|
|||||
|
|
Mutant induced pluripotent stem cell lines recapitulate aspects of TDP-43 proteinopathies and reveal cell-specific vulnerability |
|
| Authors: | Bilican Bilada Serio Andrea Barmada Sami J Nishimura Agnes Lumi Sullivan Gareth J Carrasco Monica Phatnani Hemali P Puddifoot Clare A Story David Fletcher Judy Park In-Hyun Friedman Brad A Daley George Q Wyllie David J A Hardingham Giles E Wilmut Ian Finkbeiner Steven Maniatis Tom Shaw Christopher E Chandran Siddharthan |
| Affiliation: | Medical Research Council Centre for Regenerative Medicine, University of Edinburgh, Edinburgh EH16 4SB, United Kingdom. |
| Abstract: | Transactive response DNA-binding (TDP-43) protein is the dominant disease protein in amyotrophic lateral sclerosis (ALS) and a subgroup of frontotemporal lobar degeneration (FTLD-TDP). Identification of mutations in the gene encoding TDP-43 (TARDBP) in familial ALS confirms a mechanistic link between misaccumulation of TDP-43 and neurodegeneration and provides an opportunity to study TDP-43 proteinopathies in human neurons generated from patient fibroblasts by using induced pluripotent stem cells (iPSCs). Here, we report the generation of iPSCs that carry the TDP-43 M337V mutation and their differentiation into neurons and functional motor neurons. Mutant neurons had elevated levels of soluble and detergent-resistant TDP-43 protein, decreased survival in longitudinal studies, and increased vulnerability to antagonism of the PI3K pathway. We conclude that expression of physiological levels of TDP-43 in human neurons is sufficient to reveal a mutation-specific cell-autonomous phenotype and strongly supports this approach for the study of disease mechanisms and for drug screening. |
| Keywords: | disease modeling reprogramming motor neuron disease Lou Gehrig disease |
| 本文献已被 PubMed 等数据库收录! | |