iPS Cell line: CRICKi012-A (iFCI017), c.G152A mutation in Exon 3 of SNCA

By Gurvir Virdi, MSc and James Evans, MSc
View Published Lab Material

Output Details

Description
Mutations or multiplications of the SNCA (Synuclein Alpha) gene cause rare autosomal dominant Parkinson’s disease (PD). The SNCA G51D missense mutation is associated with a synucleinopathy that shares PD and multiple system atrophy (MSA) characteristics. We generated induced pluripotent stem cell (iPSC) lines from two individuals with SNCA G51D missense mutations at risk of PD. Dermal fibroblasts were reprogrammed to pluripotency using a non-integrating mRNA-based protocol. The resulting human iPSCs displayed normal morphology, expressed markers associated with pluripotency, and differentiated into the three germ layers. The iPSC lines could facilitate disease-modelling and therapy development studies for synucleinopathies.
Tags
  • Human
Team
Team Wood
Program
Collaborative Research Network
Theme
PD Functional Genomics

Meet the Authors

  • Gurvir Virdi, MSc

    Key Personnel: Team Wood

    The Francis Crick Institute

  • User avatar fallback logo

    James Evans, MSc

    Key Personnel: Team Wood

    University College London

Related Research

iPS Cell line CRICKi011-A (iFCI016), c.G152A mutation in Exon 3 of SNCA

Mutations in the SNCA gene cause rare autosomal dominant Parkinson’s disease. iPSC lines were created from individuals with SNCA G51D mutations, showing potential for disease modeling and therapy development for synucleinopathies.

View Lab Material

EMD-40658

Structure of human ULK1 complex core (2:1:1 stoichiometry)

View Dataset

EMD-40735

Structure of human ULK1 complex core (2:2:2 stoichiometry) of the ATG13(450-517) mutant

View Dataset
View More Outputs