Proteomics

Dataset Information

0

In vivo and in vitro Genome Editing to explore GNE functions


ABSTRACT: GNE myopathy is an adult onset neuromuscular disorder characterized by slowly progressive distal and proximal muscle weakness, caused by missense recessive mutations in the GNE gene. Although the encoded bifunctional enzyme is well known as the limiting factor in the biosynthesis of sialic acid, no clear mechanisms have been recognized to account for the muscle atrophic pathology, and novel functions for GNE have been hypothesized. Two major issues impair studies on this protein. First, the expression of the GNE protein is minimal in humans and mice muscles and there is no reliable antibody to follow up endogenous expression. Second, no reliable animal model is available for the disease and cellular models from GNE myopathy patients' muscle cells (expressing the mutated protein) are less informative than expected. In order to broaden our knowledge on GNE functions in muscle, we have taken advantage of the CRISPR/Cas9 method for genome editing to first, add a tag to the endogenous Gne gene in mouse, allowing the determination of the spatiotemporal expression of the protein in the organism using well established and reliable antibodies against the specific tag. In addition we have generated a Gne knock out murine muscle cell lineage to identify the events resulting from the total lack of the protein. A thorough multi-omics analysis of both systems including transcriptomics, proteomics, phosphoproteomics and ubiquitination, unraveled novel pathways for Gne, in particular its involvement in cell cycle control and in the DNA damage/repair pathway. The elucidation of fundamental mechanisms of Gne in normal muscle may contribute to the identification of the disrupted functions in GNE myopathy, thus, to the definition of novel biomarkers and possible therapeutic targets for this disease.

INSTRUMENT(S): Q Exactive HF

ORGANISM(S): Mus Musculus (mouse)

TISSUE(S): Skeletal Muscle Fiber

SUBMITTER: Tamar Ziv  

LAB HEAD: Stella Mitrani-Rosenbaum

PROVIDER: PXD033985 | Pride | 2023-03-10

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
Seq62836_HFX.raw Raw
Seq62836_kgg_HFX.raw Raw
Seq62836_prot_HFX.raw Raw
Seq62837_HFX.raw Raw
Seq62837_kgg_HFX.raw Raw
Items per page:
1 - 5 of 39
altmetric image

Publications

<i>In vivo</i> and <i>in vitro</i> genome editing to explore GNE functions.

Ilouz Nili N   Harazi Avi A   Guttman Miriam M   Daya Alon A   Ruppo Shmuel S   Yakovlev Lena L   Mitrani-Rosenbaum Stella S  

Frontiers in genome editing 20220927


GNE myopathy is an adult onset neuromuscular disorder characterized by slowly progressive distal and proximal muscle weakness, caused by missense recessive mutations in the <i>GNE</i> gene. Although the encoded bifunctional enzyme is well known as the limiting factor in the biosynthesis of sialic acid, no clear mechanisms have been recognized to account for the muscle atrophic pathology, and novel functions for GNE have been hypothesized. Two major issues impair studies on this protein. First, t  ...[more]

Similar Datasets

2022-10-26 | GSE202046 | GEO
2019-08-30 | GSE128470 | GEO
2022-04-13 | GSE200516 | GEO
2022-10-26 | GSE207593 | GEO
2022-12-21 | GSE211885 | GEO
2024-07-26 | GSE272775 | GEO
2016-04-05 | E-GEOD-71679 | biostudies-arrayexpress
2016-04-05 | GSE71679 | GEO
2010-09-21 | E-GEOD-24239 | biostudies-arrayexpress
2005-10-14 | E-GEOD-3307 | biostudies-arrayexpress