Literature DB >> 20370501

Cellular repair in the parkinsonian nonhuman primate brain.

Donald Eugene Redmond1, Stephanie Weiss, John D Elsworth, Robert H Roth, Dustin R Wakeman, Kimberly B Bjugstad, Timothy J Collier, Barbara C Blanchard, Yang D Teng, Evan Y Synder, John R Sladek.   

Abstract

Parkinson disease (PD) is a neurodegenerative disorder that provides a useful model for testing cell replacement strategies to rejuvenate the affected dopaminergic neural systems, which have been destroyed by aging and the disease. We first showed that grafts of fetal dopaminergic neurons can reverse parkinsonian motor deficits induced by the toxin, 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP), validating the feasibility of cellular repair in a primate nervous system. Subsequent clinical trials in Parkinson patients showed encouraging results, including long-term improvement of neurological signs and reduction of medications in some patients. However, many experienced little therapeutic benefit, and some recipients experienced dyskinesias, suggesting a lack of regulated control of the grafts. We have since attempted to improve cell replacements by placing grafts in their correct anatomical location in the substantia nigra and using strategies such as co-grafting fetal striatal tissue or growth factors into the physiologic striatal targets. Moreover, the use of fetal cells depends on a variable supply of donor material, making it difficult to standardize cell quality and quantity. Therefore, we have also explored possibilities of using human neural stem cells (hNSCs) to ameliorate parkinsonism in nonhuman primates with encouraging results. hNSCs implanted into the striatum showed a remarkable migratory ability and were found in the substantia nigra, where a small number appeared to differentiate into dopamine neurons. The majority became growth factor-producing glia that could provide beneficial effects on host dopamine neurons. Studies to determine the optimum stage of differentiation from embryonic stem cells and to derive useful cells from somatic cell sources are in progress.

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Year:  2010        PMID: 20370501      PMCID: PMC2946058          DOI: 10.1089/rej.2009.0960

Source DB:  PubMed          Journal:  Rejuvenation Res        ISSN: 1549-1684            Impact factor:   4.663


  50 in total

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2.  Embryonic stem cells develop into functional dopaminergic neurons after transplantation in a Parkinson rat model.

Authors:  Lars M Bjorklund; Rosario Sánchez-Pernaute; Sangmi Chung; Therese Andersson; Iris Yin Ching Chen; Kevin St P McNaught; Anna-Liisa Brownell; Bruce G Jenkins; Claes Wahlestedt; Kwang-Soo Kim; Ole Isacson
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6.  mtDNA deletions associated with ageing and PD.

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7.  Simultaneous intrastriatal and intranigral fetal dopaminergic grafts in patients with Parkinson disease: a pilot study. Report of three cases.

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8.  Influence of age and time interval between death and autopsy on dopamine and 3-methoxytyramine levels in human basal ganglia.

Authors:  A Carlsson; B Winblad
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9.  Brain grafts reduce motor abnormalities produced by destruction of nigrostriatal dopamine system.

Authors:  M J Perlow; W J Freed; B J Hoffer; A Seiger; L Olson; R J Wyatt
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10.  Age-related decreases in Nurr1 immunoreactivity in the human substantia nigra.

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Review 2.  Defining and designing polymers and hydrogels for neural tissue engineering.

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5.  Adult human olfactory epithelial-derived progenitors: a potential autologous source for cell-based treatment for Parkinson's disease.

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Review 7.  Large animal models for stem cell therapy.

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  7 in total

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