Proteomics

Dataset Information

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LC-MSMS study of hiPSC-derived β-like cells in different 3D Eevironments


ABSTRACT: In this project hiPSC-derived β-like cells were studied in two different 3D enviromnets; size-adjusted cell aggregates (using Aggrewell™ plates) and inside alginate capsules. The hiPSC derived from a patient with maturity-onset diabetes of the young 1 (MODY1), which is a monogenic diabetes form, caused by a mutation in the HNF4A gene. We also generated and included a CRISPR/cas9 corrected isogenic control line. Human islets were also included as positive control. In the data analysis we compared to proteome of the cells in 3D environments compared to the frat 2D enviromnet. We found HNF4A mutation specific effects with both distinct 3D environments, where the cells are challenged differentially in term of oxygen, nutrient supply and cell-to-cell contact. We identified HNF4A mutation-specific phenotypes, including a unique proteome signature suggesting metabolic changes in the alginate bead environment, and mutation-specific cellular phenotypes and a unique proteome signature in the aggregation environment.

INSTRUMENT(S): Orbitrap Fusion

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Cell Culture, Fibroblast

DISEASE(S): Maturity-onset Diabetes Of The Young Type 1

SUBMITTER: Yngvild Bjoerlykke  

LAB HEAD: Helge Raeder

PROVIDER: PXD025054 | Pride | 2022-05-20

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
397247_a14161_YB.mzIdentML Mzid
397248_a14160_YB.mzIdentML Mzid
397249_a14159_YB.mzIdentML Mzid
397250_a14158_YB.mzIdentML Mzid
397251_a14157_YB.mzIdentML Mzid
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Publications


Studies of monogenic diabetes are particularly useful because we can gain insight into the molecular events of pancreatic β-cell failure. Maturity-onset diabetes of the young 1 (MODY1) is a form of monogenic diabetes caused by a mutation in the HNF4A gene. Human-induced pluripotent stem cells (hiPSCs) provide an excellent tool for disease modeling by subsequently directing differentiation toward desired pancreatic islet cells, but cellular phenotypes in terminally differentiated cells are notori  ...[more]

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