An integrated multi-omic analysis of iPSC-derived motor neurons from C9ORF72 ALS patients
- Li, J.
- Lim, R.G.
- Kaye, J.A.
- Dardov, V.
- Coyne, A.N.
- Wu, J.
- Milani, P.
- Cheng, A.
- Thompson, T.G.
- Ornelas, L.
- Frank, A.
- Adam, M.
- Banuelos, M.G.
- Casale, M.
- Cox, V.
- Escalante-Chong, R.
- Daigle, J.G.
- Gomez, E.
- Hayes, L.
- Holewenski, R.
- Lei, S.S.
- Lenail, A.
- Lima, L.
- Mandefro, B.
- Matlock, A.
- Panther, L.
- Patel-Murray, N.L.
- Pham, J.
- Ramamoorthy, D.
- Sachs, K.
- Shelley, B.
- Stocksdale, J.
- Trost, H.
- Wilhelm, M.
- Venkatraman, V.
- Wassie, B.T.
- Wyman, S.
- Yang, S.
- Eyk, J.E. van
- Lloyd, T.E.
- Finkbeiner, S.
- Fraenkel, E.
- Rothstein, J.D.
- Sareen, D.
- Svendsen, C.N.
- Thompson, L.M.
- NeuroLINCS Consortium
- NYGC ALS Consortium
DOIAbstract
Neurodegenerative diseases are challenging for systems biology because of the lack of reliable animal models or patient samples at early disease stages. Induced pluripotent stem cells (iPSCs) could address these challenges. We investigated DNA, RNA, epigenetics, and proteins in iPSC-derived motor neurons from patients with ALS carrying hexanucleotide expansions in C9ORF72. Using integrative computational methods combining all omics datasets, we identified novel and known dysregulated pathways. We used a C9ORF72 Drosophila model to distinguish pathways contributing to disease phenotypes from compensatory ones and confirmed alterations in some pathways in postmortem spinal cord tissue of patients with ALS. A different differentiation protocol...
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