Your search keyword '"Iuso, Arcangela"' showing total 37 results

1. A spatiotemporal proteomic map of human adipogenesis

Author

Klingelhuber, Felix, Frendo-Cumbo, Scott, Omar-Hmeadi, Muhmmad, Massier, Lucas, Kakimoto, Pamela, Taylor, Austin J., Couchet, Morgane, Ribicic, Sara, Wabitsch, Martin, Messias, Ana C., Iuso, Arcangela, Müller, Timo D., Rydén, Mikael, Mejhert, Niklas, and Krahmer, Natalie

Published

2024

2. A comprehensive phenotypic characterization of a whole-body Wdr45 knock-out mouse

Author

Biagosch, Caroline A., Vidali, Silvia, Faerberboeck, Michael, Hensler, Svenja-Viola, Becker, Lore, Amarie, Oana V., Aguilar-Pimentel, Antonio, Garrett, Lillian, Klein-Rodewald, Tanja, Rathkolb, Birgit, Zanuttigh, Enrica, Calzada-Wack, Julia, da Silva-Buttkus, Patricia, Rozman, Jan, Treise, Irina, Fuchs, Helmut, Gailus-Durner, Valerie, de Angelis, Martin Hrabě, Janik, Dirk, Wurst, Wolfgang, Mayr, Johannes A., Klopstock, Thomas, Meitinger, Thomas, Prokisch, Holger, and Iuso, Arcangela

Published

2021

3. Emerging variants, unique phenotypes, and transcriptomic signatures: an integrated study of COASY‐associated diseases.

Author

Cavestro, Chiara, Morra, Francesca, Legati, Andrea, D'Amato, Marco, Nasca, Alessia, Iuso, Arcangela, Lubarr, Naomi, Morrison, Jennifer L., Wheeler, Patricia G., Serra‐Juhé, Clara, Rodríguez‐Santiago, Benjamín, Turón‐Viñas, Eulalia, Prouteau, Clement, Barth, Magalie, Hayflick, Susan J., Ghezzi, Daniele, Tiranti, Valeria, and Di Meo, Ivano

Subjects

PHENOTYPES, EPILEPSY, CELL communication, COENZYME A, AUTISM spectrum disorders, TRANSCRIPTOMES

Abstract

Objective: COASY, the gene encoding the bifunctional enzyme CoA synthase, which catalyzes the last two reactions of cellular de novo coenzyme A (CoA) biosynthesis, has been linked to two exceedingly rare autosomal recessive disorders, such as COASY protein‐associated neurodegeneration (CoPAN), a form of neurodegeneration with brain iron accumulation (NBIA), and pontocerebellar hypoplasia type 12 (PCH12). We aimed to expand the phenotypic spectrum and gain insights into the pathogenesis of COASY‐related disorders. Methods: Patients were identified through targeted or exome sequencing. To unravel the molecular mechanisms of disease, RNA sequencing, bioenergetic analysis, and quantification of critical proteins were performed on fibroblasts. Results: We identified five new individuals harboring novel COASY variants. While one case exhibited classical CoPAN features, the others displayed atypical symptoms such as deafness, language and autism spectrum disorders, brain atrophy, and microcephaly. All patients experienced epilepsy, highlighting its potential frequency in COASY‐related disorders. Fibroblast transcriptomic profiling unveiled dysregulated expression in genes associated with mitochondrial respiration, responses to oxidative stress, transmembrane transport, various cellular signaling pathways, and protein translation, modification, and trafficking. Bioenergetic analysis revealed impaired mitochondrial oxygen consumption in COASY fibroblasts. Despite comparable total CoA levels to control cells, the amounts of mitochondrial 4′‐phosphopantetheinylated proteins were significantly reduced in COASY patients. Interpretation: These results not only extend the clinical phenotype associated with COASY variants but also suggest a continuum between CoPAN and PCH12. The intricate interplay of altered cellular processes and signaling pathways provides valuable insights for further research into the pathogenesis of COASY‐associated diseases. [ABSTRACT FROM AUTHOR]

Published

2024

4. A Homozygous Splice Site Mutation in SLC25A42, Encoding the Mitochondrial Transporter of Coenzyme A, Causes Metabolic Crises and Epileptic Encephalopathy

Author

Iuso, Arcangela, Alhaddad, Bader, Weigel, Corina, Kotzaeridou, Urania, Mastantuono, Elisa, Schwarzmayr, Thomas, Graf, Elisabeth, Terrile, Caterina, Prokisch, Holger, Strom, Tim M., Hoffmann, Georg F., Meitinger, Thomas, Haack, Tobias B., Baumgartner, Matthias, Series Editor, Patterson, Marc, Series Editor, Rahman, Shamima, Series Editor, Peters, Verena, Series Editor, Morava, Eva, Editor-in-Chief, and Zschocke, Johannes, Series Editor

Published

2019

5. Monogenic variants in dystonia: an exome-wide sequencing study

Author

Zech, Michael, Jech, Robert, Boesch, Sylvia, Škorvánek, Matej, Weber, Sandrina, Wagner, Matias, Zhao, Chen, Jochim, Angela, Necpál, Ján, Dincer, Yasemin, Vill, Katharina, Distelmaier, Felix, Stoklosa, Malgorzata, Krenn, Martin, Grunwald, Stephan, Bock-Bierbaum, Tobias, Fečíková, Anna, Havránková, Petra, Roth, Jan, Příhodová, Iva, Adamovičová, Miriam, Ulmanová, Olga, Bechyně, Karel, Danhofer, Pavlína, Veselý, Branislav, Haň, Vladimír, Pavelekova, Petra, Gdovinová, Zuzana, Mantel, Tobias, Meindl, Tobias, Sitzberger, Alexandra, Schröder, Sebastian, Blaschek, Astrid, Roser, Timo, Bonfert, Michaela V, Haberlandt, Edda, Plecko, Barbara, Leineweber, Birgit, Berweck, Steffen, Herberhold, Thomas, Langguth, Berthold, Švantnerová, Jana, Minár, Michal, Ramos-Rivera, Gonzalo Alonso, Wojcik, Monica H, Pajusalu, Sander, Õunap, Katrin, Schatz, Ulrich A, Pölsler, Laura, Milenkovic, Ivan, Laccone, Franco, Pilshofer, Veronika, Colombo, Roberto, Patzer, Steffi, Iuso, Arcangela, Vera, Julia, Troncoso, Monica, Fang, Fang, Prokisch, Holger, Wilbert, Friederike, Eckenweiler, Matthias, Graf, Elisabeth, Westphal, Dominik S, Riedhammer, Korbinian M, Brunet, Theresa, Alhaddad, Bader, Berutti, Riccardo, Strom, Tim M, Hecht, Martin, Baumann, Matthias, Wolf, Marc, Telegrafi, Aida, Person, Richard E, Zamora, Francisca Millan, Henderson, Lindsay B, Weise, David, Musacchio, Thomas, Volkmann, Jens, Szuto, Anna, Becker, Jessica, Cremer, Kirsten, Sycha, Thomas, Zimprich, Fritz, Kraus, Verena, Makowski, Christine, Gonzalez-Alegre, Pedro, Bardakjian, Tanya M, Ozelius, Laurie J, Vetro, Annalisa, Guerrini, Renzo, Maier, Esther, Borggraefe, Ingo, Kuster, Alice, Wortmann, Saskia B, Hackenberg, Annette, Steinfeld, Robert, Assmann, Birgit, Staufner, Christian, Opladen, Thomas, Růžička, Evžen, Cohn, Ronald D, Dyment, David, Chung, Wendy K, Engels, Hartmut, Ceballos-Baumann, Andres, Ploski, Rafal, Daumke, Oliver, Haslinger, Bernhard, Mall, Volker, Oexle, Konrad, and Winkelmann, Juliane

Published

2020

6. Generation of two human iPSC lines, HMGUi004-A and FINCBi004-A, from fibroblasts of MPAN patients carrying pathogenic recessive mutations in the gene C19orf12

Author

Zanuttigh, Enrica, primary, Rusha, Ejona, additional, Peron, Camille, additional, Brunetti, Dario, additional, Zorzi, Giovanna, additional, Pertek, Anna, additional, Nteli, Polyxeni, additional, Winkelmann, Juliane, additional, Tiranti, Valeria, additional, and Iuso, Arcangela, additional

Published

2023

7. A burning question from the first international BPAN symposium: is restoration of autophagy a promising therapeutic strategy for BPAN?

Author

Mollereau, Bertrand, primary, Hayflick, Susan J, additional, Escalante, Ricardo, additional, Mauthe, Mario, additional, Papandreou, Apostolos, additional, Iuso, Arcangela, additional, Celle, Marion, additional, Aniorte, Sahra, additional, Issa, Abdul Raouf, additional, Lasserre, Jean Paul, additional, Lesca, Gaetan, additional, Thobois, Stéphane, additional, Burger, Pauline, additional, and Walter, Ludivine, additional

Published

2023

8. A Spatiotemporal Proteomic Map of Human Adipogenesis

Author

Klingelhuber, Felix, primary, Frendo-Cumbo, Scott, additional, Omar-Hmeadi, Muhmmad, additional, Taylor, Austin J., additional, Kakimoto, Pamela, additional, Couchet, Morgane, additional, Ribicic, Sara, additional, Wabitsch, Martin, additional, Messias, Ana C., additional, Iuso, Arcangela, additional, Müller, Timo D., additional, Rydén, Mikael, additional, Mejhert, Niklas, additional, and Krahmer, Natalie, additional

Published

2023

9. A Homozygous Splice Site Mutation in SLC25A42, Encoding the Mitochondrial Transporter of Coenzyme A, Causes Metabolic Crises and Epileptic Encephalopathy

Author

Iuso, Arcangela, primary, Alhaddad, Bader, additional, Weigel, Corina, additional, Kotzaeridou, Urania, additional, Mastantuono, Elisa, additional, Schwarzmayr, Thomas, additional, Graf, Elisabeth, additional, Terrile, Caterina, additional, Prokisch, Holger, additional, Strom, Tim M., additional, Hoffmann, Georg F., additional, Meitinger, Thomas, additional, and Haack, Tobias B., additional

Published

2018

10. Arabidopsis thaliana alternative dehydrogenases: a potential therapy for mitochondrial complex I deficiency? Perspectives and pitfalls

Author

Catania, Alessia, Iuso, Arcangela, Bouchereau, Juliette, Kremer, Laura S., Paviolo, Marina, Terrile, Caterina, Bénit, Paule, Rasmusson, Allan G., Schwarzmayr, Thomas, Tiranti, Valeria, Rustin, Pierre, Rak, Malgorzata, Prokisch, Holger, and Schiff, Manuel

Published

2019

11. Identification of Autophagy as a Functional Target Suitable for the Pharmacological Treatment of Mitochondrial Membrane Protein-Associated Neurodegeneration (MPAN) In Vitro

Author

Zanuttigh, Enrica, primary, Derderian, Kevork, additional, Güra, Miriam A., additional, Geerlof, Arie, additional, Di Meo, Ivano, additional, Cavestro, Chiara, additional, Hempfling, Stefan, additional, Ortiz-Collazos, Stephanie, additional, Mauthe, Mario, additional, Kmieć, Tomasz, additional, Cammarota, Eugenia, additional, Panzeri, Maria Carla, additional, Klopstock, Thomas, additional, Sattler, Michael, additional, Winkelmann, Juliane, additional, Messias, Ana C., additional, and Iuso, Arcangela, additional

Published

2023

12. Rare causes of early-onset dystonia-parkinsonism with cognitive impairment: a de novo PSEN-1 mutation

Author

Carecchio, Miryam, Picillo, Marina, Valletta, Lorella, Elia, Antonio E., Haack, Tobias B., Cozzolino, Autilia, Vitale, Annalisa, Garavaglia, Barbara, Iuso, Arcangela, Bagella, Caterina F., Pappatà, Sabina, Barone, Paolo, Prokisch, Holger, Romito, Luigi, and Tiranti, Valeria

Published

2017

13. Assessing Mitochondrial Bioenergetics in Isolated Mitochondria from Various Mouse Tissues Using Seahorse XF96 Analyzer

Author

Iuso, Arcangela, primary, Repp, Birgit, additional, Biagosch, Caroline, additional, Terrile, Caterina, additional, and Prokisch, Holger, additional

Published

2017

14. Novel phosphopantothenoylcysteine synthetase (PPCS) mutations with prominent neuromuscular features: Expanding the phenotypical spectrum ofPPCS‐related disorders

Author

Lok, Aishin, primary, Fernandez‐Garcia, Miguel A., additional, Taylor, Robert W., additional, French, Courtney, additional, MacFarland, Robert, additional, Bodi, Istvan, additional, Champion, Michael, additional, Josifova, Dragana, additional, Raymond, Frances Lucy, additional, Iuso, Arcangela, additional, Jungbluth, Heinz, additional, Milan, Anna, additional, and Singh, Rahul R., additional

Published

2022

15. Generation of two human iPSC lines, HMGUi003-A and MRIi028-A, carrying pathogenic biallelic variants in the PPCS gene

Author

Iuso, Arcangela, primary, Zhang, Fangfang, additional, Rusha, Ejona, additional, Campbell, Birgit, additional, Dorn, Tatjana, additional, Zanuttigh, Enrica, additional, Haas, Dorothea, additional, Anikster, Yair, additional, Lederer, Gabriele, additional, Pertek, Anna, additional, Nteli, Polyxeni, additional, Laugwitz, Karl-Ludwig, additional, and Moretti, Alessandra, additional

Published

2022

16. Disturbed mitochondrial and peroxisomal dynamics due to loss of MFF causes Leigh-like encephalopathy, optic atrophy and peripheral neuropathy

Author

Koch, Johannes, Feichtinger, René G, Freisinger, Peter, Pies, Mechthild, Schrödl, Falk, Iuso, Arcangela, Sperl, Wolfgang, Mayr, Johannes A, Prokisch, Holger, and Haack, Tobias B

Published

2016

17. Novel phosphopantothenoylcysteine synthetase (PPCS) mutations with prominent neuromuscular features: Expanding the phenotypical spectrum of PPCS‐related disorders.

Author

Lok, Aishin, Fernandez‐Garcia, Miguel A., Taylor, Robert W., French, Courtney, MacFarland, Robert, Bodi, Istvan, Champion, Michael, Josifova, Dragana, Raymond, Frances Lucy, Iuso, Arcangela, Jungbluth, Heinz, Milan, Anna, and Singh, Rahul R.

Abstract

Biallelic pathogenic variants in phosphopantothenoylcysteine synthetase, PPCS, are a rare cause of a severe early‐onset dilated cardiomyopathy with high morbidity and mortality. To date, only five individuals with PPCS‐mutations have been reported. Here, we report a female infant who presented in the neonatal period with hypotonia, a necrotizing myopathy with intermittent rhabdomyolysis and other extracardiac manifestations before developing a progressive and ultimately fatal dilated cardiomyopathy. Gene agnostic trio genome sequencing revealed two rare variants in the PPCS [MIM: 609853] in trans, a previously reported pathogenic c.320_334del p. (Pro107_Ala111del) variant, and a c.613‐3C>G intronic variant of uncertain significance. Functional studies confirmed the likely pathogenicity of this variant. Our case provides clinical and histopathological evidence for an associated neuromuscular phenotype not previously recognized and expands the evolving phenotypic spectrum of PPCS‐related disorders. We also performed a literature search of all previously published cases and summarize the common features. [ABSTRACT FROM AUTHOR]

Published

2022

18. Loss‐of‐function variants in HOPS complex genes VPS16 and VPS41 cause early‐onset dystonia associated with lysosomal abnormalities

Author

Steel, Dora, Zech, Michael, Zhao, Chen, Barwick, Katy ES, Burke, Derek, Demailly, Diane, Kumar, Kishore R, Zorzi, Giovanna, Nardocci, Nardo, Kaiyrzhanov, Rauan, Wagner, Matias, Iuso, Arcangela, Berutti, Riccardo, Škorvánek, Matej, Necpál, Ján, Davis, Ryan, Wiethoff, Sarah, Mankad, Kshitij, Sudhakar, Sniya, Ferrini, Arianna, Sharma, Suvasini, Kamsteeg, Erik?Jan, Tijssen, Marina A, Verschuuren, Corien, Egmond, Martje E, Flowers, Joanna M, McEntagart, Meriel, Tucci, Arianna, Coubes, Philippe, Bustos, Bernabe I, Gonzalez-Latapi, Paulina, Tisch, Stephen, Darveniza, Paul, Gorman, Kathleen M, Peall, Kathryn J, Bötzel, Kai, Koch, Jan C, Kmiec, Tomasz, Plecko, Barbara, Boesch, Sylvia, Haslinger, Bernhard, Jech, Robert, Garavaglia, Barbara, Wood, Nick, Houlden, Henry, Gissen, Paul, Lubbe, Steven J, Sue, Carolyn M, Cif, Laura, Mencacci, Niccolò E, Anderson, Glenn, Kurian, Manju A, and Winkelmann, Juliane

Abstract

Objectives\ud The majority of people with suspected genetic dystonia remain undiagnosed after maximal investigation, implying that a number of causative genes have not yet been recognised. We aimed to investigate this paucity of diagnoses.\ud \ud Methods\ud We undertook weighted burden analysis of whole‐exome sequencing data from 138 individuals with unresolved generalised dystonia of suspected genetic aetiology, followed by additional case‐finding from international databases, first for the gene implicated by the burden analysis (VPS16), then for other functionally related genes. Electron microscopy was performed on patient‐derived cells.\ud \ud Results\ud Analysis revealed a significant burden for VPS16 (Fisher's exact test p‐value, 6.9x10−9). VPS16 encodes a subunit of the homotypic fusion and vacuole protein sorting (HOPS) complex, which plays a key role in autophagosome‐lysosome fusion. A total of 18 individuals harbouring heterozygous loss‐of‐function VPS16 variants, and one with a microdeletion, were identified. These individuals experienced early‐onset progressive dystonia with predominant cervical, bulbar, orofacial and upper limb involvement. Some patients had a more complex phenotype with additional neuropsychiatric and/or developmental comorbidities. We also identified biallelic loss‐of‐function variants in VPS41, another HOPS‐complex encoding genes, in an individual with infantile‐onset generalised dystonia. Electron microscopy of patient‐derived lymphocytes and fibroblasts from both VPS16 and VPS41 patients showed vacuolar abnormalities suggestive of impaired lysosomal function.\ud \ud Interpretation\ud Our study strongly supports a role for HOPS complex dysfunction in the pathogenesis of dystonia, though variants in different subunits display different phenotypic and inheritance characteristics.

Published

2020

19. Loss‐of‐Function Variants in HOPS Complex Genes VPS16 and VPS41 Cause Early Onset Dystonia Associated with Lysosomal Abnormalities

Author

Steel, Dora, Zech, Michael, Zhao, Chen, Barwick, Katy E. S., Burke, Derek, Demailly, Diane, Kumar, Kishore R., Zorzi, Giovanna, Nardocci, Nardo, Kaiyrzhanov, Rauan, Wagner, Matias, Iuso, Arcangela, Berutti, Riccardo, Škorvánek, Matej, Necpál, Ján, Davis, Ryan, Wiethoff, Sarah, Mankad, Kshitij, Sudhakar, Sniya, Ferrini, Arianna, Sharma, Suvasini, Kamsteeg, Erik‐Jan, Tijssen, Marina A., Verschuuren, Corien, Egmond, Martje E., Flowers, Joanna M., McEntagart, Meriel, Tucci, Arianna, Coubes, Philippe, Bustos, Bernabe I., Gonzalez‐Latapi, Paulina, Tisch, Stephen, Darveniza, Paul, Gorman, Kathleen M., Peall, Kathryn J., Bötzel, Kai, Koch, Jan C., Kmieć, Tomasz, Plecko, Barbara, Boesch, Sylvia, Haslinger, Bernhard, Jech, Robert, Garavaglia, Barbara, Wood, Nick, Houlden, Henry, Gissen, Paul, Lubbe, Steven J., Sue, Carolyn M., Cif, Laura, Mencacci, Niccolò E., Anderson, Glenn, Kurian, Manju A., and Winkelmann, Juliane

Subjects

ddc

Published

2019

20. Bi-allelic mutations in TRAPPC2L result in a neurodevelopmental disorder and have an impact on RAB11 in fibroblasts

Author

Milev, Miroslav P., Graziano, Claudio, Karall, Daniela, Kuper, Willemijn F.E., Al-Deri, Noraldin, Cordelli, Duccio Maria, Haack, Tobias B., Danhauser, Katharina, Iuso, Arcangela, Palombo, Flavia, Pippucci, Tommaso, Prokisch, Holger, Saint-Dic, Djenann, Seri, Marco, Stanga, Daniela, Cenacchi, Giovanna, Van Gassen, Koen L.I., Zschocke, Johannes, Fauth, Christine, Mayr, Johannes A., Sacher, Michael, Van Hasselt, Peter M., Milev, Miroslav P., Graziano, Claudio, Karall, Daniela, Kuper, Willemijn F.E., Al-Deri, Noraldin, Cordelli, Duccio Maria, Haack, Tobias B., Danhauser, Katharina, Iuso, Arcangela, Palombo, Flavia, Pippucci, Tommaso, Prokisch, Holger, Saint-Dic, Djenann, Seri, Marco, Stanga, Daniela, Cenacchi, Giovanna, Van Gassen, Koen L.I., Zschocke, Johannes, Fauth, Christine, Mayr, Johannes A., Sacher, Michael, and Van Hasselt, Peter M.

Published

2018

21. Bi-allelic mutations in TRAPPC2L result in a neurodevelopmental disorder and have an impact on RAB11 in fibroblasts

Author

Metabole ziekten onderzoek 1, Genetica, Genetica Sectie Genoomdiagnostiek, Child Health, Cluster C, Metabole ziekten patientenzorg, Milev, Miroslav P., Graziano, Claudio, Karall, Daniela, Kuper, Willemijn F.E., Al-Deri, Noraldin, Cordelli, Duccio Maria, Haack, Tobias B., Danhauser, Katharina, Iuso, Arcangela, Palombo, Flavia, Pippucci, Tommaso, Prokisch, Holger, Saint-Dic, Djenann, Seri, Marco, Stanga, Daniela, Cenacchi, Giovanna, Van Gassen, Koen L.I., Zschocke, Johannes, Fauth, Christine, Mayr, Johannes A., Sacher, Michael, Van Hasselt, Peter M., Metabole ziekten onderzoek 1, Genetica, Genetica Sectie Genoomdiagnostiek, Child Health, Cluster C, Metabole ziekten patientenzorg, Milev, Miroslav P., Graziano, Claudio, Karall, Daniela, Kuper, Willemijn F.E., Al-Deri, Noraldin, Cordelli, Duccio Maria, Haack, Tobias B., Danhauser, Katharina, Iuso, Arcangela, Palombo, Flavia, Pippucci, Tommaso, Prokisch, Holger, Saint-Dic, Djenann, Seri, Marco, Stanga, Daniela, Cenacchi, Giovanna, Van Gassen, Koen L.I., Zschocke, Johannes, Fauth, Christine, Mayr, Johannes A., Sacher, Michael, and Van Hasselt, Peter M.

Published

2018

22. OCR-Stats: Robust estimation and statistical testing of mitochondrial respiration activities using Seahorse XF Analyzer

Author

Yépez, Vicente A., Kremer, Laura S., Iuso, Arcangela, Gusic, Mirjana, Kopajtich, Robert, Koňaříková, Eliška, Nadel, Agnieszka, Wachutka, Leonhard, Prokisch, Holger, and Gagneur, Julien

Subjects

ddc

Published

2017

23. Bi-allelic mutations in TRAPPC2L result in a neurodevelopmental disorder and have an impact on RAB11 in fibroblasts

Author

Milev, Miroslav P, primary, Graziano, Claudio, additional, Karall, Daniela, additional, Kuper, Willemijn F E, additional, Al-Deri, Noraldin, additional, Cordelli, Duccio Maria, additional, Haack, Tobias B, additional, Danhauser, Katharina, additional, Iuso, Arcangela, additional, Palombo, Flavia, additional, Pippucci, Tommaso, additional, Prokisch, Holger, additional, Saint-Dic, Djenann, additional, Seri, Marco, additional, Stanga, Daniela, additional, Cenacchi, Giovanna, additional, van Gassen, Koen L I, additional, Zschocke, Johannes, additional, Fauth, Christine, additional, Mayr, Johannes A, additional, Sacher, Michael, additional, and van Hasselt, Peter M, additional

Published

2018

24. OCR-Stats: Robust estimation and statistical testing of mitochondrial respiration activities using Seahorse XF Analyzer

Author

Yépez, Vicente A., primary, Kremer, Laura S., additional, Iuso, Arcangela, additional, Gusic, Mirjana, additional, Kopajtich, Robert, additional, Koňaříková, Eliška, additional, Nadel, Agnieszka, additional, Wachutka, Leonhard, additional, Prokisch, Holger, additional, and Gagneur, Julien, additional

Published

2018

25. Mutations in PPCS, Encoding Phosphopantothenoylcysteine Synthetase, Cause Autosomal-Recessive Dilated Cardiomyopathy

Author

Iuso, Arcangela, primary, Wiersma, Marit, additional, Schüller, Hans-Joachim, additional, Pode-Shakked, Ben, additional, Marek-Yagel, Dina, additional, Grigat, Mathias, additional, Schwarzmayr, Thomas, additional, Berutti, Riccardo, additional, Alhaddad, Bader, additional, Kanon, Bart, additional, Grzeschik, Nicola A., additional, Okun, Jürgen G., additional, Perles, Zeev, additional, Salem, Yishay, additional, Barel, Ortal, additional, Vardi, Amir, additional, Rubinshtein, Marina, additional, Tirosh, Tal, additional, Dubnov-Raz, Gal, additional, Messias, Ana C., additional, Terrile, Caterina, additional, Barshack, Iris, additional, Volkov, Alex, additional, Avivi, Camilla, additional, Eyal, Eran, additional, Mastantuono, Elisa, additional, Kumbar, Muhamad, additional, Abudi, Shachar, additional, Braunisch, Matthias, additional, Strom, Tim M., additional, Meitinger, Thomas, additional, Hoffmann, Georg F., additional, Prokisch, Holger, additional, Haack, Tobias B., additional, Brundel, Bianca J.J.M., additional, Haas, Dorothea, additional, Sibon, Ody C.M., additional, and Anikster, Yair, additional

Published

2018

26. OCR-Stats: Robust estimation and statistical testing of mitochondrial respiration activities using Seahorse XF Analyzer

Author

Yépez, Vicente A., primary, Kremer, Laura S., additional, Iuso, Arcangela, additional, Gušić, Mirjana, additional, Kopajtich, Robert, additional, Koňaříková, Eliška, additional, Nadel, Agnieszka, additional, Wachutka, Leonhard, additional, Prokisch, Holger, additional, and Gagneur, Julien, additional

Published

2017

27. Characterization of a Leber's hereditary optic neuropathy (LHON) family harboring two primary LHON mutations m.11778G > A and m.14484T > C of the mitochondrial DNA

Author

Catarino, Claudia B., primary, Ahting, Uwe, additional, Gusic, Mirjana, additional, Iuso, Arcangela, additional, Repp, Birgit, additional, Peters, Katrin, additional, Biskup, Saskia, additional, von Livonius, Bettina, additional, Prokisch, Holger, additional, and Klopstock, Thomas, additional

Published

2017

28. Genetic diagnosis of Mendelian disorders via RNA sequencing

Author

Kremer, Laura S., primary, Bader, Daniel M., additional, Mertes, Christian, additional, Kopajtich, Robert, additional, Pichler, Garwin, additional, Iuso, Arcangela, additional, Haack, Tobias B., additional, Graf, Elisabeth, additional, Schwarzmayr, Thomas, additional, Terrile, Caterina, additional, Koňaříková, Eliška, additional, Repp, Birgit, additional, Kastenmüller, Gabi, additional, Adamski, Jerzy, additional, Lichtner, Peter, additional, Leonhardt, Christoph, additional, Funalot, Benoit, additional, Donati, Alice, additional, Tiranti, Valeria, additional, Lombes, Anne, additional, Jardel, Claude, additional, Gläser, Dieter, additional, Taylor, Robert W., additional, Ghezzi, Daniele, additional, Mayr, Johannes A., additional, Rötig, Agnes, additional, Freisinger, Peter, additional, Distelmaier, Felix, additional, Strom, Tim M., additional, Meitinger, Thomas, additional, Gagneur, Julien, additional, and Prokisch, Holger, additional

Published

2017

29. Absence of the Autophagy Adaptor SQSTM1/p62 Causes Childhood-Onset Neurodegeneration with Ataxia, Dystonia, and Gaze Palsy

Author

Haack, Tobias B., primary, Ignatius, Erika, additional, Calvo-Garrido, Javier, additional, Iuso, Arcangela, additional, Isohanni, Pirjo, additional, Maffezzini, Camilla, additional, Lönnqvist, Tuula, additional, Suomalainen, Anu, additional, Gorza, Matteo, additional, Kremer, Laura S., additional, Graf, Elisabeth, additional, Hartig, Monika, additional, Berutti, Riccardo, additional, Paucar, Martin, additional, Svenningsson, Per, additional, Stranneheim, Henrik, additional, Brandberg, Göran, additional, Wedell, Anna, additional, Kurian, Manju A., additional, Hayflick, Susan A., additional, Venco, Paola, additional, Tiranti, Valeria, additional, Strom, Tim M., additional, Dichgans, Martin, additional, Horvath, Rita, additional, Holinski-Feder, Elke, additional, Freyer, Christoph, additional, Meitinger, Thomas, additional, Prokisch, Holger, additional, Senderek, Jan, additional, Wredenberg, Anna, additional, Carroll, Christopher J., additional, and Klopstock, Thomas, additional

Published

2016

30. Genetic diagnosis of Mendelian disorders via RNA sequencing

Author

Kremer, Laura S, primary, Bader, Daniel M, additional, Mertes, Christian, additional, Kopajtich, Robert, additional, Pichler, Garwin, additional, Iuso, Arcangela, additional, Haack, Tobias B, additional, Graf, Elisabeth, additional, Schwarzmayr, Thomas, additional, Terrile, Caterina, additional, Koňařiková, Eliška, additional, Repp, Birgit, additional, Kastenmüller, Gabi, additional, Adamski, Jerzy, additional, Lichtner, Peter, additional, Leonhardt, Christoph, additional, Funalot, Benoit, additional, Donati, Alice, additional, Tiranti, Valeria, additional, Lombes, Anne, additional, Jardel, Claude, additional, Gläser, Dieter, additional, Taylor, Robert W., additional, Ghezzi, Daniele, additional, Mayr, Johannes A, additional, Rötig, Agnes, additional, Freisinger, Peter, additional, Distelmaier, Felix, additional, Strom, Tim M, additional, Meitinger, Thomas, additional, Gagneur, Julien, additional, and Prokisch, Holger, additional

Published

2016

31. Bi-allelic Truncating Mutations in TANGO2 Cause Infancy-Onset Recurrent Metabolic Crises with Encephalocardiomyopathy

Author

Kremer, Laura S., primary, Distelmaier, Felix, additional, Alhaddad, Bader, additional, Hempel, Maja, additional, Iuso, Arcangela, additional, Küpper, Clemens, additional, Mühlhausen, Chris, additional, Kovacs-Nagy, Reka, additional, Satanovskij, Robin, additional, Graf, Elisabeth, additional, Berutti, Riccardo, additional, Eckstein, Gertrud, additional, Durbin, Richard, additional, Sauer, Sascha, additional, Hoffmann, Georg F., additional, Strom, Tim M., additional, Santer, René, additional, Meitinger, Thomas, additional, Klopstock, Thomas, additional, Prokisch, Holger, additional, and Haack, Tobias B., additional

Published

2016

32. Mutations of C19orf12, coding for a transmembrane glycine zipper containing mitochondrial protein, cause mis-localization of the protein, inability to respond to oxidative stress and increased mitochondrial Ca2+

Author

Venco, Paola, Bonora, Massimo, Giorgi, Carlotta, Papaleo, Elena, Iuso, Arcangela, Prokisch, Holger, Pinton, Paolo, Tiranti, Valeria, Venco, Paola, Bonora, Massimo, Giorgi, Carlotta, Papaleo, Elena, Iuso, Arcangela, Prokisch, Holger, Pinton, Paolo, and Tiranti, Valeria

Abstract

Mutations in C19orf12 have been identified in patients affected by Neurodegeneration with Brain Iron Accumulation (NBIA), a clinical entity characterized by iron accumulation in the basal ganglia. By using western blot analysis with specific antibody and confocal studies, we showed that wild-type C19orf12 protein was not exclusively present in mitochondria, but also in the Endoplasmic Reticulum (ER) and MAM (Mitochondria Associated Membrane), while mutant C19orf12 variants presented a different localization. Moreover, after induction of oxidative stress, a GFP-tagged C19orf12 wild-type protein was able to relocate to the cytosol. On the contrary, mutant isoforms were not able to respond to oxidative stress. High mitochondrial calcium concentration and increased H2O2 induced apoptosis were found in fibroblasts derived from one patient as compared to controls. C19orf12 protein is a 17 kDa mitochondrial membrane-associated protein whose function is still unknown. Our in silico investigation suggests that, the glycine zipper motifs of C19orf12 form helical regions spanning the membrane. The N- and C-terminal regions with respect to the transmembrane portion, on the contrary, are predicted to rearrange in a structural domain, which is homologs to the N-terminal regulatory domain of the magnesium transporter MgtE, suggesting that C19orf12 may act as a regulatory protein for human MgtE transporters. The mutations here described affect respectively one glycine residue of the glycine zipper motifs, which are involved in dimerization of transmembrane helices and predicted to impair the correct localization of the protein into the membranes, and one residue present in the regulatory domain, which is important for protein-protein interaction.

Published

2015

33. Mutations of C19orf12, coding for a transmembrane glycine zipper containing mitochondrial protein, cause mis-localization of the protein, inability to respond to oxidative stress and increased mitochondrial Ca2+

Author

Venco, Paola, primary, Bonora, Massimo, additional, Giorgi, Carlotta, additional, Papaleo, Elena, additional, Iuso, Arcangela, additional, Prokisch, Holger, additional, Pinton, Paolo, additional, and Tiranti, Valeria, additional

Published

2015

34. Bi-allelic mutations in TRAPPC2Lresult in a neurodevelopmental disorder and have an impact on RAB11 in fibroblasts

Author

Milev, Miroslav P, Graziano, Claudio, Karall, Daniela, Kuper, Willemijn F E, Al-Deri, Noraldin, Cordelli, Duccio Maria, Haack, Tobias B, Danhauser, Katharina, Iuso, Arcangela, Palombo, Flavia, Pippucci, Tommaso, Prokisch, Holger, Saint-Dic, Djenann, Seri, Marco, Stanga, Daniela, Cenacchi, Giovanna, van Gassen, Koen L I, Zschocke, Johannes, Fauth, Christine, Mayr, Johannes A, Sacher, Michael, and van Hasselt, Peter M

Abstract

BackgroundThe combination of febrile illness-induced encephalopathy and rhabdomyolysis has thus far only been described in disorders that affect cellular energy status. In the absence of specific metabolic abnormalities, diagnosis can be challenging.ObjectiveThe objective of this study was to identify and characterise pathogenic variants in two individuals from unrelated families, both of whom presented clinically with a similar phenotype that included neurodevelopmental delay, febrile illness-induced encephalopathy and episodes of rhabdomyolysis, followed by developmental arrest, epilepsy and tetraplegia.MethodsWhole exome sequencing was used to identify pathogenic variants in the two individuals. Biochemical and cell biological analyses were performed on fibroblasts from these individuals and a yeast two-hybrid analysis was used to assess protein-protein interactions.ResultsProbands shared a homozygous TRAPPC2Lvariant (c.109G>T) resulting in a p.Asp37Tyr missense variant. TRAPPC2L is a component of transport protein particle (TRAPP), a group of multisubunit complexes that function in membrane traffic and autophagy. Studies in patient fibroblasts as well as in a yeast system showed that the p.Asp37Tyr protein was present but not functional and resulted in specific membrane trafficking delays. The human missense mutation and the analogous mutation in the yeast homologue Tca17 ablated the interaction between TRAPPC2L and TRAPPC10/Trs130, a component of the TRAPP II complex. Since TRAPP II activates the GTPase RAB11, we examined the activation state of this protein and found increased levels of the active RAB, correlating with changes in its cellular morphology.ConclusionsOur study implicates a RAB11 pathway in the aetiology of the TRAPPC2L disorder and has implications for other TRAPP-related disorders with similar phenotypes.

Published

2018

35. Mutations of C19orf12, coding for a transmembrane glycine zipper containing mitochondrial protein, cause mis-localization of the protein, inability to respond to oxidative stress and increased mitochondrial Ca2+.

Author

Venco, Paola, Bonora, Massimo, Giorgi, Carlotta, Papaleo, Elena, Iuso, Arcangela, Prokisch, Holger, Pinton, Paolo, and Tiranti, Valeria

Subjects

NEURODEGENERATION, BASAL ganglia, MITOCHONDRIA, ENDOPLASMIC reticulum, PROTEIN-protein interactions

Abstract

Mutations in C19orf12 have been identified in patients affected by Neurodegeneration with Brain Iron Accumulation (NBIA), a clinical entity characterized by iron accumulation in the basal ganglia. By using western blot analysis with specific antibody and confocal studies, we showed that wild-type C19orf12 protein was not exclusively present in mitochondria, but also in the Endoplasmic Reticulum (ER) and MAM (Mitochondria Associated Membrane), while mutant C19orf12 variants presented a different localization. Moreover, after induction of oxidative stress, a GFP-tagged C19orf12 wild-type protein was able to relocate to the cytosol. On the contrary, mutant isoforms were not able to respond to oxidative stress. High mitochondrial calcium concentration and increased H2O2 induced apoptosis were found in fibroblasts derived from one patient as compared to controls. C19orf12 protein is a 17 kDa mitochondrial membrane-associated protein whose function is still unknown. Our in silico investigation suggests that, the glycine zipper motifs of C19orf12 form helical regions spanning the membrane. The N- and C-terminal regions with respect to the transmembrane portion, on the contrary, are predicted to rearrange in a structural domain, which is homologs to the N-terminal regulatory domain of the magnesium transporter MgtE, suggesting that C19orf12 may act as a regulatory protein for human MgtE transporters. The mutations here described affect respectively one glycine residue of the glycine zipper motifs, which are involved in dimerization of transmembrane helices and predicted to impair the correct localization of the protein into the membranes, and one residue present in the regulatory domain, which is important for protein-protein interaction. [ABSTRACT FROM AUTHOR]

Published

2015

36. Loss-of-Function Variants in HOPS Complex Genes VPS16 and VPS41 Cause Early Onset Dystonia Associated with Lysosomal Abnormalities.

Author

Steel D, Zech M, Zhao C, Barwick KES, Burke D, Demailly D, Kumar KR, Zorzi G, Nardocci N, Kaiyrzhanov R, Wagner M, Iuso A, Berutti R, Škorvánek M, Necpál J, Davis R, Wiethoff S, Mankad K, Sudhakar S, Ferrini A, Sharma S, Kamsteeg EJ, Tijssen MA, Verschuuren C, van Egmond ME, Flowers JM, McEntagart M, Tucci A, Coubes P, Bustos BI, Gonzalez-Latapi P, Tisch S, Darveniza P, Gorman KM, Peall KJ, Bötzel K, Koch JC, Kmieć T, Plecko B, Boesch S, Haslinger B, Jech R, Garavaglia B, Wood N, Houlden H, Gissen P, Lubbe SJ, Sue CM, Cif L, Mencacci NE, Anderson G, Kurian MA, and Winkelmann J

Subjects

Adult, Cost of Illness, Dystonia pathology, Exome genetics, Female, Fibroblasts pathology, Genetic Predisposition to Disease genetics, Genetic Variation, Humans, Lysosomal Storage Diseases pathology, Male, Middle Aged, Mutation genetics, Pedigree, Dystonia genetics, Lysosomal Storage Diseases genetics, Vesicular Transport Proteins genetics

Abstract

Objectives: The majority of people with suspected genetic dystonia remain undiagnosed after maximal investigation, implying that a number of causative genes have not yet been recognized. We aimed to investigate this paucity of diagnoses., Methods: We undertook weighted burden analysis of whole-exome sequencing (WES) data from 138 individuals with unresolved generalized dystonia of suspected genetic etiology, followed by additional case-finding from international databases, first for the gene implicated by the burden analysis (VPS16), and then for other functionally related genes. Electron microscopy was performed on patient-derived cells., Results: Analysis revealed a significant burden for VPS16 (Fisher's exact test p value, 6.9 × 10 9 ). VPS16 encodes a subunit of the homotypic fusion and vacuole protein sorting (HOPS) complex, which plays a key role in autophagosome-lysosome fusion. A total of 18 individuals harboring heterozygous loss-of-function VPS16 variants, and one with a microdeletion, were identified. These individuals experienced early onset progressive dystonia with predominant cervical, bulbar, orofacial, and upper limb involvement. Some patients had a more complex phenotype with additional neuropsychiatric and/or developmental comorbidities. We also identified biallelic loss-of-function variants in VPS41, another HOPS-complex encoding gene, in an individual with infantile-onset generalized dystonia. Electron microscopy of patient-derived lymphocytes and fibroblasts from both patients with VPS16 and VPS41 showed vacuolar abnormalities suggestive of impaired lysosomal function., Interpretation: Our study strongly supports a role for HOPS complex dysfunction in the pathogenesis of dystonia, although variants in different subunits display different phenotypic and inheritance characteristics. ANN NEUROL 2020;88:867-877., (© 2020 The Authors. Annals of Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association.)

Published

2020

37. Characterization of a Leber's hereditary optic neuropathy (LHON) family harboring two primary LHON mutations m.11778G>A and m.14484T>C of the mitochondrial DNA.

Author

Catarino CB, Ahting U, Gusic M, Iuso A, Repp B, Peters K, Biskup S, von Livonius B, Prokisch H, and Klopstock T

Subjects

Adult, Age Factors, Aged, Female, Humans, Male, Middle Aged, Sex Ratio, DNA, Mitochondrial genetics, Family Health, Optic Atrophy, Hereditary, Leber genetics, Optic Atrophy, Hereditary, Leber pathology, Point Mutation

Abstract

Leber's hereditary optic neuropathy (LHON) is an inherited mitochondrial disease that usually leads to acute or subacute bilateral central vision loss. In 95% of cases, LHON is caused by one of three primary mutations of the mitochondrial DNA (mtDNA), m.11778G>A in the MT-ND4 gene, m.14484T>C in the MT-ND6 gene, or m.3460G>A in the MT-ND1 gene. Here we characterize clinically, genetically, and biochemically a LHON family with multiple patients harboring two of these primary LHON mutations, m.11778G>A homoplasmic and m.14484T>C heteroplasmic. The unusually low male-to-female ratio of affected family members is also seen among the other patients previously reported with two primary LHON mutations m.11778G>A and m.14484T>C. While the index patient had very late onset of symptoms at 75years and severe visual loss, her two daughters had both onset in childhood (6 and 9years), with moderate to mild visual loss. A higher degree of heteroplasmy of the m.14484T>C mutation was found to correlate with an earlier age at onset in this family. Ours is the first LHON family harboring two primary LHON mutations where functional studies were performed in several affected family members. A more pronounced bioenergetic defect was found to correlate with an earlier age at onset. The patient with the earliest age at onset had a more significant complex I dysfunction than all controls, including the LHON patient with only the m.11778G>A mutation, suggesting a synergistic effect of the two primary LHON mutations in this patient., (Copyright © 2017 Elsevier B.V. and Mitochondria Research Society. All rights reserved.)

Published

2017