ASAP announces new teams joining the Collaborative Research Network! Learn More
Aligning Science Across Parkinson's Logo Text

Chromatin accessibility profiling (ATAC-seq) of human iPSC-derived midbrain astrocytes in ATP13A2 c.1306 deficiency models

By Elena Coccia
View Published Dataset

Output Details

Description
This dataset contains bulk Assay for Transposase-Accessible Chromatin using sequencing (ATAC-seq) data from human iPSC-derived midbrain astrocytes. The study compares Wild Type (WT) astrocytes and ATP13A2 c.1306 loss-of-function mutants. The objective was to characterize the epigenomic landscape and changes in genome-wide accessibility driven by the genotype.
Identifier (DOI)
10.5281/zenodo.19226012
Tags
  • iPSC
Discovery Team
Team Vangheluwe
Program
Collaborative Research Network
Theme
PD Functional Genomics

Meet the Authors

  • User avatar fallback logo

    Elena Coccia

    External Collaborator

Related Research

Transcriptomic profiling of human iPSC-derived midbrain astrocytes in ATP13A2 deficiency (c.1306) models

Dataset compares gene expression in WT and ATP13A2 c.1306 mutants in midbrain astrocytes to understand transcriptional effects on neuroinflammation and lysosome dysfunction linked to early-onset Parkinson's Disease.

View Dataset

DNA methylome profiling (Bisulfite Sequencing) of human iPSC-derived midbrain astrocytes in ATP13A2 c.1306deficiency models

Dataset offers DNA methylation profiles of human midbrain astrocytes comparing ATP13A2 c.1306 mutants with Wild Type controls using WGBS.

View Dataset

Sample preparation for aCGH karyotyping

This protocol describes the standard procedure preparing cell pellets from human pluripotent stem cells (hPSCs) cultured on MEFs for outsourced aCGH karyotyping.

View Protocol
View More Outputs
Aligning Science Across Parkinson's
Powered by  GDPR Cookie Compliance
Privacy Overview

This website uses cookies so that we can provide you with the best user experience possible. Cookie information is stored in your browser and performs functions such as recognising you when you return to our website and helping our team to understand which sections of the website you find most interesting and useful.