Mutations in SLC39A14 disrupt manganese homeostasis and cause childhood-onset parkinsonism–dystonia

被引:0
|
作者
Karin Tuschl
Esther Meyer
Leonardo E. Valdivia
Ningning Zhao
Chris Dadswell
Alaa Abdul-Sada
Christina Y. Hung
Michael A. Simpson
W. K. Chong
Thomas S. Jacques
Randy L. Woltjer
Simon Eaton
Allison Gregory
Lynn Sanford
Eleanna Kara
Henry Houlden
Stephan M. Cuno
Holger Prokisch
Lorella Valletta
Valeria Tiranti
Rasha Younis
Eamonn R. Maher
John Spencer
Ania Straatman-Iwanowska
Paul Gissen
Laila A. M. Selim
Guillem Pintos-Morell
Wifredo Coroleu-Lletget
Shekeeb S. Mohammad
Sangeetha Yoganathan
Russell C. Dale
Maya Thomas
Jason Rihel
Olaf A. Bodamer
Caroline A. Enns
Susan J. Hayflick
Peter T. Clayton
Philippa B. Mills
Manju A. Kurian
Stephen W. Wilson
机构
[1] Genetics and Genomic Medicine,Department of Cell and Developmental Biology
[2] UCL Institute of Child Health,Department of Cell
[3] University College London,Department of Chemistry
[4] University College London,Division of Genetics and Genomics, Department of Medicine
[5] Developmental Neurosciences,Division of Genetics and Molecular Medicine
[6] UCL Institute of Child Health,Department of Radiology
[7] University College London,UCL Institute of Child Health and Department of Histopathology
[8] ,Department of Pathology
[9] Development and Cancer Biology,Department of Molecular & Medical Genetics
[10] Oregon Health & Sciences University,Department of Neurology
[11] School of Life Sciences,Department of Medical and Molecular Genetics
[12] University of Sussex,Department of Medical Genetics
[13] Boston Children’s Hospital and Harvard Medical School,Department of Metabolic Medicine
[14] King’s College London School of Medicine,Department of Paediatric Neurology
[15] Great Ormond Street Hospital for Children NHS Trust,Department of Paediatrics
[16] Developmental Biology and Cancer,Department of Paediatrics
[17] Great Ormond Street Hospital for Children NHS Trust,Department of Neurological Sciences
[18] Oregon Health & Science University,Department of Neurology
[19] Developmental Biology and Cancer Programme,Department of Pediatrics
[20] UCL Institute of Child Health,undefined
[21] University College London,undefined
[22] Oregon Health & Science University,undefined
[23] Institute of Neurology,undefined
[24] University College London,undefined
[25] Alzheimer’s Disease Research Centre,undefined
[26] Harvard Medical School and Massachusetts General Hospital,undefined
[27] Institute of Human Genetics,undefined
[28] Technische Universität München,undefined
[29] Institute of Human Genetics,undefined
[30] Helmholtz Zentrum München,undefined
[31] German Research Center for Environmental Health,undefined
[32] Unit of Molecular Neurogenetics,undefined
[33] IRCCS,undefined
[34] Foundation Neurological Institute ‘C. Besta’,undefined
[35] University of Birmingham,undefined
[36] Centre for Rare Diseases and Personalised Medicine,undefined
[37] School of Clinical and Experimental Medicine,undefined
[38] College of Medical and Dental Sciences,undefined
[39] University of Birmingham,undefined
[40] School of Clinical Medicine,undefined
[41] University of Cambridge,undefined
[42] and Cambridge NIHR Biomedical Research Centre,undefined
[43] MRC Laboratory for Molecular Cell Biology and Cell Biology Unit,undefined
[44] University College London,undefined
[45] Great Ormond Street Hospital for Children NHS Trust,undefined
[46] Faculty of Medicine,undefined
[47] Cairo University Children’s Hospital,undefined
[48] Section of Paediatric Nephrology,undefined
[49] Genetics and Metabolism,undefined
[50] Unit of Rare Diseases,undefined
来源
Nature Communications | / 7卷
关键词
D O I
暂无
中图分类号
学科分类号
摘要
Although manganese is an essential trace metal, little is known about its transport and homeostatic regulation. Here we have identified a cohort of patients with a novel autosomal recessive manganese transporter defect caused by mutations in SLC39A14. Excessive accumulation of manganese in these patients results in rapidly progressive childhood-onset parkinsonism–dystonia with distinctive brain magnetic resonance imaging appearances and neurodegenerative features on post-mortem examination. We show that mutations in SLC39A14 impair manganese transport in vitro and lead to manganese dyshomeostasis and altered locomotor activity in zebrafish with CRISPR-induced slc39a14 null mutations. Chelation with disodium calcium edetate lowers blood manganese levels in patients and can lead to striking clinical improvement. Our results demonstrate that SLC39A14 functions as a pivotal manganese transporter in vertebrates.
引用
收藏
相关论文
共 50 条
  • [21] A case of childhood-onset dystonia-parkinsonism due to homozygous parkin mutations and effect of globus pallidus deep brain stimulation
    Federica Garrì
    Dario Ciprietti
    Lisa Lerjefors
    Andrea Landi
    Manuela Pilleri
    Roberta Biundo
    Leonardo Salviati
    Miryam Carecchio
    Angelo Antonini
    Neurological Sciences, 2023, 44 : 3323 - 3326
  • [22] Hypermanganesemia due to mutations in SLC39A14: further insights into Mn deposition in the central nervous system
    L. Marti-Sanchez
    J. D. Ortigoza-Escobar
    A. Darling
    M. Villaronga
    H. Baide
    M. Molero-Luis
    M. Batllori
    M. I. Vanegas
    J. Muchart
    L. Aquino
    R. Artuch
    A. Macaya
    M. A. Kurian
    Pérez Dueñas
    Orphanet Journal of Rare Diseases, 13
  • [23] Phenotypic evaluation of a childhood-onset parkinsonism-dystonia mouse model with inherent postural abnormalities
    Giraldo, Genesys
    Janus, Christopher
    BRAIN RESEARCH BULLETIN, 2021, 166 : 54 - 63
  • [24] SLC39A14 deficiency alters manganese homeostasis and excretion resulting in brain manganese accumulation and motor deficits in mice (vol 115, pg E1769, 2018)
    Jenkitkasemwong, Supak
    Akinyode, Adenike
    Paulus, Elizabeth
    Weiskirchen, Ralf
    Hojyo, Shintaro
    Fukada, Toshiyuki
    Giraldo, Genesys
    Schrier, Jessica
    Garcia, Armin
    Janus, Christopher
    Giasson, Benoit
    Knutson, Mitchell D.
    PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2018, 115 (20) : E4730 - E4730
  • [25] Conditional mouse models support the role of SLC39A14 (ZIP14) in Hyperostosis Cranialis Interna and in bone homeostasis
    Hendrickx, Gretl
    Borra, Vere M.
    Steenackers, Ellen
    Yorgan, Timur A.
    Hermans, Christophe
    Boudin, Eveline
    Waterval, Jerome J.
    Jansen, Ineke D. C.
    Aydemir, Tolunay Beker
    Kamerling, Niels
    Behets, Geert J.
    Plumeyer, Christine
    D'Haese, Patrick C.
    Busse, Bjoern
    Everts, Vincent
    Lammens, Martin
    Mortier, Geert
    Cousins, Robert J.
    Schinke, Thorsten
    Stokroos, Robert J.
    Manni, Johannes J.
    Van Hul, Wim
    PLOS GENETICS, 2018, 14 (04): : e1007321
  • [26] Mutations in EMP2 Cause Childhood-Onset Nephrotic Syndrome
    Gee, Heon Yung
    Ashraf, Shazia
    Wan, Xiaoyang
    Vega-Warner, Virginia
    Esteve-Rudd, Julian
    Lovric, Svjetlana
    Fang, Humphrey
    Hurd, Toby W.
    Sadowski, Carolin E.
    Allen, Susan J.
    Otto, Edgar A.
    Korkmaz, Emine
    Washburn, Joseph
    Levy, Shawn
    Williams, David S.
    Bakkaloglu, Sevcan A.
    Zolotnitskaya, Anna
    Ozaltin, Fatih
    Zhou, Weibin
    Hildebrandt, Friedhelm
    AMERICAN JOURNAL OF HUMAN GENETICS, 2014, 94 (06) : 884 - 890
  • [27] GATA4 Mutations Are a Cause of Neonatal and Childhood-Onset Diabetes
    Shaw-Smith, Charles
    De Franco, Elisa
    Allen, Hana Lango
    Batlle, Marta
    Flanagan, Sarah E.
    Borowiec, Maciej
    Taplin, Craig E.
    van Alfen-van der Velden, Janielle
    Cruz-Rojo, Jaime
    Perez de Nanclares, Guiomar
    Miedzybrodzka, Zosia
    Deja, Grazyna
    Wlodarska, Iwona
    Mlynarski, Wojciech
    Ferrer, Jorge
    Hattersley, Andrew T.
    Ellard, Sian
    DIABETES, 2014, 63 (08) : 2888 - 2894
  • [28] BCL11B-Related Dystonia: Further Evidence of an Emerging Cause of Childhood-Onset Generalized Dystonia
    Garone, Giacomo
    Capuano, Alessandro
    Amodio, Donato
    Nicita, Francesco
    Travaglini, Lorena
    Graziola, Federica
    De Benedictis, Alessandro
    Frascarelli, Flaminia
    Parisi, Pasquale
    Pizzi, Simone
    Tartaglia, Marco
    Marras, Carlo Efisio
    Niceta, Marcello
    MOVEMENT DISORDERS CLINICAL PRACTICE, 2024, 11 (07): : 897 - 901
  • [29] Mutations in SLC30A10 Cause Parkinsonism and Dystonia with Hypermanganesemia, Polycythemia, and Chronic Liver Disease
    Quadri, Marialuisa
    Federico, Antonio
    Zhao, Tianna
    Breedveld, Guido J.
    Battisti, Carla
    Delnooz, Catherine
    Severijnen, Lies-Anne
    Mammarella, Lara Di Toro
    Mignarri, Andrea
    Monti, Lucia
    Sanna, Antioco
    Lu, Peng
    Punzo, Francesca
    Cossu, Giovanni
    Willemsen, Rob
    Rasi, Fabrizio
    Oostra, Ben A.
    van de Warrenburg, Bart P.
    Bonifati, Vincenzo
    AMERICAN JOURNAL OF HUMAN GENETICS, 2012, 90 (03) : 467 - 477
  • [30] TBCD mutations cause autosomal recessive early childhood-onset neurodegenerative encephalopathy
    Miyake, N.
    Chihara, T.
    Miura, M.
    Shimizu, H.
    Kakita, A.
    Matsumoto, N.
    EUROPEAN JOURNAL OF HUMAN GENETICS, 2018, 26 : 362 - 363
12345