Motor Unit Integrity in Pathophysiological States and the Assessment of Potential Neuroprotective Therapeutics

Wier, Christopher G.

January 2018

No description available.

Neurosciences

Motor Unit

Connectivity

Contractility

ALS

SOD1G93A

PNI

Gene Therapy

AAV9

HSPB1

SMN

Elucidating the Mechanism of Disease Pathogenesis in SMA by Studying SMN Missense Mutant Function

Blatnik, Anton J., III

January 2020

No description available.

Biochemistry

Genetics

Molecular Biology

SMN promotes mitochondrial metabolic maturation during myogenesis by regulating the MYOD-miRNA axis / SMNは、骨格筋分化においてMYOD-miRNA 経路を制御することにより、ミトコンドリアの機能的成熟を促進する

Uehara(Ikenaka), Akihiro

24 July 2023

京都大学 / 新制・論文博士 / 博士(医学) / 乙第13564号 / 論医博第2291号 / 新制||医||1068(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 齊藤, 博英, 教授 滝田, 順子, 教授 萩原, 正敏 / 学位規則第4条第2項該当 / Doctor of Medical Science / Kyoto University / DFAM

脊髄性筋萎縮症

骨格筋

SMN

MYOD1

miRNA

490

Characterization of Mutant SMN and Development of Mutant SMN Transgenic Mice

Workman, Eileen

26 June 2009

No description available.

Biochemistry

Biomedical Research

Cellular Biology

Molecular Biology

Neurology

SMN

Survival Motor Neuron

SMA

Spinal Muscular Atrophy

Generation and Analysis of Motor Neuron Disease Models in Zebrafish

Lyon, Alison Nicole

22 June 2012

No description available.

Biomedical Research

Molecular Biology

Neurosciences

motor neuron

zebrafish

ALS

SOD1

SMA

SMN

plastin 3

Characterization of three SMN missense mutations using mouse models of Spinal Muscular Atrophy

Madabusi, Narasimhan Kandaye

18 July 2012

No description available.

Biochemistry

Genetics

Molecular Biology

Spinal Muscular Atrophy

SMN

missense mutations

mouse models

Étude des interactions protéine-protéine entre le complexe de Survie des MotoNeurones (SMN) et les facteurs d'assemblage des RNP à boîtes C/D et H/ACA / Study of the protein-protein interactions between the SMN complex and the factors required for box C/D and H/ACA RNP assembly

Huttin, Alexandra

11 December 2012

Les particules ribonucléoprotéiques (RNP) à boîtes C/D et H/ACA sont impliquées dans la maturation des UsnRNA et des précurseurs des ARNr. L'assemblage de ces RNP dans les cellules est un processus complexe faisant intervenir de nombreux facteurs cellulaires dont NUFIP, commun aux deux RNP, et NAF1, spécifique aux RNP à boîtes H/ACA. Le complexe de Survie des Motoneurones (SMN) est essentiel à la survie cellulaire et est nécessaire à l'assemblage d'une autre RNP, les UsnRNP, composants des spliceosomes. Un déficit en protéine SMN conduit à une pathologie grave, l'amyotrophie spinale. Plusieurs études suggèrent que le complexe SMN puisse également jouer un rôle dans l'assemblage des RNP à boîtes C/D et H/ACA. Dans le but d'obtenir de plus amples informations, nous avons testé si des interactions existent entre les constituants du complexe SMN et i) les protéines associées aux RNP matures, ainsi que ii) les autres facteurs d'assemblage déjà connus. Ainsi, par une approche de double hybride chez la levure, nous avons observé des interactions fortes entre NAF1 et les protéines Gemin3 et Gemin8 du complexe SMN. Comme la protéine coeur GAR1 des RNP à boîte H/ACA interagit avec la protéine SMN, ces données suggèrent que le complexe SMN participe à l'échange de NAF1 par GAR1, qui est une étape clé de la biogenèse des RNP à boîtes H/ACA. De plus, nous avons mis en évidence des interactions entre Gemin3/NUFIP, Gemin4/NUFIP et Gemin6/NUFIP. L'étude de cette dernière interaction a été approfondie. Nous avons montré que l'interaction est directe, qu'elle existe dans les cellules de mammifères à la fois dans le cytoplasme et le noyau, et nous avons défini les domaines de chaque protéine nécessaires à l'interaction, en collaboration avec l'équipe d'E. Bertrand (IGM Montpellier). Ces résultats ouvrent de larges perspectives quant à un lien fonctionnel entre le complexe SMN et NUFIP dans l'assemblage des RNP à boîtes C/D et H/ACA, mais aussi dans l'assemblage de la snRNP U4 et dans le mécanisme de traduction localisée dans les cellules / Box C/D and H/ACA ribonucleoparticles (RNPs) are required for UsnRNA and ribosomal RNA maturation. Their assembly in cells is a complex process, which implicates numerous cellular factors, such as NUFIP, a common assembly factor, and NAF1, which is a specific factor for H/ACA box RNP assembly. The Survival of Motoneurons (SMN) complex is essential for cell survival and is required for the assembly of another class of RNPs, the UsnRNPs, which are essential components of the splicing machinery. Decreased levels of the SMN protein lead to a severe disease, the spinal muscular atrophy. Several studies led to the proposal that the SMN complex also plays a role in the assembly of box C/D and H/ACA RNPs. In order to obtain more information, we analyzed whether some interactions may exist between components of the SMN complex and i) core proteins of mature RNPs, or ii) factors already known to be involved in the assembly. Using a yeast two-hybrid approach, we observed strong interactions between NAF1 and the SMN complex components, Gemin3 and Gemin8. Since the core H/ACA protein GAR1 interacts with the SMN protein, our data suggest that the SMN complex participates to the exchange of NAF1 by GAR1, which is a crucial step of H/ACA box RNP biogenesis. Furthermore, we discovered strong interactions between Gemin3/NUFIP, Gemin4/NUFIP and Gemin6/NUFIP. Concerning the Gemin6/NUFIP interaction, we showed that is direct, that it exists in both compartments in mammalian cells and we defined domains of both proteins necessary for the interaction in collaboration with the E. Bertrand team (IGM Montpellier). These results open new perspectives concerning functional links between the SMN complex and NUFIP in box H/ACA and C/D RNP assembly, but also in U4 snRNP assembly and in the mechanism of localized translation

Complexe SMN

RNP à boîtes C/D et H/ACA

NUFIP

NAF1

Assemblage de RNP

Double hybride

Interactions protéine-protéine

SMN complex

Box C/D and H/ACA RNPs

NUFIP

NAF1

RNP biogenesis

Yeast two-hybrid

Protein-protein interactions

572.6

Identification and Characterization of an Arginine-methylated Survival of Motor Neuron (SMN) Interactor in Spinal Muscular Atrophy (SMA)

Tadesse, Helina

19 December 2012

Spinal Muscular Atrophy (SMA) is a neuronal degenerative disease caused by the mutation or loss of the Survival Motor Neuron (SMN) gene. The cause for the specific motor neuron susceptibility in SMA has not been identified. The high axonal transport/localization demand on motor neurons may be one potentially disrupted function, more specific to these cells. We therefore used a large-scale immunoprecipitation (IP) experiment, to identify potential interactors of SMN involved in neuronal transport and localization of mRNA targets. We identified KH-type splicing regulatory protein (KSRP), a multifunctional RNA-binding protein that has been implicated in transcriptional regulation, neuro-specific alternative splicing, and mRNA decay. KSRP is closely related to chick zipcode-binding protein 2 and rat MARTA1, proteins involved in neuronal transport/localization of beta-actin and microtubule-associated protein 2 mRNAs, respectively. We demonstrated that KSRP is arginine methylated, a novel SMN interactor (specifically with the SMN Tudor domain; and not with SMA causing mutants). We also found this protein to be misregulated in the absence of SMN, resulting in increased mRNA stability of KSRP mRNA target, p21cip/waf1. A role for SMN as an axonal chaperone of methylated RBPs could thus be key in SMA pathophysiology.

Spinal Muscular Atrophy (SMA)

Survival Motor Neuron (SMN)

Neurodegenerative Disease

Arginine Methylation

Identification and Characterization of an Arginine-methylated Survival of Motor Neuron (SMN) Interactor in Spinal Muscular Atrophy (SMA)

Tadesse, Helina

19 December 2012

Spinal Muscular Atrophy (SMA) is a neuronal degenerative disease caused by the mutation or loss of the Survival Motor Neuron (SMN) gene. The cause for the specific motor neuron susceptibility in SMA has not been identified. The high axonal transport/localization demand on motor neurons may be one potentially disrupted function, more specific to these cells. We therefore used a large-scale immunoprecipitation (IP) experiment, to identify potential interactors of SMN involved in neuronal transport and localization of mRNA targets. We identified KH-type splicing regulatory protein (KSRP), a multifunctional RNA-binding protein that has been implicated in transcriptional regulation, neuro-specific alternative splicing, and mRNA decay. KSRP is closely related to chick zipcode-binding protein 2 and rat MARTA1, proteins involved in neuronal transport/localization of beta-actin and microtubule-associated protein 2 mRNAs, respectively. We demonstrated that KSRP is arginine methylated, a novel SMN interactor (specifically with the SMN Tudor domain; and not with SMA causing mutants). We also found this protein to be misregulated in the absence of SMN, resulting in increased mRNA stability of KSRP mRNA target, p21cip/waf1. A role for SMN as an axonal chaperone of methylated RBPs could thus be key in SMA pathophysiology.

Spinal Muscular Atrophy (SMA)

Survival Motor Neuron (SMN)

Neurodegenerative Disease

Arginine Methylation

Identification and Characterization of an Arginine-methylated Survival of Motor Neuron (SMN) Interactor in Spinal Muscular Atrophy (SMA)

Tadesse, Helina

January 2012

Spinal Muscular Atrophy (SMA) is a neuronal degenerative disease caused by the mutation or loss of the Survival Motor Neuron (SMN) gene. The cause for the specific motor neuron susceptibility in SMA has not been identified. The high axonal transport/localization demand on motor neurons may be one potentially disrupted function, more specific to these cells. We therefore used a large-scale immunoprecipitation (IP) experiment, to identify potential interactors of SMN involved in neuronal transport and localization of mRNA targets. We identified KH-type splicing regulatory protein (KSRP), a multifunctional RNA-binding protein that has been implicated in transcriptional regulation, neuro-specific alternative splicing, and mRNA decay. KSRP is closely related to chick zipcode-binding protein 2 and rat MARTA1, proteins involved in neuronal transport/localization of beta-actin and microtubule-associated protein 2 mRNAs, respectively. We demonstrated that KSRP is arginine methylated, a novel SMN interactor (specifically with the SMN Tudor domain; and not with SMA causing mutants). We also found this protein to be misregulated in the absence of SMN, resulting in increased mRNA stability of KSRP mRNA target, p21cip/waf1. A role for SMN as an axonal chaperone of methylated RBPs could thus be key in SMA pathophysiology.

Spinal Muscular Atrophy (SMA)

Survival Motor Neuron (SMN)

Neurodegenerative Disease

Arginine Methylation