Your search keyword '"Danzi, Matt"' showing total 241 results

1. Spinocerebellar ataxia 27B: a frequent and slowly progressive autosomal-dominant cerebellar ataxia—experience from an Italian cohort

Author

Satolli, Sara, Rossi, Salvatore, Vegezzi, Elisa, Pellerin, David, Manca, Maria Laura, Barghigiani, Melissa, Battisti, Carla, Bilancieri, Giusi, Bruno, Giorgia, Capacci, Elena, Casali, Carlo, Ceravolo, Roberto, Cocozza, Sirio, Cotti Piccinelli, Stefano, Criscuolo, Chiara, Danzi, Matt C., De Micco, Rosa, De Michele, Giuseppe, Dicaire, Marie-Josée, Falcone, Grazia Maria Igea, Fancellu, Roberto, Ferchichi, Yasmine, Ferrari, Camilla, Filla, Alessandro, Fini, Nicola, Govoni, Alessandra, Lo Vecchio, Filomena, Malandrini, Alessandro, Mignarri, Andrea, Musumeci, Olimpia, Nesti, Claudia, Pappatà, Sabina, Pellecchia, Maria Teresa, Perna, Alessia, Petrucci, Antonio, Pomponi, Maria Grazia, Ravenni, Roberta, Ricca, Ivana, Rufa, Alessandra, Tabolacci, Elisabetta, Tessa, Alessandra, Tessitore, Alessandro, Zuchner, Stephan, Silvestri, Gabriella, Cortese, Andrea, Brais, Bernard, and Santorelli, Filippo M.

Published

2024

2. A common flanking variant is associated with enhanced stability of the FGF14-SCA27B repeat locus

Author

Pellerin, David, Del Gobbo, Giulia F., Couse, Madeline, Dolzhenko, Egor, Nageshwaran, Sathiji K., Cheung, Warren A., Xu, Isaac R. L., Dicaire, Marie-Josée, Spurdens, Guinevere, Matos-Rodrigues, Gabriel, Stevanovski, Igor, Scriba, Carolin K., Rebelo, Adriana, Roth, Virginie, Wandzel, Marion, Bonnet, Céline, Ashton, Catherine, Agarwal, Aman, Peter, Cyril, Hasson, Dan, Tsankova, Nadejda M., Dewar, Ken, Lamont, Phillipa J., Laing, Nigel G., Renaud, Mathilde, Houlden, Henry, Synofzik, Matthis, Usdin, Karen, Nussenzweig, Andre, Napierala, Marek, Chen, Zhao, Jiang, Hong, Deveson, Ira W., Ravenscroft, Gianina, Akbarian, Schahram, Eberle, Michael A., Boycott, Kym M., Pastinen, Tomi, Brais, Bernard, Zuchner, Stephan, and Danzi, Matt C.

Published

2024

3. Standards of NGS Data Sharing and Analysis in Ataxias: Recommendations by the NGS Working Group of the Ataxia Global Initiative

Author

Beijer, Danique, Fogel, Brent L., Beltran, Sergi, Danzi, Matt C., Németh, Andrea H., Züchner, Stephan, and Synofzik, Matthis

Published

2024

4. The genetic landscape and phenotypic spectrum of GAA-FGF14 ataxia in China: a large cohort study

Author

Ouyang, Riwei, Wan, Linlin, Pellerin, David, Long, Zhe, Hu, Jian, Jiang, Qian, Wang, Chunrong, Peng, Linliu, Peng, Huirong, He, Lang, Qiu, Rong, Wang, Junling, Guo, Jifeng, Shen, Lu, Brais, Bernard, Danzi, Matt C., Zuchner, Stephan, Tang, Beisha, Chen, Zhao, and Jiang, Hong

Published

2024

5. GAA-FGF14 disease: defining its frequency, molecular basis, and 4-aminopyridine response in a large downbeat nystagmus cohort

Author

Pellerin, David, Heindl, Felix, Wilke, Carlo, Danzi, Matt C., Traschütz, Andreas, Ashton, Catherine, Dicaire, Marie-Josée, Cuillerier, Alexanne, Del Gobbo, Giulia, Boycott, Kym M., Claassen, Jens, Rujescu, Dan, Hartmann, Annette M., Zuchner, Stephan, Brais, Bernard, Strupp, Michael, and Synofzik, Matthis

Published

2024

6. Deep structured learning for variant prioritization in Mendelian diseases

Author

Danzi, Matt C., Dohrn, Maike F., Fazal, Sarah, Beijer, Danique, Rebelo, Adriana P., Cintra, Vivian, and Züchner, Stephan

Published

2023

7. The circadian clock time tunes axonal regeneration

Author

De Virgiliis, Francesco, Mueller, Franziska, Palmisano, Ilaria, Chadwick, Jessica Sarah, Luengo-Gutierrez, Lucia, Giarrizzo, Angela, Yan, Yuyang, Danzi, Matt Christopher, Picon-Muñoz, Carmen, Zhou, Luming, Kong, Guiping, Serger, Elisabeth, Hutson, Thomas Haynes, Maldonado-Lasuncion, Ines, Song, Yayue, Scheiermann, Christoph, Brancaccio, Marco, and Di Giovanni, Simone

Published

2023

8. The gut metabolite indole-3 propionate promotes nerve regeneration and repair

Author

Serger, Elisabeth, Luengo-Gutierrez, Lucia, Chadwick, Jessica S., Kong, Guiping, Zhou, Luming, Crawford, Greg, Danzi, Matt C., Myridakis, Antonis, Brandis, Alexander, Bello, Adesola Temitope, Müller, Franziska, Sanchez-Vassopoulos, Alexandros, De Virgiliis, Francesco, Liddell, Phoebe, Dumas, Marc Emmanuel, Strid, Jessica, Mani, Sridhar, Dodd, Dylan, and Di Giovanni, Simone

Published

2022

9. Comparative RNAseq analysis for the study of motoneuron diseases in multi-omics approaches

Author

Chen, Sitong, primary, Ulmer, Ulrike, additional, Synofzik, Matthis, additional, Schule, Rebecca, additional, Zuchner, Stephan, additional, and Danzi, Matt C., additional

Published

2024

10. GAA-FGF14 Disease: Defining Its Frequency, Molecular Basis, and 4-aminopyridine Response in a Large Cohort of Patients with Downbeat Nystagmus (P6-3.013)

Author

Pellerin, David, primary, Heindl, Felix, additional, Wilke, Carlo, additional, Danzi, Matt, additional, Traschutz, Andreas, additional, Ashton, Catherine, additional, Dicaire, Marie-Josee, additional, Cuillerier, Alexanne, additional, Del Gobbo, Giulia, additional, Boycott, Kym, additional, Claassen, Jens, additional, Rujescu, Dan, additional, Hartmann, Annette, additional, Zuchner, Stephan, additional, Brais, Bernard, additional, Strupp, Michael, additional, and Synofzik, Matthis, additional

Published

2024

11. Childhood Onset Amyotrophic Lateral Sclerosis Associated with SPTLC2 Gain-of-Function Pathogenic Variants: Clinical, Genetic, and Biochemical Insights (P4-8.001)

Author

Orbach, Rotem, primary, Syeda, Safoora, additional, Mohassel, Payam, additional, Dohrn, Maike, additional, Lone, Museer A., additional, Donkervoort, Sandra, additional, Foley, A. Reghan, additional, Beijer, Danique, additional, Bayraktar, Elif, additional, Oflazer, Piraye, additional, Munot, Pinki, additional, Rose, Aubrey, additional, Lyons, Michael, additional, Louie, Raymond, additional, Gable, Kenneth, additional, Franca, Marcondes C., additional, Galarza-Brito, Juan E., additional, Eckenweiler, Matthias, additional, Asamoah, Alexander, additional, Majumdar, Anirban, additional, Shieh, Perry, additional, Schumann, Anke, additional, Gupta, Sita D., additional, Lakhotia, Arpita, additional, Jackson, Kelly, additional, Chao, Kathrine R., additional, Winder, Thomas, additional, Catapano, Francesco, additional, Feng, Lucy, additional, Kirschner, Janbernd, additional, Chen, Sitong, additional, Danzi, Matt, additional, Synofzik, Matthis, additional, Muntoni, Francesco, additional, Başak, A. Nazli, additional, Dunn, Teresa M., additional, Hornemann, Thorsten, additional, Zuchner, Stephan, additional, and Bonnemann, Carsten, additional

Published

2024

12. Mechanisms of Neurodegeneration and Mini-gene Therapeutic Approach for Charcot-Marie-Tooth Disease Type 4B3 (S37.007)

Author

Jacobs, Elizabeth, primary, Danzi, Matt, additional, Rebelo, Adriana, additional, Zuchner, Stephan, additional, and Saporta, Mario, additional

Published

2024

13. Pre-clinical Antisense Oligonucleotide Treatment of CMT2E in a Human Induced Pluripotent Stem Cell (iPSC)-derived Motor Neuron Model (S5.008)

Author

Medina, Jessica, primary, Rebelo, Adriana, additional, Jacobs, Elizabeth, additional, Danzi, Matt, additional, Zuchner, Stephan, additional, and Saporta, Mario, additional

Published

2024

14. PP4‐dependent HDAC3 dephosphorylation discriminates between axonal regeneration and regenerative failure

Author

Hervera, Arnau, Zhou, Luming, Palmisano, Ilaria, McLachlan, Eilidh, Kong, Guiping, Hutson, Thomas H, Danzi, Matt C, Lemmon, Vance P, Bixby, John L, Matamoros‐Angles, Andreu, Forsberg, Kirsi, De Virgiliis, Francesco, Matheos, Dina P, Kwapis, Janine, Wood, Marcelo A, Puttagunta, Radhika, del Río, José Antonio, and Di Giovanni, Simone

Subjects

Neurodegenerative, Traumatic Head and Spine Injury, Neurosciences, Physical Injury - Accidents and Adverse Effects, Genetics, Regenerative Medicine, Spinal Cord Injury, Biotechnology, Underpinning research, 2.1 Biological and endogenous factors, Aetiology, 1.1 Normal biological development and functioning, Neurological, Animals, Axons, Cells, Cultured, Disease Models, Animal, Epigenesis, Genetic, Female, Ganglia, Spinal, Histone Deacetylases, Male, Mice, Nerve Regeneration, Peripheral Nerve Injuries, Phosphoprotein Phosphatases, Phosphorylation, Signal Transduction, Small Molecule Libraries, Injury (total) Accidents/Adverse Effects, Injury - Trauma - (Head and Spine), calcium, HDAC3, nerve regeneration, spinal cord injury, transcription, Biological Sciences, Information and Computing Sciences, Medical and Health Sciences, Developmental Biology

Abstract

The molecular mechanisms discriminating between regenerative failure and success remain elusive. While a regeneration-competent peripheral nerve injury mounts a regenerative gene expression response in bipolar dorsal root ganglia (DRG) sensory neurons, a regeneration-incompetent central spinal cord injury does not. This dichotomic response offers a unique opportunity to investigate the fundamental biological mechanisms underpinning regenerative ability. Following a pharmacological screen with small-molecule inhibitors targeting key epigenetic enzymes in DRG neurons, we identified HDAC3 signalling as a novel candidate brake to axonal regenerative growth. In vivo, we determined that only a regenerative peripheral but not a central spinal injury induces an increase in calcium, which activates protein phosphatase 4 that in turn dephosphorylates HDAC3, thus impairing its activity and enhancing histone acetylation. Bioinformatics analysis of ex vivo H3K9ac ChIPseq and RNAseq from DRG followed by promoter acetylation and protein expression studies implicated HDAC3 in the regulation of multiple regenerative pathways. Finally, genetic or pharmacological HDAC3 inhibition overcame regenerative failure of sensory axons following spinal cord injury. Together, these data indicate that PP4-dependent HDAC3 dephosphorylation discriminates between axonal regeneration and regenerative failure.

Published

2019

15. REViewer: haplotype-resolved visualization of read alignments in and around tandem repeats

Author

Dolzhenko, Egor, Weisburd, Ben, Ibañez, Kristina, Rajan-Babu, Indhu-Shree, Anyansi, Christine, Bennett, Mark F., Billingsley, Kimberley, Carroll, Ashley, Clamons, Samuel, Danzi, Matt C., Deshpande, Viraj, Ding, Jinhui, Fazal, Sarah, Halman, Andreas, Jadhav, Bharati, Qiu, Yunjiang, Richmond, Phillip A., Saunders, Christopher T., Scheffler, Konrad, van Vugt, Joke J. F. A., Zwamborn, Ramona R. A. J., Chong, Samuel S., Friedman, Jan M., Tucci, Arianna, Rehm, Heidi L., and Eberle, Michael A.

Published

2022

16. Phenotypic Screening Following Transcriptomic Deconvolution to Identify Transcription Factors Mediating Axon Growth Induced by a Kinase Inhibitor

Author

Lowell, Jeffrey A., O’Neill, Nicholas, Danzi, Matt C., Al-Ali, Hassan, Bixby, John L., and Lemmon, Vance P.

Published

2021

17. Neuroradiological findings in GAA-FGF14 ataxia (SCA27B): more than cerebellar atrophy.

Author

Chen, Shihan, primary, Ashton, Catherine, additional, Sakalla, Rawan, additional, Clement, Guillemette, additional, Planel, Sophie, additional, Bonnet, Celine, additional, Lamont, Phillipa, additional, Kulanthaivelu, Karthik, additional, Nalini, Atchayaram, additional, Houlden, Henry, additional, Duquette, Antoine, additional, Dicaire, Marie-Josee, additional, Iruzubieta Agudo, Pablo, additional, Ruiz Martinez, Javier, additional, Marco de Lucas, Enrique, additional, Sutil Berjon, Rodrigo, additional, Infante Ceberio, Jon, additional, Indelicato, Elisabetta, additional, Boesch, Sylvia, additional, Synofzik, Matthis, additional, Bender, Benjamin, additional, Danzi, Matt C., additional, Zuchner, Stephan, additional, Pellerin, David, additional, Brais, Bernard, additional, Renaud, Mathilde, additional, and La Piana, Roberta, additional

Published

2024

18. RExPRT: a machine learning tool to predict pathogenicity of tandem repeat loci

Author

Fazal, Sarah, primary, Danzi, Matt C., additional, Xu, Isaac, additional, Kobren, Shilpa Nadimpalli, additional, Sunyaev, Shamil, additional, Reuter, Chloe, additional, Marwaha, Shruti, additional, Wheeler, Matthew, additional, Dolzhenko, Egor, additional, Lucas, Francesca, additional, Wuchty, Stefan, additional, Tekin, Mustafa, additional, Züchner, Stephan, additional, and Aguiar-Pulido, Vanessa, additional

Published

2024

19. The FGF14GAA repeat expansion in Greek patients with late‐onset cerebellar ataxia and an overview of the SCA27B phenotype across populations

Author

Kartanou, Chrisoula, primary, Mitrousias, Alexandros, additional, Pellerin, David, additional, Kontogeorgiou, Zoi, additional, Iruzubieta, Pablo, additional, Dicaire, Marie‐Josée, additional, Danzi, Matt C., additional, Koniari, Chrysoula, additional, Athanassopoulos, Konstantinos, additional, Panas, Marios, additional, Stefanis, Leonidas, additional, Zuchner, Stephan, additional, Brais, Bernard, additional, Houlden, Henry, additional, Karadima, Georgia, additional, and Koutsis, Georgios, additional

Published

2024

20. Characterization and visualization of tandem repeats at genome scale

Author

Dolzhenko, Egor, primary, English, Adam, additional, Dashnow, Harriet, additional, De Sena Brandine, Guilherme, additional, Mokveld, Tom, additional, Rowell, William J., additional, Karniski, Caitlin, additional, Kronenberg, Zev, additional, Danzi, Matt C., additional, Cheung, Warren A., additional, Bi, Chengpeng, additional, Farrow, Emily, additional, Wenger, Aaron, additional, Chua, Khi Pin, additional, Martínez-Cerdeño, Verónica, additional, Bartley, Trevor D., additional, Jin, Peng, additional, Nelson, David L., additional, Zuchner, Stephan, additional, Pastinen, Tomi, additional, Quinlan, Aaron R., additional, Sedlazeck, Fritz J., additional, and Eberle, Michael A., additional

Published

2024

21. A study concept of expeditious clinical enrollment for genetic modifier studies in Charcot–Marie–Tooth neuropathy 1A.

Author

Xu, Isaac R. L., Danzi, Matt C., Ruiz, Ariel, Raposo, Jacquelyn, De Jesus, Yeisha Arcia, Reilly, Mary M., Cortese, Andrea, Shy, Michael E., Scherer, Steven S., Herrmann, David N., Fridman, Vera, Baets, Jonathan, Saporta, Mario, Seyedsadjadi, Reza, Stojkovic, Tanya, Claeys, Kristl G., Patel, Pooja, Feely, Shawna, Rebelo, Adriana P., and Dohrn, Maike F.

Subjects

*DORSIFLEXION, *EFFECT sizes (Statistics), *RESEARCH funding, *SEVERITY of illness index, *GENETIC variation, *NUCLEOTIDES, *CHARCOT-Marie-Tooth disease, *GENOMES, *DISEASE progression, *GENETICS, *SEQUENCE analysis, *PHENOTYPES

Abstract

Background: Caused by duplications of the gene encoding peripheral myelin protein 22 (PMP22), Charcot–Marie–Tooth disease type 1A (CMT1A) is the most common hereditary neuropathy. Despite this shared genetic origin, there is considerable variability in clinical severity. It is hypothesized that genetic modifiers contribute to this heterogeneity, the identification of which may reveal novel therapeutic targets. In this study, we present a comprehensive analysis of clinical examination results from 1564 CMT1A patients sourced from a prospective natural history study conducted by the RDCRN‐INC (Inherited Neuropathy Consortium). Our primary objective is to delineate extreme phenotype profiles (mild and severe) within this patient cohort, thereby enhancing our ability to detect genetic modifiers with large effects. Methods: We have conducted large‐scale statistical analyses of the RDCRN‐INC database to characterize CMT1A severity across multiple metrics. Results: We defined patients below the 10th (mild) and above the 90th (severe) percentiles of age‐normalized disease severity based on the CMT Examination Score V2 and foot dorsiflexion strength (MRC scale). Based on extreme phenotype categories, we defined a statistically justified recruitment strategy, which we propose to use in future modifier studies. Interpretation: Leveraging whole genome sequencing with base pair resolution, a future genetic modifier evaluation will include single nucleotide association, gene burden tests, and structural variant analysis. The present work not only provides insight into the severity and course of CMT1A, but also elucidates the statistical foundation and practical considerations for a cost‐efficient and straightforward patient enrollment strategy that we intend to conduct on additional patients recruited globally. [ABSTRACT FROM AUTHOR]

Published

2024

22. Recurrent ATP1A1 variant Gly903Arg causes developmental delay, intellectual disability, and autism.

Author

Dohrn, Maike F., Bademci, Guney, Rebelo, Adriana P., Jeanne, Médéric, Borja, Nicholas A., Beijer, Danique, Danzi, Matt C., Bivona, Stephanie A., Gueguen, Paul, Zafeer, Mohammad F., Tekin, Mustafa, Züchner, Stephan, Acosta, Maria T., Adams, David R., Afzali, Ben, Allworth, Aimee, Alvarez, Raquel L., Alvey, Justin, Andrews, Ashley, and Ashley, Euan A.

Subjects

DEVELOPMENTAL delay, INTELLECTUAL disabilities, AUTISM, GENETIC variation, NEUROLOGICAL disorders, CHILDREN with developmental disabilities, CHILDREN with autism spectrum disorders

Abstract

ATP1A1 encodes a sodium‐potassium ATPase that has been linked to several neurological diseases. Using exome and genome sequencing, we identified the heterozygous ATP1A1 variant NM_000701.8: c.2707G>A;p.(Gly903Arg) in two unrelated children presenting with delayed motor and speech development and autism. While absent in controls, the variant occurred de novo in one proband and co‐segregated in two affected half‐siblings, with mosaicism in the healthy mother. Using a specific ouabain resistance assay in mutant transfected HEK cells, we found significantly reduced cell viability. Demonstrating loss of ATPase function, we conclude that this novel variant is pathogenic, expanding the phenotype spectrum of ATP1A1. [ABSTRACT FROM AUTHOR]

Published

2024

23. Computational Identification of Kinases That Control Axon Growth in Mouse

Author

Devkota, Prajwal, Danzi, Matt C., Lemmon, Vance P., Bixby, John L., and Wuchty, Stefan

Published

2020

24. A deep intronic FGF14 GAA repeat expansion causes late-onset cerebellar ataxia

Author

Pellerin, David, primary, Danzi, Matt, additional, Wilke, Carlo, additional, Renaud, Mathilde, additional, Fazal, Sarah, additional, Dicaire, Marie-Josée, additional, Scriba, Carolin, additional, Ashton, Catherine, additional, Genís, David, additional, Porcel, Laura Molina, additional, Nagy, Sara, additional, Nalini, Atchayaram, additional, Boycott, Kym, additional, Duquette, Antoine, additional, Houlden, Henry, additional, Ravenscroft, Gianina, additional, Laing, Nigel, additional, Lamont, Phillipa, additional, Schöls, Ludger, additional, La Piana, Roberta, additional, Synofzik, Matthis, additional, Zuchner, Stephan, additional, and Brais, Bernard, additional

Published

2023

25. Recurrentde-novo gain-of-functionmutation inSPTLC2confirms dysregulated sphingolipid production to cause juvenile amyotrophic lateral sclerosis

Author

Dohrn, Maike F, primary, Beijer, Danique, additional, Lone, Museer A, additional, Bayraktar, Elif, additional, Oflazer, Piraye, additional, Orbach, Rotem, additional, Donkervoort, Sandra, additional, Foley, A Reghan, additional, Rose, Aubrey, additional, Lyons, Michael, additional, Louie, Raymond J, additional, Gable, Kenneth, additional, Dunn, Teresa, additional, Chen, Sitong, additional, Danzi, Matt C, additional, Synofzik, Matthis, additional, Bönnemann, Carsten G, additional, Nazlı Başak, A, additional, Hornemann, Thorsten, additional, and Zuchner, Stephan, additional

Published

2023

26. Epigenomic signatures underpin the axonal regenerative ability of dorsal root ganglia sensory neurons

Author

Palmisano, Ilaria, Danzi, Matt C., Hutson, Thomas H., Zhou, Luming, McLachlan, Eilidh, Serger, Elisabeth, Shkura, Kirill, Srivastava, Prashant K., Hervera, Arnau, Neill, Nick O’, Liu, Tong, Dhrif, Hassen, Wang, Zheng, Kubat, Miroslav, Wuchty, Stefan, Merkenschlager, Matthias, Levi, Liron, Elliott, Evan, Bixby, John L., Lemmon, Vance P., and Di Giovanni, Simone

Published

2019

27. Recurrent de-novo gain-of-function mutation in SPTLC2 confirms dysregulated sphingolipid production to cause juvenile amyotrophic lateral sclerosis.

Author

Dohrn, Maike F., Beijer, Danique, Lone, Museer A., Bayraktar, Elif, Oflazer, Piraye, Orbach, Rotem, Donkervoort, Sandra, Foley, A. Reghan, Rose, Aubrey, Lyons, Michael, Louie, Raymond J., Gable, Kenneth, Dunn, Teresa, Sitong Chen, Danzi, Matt C., Synofzik, Matthis, Bönnemann, Carsten G., Başak, A. Nazlı, Hornemann, Thorsten, and Zuchner, Stephan

Subjects

MOTOR neuron diseases, AMYOTROPHIC lateral sclerosis, GAIN-of-function mutations, MOLECULAR biology

Abstract

This document summarizes a study on the genetic mutation SPTLC2 and its connection to juvenile amyotrophic lateral sclerosis (ALS). The researchers used genetic data to identify variants in SPTLC2 in ALS patients and discovered a recurring gain-of-function mutation that led to abnormal sphingolipid production and the development of juvenile ALS. The study suggests that dysregulated sphingolipid synthesis plays a role in the development of ALS and proposes potential therapeutic options for motor neuron diseases. Additionally, the document compares the lipid profiles of ALS patients with SPTLC2 mutations to those with mutations in the SPTLC1 gene, which have a different phenotype. [Extracted from the article]

Published

2024

28. Spinocerebellar ataxia 27B: A novel, frequent and potentially treatable ataxia.

Author

Pellerin, David, Danzi, Matt C., Renaud, Mathilde, Houlden, Henry, Synofzik, Matthis, Zuchner, Stephan, and Brais, Bernard

Subjects

*SPINOCEREBELLAR ataxia, *FRIEDREICH'S ataxia, *FIBROBLAST growth factors, *ATAXIA, *CEREBELLAR ataxia, *GENETIC disorder diagnosis

Abstract

Hereditary ataxias, especially when presenting sporadically in adulthood, present a particular diagnostic challenge owing to their great clinical and genetic heterogeneity. Currently, up to 75% of such patients remain without a genetic diagnosis. In an era of emerging disease‐modifying gene‐stratified therapies, the identification of causative alleles has become increasingly important. Over the past few years, the implementation of advanced bioinformatics tools and long‐read sequencing has allowed the identification of a number of novel repeat expansion disorders, such as the recently described spinocerebellar ataxia 27B (SCA27B) caused by a (GAA)•(TTC) repeat expansion in intron 1 of the fibroblast growth factor 14 (FGF14) gene. SCA27B is rapidly gaining recognition as one of the most common forms of adult‐onset hereditary ataxia, with several studies showing that it accounts for a substantial number (9–61%) of previously undiagnosed cases from different cohorts. First natural history studies and multiple reports have already outlined the progression and core phenotype of this novel disease, which consists of a late‐onset slowly progressive pan‐cerebellar syndrome that is frequently associated with cerebellar oculomotor signs, such as downbeat nystagmus, and episodic symptoms. Furthermore, preliminary studies in patients with SCA27B have shown promising symptomatic benefits of 4‐aminopyridine, an already marketed drug. This review describes the current knowledge of the genetic and molecular basis, epidemiology, clinical features and prospective treatment strategies in SCA27B. [ABSTRACT FROM AUTHOR]

Published

2024

29. Frequency of GAA-FGF14Ataxia in a Large Cohort of Brazilian Patients With Unsolved Adult-Onset Cerebellar Ataxia

Author

Novis, Luiz Eduardo, primary, Frezatti, Rodrigo S., additional, Pellerin, David, additional, Tomaselli, Pedro J., additional, Alavi, Shahryar, additional, Della Coleta, Marcus Vinícius, additional, Spitz, Mariana, additional, Dicaire, Marie-Josée, additional, Iruzubieta, Pablo, additional, Pedroso, José Luiz, additional, Barsottini, Orlando, additional, Cortese, Andrea, additional, Danzi, Matt C., additional, França, Marcondes C., additional, Brais, Bernard, additional, Zuchner, Stephan, additional, Houlden, Henry, additional, Raskin, Salmo, additional, Marques, Wilson, additional, and Teive, Helio A., additional

Published

2023

30. Frequency and phenotypic spectrum of spinocerebellar ataxia 27B and other genetic ataxias in a Spanish cohort of late‐onset cerebellar ataxia

Author

Iruzubieta, Pablo, primary, Pellerin, David, additional, Bergareche, Alberto, additional, Albajar, Inés, additional, Mondragón, Elisabet, additional, Vinagre, Ana, additional, Fernández‐Torrón, Roberto, additional, Moreno, Fermín, additional, Equiza, Jon, additional, Campo‐Caballero, David, additional, Poza, Juan José, additional, Ruibal, Marta, additional, Formica, Alessandro, additional, Dicaire, Marie‐Josée, additional, Danzi, Matt C., additional, Zuchner, Stephan, additional, Croitoru, Ioana, additional, Ruiz, Montserrat, additional, Schlüter, Agatha, additional, Casasnovas, Carlos, additional, Pujol, Aurora, additional, Brais, Bernard, additional, Houlden, Henry, additional, de Munain, Adolfo López, additional, and Ruiz‐Martínez, Javier, additional

Published

2023

31. The circadian clock is a pacemaker of the axonal regenerative ability

Author

De Virgiliis, Francesco, primary, Mueller, Franziska, additional, Palmisano, Ilaria, additional, Chadwick, Jessica S, additional, Luengo Gutierrez, Lucia, additional, Giarrizzo, Angela, additional, Yan, Yuyang, additional, Danzi, Matt Christopher, additional, Picon Munoz, Carmen, additional, Zhou, Luming, additional, Kong, Guiping, additional, Serger, Elisabeth, additional, Hutson, Thomas Haynes, additional, Scheiermann, Christoph, additional, Brancaccio, Marco, additional, and Di Giovanni, Simone, additional

Published

2023

32. IntronicFGF14GAA repeat expansions are a common cause of downbeat nystagmus syndromes: frequency, phenotypic profile, and 4-aminopyridine treatment response

Author

Pellerin, David, primary, Heindl, Felix, additional, Wilke, Carlo, additional, Danzi, Matt C., additional, Traschütz, Andreas, additional, Ashton, Catherine, additional, Dicaire, Marie-Josée, additional, Cuillerier, Alexanne, additional, Del Gobbo, Giulia, additional, Boycott, Kym M., additional, Claassen, Jens, additional, Rujescu, Dan, additional, Hartmann, Annette M., additional, Zuchner, Stephan, additional, Brais, Bernard, additional, Strupp, Michael, additional, and Synofzik, Matthis, additional

Published

2023

33. Non‐GAA Repeat Expansions in FGF14 Are Likely Not Pathogenic—Reply to: “Shaking Up Ataxia: FGF14 and RFC1 Repeat Expansions in Affected and Unaffected Members of a Chilean Family”

Author

Pellerin, David, primary, Iruzubieta, Pablo, additional, Tekgül, Şeyma, additional, Danzi, Matt C., additional, Ashton, Catherine, additional, Dicaire, Marie‐Josée, additional, Wandzel, Marion, additional, Roth, Virginie, additional, Lamont, Phillipa J., additional, Bonnet, Céline, additional, Renaud, Mathilde, additional, Synofzik, Matthis, additional, Zuchner, Stephan, additional, Brais, Bernard, additional, Başak, Nazlı A., additional, and Houlden, Henry, additional

Published

2023

34. Enriched conditioning expands the regenerative ability of sensory neurons after spinal cord injury via neuronal intrinsic redox signaling

Author

De Virgiliis, Francesco, Hutson, Thomas H., Palmisano, Ilaria, Amachree, Sarah, Miao, Jian, Zhou, Luming, Todorova, Rositsa, Thompson, Richard, Danzi, Matt C., Lemmon, Vance P., Bixby, John L., Wittig, Ilka, Shah, Ajay M., and Di Giovanni, Simone

Published

2020

35. Optimized testing strategy for the diagnosis of GAA-FGF14 ataxia/spinocerebellar ataxia 27B

Author

Bonnet, Céline, primary, Pellerin, David, additional, Roth, Virginie, additional, Clément, Guillemette, additional, Wandzel, Marion, additional, Lambert, Laëtitia, additional, Frismand, Solène, additional, Douarinou, Marian, additional, Grosset, Anais, additional, Bekkour, Ines, additional, Weber, Frédéric, additional, Girardier, Florent, additional, Robin, Clément, additional, Cacciatore, Stéphanie, additional, Bronner, Myriam, additional, Pourié, Carine, additional, Dreumont, Natacha, additional, Puisieux, Salomé, additional, Iruzubieta, Pablo, additional, Dicaire, Marie-Josée, additional, Evoy, François, additional, Rioux, Marie-France, additional, Hocquel, Armand, additional, La Piana, Roberta, additional, Synofzik, Matthis, additional, Houlden, Henry, additional, Danzi, Matt C., additional, Zuchner, Stephan, additional, Brais, Bernard, additional, and Renaud, Mathilde, additional

Published

2023

36. A common flanking variant is associated with enhanced meiotic stability of theFGF14-SCA27B locus

Author

Pellerin, David, primary, Del Gobbo, Giulia, additional, Couse, Madeline, additional, Dolzhenko, Egor, additional, Dicaire, Marie-Josée, additional, Rebelo, Adriana, additional, Roth, Virginie, additional, Wandzel, Marion, additional, Bonnet, Céline, additional, Ashton, Catherine, additional, Lamont, Phillipa J., additional, Laing, Nigel G., additional, Renaud, Mathilde, additional, Ravenscroft, Gianina, additional, Houlden, Henry, additional, Synofzik, Matthis, additional, Eberle, Michael A., additional, Boycott, Kym M., additional, Pastinen, Tomi, additional, Brais, Bernard, additional, Zuchner, Stephan, additional, and Danzi, Matt C., additional

Published

2023

37. Resolving the unsolved: Comprehensive assessment of tandem repeats at scale

Author

Dolzhenko, Egor, primary, English, Adam, additional, Dashnow, Harriet, additional, De Sena Brandine, Guilherme, additional, Mokveld, Tom, additional, Rowell, William J, additional, Karniski, Caitlin, additional, Kronenberg, Zev, additional, Danzi, Matt C, additional, Cheung, Warren A, additional, Bi, Chengpeng, additional, Farrow, Emily, additional, Wenger, Aaron, additional, Martínez-Cerdeño, Verónica, additional, Bartley, Trevor D, additional, Jin, Peng, additional, Nelson, David, additional, Zuchner, Stephan, additional, Pastinen, Tomi, additional, Quinlan, Aaron R, additional, Sedlazeck, Fritz J, additional, and Eberle, Michael A, additional

Published

2023

38. Recurrent de-novo gain-of-functionmutation in SPTLC2confirms dysregulated sphingolipid production to cause juvenile amyotrophic lateral sclerosis

Author

Dohrn, Maike F, Beijer, Danique, Lone, Museer A, Bayraktar, Elif, Oflazer, Piraye, Orbach, Rotem, Donkervoort, Sandra, Foley, A Reghan, Rose, Aubrey, Lyons, Michael, Louie, Raymond J, Gable, Kenneth, Dunn, Teresa, Chen, Sitong, Danzi, Matt C, Synofzik, Matthis, Bo¨nnemann, Carsten G, Nazlı Basak, A, Hornemann, Thorsten, and Zuchner, Stephan

Abstract

BackgroundAmyotrophic lateral sclerosis (ALS) leads to paralysis and death by progressive degeneration of motor neurons. Recently, specific gain-of-functionmutations in SPTLC1were identified in patients with juvenile form of ALS. SPTLC2encodes the second catalytic subunit of the serine-palmitoyltransferase (SPT) complex.MethodsWe used the GENESIS platform to screen 700 ALS whole-genome and whole-exome data sets for variants in SPTLC2. The de-novostatus was confirmed by Sanger sequencing. Sphingolipidomics was performed using liquid chromatography and high-resolution mass spectrometry.ResultsTwo unrelated patients presented with early-onset progressive proximal and distal muscle weakness, oral fasciculations, and pyramidal signs. Both patients carried the novel de-novo SPTLC2mutation, c.203T>G, p.Met68Arg. This variant lies within a single short transmembrane domain of SPTLC2, suggesting that the mutation renders the SPT complex irresponsive to regulation through ORMDL3. Confirming this hypothesis, ceramide and complex sphingolipid levels were significantly increased in patient plasma. Accordingly, excessive sphingolipid production was shown in mutant-expressing human embryonic kindney (HEK) cells.ConclusionsSpecific gain-of-functionmutations in both core subunits affect the homoeostatic control of SPT. SPTLC2represents a new Mendelian ALS gene, highlighting a key role of dysregulated sphingolipid synthesis in the pathogenesis of juvenile ALS. Given the direct interaction of SPTLC1 and SPTLC2, this knowledge might open new therapeutic avenues for motor neuron diseases.

Published

2024

39. Large scale in silico characterization of repeat expansion variation in human genomes

Author

Fazal, Sarah, Danzi, Matt C., Cintra, Vivian P., Bis-Brewer, Dana M., Dolzhenko, Egor, Eberle, Michael A., and Zuchner, Stephan

Published

2020

40. Biallelic variants in COQ7 cause distal hereditary motor neuropathy with upper motor neuron signs.

Author

Rebelo, Adriana P, Tomaselli, Pedro J, Medina, Jessica, Wang, Ying, Dohrn, Maike F, Nyvltova, Eva, Danzi, Matt C, Garrett, Mark, Smith, Sean E, Pestronk, Alan, Li, Chengcheng, Ruiz, Ariel, Jacobs, Elizabeth, Feely, Shawna M E, França, Marcondes C, Gomes, Marcus V, Santos, Diogo F, Kumar, Surinder, Lombard, David B, and Saporta, Mario

Subjects

MOTOR neuron diseases, MOTOR neurons, CELL physiology, HIGH performance liquid chromatography, UBIQUINONES, MITOCHONDRIAL pathology

Abstract

COQ7 encodes a hydroxylase responsible for the penultimate step of coenzyme Q10 (CoQ10) biosynthesis in mitochondria. CoQ10 is essential for multiple cellular functions, including mitochondrial oxidative phosphorylation, lipid metabolism, and reactive oxygen species homeostasis. Mutations in COQ7 have been previously associated with primary CoQ10 deficiency, a clinically heterogeneous multisystemic mitochondrial disorder. We identified COQ7 biallelic variants in nine families diagnosed with distal hereditary motor neuropathy with upper neuron involvement, expending the clinical phenotype associated with defects in this gene. A recurrent p.Met1? change was identified in five families from Brazil with evidence of a founder effect. Fibroblasts isolated from patients revealed a substantial depletion of COQ7 protein levels, indicating protein instability leading to loss of enzyme function. High-performance liquid chromatography assay showed that fibroblasts from patients had reduced levels of CoQ10, and abnormal accumulation of the biosynthetic precursor DMQ10. Accordingly, fibroblasts from patients displayed significantly decreased oxygen consumption rates in patients, suggesting mitochondrial respiration deficiency. Induced pluripotent stem cell-derived motor neurons from patient fibroblasts showed significantly increased levels of extracellular neurofilament light protein, indicating axonal degeneration. Our findings indicate a molecular pathway involving CoQ10 biosynthesis deficiency and mitochondrial dysfunction in patients with distal hereditary motor neuropathy. Further studies will be important to evaluate the potential benefits of CoQ10 supplementation in the clinical outcome of the disease. [ABSTRACT FROM AUTHOR]

Published

2023

41. GAA-FGF14 ataxia (SCA27B): phenotypic profile, natural history progression and 4-aminopyridine treatment response.

Author

Wilke, Carlo, Pellerin, David, Mengel, David, Traschütz, Andreas, Danzi, Matt C, Dicaire, Marie-Josée, Neumann, Manuela, Lerche, Holger, Bender, Benjamin, Houlden, Henry, group, RFC1 study, Züchner, Stephan, Schöls, Ludger, Brais, Bernard, and Synofzik, Matthis

Subjects

SPINOCEREBELLAR ataxia, PROGRESSIVE supranuclear palsy, NATURAL history, ATAXIA, PHENOTYPES

Abstract

Ataxia due to an autosomal dominant intronic GAA repeat expansion in FGF14 [GAA- FGF14 ataxia, spinocerebellar ataxia 27B (SCA27B)] has recently been identified as one of the most common genetic late-onset ataxias. We here aimed to characterize its phenotypic profile, natural history progression, and 4-aminopyridine (4-AP) treatment response. We conducted a multi-modal cohort study of 50 GAA- FGF14 patients, comprising in-depth phenotyping, cross-sectional and longitudinal progression data (up to 7 years), MRI findings, serum neurofilament light (sNfL) levels, neuropathology, and 4-AP treatment response data, including a series of n -of-1 treatment studies. GAA- FGF14 ataxia consistently presented as late-onset [60.0 years (53.5–68.5), median (interquartile range)] pancerebellar syndrome, partly combined with afferent sensory deficits (55%) and dysautonomia (28%). Dysautonomia increased with duration while cognitive impairment remained infrequent, even in advanced stages. Cross-sectional and longitudinal assessments consistently indicated mild progression of ataxia [0.29 Scale for the Assessment and Rating of Ataxia (SARA) points/year], not exceeding a moderate disease severity even in advanced stages (maximum SARA score: 18 points). Functional impairment increased relatively slowly (unilateral mobility aids after 8 years in 50% of patients). Corresponding to slow progression and low extra-cerebellar involvement, sNfL was not increased relative to controls. Concurrent second diseases (including progressive supranuclear palsy neuropathology) represented major individual aggravators of disease severity, constituting important caveats for planning future GAA- FGF14 trials. A treatment response to 4-AP with relevance for everyday living was reported by 86% of treated patients. A series of three prospective n -of-1 treatment experiences with on/off design showed marked reduction in daily symptomatic time and symptom severity on 4-AP. Our study characterizes the phenotypic profile, natural history progression, and 4-AP treatment response of GAA- FGF14 ataxia. It paves the way towards large-scale natural history studies and 4-AP treatment trials in this newly discovered, possibly most frequent, and treatable late-onset ataxia. [ABSTRACT FROM AUTHOR]

Published

2023

42. Frequency of GAA-FGF14 Ataxia in a Large Cohort of Brazilian Patients With Unsolved Adult-Onset Cerebellar Ataxia.

Author

Novis, Luiz Eduardo, Frezatti, Rodrigo S., Pellerin, David, Tomaselli, Pedro J., Alavi, Shahryar, Della Coleta, Marcus Vinícius, Spitz, Mariana, Dicaire, Marie-Josée, Iruzubieta, Pablo, Pedroso, José Luiz, Barsottini, Orlando, Cortese, Andrea, Danzi, Matt C., França Jr, Marcondes C., Brais, Bernard, Zuchner, Stephan, Houlden, Henry, Raskin, Salmo, Marques, Wilson, and Teive, Helio A.

Published

2023

43. Reactive oxygen species regulate axonal regeneration through the release of exosomal NADPH oxidase 2 complexes into injured axons

Author

Hervera, Arnau, De Virgiliis, Francesco, Palmisano, Ilaria, Zhou, Luming, Tantardini, Elena, Kong, Guiping, Hutson, Thomas, Danzi, Matt C., Perry, Rotem Ben-Tov, Santos, Celio X. C., Kapustin, Alexander N., Fleck, Roland A., Del Río, José Antonio, Carroll, Thomas, Lemmon, Vance, Bixby, John L., Shah, Ajay M., Fainzilber, Mike, and Di Giovanni, Simone

Published

2018

44. RExPRT: a machine learning tool to predict pathogenicity of tandem repeat loci

Author

Fazal, Sarah, primary, Danzi, Matt, additional, Xu, Isaac, additional, Kobren, Shilpa Nadimpalli, additional, Sunyaev, Shamil, additional, Reuter, Chloe, additional, Marwaha, Shruti, additional, Wheeler, Matthew T, additional, Dolzhenko, Egor, additional, Lucas, Francesca, additional, Wuchty, Stefan, additional, Tekin, Mustafa, additional, Zuchner, Stephan, additional, and Aguiar-Pulido, Vanessa, additional

Published

2023

45. Optimized testing strategy for the diagnosis of GAA-FGF14ataxia

Author

Bonnet, Céline, primary, Pellerin, David, additional, Roth, Virginie, additional, Clément, Guillemette, additional, Wandzel, Marion, additional, Lambert, Laëtitia, additional, Frismand, Solène, additional, Douarinou, Marian, additional, Grosset, Anais, additional, Bekkour, Ines, additional, Weber, Frédéric, additional, Girardier, Florent, additional, Robin, Clément, additional, Cacciatore, Stéphanie, additional, Bronner, Myriam, additional, Pourié, Carine, additional, Dreumont, Natacha, additional, Puisieux, Salomé, additional, Dicaire, Marie-Josée, additional, Evoy, François, additional, Rioux, Marie-France, additional, Hocquel, Armand, additional, La Piana, Roberta, additional, Synofzik, Matthis, additional, Houlden, Henry, additional, Danzi, Matt C., additional, Zuchner, Stephan, additional, Brais, Bernard, additional, and Renaud, Mathilde, additional

Published

2023

46. Deep Intronic FGF14 GAA Repeat Expansion in Late-Onset Cerebellar Ataxia

Author

Pellerin, David, primary, Danzi, Matt C., additional, Wilke, Carlo, additional, Renaud, Mathilde, additional, Fazal, Sarah, additional, Dicaire, Marie-Josée, additional, Scriba, Carolin K., additional, Ashton, Catherine, additional, Yanick, Christopher, additional, Beijer, Danique, additional, Rebelo, Adriana, additional, Rocca, Clarissa, additional, Jaunmuktane, Zane, additional, Sonnen, Joshua A., additional, Larivière, Roxanne, additional, Genís, David, additional, Molina Porcel, Laura, additional, Choquet, Karine, additional, Sakalla, Rawan, additional, Provost, Sylvie, additional, Robertson, Rebecca, additional, Allard-Chamard, Xavier, additional, Tétreault, Martine, additional, Reiling, Sarah J., additional, Nagy, Sara, additional, Nishadham, Vikas, additional, Purushottam, Meera, additional, Vengalil, Seena, additional, Bardhan, Mainak, additional, Nalini, Atchayaram, additional, Chen, Zhongbo, additional, Mathieu, Jean, additional, Massie, Rami, additional, Chalk, Colin H., additional, Lafontaine, Anne-Louise, additional, Evoy, François, additional, Rioux, Marie-France, additional, Ragoussis, Jiannis, additional, Boycott, Kym M., additional, Dubé, Marie-Pierre, additional, Duquette, Antoine, additional, Houlden, Henry, additional, Ravenscroft, Gianina, additional, Laing, Nigel G., additional, Lamont, Phillipa J., additional, Saporta, Mario A., additional, Schüle, Rebecca, additional, Schöls, Ludger, additional, La Piana, Roberta, additional, Synofzik, Matthis, additional, Zuchner, Stephan, additional, and Brais, Bernard, additional

Published

2023

47. Standards of NGS Data Sharing and Analysis in Ataxias: Recommendations by the NGS Working Group of the Ataxia Global Initiative

Author

Beijer, Danique, Fogel, Brent L, Beltran, Sergi, Danzi, Matt C, Németh, Andrea H, Züchner, Stephan, Synofzik, Matthis, AGI Ataxia NGS genomics, platforms Working Group, Ashrafi, Mahmoud Reza, Bataller, Luis, Bertini, Enrico, Boesch, Sylvia, Buijsen, Ronald, Cassou, Emanuel, Chan, Edwin, Damásio, Joana, Donis, Karina, Elert-Dobkowska, Ewelina, Elsayed, Liena, Espinos, Carmen, Hanağasi, Haşmet, Heidari, Morteza, Nachbauer, Wolfgang, Oliveira, Jorge, Opal, Puneet, Paisan-Ruiz, Coro, Puccio, Hélène, Saccà, Francesco, Saraiva-Pereira, Maria Luiza, Schmidt, Thorsten, Schüle-Freyer, Rebecca, Stevanin, Giovanni, Wilke, Carlo, Yoon, Grace, Zach, Neta, Zanni, Ginevra, Adarmes, Astrid, and Alhusaini, Saud

Subjects

Consensus, Neurology, Information dissemination, ddc:610, Genomics, Neurology (clinical), High-throughput nucleotide sequencing, Cerebellar ataxia

Abstract

Data de publicació electrònica: 04-03-2023 The Ataxia Global Initiative (AGI) is a worldwide multi-stakeholder research platform to systematically enhance trial-readiness in degenerative ataxias. The next-generation sequencing (NGS) working group of the AGI aims to improve methods, platforms, and international standards for ataxia NGS analysis and data sharing, ultimately allowing to increase the number of genetically ataxia patients amenable for natural history and treatment trials. Despite extensive implementation of NGS for ataxia patients in clinical and research settings, the diagnostic gap remains sizeable, as approximately 50% of patients with hereditary ataxia remain genetically undiagnosed. One current shortcoming is the fragmentation of patients and NGS datasets on different analysis platforms and databases around the world. The AGI NGS working group in collaboration with the AGI associated research platforms—CAGC, GENESIS, and RD-Connect GPAP—provides clinicians and scientists access to user-friendly and adaptable interfaces to analyze genome-scale patient data. These platforms also foster collaboration within the ataxia community. These efforts and tools have led to the diagnosis of > 500 ataxia patients and the discovery of > 30 novel ataxia genes. Here, the AGI NGS working group presents their consensus recommendations for NGS data sharing initiatives in the ataxia field, focusing on harmonized NGS variant analysis and standardized clinical and metadata collection, combined with collaborative data and analysis tool sharing across platforms. Open Access funding enabled and organized by Projekt DEAL. This work was supported by the Horizon 2020 research and innovation programme (grant 779257 Solve-RD to MS and SB), and the European Joint Programme on Rare Diseases (grant 825575 EJP RD to SB) under the EJP RD COFUND-EJP No. 825575 (PROSPAX consortium, to MS and—as an associated partner—SZ). DB is supported by a Postdoctoral Fellowship from the Alexander von Humboldt Foundation.

Published

2023

48. Optimized testing strategy for the diagnosis of GAA-FGF14 ataxia/spinocerebellar ataxia 27B

Author

Bonnet, Céline, Pellerin, David, Weber, Frédéric, Girardier, Florent, Robin, Clément, Cacciatore, Stéphanie, Bronner, Myriam, Pourié, Carine, Dreumont, Natacha, Puisieux, Salomé, Iruzubieta, Pablo, Dicaire, Marie-Josée, Roth, Virginie, Evoy, François, Rioux, Marie-France, Hocquel, Armand, La Piana, Roberta, Synofzik, Matthis, Houlden, Henry, Danzi, Matt C, Zuchner, Stephan, Brais, Bernard, Renaud, Mathilde, Clément, Guillemette, Wandzel, Marion, Lambert, Laëtitia, Frismand, Solène, Douarinou, Marian, Grosset, Anais, and Bekkour, Ines

Subjects

Canada, Humans, genetics [Spinocerebellar Ataxias], Trinucleotide Repeat Expansion, ddc:600, genetics [Friedreich Ataxia]

Abstract

Dominantly inherited GAA repeat expansions in FGF14 are a common cause of spinocerebellar ataxia (GAA-FGF14 ataxia; spinocerebellar ataxia 27B). Molecular confirmation of FGF14 GAA repeat expansions has thus far mostly relied on long-read sequencing, a technology that is not yet widely available in clinical laboratories. We developed and validated a strategy to detect FGF14 GAA repeat expansions using long-range PCR, bidirectional repeat-primed PCRs, and Sanger sequencing. We compared this strategy to targeted nanopore sequencing in a cohort of 22 French Canadian patients and next validated it in a cohort of 53 French index patients with unsolved ataxia. Method comparison showed that capillary electrophoresis of long-range PCR amplification products significantly underestimated expansion sizes compared to nanopore sequencing (slope, 0.87 [95% CI, 0.81 to 0.93]; intercept, 14.58 [95% CI, - 2.48 to 31.12]) and gel electrophoresis (slope, 0.84 [95% CI, 0.78 to 0.97]; intercept, 21.34 [95% CI, - 27.66 to 40.22]). The latter techniques yielded similar size estimates. Following calibration with internal controls, expansion size estimates were similar between capillary electrophoresis and nanopore sequencing (slope: 0.98 [95% CI, 0.92 to 1.04]; intercept: 10.62 [95% CI, - 7.49 to 27.71]), and gel electrophoresis (slope: 0.94 [95% CI, 0.88 to 1.09]; intercept: 18.81 [95% CI, - 41.93 to 39.15]). Diagnosis was accurately confirmed for all 22 French Canadian patients using this strategy. We also identified 9 French patients (9/53; 17%) and 2 of their relatives who carried an FGF14 (GAA)≥250 expansion. This novel strategy reliably detected and sized FGF14 GAA expansions, and compared favorably to long-read sequencing.

Published

2023

49. A network biology approach to unraveling inherited axonopathies

Author

Bis-Brewer, Dana M., Danzi, Matt C., Wuchty, Stefan, and Züchner, Stephan

Published

2019

50. Spinocerebellar ataxia 27B: episodic symptoms and acetazolamide response in 34 patients.

Author

Ashton, Catherine, Indelicato, Elisabetta, Pellerin, David, Clément, Guillemette, Danzi, Matt C., Dicaire, Marie-Josée, Bonnet, Céline, Houlden, Henry, Züchner, Stephan, Synofzik, Matthis, Lamont, Phillipa J., Renaud, Mathilde, Boesch, Sylvia, and Brais, Bernard

Published

2023