Article
Clinical Neurology
Jonai Pujol-Gimenez, Ghayda Mirzaa, Elizabeth E. Blue, Giuseppe Albano, Danny E. Miller, Aimee Allworth, James T. Bennett, Peter H. Byers, Sirisak Chanprasert, Jingheng Chen, Daniel Doherty, Andrew B. Folta, Madelyn A. Gillentine, Ian Glass, Anne Hing, Martha Horike-Pyne, Kathleen A. Leppig, Azma Parhin, Jane Ranchalis, Wendy H. Raskind, Elisabeth A. Rosenthal, Ulrike Schwarze, Sam Sheppeard, Samuel Strohbehn, Virginia P. Sybert, Andrew Timms, Mark Wener, Michael J. Bamshad, Fuki M. Hisama, Gail P. Jarvik, Katrina M. Dipple, Matthias A. Hediger, Andrew B. Stergachis
Summary: SLC1A4 is important for transporting L-serine from astrocytes into neurons. Biallelic variants in SLC1A4 cause SPATCCM syndrome, while heterozygous variants are not associated with disease. We identified a patient with developmental delay, spasticity, epilepsy, and microcephaly who had a de novo heterozygous three amino acid duplication in SLC1A4, resulting in a dominant-negative defect of the protein.
ANNALS OF CLINICAL AND TRANSLATIONAL NEUROLOGY
(2023)
Article
Neurosciences
Majida Charif, Yvette C. Wong, Soojin Kim, Agnes Guichet, Catherine Vignal, Xavier Zanlonghi, Philippe Bensaid, Vincent Procaccio, Dominique Bonneau, Patrizia Amati-Bonneau, Pascal Reynier, Dimitri Krainc, Guy Lenaers
Summary: Inherited optic neuropathies are the most common mitochondrial diseases, with neurodegeneration and loss of retinal ganglion cells being key characteristics. Mutations in the MIEF1 gene, which encodes the MID51 protein, have been identified as a cause for a rare form of late-onset progressive optic neuropathy. These mutations disrupt mitochondrial network dynamics without affecting MID51's localization or oligomerization on the outer mitochondrial membrane. Properly regulated mitochondrial dynamics play a crucial role in neurodegeneration.
MOLECULAR NEURODEGENERATION
(2021)
Review
Ophthalmology
Guy Lenaers, Albert Neutzner, Yannick Le Dantec, Christoph Juschke, Ting Xiao, Sarah Decembrini, Sebastian Swirski, Sinja Kieninger, Cavit Agca, Ungsoo S. Kim, Pascal Reynier, Patrick Yu-Wai-Man, John Neidhardt, Bernd Wissinger
Summary: Dominant optic atrophy is an inherited mitochondrial disease characterized by specific degeneration of retinal ganglion cells, primarily caused by OPA1 mutations. OPA1 is crucial for mitochondrial function, and understanding RGC peculiarities is important for studying DOA pathophysiology.
PROGRESS IN RETINAL AND EYE RESEARCH
(2021)
Article
Biology
Ethiraj Ravindran, Nobuto Arashiki, Lena-Luise Becker, Kohtaro Takizawa, Jonathan Levy, Thomas Rambaud, Konstantin L. Makridis, Yoshio Goshima, Na Li, Maaike Vreeburg, Benedicte Demeer, Achim Dickmanns, Alexander P. A. Stegmann, Hao Hu, Fumio Nakamura, Angela M. Kaindl
Summary: Variants in the CRMP1 gene are discovered to be associated with neurodevelopmental disorders such as muscular hypotonia, intellectual disability, and/or autism spectrum disorder. These variants may affect the protein structure and function of CRMP1, leading to alterations in cellular processes and neurite outgrowth.
Article
Medicine, General & Internal
Tao Zhang, Jingshan Bai, Xinyi Zhang, Xiaowei Zheng, Nan Lu, Zhongyin Liang, Ling Lin, Yongsong Chen
Summary: This study identified a novel heterozygous SNRNP200(c.C6088T) mutation that causes retinitis pigmentosa through a dominant-negative effect.
FRONTIERS IN MEDICINE
(2021)
Article
Genetics & Heredity
Lettie E. Rawlins, Hashem Almousa, Shazia Khan, Stephan C. Collins, Miroslav P. Milev, Joseph Leslie, Djenann Saint-Dic, Valeed Khan, Ana Maria Hincapie, Jacob O. Day, Lucy McGavin, Christine Rowley, Gaurav V. Harlalka, Valerie E. Vancollie, Wasim Ahmad, Christopher J. Lelliott, Asma Gul, Binnaz Yalcin, Andrew H. Crosby, Michael Sacher, Emma L. Baple
Summary: The research identified biallelic sequence alterations in the TRAPPC10 gene as a cause of severe microcephalic neurodevelopmental disorder, leading to reduced levels of TRAPPC9 and cellular transport defects. Wild type TRAPPC10 gene constructs were able to rescue the reduction in TRAPPC9 levels and the trafficking defect in cells. Studies in mice lacking the TRAPPC10 gene showed similar features to affected humans, confirming alterations in TRAPPC10 as a cause of microcephalic neurodevelopmental disorder.
Article
Clinical Neurology
Leonie von Elsner, Guoliang Chai, Pauline E. Schneeberger, Frederike L. Harms, Christian Casar, Minyue Qi, Malik Alawi, Ghada M. H. Abdel-Salam, Maha S. Zaki, Florian Arndt, Xiaoxu Yang, Valentina Stanley, Maja Hempel, Joseph G. Gleeson, Kerstin Kutsche
Summary: The peripheral protein FRA10AC1 of the spliceosomal C complex plays a crucial role in neurodevelopment, with mutations potentially leading to intellectual disabilities and other symptoms.
Article
Clinical Neurology
Pauline E. Schneeberger, Sheela Nampoothiri, Tess Holling, Dhanya Yesodharan, Malik Alawi, A. S. Knisely, Thomas Mueller, Barbara Plecko, Andreas R. Janecke, Kerstin Kutsche
Summary: GARP and EARP are membrane-tethering heterotetramers located at the trans-Golgi network and recycling endosomes, mediating retrograde transport and endocytic recycling. Patients with VPS50 variants exhibit severe developmental delay, microcephaly, seizures, and liver abnormalities.
Article
Cell Biology
Lin Yang, Xiuxiu Jin, Ya Li, Qingge Guo, Mingzhu Yang, Ya You, Shun Yao, Xiaoli Zhang, Zhongfeng Wang, Bo Lei
Summary: In this study, a novel pathogenic mutation in the AFG3L2 intermembrane space domain was identified in a family with DOA. The mutation may impair mitochondrial function and decrease the ability of AFG3L2 protein to enter the mitochondrial inner membrane, leading to protein degradation and reduced stability.
CELL DEATH DISCOVERY
(2022)
Article
Genetics & Heredity
Silvestre Cuinat, Mathilde Nizon, Bertrand Isidor, Alexander Stegmann, Richard H. van Jaarsveld, Koen L. van Gassen, Jasper J. van der Smagt, Catharina M. L. Volker-Touw, Sjoerd J. B. Holwerda, Paulien A. Terhal, Sarah Schuhmann, Georgia Vasileiou, Mohamed Khalifa, Alaa A. Nugud, Hemad Yasaei, Lilian Bomme Ousager, Charlotte Brasch-Andersen, Wallid Deb, Thomas Besnard, Marleen E. H. Simon, Karin Huijsdens-van Amsterdam, Nienke E. Verbeek, Dena Matalon, Natalie Dykzeul, Shana White, Elizabeth Spiteri, Koen Devriendt, Anneleen Boogaerts, Marjolein Willemsen, Han G. Brunner, Margje Sinnema, Bert B. A. De Vries, Erica H. Gerkes, Rolph Pfundt, Kosuke Izumi, Ian D. Krantz, Zhou L. Xu, Jill R. Murrell, Irene Valenzuela, Ivon Cusco, Eulalia Rovira-Moreno, Yaping Yang, Varoona Bizaoui, Olivier Patat, Laurence Faivre, Frederic Tran-Mau-Them, Antonio Vitobello, Anne-Sophie Denomme-Pichon, Christophe Philippe, Stephane Bezieau, Benjamin Cogne
Summary: This study reports an association between SRRM2 gene variants and a rare neurodevelopmental disorder. It includes 22 patients with loss-of-function variants and provides a description of the phenotype. The patients exhibited mild developmental delay, predominant speech delay, autistic or attention-deficit/hyperactivity disorder features, overfriendliness, generalized hypotonia, overweight, and dysmorphic facial features. The intellectual disability varied and was mild when present.
GENETICS IN MEDICINE
(2022)
Article
Biochemistry & Molecular Biology
Natalia Arruti, Patricia Rodriguez-Solana, Maria Nieves-Moreno, Marta Guerrero-Carretero, Angela del Pozo, Victoria E. F. Montano, Fernando Santos-Simarro, Emi Rikeros-Orozco, Luna Delgado-Mora, Elena Vallespin, Susana Noval
Summary: A clinical and genetic study was conducted to investigate the correlation between genotype and phenotype in pediatric patients with optic atrophy 1 (OPA1) mutations. Eleven children with confirmed OPA1 mutations were identified, with reduced visual acuity being the main complaint. Most patients had a positive family history of optic atrophy. The study found various mutations in the OPA1 gene, including one that has not been previously reported.
CURRENT ISSUES IN MOLECULAR BIOLOGY
(2023)
Article
Genetics & Heredity
Daniel L. Polla, Mohammad Ali Farazi Fard, Zahra Tabatabaei, Parham Habibzadeh, Olga A. Levchenko, Pooneh Nikuei, Periklis Makrythanasis, Mureed Hussain, Sandra von Hardenberg, Sirous Zeinali, Mohammad-Sadegh Fallah, Janneke H. M. Schuurs-Hoeijmakers, Mohsin Shahzad, Fareeha Fatima, Neelam Fatima, Laura Donker Kaat, Hennie T. Bruggenwirth, Leah R. Fleming, John Condie, Rafal Ploski, Agnieszka Pollak, Jacek Pilch, Nina A. Demina, Alena L. Chukhrova, Vasilina S. Sergeeva, Hanka Venselaar, Amira T. Masri, Hanan Hamamy, Federico A. Santoni, Katrin Linda, Zubair M. Ahmed, Nael Nadif Kasri, Arjan P. M. de Brouwer, Anke K. Bergmann, Sven Hethey, Majid Yavarian, Muhammad Ansar, Saima Riazuddin, Sheikh Riazuddin, Mohammad Silawi, Gaia Ruggeri, Filomena Pirozzi, Ebrahim Eftekhar, Afsaneh Taghipour Sheshdeh, Shima Bahramjahan, Ghayda M. Mirzaa, Alexander V. Lavrov, Stylianos E. Antonarakis, Mohammad Ali Faghihi, Hans van Bokhoven
Summary: The study identified biallelic variants in the TMEM222 gene as a novel underlying cause of an autosomal recessive neurodevelopmental disorder in 17 individuals from nine unrelated families. Further investigation revealed relatively high levels of TMEM222 expression in the human brain, particularly in the parietal and occipital cortex, with subcellular localization analysis showing TMEM222 localizing to early endosomes in synapses of mature neurons.
GENETICS IN MEDICINE
(2021)
Article
Health Care Sciences & Services
Youn Jung Kim, Yejin Lee, Wonseon Chae, Jung-Wook Kim
Summary: In this study, two families with amelogenesis imperfecta (AI) were recruited and mutational analysis was performed using whole-exome sequencing. Different mutation genes were identified by analyzing the genetic variations of the patients, providing insights into the genetic mechanisms of AI.
JOURNAL OF PERSONALIZED MEDICINE
(2023)
Article
Genetics & Heredity
Yanxin Wang, Yuqiang Lv, Zilong Li, Min Gao, Xiaomeng Yang, Yue Li, Jianguo Shi, Zaifen Gao, Yi Liu, Zhongtao Gai
Summary: This study investigated SYNGAP1 mutations in a clinical cohort with intellectual disability and developmental delay in Shandong, China. Ten unrelated affected individuals were found to carry SYNGAP1 mutations, with all mutations being de novo. Five novel genetic mutations were identified, expanding the mutational spectrum of the SYNGAP1 gene.
FRONTIERS IN GENETICS
(2022)
Article
Medical Laboratory Technology
Shimeng Chen, Xiaolu Deng, Juan Xiong, Fang He, Lifen Yang, Baiyu Chen, Chen Chen, Ciliu Zhang, Li Yang, Jing Peng, Fei Yin
Summary: This study explored the clinical and genetic characteristics of Chinese patients with de novo DEAF1 variants. The patients exhibited intellectual disability, language delay, and behavior problems. Interestingly, the DEAF1-related epilepsy in Eastern-Asian individuals was found to be completely treatable. The study expanded the knowledge of DEAF1-related neurodevelopmental disorder and the de novo variant database of DEAF1.
CLINICA CHIMICA ACTA
(2021)
Article
Clinical Neurology
Christelle M. Durand, Chloe Angelini, Vincent Michaud, Claire Delleci, Isabelle Coupry, Cyril Goizet, Aurelien Trimouille
Summary: This study identified the genetic etiology of a patient with early onset sporadic progressive spastic ataxia and investigated the pathogenicity of VPS13D variants through functional studies. The findings confirmed the role of VPS13D in spastic ataxia and provided support for mitochondrial defects in patient's skin fibroblasts with VPS13D variants. The functional studies performed in this study could serve as biomarkers for diagnosis of VPS13D-related neurological disorders.
Article
Clinical Neurology
Jean-Loup Mereaux, Guillaume Banneau, Melanie Papin, Giulia Coarelli, Remi Valter, Laure Raymond, Bophara Kol, Olivier Ariste, Livia Parodi, Laurene Tissier, Mathilde Mairey, Samia Ait Said, Celia Gautier, Marine Guillaud-Bataille, Sylvie Forlani, Pierre de la Grange, Alexis Brice, Giovanni Vazza, Alexandra Durr, Eric Leguern, Giovanni Stevanin
Summary: This study reports the clinical and genetic results of a large cohort of patients with hereditary spastic paraplegia. A causative variant was found in 30.7% of the patients, with SPAST and SPG7 being the most frequently mutated genes. A two-step strategy combining gene panels and whole-exome sequencing is proposed to improve the diagnostic yield.
Article
Genetics & Heredity
Benjamin Billiet, Patrizia Amati-Bonneau, Valerie Desquiret-Dumas, Khadidja Guehlouz, Dan Milea, Philippe Gohier, Guy Lenaers, Delphine Mirebeau-Prunier, Johan T. den Dunnen, Pascal Reynier, Marc Ferre
Summary: A public database for NR2F1 gene was established to refine the clinical description of BBSOAS, suggesting additional signs and features for neurological and motor functions.
Article
Health Care Sciences & Services
Ioanna Pyromali, Nesrine Benslimane, Frederic Favreau, Cyril Goizet, Leila Lazaro, Martine Vitry, Paco Derouault, Franck Sturtz, Corinne Magdelaine, Anne-Sophie Lia
Summary: Next-generation sequencing (NGS) has increased the ability to diagnose patients through the detection of numerous mutations, however, structural variations (SVs) such as copy number variants (CNVs) are often overlooked. This study presents a personalized approach for the positive diagnosis of a patient with demyelinating Charcot-Marie-Tooth disease (CMT) using NGS data and specialized software to detect CNVs. This approach revealed the presence of a previously undetected mutation in SH3TC2, highlighting the importance of systematically searching for SVs in peripheral neuropathy diagnoses.
JOURNAL OF PERSONALIZED MEDICINE
(2022)
Article
Genetics & Heredity
Al Mehdi Krami, Aymane Bouzidi, Majida Charif, Ghita Amalou, Hicham Charoute, Hassan Rouba, Rachida Roky, Guy Lenaers, Abdelhamid Barakat, Halima Nahili
Summary: Intellectual disability is a condition characterized by impaired intellectual and adaptive functioning, affecting approximately 1-3% of the population. Recent research has found that mutations in the HECW2 gene are associated with neurodevelopmental disorders such as hypotonia, seizures, and absent language. HECW2 encodes an enzyme that plays a role in brain development by regulating key factors involved in proliferation, apoptosis, and neuronal differentiation. This study identified a homozygous HECW2 mutation in a Moroccan family, inherited in an autosomal recessive pattern, contrasting with previous findings of de novo mutations in HECW2 patients.
EUROPEAN JOURNAL OF MEDICAL GENETICS
(2022)
Article
Clinical Neurology
Giulia Coarelli, Anna Heinzmann, Claire Ewenczyk, Clara Fischer, Marie Chupin, Marie-Lorraine Monin, Hortense Hurmic, Fabienne Calvas, Patrick Calvas, Cyril Goizet, Stephane Thobois, Mathieu Anheim, Karine Nguyen, David Devos, Christophe Verny, Vito A. G. Ricigliano, Jean-Francois Mangin, Alexis Brice, Sophie Tezenas du Montcel, Alexandra Durr
Summary: A randomized, double-blind, placebo-controlled trial was conducted in France to assess the effectiveness of riluzole in patients with spinocerebellar ataxia type 2, involving 45 moderately affected patients. The study found that riluzole did not show improvement in clinical or radiological outcomes in these patients, but provided valuable data for the design of future clinical trials.
Review
Genetics & Heredity
Aymane Bouzidi, Hicham Charoute, Majida Charif, Ghita Amalou, Mostafa Kandil, Abdelhamid Barakat, Guy Lenaers
Summary: Inherited retinal dystrophies (IRD) and optic neuropathies (ION) are major causes of visual impairment worldwide, but there is a lack of accurate epidemiological studies and comprehensive genetic research in North Africa.
ORPHANET JOURNAL OF RARE DISEASES
(2022)
Review
Nutrition & Dietetics
Valentin Lacombe, Guy Lenaers, Geoffrey Urbanski
Summary: Cobalamin and transcobalamins play important roles in cancer development, affecting cellular metabolism and being associated with cancer diagnosis and prognosis.
Article
Biochemistry & Molecular Biology
Ahmad Chehaitly, Anne-Laure Guihot, Coralyne Proux, Linda Grimaud, Jade Aurriere, Benoit Legouriellec, Jordan Rivron, Emilie Vessieres, Clement Tetaud, Antonio Zorzano, Vincent Procaccio, Francoise Joubaud, Pascal Reynier, Guy Lenaers, Laurent Loufrani, Daniel Henrion
Summary: The reduction in mitochondrial fusion in mouse endothelial cells was found to impair the dilator response to shear stress, leading to excessive superoxide production and promoting greater atherosclerosis development.
Article
Multidisciplinary Sciences
C. Liautard-Haag, G. Durif, C. VanGoethem, D. Baux, A. Louis, L. Cayrefourcq, M. Lamairia, M. Willems, C. Zordan, V. Dorian, C. Rooryck, C. Goizet, A. Chaussenot, L. Monteil, P. Calvas, C. Miry, R. Favre, E. Le Boette, M. Fradin, A. F. Roux, M. Cossee, M. Koenig, C. Alix-Panabiere, C. Guissart, M. C. Vincent
Summary: The field of noninvasive prenatal diagnosis (NIPD) has made significant progress, but technical issues remain for triplet-repeat expansions. This study developed an NIPD approach for couples at risk of transmitting dynamic mutations and showed that linked-read sequencing and parental haplotype phasing can be successfully used for NIPD of triplet-repeat expansion diseases.
SCIENTIFIC REPORTS
(2022)
Review
Biochemistry & Molecular Biology
Florian Beignon, Naig Gueguen, Helene Tricoire-Leignel, Cesar Mattei, Guy Lenaers
Summary: Understanding temperature production and regulation in endotherm organisms is a crucial challenge. Mitochondria can act as cellular radiators, controlling heat production and cell temperature. Considering these new thermic paradigms, we discuss conventional wisdom linking mitochondrial functions to cellular thermogenesis.
CELLULAR AND MOLECULAR LIFE SCIENCES
(2022)
Article
Urology & Nephrology
Hugo Bakis, Aurelien Trimouille, Agathe Vermorel, Cyril Goizet, Yaniss Belaroussi, Sacha Schutz, Guilhem Sole, Christian Combe, Marie-Laure Martin-Negrier, Claire Rigothier
Summary: Adults with mitochondrial disorders (MIDs) can also develop mitochondrial disorder-associated nephropathies (MIDANs), which are characterized by tubulointerstitial nephropathy or glomerular disease. Hypertension, albumin level, and vision abnormalities are associated with MIDANs.
CLINICAL KIDNEY JOURNAL
(2023)
Article
Biochemistry & Molecular Biology
Jean-Baptiste Domergue, Cinzia Bocca, Rosine De Paepe, Guy Lenaers, Anis M. Limami, Guillaume Tcherkez
Summary: Disruption of mitochondrial complex I (CI) has been found to cause multiple changes in cellular lipids, including leaf, pollen, and seed lipids. This suggests that mitochondrial homeostasis plays a crucial role in regulating the whole cellular lipidome through specific signaling pathways.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2023)
Article
Endocrinology & Metabolism
Rahma Felhi, Lamia Sfaihi, Majida Charif, Fakher Frikha, Nissaf Aoiadni, Thouraya Kamoun, Guy Lenaers, Faiza Fakhfakh
Summary: Leigh syndrome (LS) and Leigh-like spectrum are common mitochondrial disorders in infants, caused by pathogenic variants in SLC carriers. A homozygous c.1264 A > G (p.T422A) variant in SLC19A3 was identified in a patient with LS from a consanguineous Tunisian family. This variant affects vitamin-B1 transport, induces mtDNA depletion, and reduces the expression of oxidative stress enzymes, contributing to the LS phenotype.
METABOLIC BRAIN DISEASE
(2023)
Meeting Abstract
Clinical Neurology
Ioanna Pyromali, Nesrine Benslimane, Federica Miressi, Frederic Favreau, Pierre-Antoine Faye, Cyril Goizet, Leila Lazaro, Martine Vitry, Paco Derouault, Sylvie Bourthoumieu, Marie Husson, Franck Sturtz, Corinne Magdelaine, Anne-Sophie Lia
JOURNAL OF THE PERIPHERAL NERVOUS SYSTEM
(2022)
