4.8 Article

Direct conversion of human fibroblasts to dopaminergic neurons

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1105135108

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Funding

  1. European Community [22943]
  2. Swedish Research Council [K2007-62X-20391-01-4, K2007-62P-20390-01-4, K2010-80P-21583-01-4]
  3. Bagadilico Grant [349-2007-8626]
  4. Stem-Therapy
  5. Crafoord Foundation
  6. Swedish Parkinson Foundation
  7. Jeansson Foundation
  8. Lundbeck Foundation [R44-A3856]
  9. M. Lundqvist Foundation
  10. Knut and Alice Wallenberg Foundation
  11. Human Frontiers Science Program
  12. Lundbeck Foundation [R44-2009-3856] Funding Source: researchfish

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Recent reports demonstrate that somatic mouse cells can be directly converted to other mature cell types by using combined expression of defined factors. Here we show that the same strategy can be applied to human embryonic and postnatal fibroblasts. By overexpression of the transcription factors Ascl1, Brn2, and Myt1l, human fibroblasts were efficiently converted to functional neurons. We also demonstrate that the converted neurons can be directed toward distinct functional neurotransmitter phenotypes when the appropriate transcriptional cues are provided together with the three conversion factors. By combining expression of the three conversion factors with expression of two genes involved in dopamine neuron generation, Lmx1a and FoxA2, we could direct the phenotype of the converted cells toward dopaminergic neurons. Such subtype-specific induced neurons derived from human somatic cells could be valuable for disease modeling and cell replacement therapy.

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