[51] When multiple human iPSC lines derived by virus- and protein

[51] When multiple human iPSC lines derived by virus- and protein-based reprogramming were compared, DA neurons derived from protein-based iPSCs were best suited for transplantation since they exhibited gene expression, physiological and electrophysiological properties similar to those of human midbrain DA neurons.[52] DA neurons were also generated from

iPS cells from PD patients and these DA neurons can be transplanted without signs of neurodegeneration into the PD animal model. The PDiPS cell-derived DA neurons survived at high numbers, and mediated functional effects in PD animals.[53] These PDiPS cell-derived DA neurons could be used for screening new drug development in PD. More recently human fibroblasts were directly converted into DA neuron-like cells by the Selleckchem PD-1/PD-L1 inhibitor use of combination of five transcriptional factors Mash1, Ngn2, Sox2, Nurr1 and Pitx3, and the reprogrammed cells

stained positive for various markers for DA neurons.[6] Although further research is still required, cell therapy based on DA neurons derived from iPS cells[54] or DA neurons directly converted from fibroblasts may become a promising treatement for PD patients in the coming years. A summary of preclinical studies of stem cell transplantation in PD animal models in rat and monkey is shown in Table 1. TH/GTPCH1 Gene transfer TH/GTPCH1 Gene transfer Monkey MPTP Rotation Beam walking Wnt signal Shh Huntington’s disease is an autosomal dominant neurodegenerative disorder characterized by involuntary Sunitinib supplier choreic movements, cognitive impairment and emotional disturbances.[55, 56] Niclosamide Despite identification of the HD gene and associated protein, the mechanisms involved in the pathogenesis of HD remain largely unknown and this hampers effective therapeutic interventions. Transplantation of fetal human brain tissue may serve as a useful strategy in reducing neuronal damage in the HD brain and a recent study has documented improvements in motor and cognition performance in HD patients following fetal cell transplantation.[57] This trial follows previous reports in HD experimental

animals that positive effects of fetal striatal cell transplantation to ameliorate neuronal dysfunction[58] and that striatal graft tissue could integrate and survive within the progressively degenerated striatum in a transgenic HD mouse model.[59] The latter study is consistent with results obtained from HD patients indicating survival and differentiation of implanted human fetal tissue in the affected regions.[60] Cell replacement therapy using human fetal striatal grafts has shown clinical success in HD patients. However, a recent study has reported neural overgrowth of grafted tissue in an HD patient who survived 5 years post-transplantaion.[61] Overgrown grafts were composed of neurons and glia embedded in disorganized neurpil.

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