenital disorder of glycosylation resulting in severe symptoms such as global developmental delay and epilepsy, expanding the understanding of the genotype and phenotype of PIGS-related disorders. This highlights the importance of delineating the molecular spectrum of PIGS-related disorders for improved management, treatment development, and diagnostic testing expansion.
Article
Behavioral Sciences
Guihai Suo, Xing Cao, Yuqin Zheng, Haiying Li, Qi Zhang, Jihong Tang, Youjia Wu
Summary: Mutations in STXBP1 gene are associated with neurodevelopmental disorders and early-onset epileptic encephalopathies. Using a zebrafish model with mutant STXBP1, researchers demonstrated clinical phenotypes related to human STXBP1 mutation and evaluated antiepileptic drugs effects on seizures.
EPILEPSY & BEHAVIOR
(2021)
Article
Behavioral Sciences
Mary E. Moya-Mendez, David M. Mueller, Milton Pratt, Melanie Bonner, Courtney Elliott, Arsen Hunanyan, Gary Kucera, Cheryl Bock, Lyndsey Prange, Joan Jasien, Karen Keough, Vandana Shashi, Marie McDonald, Mohamad A. Mikati
Summary: ATP1A2 mutations can cause early-onset severe epileptic encephalopathy, leading to symptoms such as drug-resistant seizures and developmental delay. Memantine therapy, an NMDA receptor antagonist, showed tolerability and some improvements in patients with ATP1A2 mutations. Future studies on NMDAR antagonist therapy in ATP1A2-encephalopathy are warranted.
EPILEPSY & BEHAVIOR
(2021)
Article
Cell & Tissue Engineering
Manting Xu, Xin Duan, Xiaotun Ren, Zhimei Liu, Shuhua Chen, Fang Fang
Summary: In this study, an iPSC line carrying a homozygous mutation in the CARS2 gene was generated from HDFs of a one-year-old boy with EOEE. Through the characterization of the iPSCs, it was found that the CARS2 mutation was associated with EOEE, providing a model for further research on the disease.
STEM CELL RESEARCH
(2022)
Article
Clinical Neurology
Xianyu Liu, Qiyang Shen, Guo Zheng, Hu Guo, Xiaopeng Lu, Xiaoyu Wang, Xiao Yang, Zixuan Cao, Jing Chen
Summary: NGS has revealed genetic causes of epileptic encephalopathy in Chinese children, with pathogenic variants identified in 34% of the cohort. The phenotypes of genes with pathogenic variants were diverse, and early diagnosis through NGS may lead to precise therapeutic interventions and potentially improve developmental outcomes.
FRONTIERS IN NEUROLOGY
(2021)
Review
Biochemistry & Molecular Biology
Carlotta Spagnoli, Carlo Fusco, Francesco Pisani
Summary: Genetic early-onset Parkinsonism in children can be classified into several distinct presentations, including Parkinsonism as a late manifestation of complex neurodevelopmental disorders, syndromic conditions with reduced seizure threshold, neurodegenerative conditions with brain iron accumulation, and monogenic juvenile Parkinsonism. These conditions often involve epilepsy or developmental and epileptic encephalopathies (DE-EE) in childhood, highlighting the importance of long-term follow-up in individuals with intellectual disability or developmental delay (ID/DD) to identify those at increased risk of later Parkinsonism.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2023)
Review
Pharmacology & Pharmacy
Kenneth A. Myers, Ingrid E. Scheffer
Summary: Epilepsy is a genetically heterogeneous condition, with genetic factors playing a role in most patients. Over 50% of patients with infantile-onset developmental and epileptic encephalopathy (DEE) now have a genetic diagnosis. Precision medicine approaches have the potential to significantly improve the quality of life for these children and their families.
ANNUAL REVIEW OF PHARMACOLOGY AND TOXICOLOGY
(2022)
Review
Clinical Neurology
Yi Liu, Chih-Wei Wang, Yueh-Feng Sung, Fu-Chi Yang
Summary: Susac syndrome is a rare disease with a classic triad of symptoms, including sensorineural hearing loss, encephalopathy, and branch retinal artery occlusions. Early symptoms may lead to misdiagnosis, making neurological and retinal examinations crucial for accurate diagnosis. Case reviews and treatment guidelines are available for Susac syndrome presenting as sudden sensorineural hearing loss.
NEUROLOGICAL SCIENCES
(2022)
Article
Genetics & Heredity
Anca-Lelia Riza, Ioana Streata, Eugenia Roza, Magdalena Budisteanu, Catrinel Iliescu, Carmen Burloiu, Mihaela-Amelia Dobrescu, Stefania Dorobantu, Adina Dragos, Andra Grigorescu, Tiberiu Tataru, Mihai Ioana, Raluca Teleanu
Summary: This study conducted genetic testing on 36 Romanian patients and found a 25% diagnostic rate for known gene variants associated with epilepsy syndromes. The study emphasizes the importance of comprehensive clinical phenotyping in variant interpretation and highlights the significance of genetic assessment for the diagnosis and management of early-onset DEE patients.
Article
Multidisciplinary Sciences
Lauri Weman, Henri Salo, Laura Kuusalo, Johanna Huhtakangas, Johanna Karki, Paula Vahasalo, Maria Backstrom, Tuulikki Sokka-Isler
Summary: The study aims to assess the joint distribution and clinical presentation of rheumatoid arthritis (RA) in seropositive and negative patients at the initial stage, as well as the impact of symptom duration on the clinical picture. The results showed that symmetrical swelling was observed in 75% of the patients. Seronegative patients had higher values for disease activity measures and patient reported outcomes (PROs) compared to seropositive patients. Patients diagnosed within three months had more severe pain and functional impairment, while those diagnosed after six months were more likely to be ACPA-positive.
Article
Clinical Neurology
Annalisa Vetro, Hang N. Nielsen, Rikke Holm, Robert F. Hevner, Elena Parrini, Zoe Powis, Rikke S. Moller, Cristina Bellan, Alessandro Simonati, Gaetan Lesca, Katherine L. Helbig, Elizabeth E. Palmer, Davide Mei, Elisa Ballardini, Arie Van Haeringen, Steffen Syrbe, Vincenzo Leuzzi, Giovanni Cioni, Cynthia J. Curry, Gregory Costain, Margherita Santucci, Karen Chong, Grazia M. S. Mancini, Jill Clayton-Smith, Stefania Bigoni, Ingrid E. Scheffer, William B. Dobyns, Bente Vilsen, Renzo Guerrini
Summary: Constitutional heterozygous mutations of ATP1A2 and ATP1A3 have been associated with various neurological disorders, including familial hemiplegic migraine and alternating hemiplegia of childhood. This study identified 22 patients with de novo or inherited heterozygous mutations in ATP1A2 or ATP1A3, leading to severe and novel phenotypes of developmental and epileptic encephalopathies. Mutations in these genes resulted in impaired NKA-pump activity and a wide range of severity in phenotype, indicating a complex genotype-phenotype relationship.
Article
Medicine, General & Internal
Xiaoyu Tian, Yange Zhang, Jinhong Zhang, Yan Lu, Xinyi Men, Xiuxia Wang
Summary: Research has shown that mutations in the SCN2A gene are associated with developmental delays and infantile seizures in patients with EOEEs. This case report highlights the effectiveness of a ketogenic diet in managing medically refractory seizures caused by a de novo SCN2A mutation in an infant. Personalized genomics can play a crucial role in identifying the etiology of illnesses, and the ketogenic diet may be a feasible and effective treatment option for EOEE associated with SCN2A mutations in infants younger than 2 months old.
YONSEI MEDICAL JOURNAL
(2021)
Article
Clinical Neurology
Lin Li, Zili Liu, Haiyang Yang, Yang Li, Qi Zeng, Li Chen, Yidi Liu, Yan Chen, Fengjun Zhu, Dezhi Cao, Jun Hu, Xuefeng Shen
Summary: This study identified two novel KCNC2 variants in patients with early onset developmental and epileptic encephalopathy, providing evidence supporting the role of KCNC2 as a disease-causing gene in human neurodevelopmental delay and epilepsy.
SEIZURE-EUROPEAN JOURNAL OF EPILEPSY
(2022)
Review
Pediatrics
M- Andre, P. Cacciagli, A. Cano, L. Vaugier, M. Roussel, N. Girard, B. Chabrol, L. Villard, M. Milh
Summary: We present the case of a patient with developmental and epileptic encephalopathy due to a homozygous pathogenic variant of mitochondrial glutamate/H+ symporter SLC25A22. The patient started experiencing focal onset seizures in the first week of life, with interictal EEG showing a suppression-burst pattern. Long-term follow-up revealed ongoing active epilepsy and almost no developmental progress by 8 years of age, confirming the severe consequences of SLC25A22 recessive variations. This study provides insight into a rare genetic cause of neonatal onset epilepsy.
ARCHIVES DE PEDIATRIE
(2021)
Article
Biochemistry & Molecular Biology
Sandra Whalen, Marie Shaw, Cyril Mignot, Delphine Heron, Sandra Chantot Bastaraud, Cecile Cieuta Walti, Jan Liebelt, Frances Elmslie, Patrick Yap, Jane Hurst, Elisabeth Forsythe, Brian Kirmse, Jillian Ozmore, Alessandro Mauro Spinelli, Olga Calabrese, Thierry Billette de Villemeur, Anne Claude Tabet, Jonathan Levy, Agnes Guet, Manoelle Kossorotoff, Benjamin Kamien, Jenny Morton, Anne McCabe, Elise Brischoux-Boucher, Annick Raas-Rothschild, Antonella Pini, Renee Carroll, Jessica N. Hartley, Patrick Frosk, Anne Slavotinek, Kristen Truxal, Carroll Jennifer, Annelies Dheedene, Hong Cui, Vishal Kumar, Glen Thomson, Florence Riccardi, Jozef Gecz, Laurent Villard
Summary: The BCAP31 gene, located at Xq28, encodes BAP31, which plays a role in ER-to-Golgi anterograde transport. Pathogenic variants in BCAP31 can result in severe intellectual disability, dystonia, deafness, and central hypomyelination. Deletions involving BCAP31 and adjacent genes may lead to a more severe neurological phenotype.
EUROPEAN JOURNAL OF HUMAN GENETICS
(2021)
Article
Genetics & Heredity
Marion Aubert Mucca, Olivier Patat, Sandra Whalen, Lionel Arnaud, Giulia Barcia, Julien Buratti, Benjamin Cogne, Diane Doummar, Caroline Karsenty, Sandra Kenis, Eric Leguern, Gaetan Lesca, Caroline Nava, Mathilde Nizon, Amelie Piton, Stephanie Valence, Laurent Villard, Sarah Weckhuysen, Boris Keren, Cyril Mignot
Summary: De novo missense variants in KCNH1 cause Temple-Baraitser syndrome (TBS) and Zimmermann-Laband syndrome (ZLS), which overlap clinically and suggest a spectrum of KCNH1-related encephalopathies. Affected patients exhibit severe intellectual disability, hypertrichosis, and distinctive features such as gingival hyperplasia and nail hypoplasia/aplasia. A study identified pathogenic KCNH1 variants in patients with atypical features expanding the phenotypical spectrum of KCNH1-related encephalopathies.
JOURNAL OF MEDICAL GENETICS
(2022)
Article
Genetics & Heredity
Lionel Arnaud, Marie-Therese Abi Warde, Giulia Barcia, Julitta de Bellescize, Nicolas Chatron, Marie Faoucher, Anne de Saint Martin, Delphine Heron, Guillaume Jedraszak, Caroline Lacoste, Anne-Sophie Lebre, Melanie Jenneson-Lyver, Audrey Labalme, Eric Leguern, Cyril Mignot, Mathieu Milh, Rima Nabbout, Caroline Nava, Eleni Panagiotakaki, Amelie Piton, Elise Schaefer, Julien Thevenon, Laurent Villard, Dorothee Ville, Gaetan Lesca
Summary: The EPIGENE network, consisting of geneticists, pediatric neurologists, and specialists in epileptology, aims to improve the diagnostic strategy for Mendelian epileptic disorders in France. Their gene panel approach has shown positive results, with a diagnostic yield of 31% for epileptic patients. Whole-genome sequencing is expected to be implemented as a second-line screening method in the near future, benefiting French patients with drug-resistant epilepsies.
EUROPEAN JOURNAL OF MEDICAL GENETICS
(2022)
Article
Genetics & Heredity
Stefanie Brock, Annie Laquerriere, Florent Marguet, Scott J. Myers, Yuan Hongjie, Diana Baralle, Tim Vanderhasselt, Katrien Stouffs, Kathelijn Keymolen, Sukhan Kim, James Allen, Gil Shaulsky, Jamel Chelly, Pascale Marcorelle, Jacqueline Aziza, Laurent Villard, Elise Sacaze, Marie C. Y. de Wit, Martina Wilke, Grazia Maria Simonetta Mancini, Ute Hehr, Derek Lim, Sahar Mansour, Stephen F. Traynelis, Claire Beneteau, Marie Denis-Musquer, Anna C. Jansen, Andrew E. Fry, Nadia Bahi-Buisson
Summary: This study aimed to further define the phenotypic spectrum of NMDAR-related malformations of cortical development (MCDs). Clinical, radiological, and molecular features of new and previously reported patients were analyzed and neuropathological findings were presented. The study provides new insights into the clinical and imaging features of NMDAR-related MCDs and contributes to our understanding of the underlying pathogenic mechanisms.
JOURNAL OF MEDICAL GENETICS
(2023)
Article
Neurosciences
Najoua Biba-Maazou, Helene Becq, Emilie Pallesi-Pocachard, Stefania Sarno, Samuel Granjeaud, Aurelie Montheil, Marie Kurz, Laurent Villard, Mathieu Milh, Pierre-Pascal Lenck Santini, Laurent Aniksztejn
Summary: Mutations in the KCNQ2 gene can cause developmental and epileptic encephalopathy, affecting the electrophysiological properties of brain cells at different developmental stages, but the effects vary during the course of development.
JOURNAL OF PHYSIOLOGY-LONDON
(2022)
Review
Clinical Neurology
Pierre-Yves Maillard, Sarah Baer, Elise Schaefer, Beatrice Desnous, Nathalie Villeneuve, Anne Lepine, Alexandre Fabre, Caroline Lacoste, Salima El Chehadeh, Amelie Piton, Louise Frances Porter, Caroline Perriard, Marie-Therese Abi Warde, Marie-Aude Spitz, Vincent Laugel, Gaetan Lesca, Audrey Putoux, Dorothee Ville, Cyril Mignot, Delphine Heron, Rima Nabbout, Giulia Barcia, Marlene Rio, Agathe Roubertie, Pierre Meyer, Veronique Paquis-Flucklinger, Olivier Patat, Jeremie Lefranc, Marion Gerard, Julietta de Bellescize, Laurent Villard, Anne De Saint Martin, Mathieu Milh
Summary: This study describes the phenotypes associated with GABA(A)-receptor subunit variants and investigates potential genotype-phenotype correlations. The results show that despite the similarities in molecular structure and physiological role, GABA(A)-receptor subunit variants are associated with highly variable phenotypes. Furthermore, the location of the variant on the protein may be a marker of severity.
Review
Clinical Neurology
Lucile Brun, Jean-Charles Viemari, Laurent Villard
Summary: Variants in the KCNQ2 gene can cause epileptic disorders of different severities, but the biological mechanisms are still unclear. Previous studies using KCNQ2 models have helped to elucidate the pathological mechanisms and identify new therapeutic targets.
Article
Multidisciplinary Sciences
Elsa Leitao, Christopher Schroeder, Ilaria Parenti, Carine Dalle, Agnes Rastetter, Theresa Kuehnel, Alma Kuechler, Sabine Kaya, Benedicte Gerard, Elise Schaefer, Caroline Nava, Nathalie Drouot, Camille Engel, Juliette Piard, Benedicte Duban-Bedu, Laurent Villard, Alexander P. A. Stegmann, Els K. Vanhoutte, Job A. J. Verdonschot, Frank J. Kaiser, Frederic Tran Mau-Them, Marcello Scala, Pasquale Striano, Suzanna G. M. Frints, Emanuela Argilli, Elliott H. Sherr, Fikret Elder, Julien Buratti, Boris Keren, Cyril Mignot, Delphine Heron, Jean-Louis Mandel, Jozef Gecz, Vera M. Kalscheuer, Bernhard Horsthemke, Amelie Piton, Christel Depienne
Summary: This study predicts gene-disease associations on the X chromosome using known disease gene features and machine learning techniques.
NATURE COMMUNICATIONS
(2022)
Article
Obstetrics & Gynecology
Raphaelle Eydoux, Emmanuelle Lesieur, Julie Blanc, Nadine Girard, Claude D'Ercole, Sabine Sigaudy, Kathia Chaumoitre, Florence Bretelle
Summary: The study aimed to evaluate the relevance of fetal brain MRI in cases of cleft lip and/or palate. The results showed that MRI could detect severe abnormalities in cases of clefts associated with other anomalies, leading to changed prognoses. However, for isolated cleft lip cases, MRI only found minor abnormalities and no postnatal disorders were found in these children.
FETAL DIAGNOSIS AND THERAPY
(2023)
Article
Cell Biology
Ilaria Parenti, Elsa Leitao, Alma Kuechler, Laurent Villard, Cyril Goizet, Cecile Courdier, Allan Bayat, Alessandra Rossi, Sophie Julia, Ange-Line Bruel, Frederic Tran Mau-Them, Sophie Nambot, Daphne Lehalle, Marjolaine Willems, James Lespinasse, Jamal Ghoumid, Roseline Caumes, Thomas Smol, Salima El Chehadeh, Elise Schaefer, Marie-Therese Abi-Warde, Boris Keren, Alexandra Afenjar, Anne-Claude Tabet, Jonathan Levy, Anna Maruani, Angel Aledo-Serrano, Waltraud Garming, Clara Milleret-Pignot, Anna Chassevent, Marije Koopmans, Nienke E. Verbeek, Richard Person, Rebecca Belles, Gary Bellus, Bonnie A. Salbert, Frank J. Kaiser, Laure Mazzola, Philippe Convers, Laurine Perrin, Amelie Piton, Gert Wiegand, Andrea Accogli, Francesco Brancati, Fabio Benfenati, Nicolas Chatron, David Lewis-Smith, Rhys H. Thomas, Federico Zara, Pasquale Striano, Gaetan Lesca, Christel Depienne
Summary: This study expands on the clinical and molecular spectrum of SYN1-related neurodevelopmental disorders and provides analysis on the association between these disorders and features such as epilepsy and intellectual disability. Additionally, the study reveals an association between early seizure onset and more severe impairment of cognitive functions.
FRONTIERS IN CELL AND DEVELOPMENTAL BIOLOGY
(2022)
Article
Clinical Neurology
Cecile Mignon-Ravix, Florence Riccardi, Geraldine Daquin, Pierre Cacciagli, Sylvie Lamoureux-Toth, Laurent Villard, Nathalie Villeneuve, Florence Molinari
Summary: Developmental and epileptic encephalopathies (DEE) are a group of neurodevelopmental disorders characterized by epileptic seizures associated with developmental delay or regression. We identified a novel homozygous protein-truncating variant in the NAPB gene that encodes the beta SNAP protein. Our findings strengthen the association between biallelic variants in NAPB and DEE and suggest including this gene in the targeted epilepsy gene panels used for routine diagnosis of unexplained epilepsy.
Article
Genetics & Heredity
Mario Abaji, Cecile Mignon-Ravix, Svetlana Gorokhova, Pierre Cacciagli, Jeremie Mortreux, Florence Molinari, Brigitte Chabrol, Sabine Sigaudy, Laurent Villard, Florence Riccardi
Summary: The TRAPP complexes are involved in intracellular transport and are related to ultra-rare human diseases called TRAPPopathies. Pathogenic variants in 8 genes encoding TRAPP proteins have been associated with neurodevelopmental disorders. This report describes a new protein-truncating variant in the TRAPPC2L gene found in two affected siblings, providing important genetic evidence and insights into the TRAPPC2L phenotype. The TRAPPC2L syndrome is characterized by severe neurodevelopmental disorder and variable muscle involvement, suggesting it belongs to the clinical entity of rare congenital muscular dystrophies.
JOURNAL OF MEDICAL GENETICS
(2023)
Article
Radiology, Nuclear Medicine & Medical Imaging
Sameer Omer Jin, Ines Merida, Ioannis Stavropoulos, Robert D. C. Elwes, Tanya Lam, Eric Guedj, Nadine Girard, Nicolas Costes, Alexander Hammers
Summary: This study compared two different databases of [F-18]FDG PET data and achieved a higher abnormality detection rate by adjusting spatial resolution and global values. The results demonstrate the importance of increasing database size and overcoming database differences, which can be applicable to traditional statistical analysis or machine learning, as well as clinical implementation.
Meeting Abstract
Biochemistry & Molecular Biology
Maude Vecten, Emmanuelle Pion, Raul Juntas Morales, Damien Sternberg, John Rendu, Tania Stojkovic, Cecile Acquaviva-Bourdain, Corrine Metay, Isabelle Richard, Laurent Villard, Mathieu Cerino, Mathieu Milh, Sevtlana Gorokhova, Nicolas Levy, Xenia Martin, Gisele Bonne, Valerie Biancalana, Francois Petit, Aurelien Perrin, Pascal Laforet, Marc Bartoli, Mireille Cossee, Martin Krahn
EUROPEAN JOURNAL OF HUMAN GENETICS
(2022)
