Mitochondrial complex I NUBPL mutations cause combined dystonia with bilateral striatal necrosis and cerebellar atrophy

被引：8

作者：

Balint, B. ^{[1
,2
]}

Charlesworth, G. ^{[3
]}

Stamelou, M. ^{[4
,5
]}

Carr, L. ^{[6
]}

Mencacci, N. E. ^{[7
]}

Wood, N. W. ^{[8
]}

Bhatia, K. P. ^{[1
]}

机构：

[1] UCL Queen Sq Inst Neurol, Dept Clin & Movement Neurosci, Queen Sq, London WC1X 8EB, England

[2] Univ Hosp Heidelberg, Dept Neurol, Heidelberg, Germany

[3] Charing Cross Hosp, Dept Neurol, London, England

[4] Univ Athens, Dept Neurol 2, Attiko Hosp, Athens, Greece

[5] HYGEIA Hosp, Parkinsons Dis & Movement Disorders Dept, Athens, Greece

[6] GOSH, Neurosci Dept, London, England

[7] Northwestern Univ, Dept Neurol, Chicago, IL 60611 USA

[8] UCL, Dept Mol Neurosci, Inst Neurol, London, England

来源：

EUROPEAN JOURNAL OF NEUROLOGY | 2019年 / 26卷 / 09期

基金：

英国惠康基金;

关键词：

ataxia; autosomal recessive; bilateral striatal necrosis; dystonia; NUBPL;

D O I：

10.1111/ene.13956

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Background and purpose The recent advances in genetics have helped to unravel the cause of many dystonia syndromes. With the broadening spectrum of genetically defined dystonia syndromes, distinct clinico-radiological phenotypes are a welcome handle to guide the diagnostic work-up. Methods Exome sequencing was used to elucidate the genetic cause of a syndrome characterized by generalized dystonia, pyramidal and cerebellar involvement, with bilateral striatal necrosis (BSN) and cerebellar atrophy on magnetic resonance imaging. Homozygosity mapping and linkage analysis were used in a supportive role. Known genetic causes of BSN were excluded by use of exome data or Sanger sequencing. Results Compound heterozygous mutations were identified in the NUBPL gene in a small UK kindred. The gene lay in a region of positive linkage and segregated with disease in a family of six individuals. Conclusion NUBPL mutations cause early onset, autosomal recessive generalized dystonia with cerebellar ataxia, pyramidal signs, preserved cognition and a distinct magnetic resonance imaging appearance with BSN and cerebellar atrophy.

引用

页码：1240 / 1243

页数：4

共 34 条

[1] NUBPL mutations cause combined dystonia with bilateral striatal necrosis and cerebellar atrophy
Balint, B.
Charlesworth, G.
Stamelou, M.
Carr, L.
Wood, N. W.
Bhatia, K.
EUROPEAN JOURNAL OF NEUROLOGY, 2017, 24 : 474 - 475
[2] NUBPL mutations cause combined dystonia with bilateral striatal necrosis and cerebellar atrophy
Balint, B.
Charlesworth, G.
Stamelou, M.
Carr, L.
Wood, N.
Bhatia, K.
MOVEMENT DISORDERS, 2017, 32
[3] Mutations in the mitochondrial complex I assembly factor NDUFAF6 cause isolated bilateral striatal necrosis and progressive dystonia in childhood
Baide-Mairena, Heidy
Gaudo, Paula
Marti-Sanchez, Laura
Emperador, Sonia
Sanchez-Montanez, Angel
Alonso-Luengo, Olga
Correa, Marta
Marce Grau, Anna
Dario Ortigoza-Escobar, Juan
Artuch, Rafael
Vazquez, Elida
Del Toro, Mireia
Garrido-Perez, Nuria
Ruiz-Pesini, Eduardo
Montoya, Julio
Pilar Bayona-Bafaluy, Maria
Perez-Duenas, Belen
MOLECULAR GENETICS AND METABOLISM, 2019, 126 (03) : 250 - 258
[4] BILATERAL STRIATAL NECROSIS, DYSTONIA AND OPTIC ATROPHY IN 2 SIBLINGS
LEUZZI, V
BERTINI, E
DENEGRI, AM
GALLUCCI, M
GARAVAGLIA, B
JOURNAL OF NEUROLOGY NEUROSURGERY AND PSYCHIATRY, 1992, 55 (01): : 16 - 19
[5] Bilateral striatal necrosis, dystonia and multiple mitochondrial DNA deletions: Case study and effect of deep brain stimulation
Aniello, Maria Stella
Martino, Davide
Petruzzella, Vittoria
Eleopra, Roberto
Mancuso, Michelangelo
Dell'Aglio, Rosa
Cavallo, Michele
Siciliano, Gabriele
Defazio, Giovanni
MOVEMENT DISORDERS, 2008, 23 (01) : 114 - 118
[6] A Novel Variation in the Mitochondrial Complex I Assembly Factor NDUFAF5 Causes Isolated Bilateral Striatal Necrosis in Childhood
Bi, Hongyan
Guo, Hui
Wang, Qianfei
Zhang, Xiao
Zhao, Yaming
Li, Jimei
Zhao, Weiqin
Tuo, Houzhen
Zhang, Yongbo
FRONTIERS IN NEUROLOGY, 2021, 12
[7] MECR Mutations Cause Childhood-Onset Dystonia and Optic Atrophy, a Mitochondrial Fatty Acid Synthesis Disorder
Heimer, Gali
Keraetaer, Juha M.
Riley, Lisa G.
Balasubramaniam, Shanti
Eyal, Eran
Pietikaeinen, Laura P.
Hiltunen, J. Kalervo
Marek-Yagel, Dina
Hamada, Jeffrey
Gregory, Allison
Rogers, Caleb
Hogarth, Penelope
Nance, Martha A.
Shalva, Nechama
Veber, Alvit
Tzadok, Michal
Nissenkorn, Andreea
Tonduti, Davide
Renaldo, Florence
Kraoua, Ichraf
Panteghini, Celeste
Valletta, Lorella
Garavaglia, Barbara
Cowley, Mark J.
Gayevskiy, Velimir
Roscioli, Tony
Silberstein, Jonathon M.
Hoffmann, Chen
Raas-Rothschild, Annick
Tiranti, Valeria
Anikster, Yair
Christodoulou, John
Kastaniotis, Alexander J.
Ben-Zeev, Bruria
Hayflick, Susan J.
AMERICAN JOURNAL OF HUMAN GENETICS, 2016, 99 (06) : 1229 - 1244
[8] A type I interferon signature identifies bilateral striatal necrosis due to mutations in ADAR1
Livingston, John H.
Lin, Jean-Pierre
Dale, Russell C.
Gill, Deepak
Brogan, Paul
Munnich, Arnold
Kurian, Manju A.
Gonzalez-Martinez, Victoria
De Goede, Christian G. E. L.
Falconer, Alastair
Forte, Gabriella
Jenkinson, Emma M.
Kasher, Paul R.
Szynkiewicz, Marcin
Rice, Gillian I.
Crow, Yanick J.
JOURNAL OF MEDICAL GENETICS, 2014, 51 (02) : 76 - 82
[9] FOXRED1 mutations are a novel cause of mitochondrial complex I deficiency
Fassone, E.
Duncan, A. J.
Taanman, J. W.
Pagnamenta, A. T.
Sadowski, M. I.
Holand, T.
Qasim, W.
Rutland, P.
Calvo, S. E.
Mootha, V. K.
Bitner-Glindzicz, M.
Rahman, S.
NEUROPATHOLOGY AND APPLIED NEUROBIOLOGY, 2011, 37 : 37 - 37
[10] SSBP1 mutations cause a complex optic atrophy spectrum disorder with mitochondrial DNA depletion
Pippucci, T.
Del Dotto, V.
Di Meo, I.
Magini, P.
Gusic, M.
Maresca, A.
Caporali, L.
Palombo, F.
Tagliavini, F.
Baugh, E. H.
La Morgia, C.
Barboni, P.
Carbonelli, M.
Valentino, M. L.
Liguori, R.
Shashi, V.
Sullivan, J.
Nagaraj, S.
Bertini, E.
Carrozzo, R.
Emma, F.
Cutcutache, I.
Armstrong, M.
Page, M.
Stong, N.
Davies, E.
Karall, D.
Boesch, S.
Seri, M.
Falkenberg, M.
Prokisch, H.
Katsanis, N.
Tiranti, V.
Carelli, V.
EUROPEAN JOURNAL OF HUMAN GENETICS, 2019, 27 : 1162 - 1163

← 1 2 3 4 →