Recessive <scp><i>NUP54</i></scp> Variants Underlie Early‐Onset Dystonia with Striatal Lesions

Harrer, Philip; Schalk, Audrey; Shimura, Masaru; Baer, Sarah; Calmels, Nadège; Spitz, Marie Aude; Wardé, Marie‐Thérèse Abi; Schaefer, Élise; Kittke, Volker; Dincer, Yasemin; Wagner, Matias; Dzinovic, Ivana; Berutti, Riccardo; Sato, Tatsuharu; Shirakawa, Toshihiko; Okazaki, Yasushi; Murayama, Kei; Oexle, Konrad; Prokisch, Holger; Mall, Volker; Melčák, Ivo; Winkelmann, Juliane; Zech, Michael

doi:10.1002/ana.26544

Cited by 8 publications

(5 citation statements)

References 20 publications

(56 reference statements)

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“…Neurons are heavily dependent on NPC function; neuronal plasticity requires transport of signaling molecules and transcription factors [3][4][5][6] and mRNA export for local translation is essential for several neurodevelopmental processes [7][8][9][10][11] . Accordingly, NPC defects are present in several nervous system diseases [12][13][14][15][16] and mutations in nucleoporins cause earlyonset neurological illness 17,18 . Indeed, neurons face a considerable challenge in maintaining proper nuclear function throughout their lifetime.…”

Section: Introductionmentioning

confidence: 99%

TorsinA is essential for the timing and localization of neuronal nuclear pore complex biogenesis

Kim

Phan

Ellisman

et al. 2023

Preprint

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Nuclear pore complexes (NPCs) regulate information transfer between the nucleus and cytoplasm. NPC defects are linked to several neurological diseases, but the processes governing NPC biogenesis and spatial organization are poorly understood. Here, we identify a temporal window of strongly upregulated NPC biogenesis during neuronal maturation. We demonstrate that the AAA+ protein torsinA, whose loss of function causes the neurodevelopmental movement disorder DYT-TOR1A (DYT1) dystonia, coordinates NPC spatial organization during this period without impacting total NPC density. Using a new mouse line in which endogenous Nup107 is Halo-Tagged, we find that torsinA is essential for correct localization of NPC formation. In the absence of torsinA, the inner nuclear membrane buds excessively at sites of mislocalized, nascent NPCs, and NPC assembly completion is delayed. Our work implies that NPC spatial organization and number are independently regulated and suggests that torsinA is critical for the normal localization and assembly kinetics of NPCs.

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Section: Introductionmentioning

confidence: 99%

TorsinA is essential for the timing and localization of neuronal nuclear pore complex biogenesis

Kim

Phan

Ellisman

et al. 2023

Preprint

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Section: Nucleoporin Variation and Diseasementioning

confidence: 99%

“…In the central channel, Nup54 mutations have been linked to infantile striatonigral degeneration, a disease that results in dystonia, ataxia, spasms, and difficulty swallowing [ 256 ]. Interestingly, disease-related Nup54 mutations are clustered in the C-terminus of the protein, which interacts with Nup62 [ 256 ]. Separate work had previously identified Nup62 mutations which lead to bilateral striatal necrosis, a neurodegenerative disorder that affects the caudate nucleus and putamen of the basal ganglia [ 257 ].…”

Section: Nucleoporin Variation and Diseasementioning

confidence: 99%

“…Separate work had previously identified Nup62 mutations which lead to bilateral striatal necrosis, a neurodegenerative disorder that affects the caudate nucleus and putamen of the basal ganglia [ 257 ]. The phenotypes of patients with Nup54 and Nup62 mutations are remarkably similar [ 256 ], suggesting that proper interaction between central channel Nups is critical for neurological and motor functioning.…”

Section: Nucleoporin Variation and Diseasementioning

confidence: 99%

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Nuclear pore dysfunction and disease: a complex opportunity

Fare,

Rothstein

2024

Nucleus

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The separation of genetic material from bulk cytoplasm has enabled the evolution of increasingly complex organisms, allowing for the development of sophisticated forms of life. However, this complexity has created new categories of dysfunction, including those related to the movement of material between cellular compartments. In eukaryotic cells, nucleocytoplasmic trafficking is a fundamental biological process, and cumulative disruptions to nuclear integrity and nucleocytoplasmic transport are detrimental to cell survival. This is particularly true in post-mitotic neurons, where nuclear pore injury and errors to nucleocytoplasmic trafficking are strongly associated with neurodegenerative disease. In this review, we summarize the current understanding of nuclear pore biology in physiological and pathological contexts and discuss potential therapeutic approaches for addressing nuclear pore injury and dysfunctional nucleocytoplasmic transport.

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“…Recently, loss of NPC integrity and nucleocytoplasmic shuttling have emerged as processes that are disturbed in in several aging-related neurodegenerative diseases, including Alzheimer's disease and ALS [124]. Mutations in Nups themselves can lead to diseases, including Dystonia [125,126], and nucleocytoplasmic transport can become disturbed by mutations in aggregation-prone proteins that sequester importins, Nups, or components of the Ran gradient needed for efficient transport [122][123][124][127][128][129][130]. These findings highlight the need for protein quality control at the nuclear envelope to ensure maintenance of the NPC and its efficient transport capabilities [131].…”

Section: Npc Maintenancementioning

confidence: 99%

Coordinating nucleoporin condensation and nuclear pore complex assembly

Kuiper,

Prophet,

Schlieker

2023

FEBS Letters

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The nuclear pore complex (NPC) is among the most elaborate protein complexes in eukaryotes. While ribosomes and proteasomes are known to require dedicated assembly machinery, our understanding of NPC assembly is at a relatively early stage. Defects in NPC assembly or homeostasis are tied to movement disorders, including dystonia and amyotrophic lateral sclerosis (ALS), as well as aging, requiring a better understanding of these processes to enable therapeutic intervention. Here, we discuss recent progress in the understanding of NPC assembly and highlight how related defects in human disorders can shed light on NPC biogenesis. We propose that the condensation of phenylalanine‐glycine repeat nucleoporins needs to be carefully controlled during NPC assembly to prevent aberrant condensation, aggregation, or amyloid formation.

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Recessive NUP54 Variants Underlie Early‐Onset Dystonia with Striatal Lesions

Cited by 8 publications

References 20 publications

TorsinA is essential for the timing and localization of neuronal nuclear pore complex biogenesis

TorsinA is essential for the timing and localization of neuronal nuclear pore complex biogenesis

Nuclear pore dysfunction and disease: a complex opportunity

Coordinating nucleoporin condensation and nuclear pore complex assembly

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