The DaNeX Study of Embryonic Mesencephalic, Dopaminergic Tissue Grafted to a Minipig Model of Parkinson's Disease: Preliminary Findings of Effect of MPTP Poisoning on Striatal Dopaminergic Markers

Author:

Danielsen Erik Hvid1,Dimming P.1,Andersen F.1,Bender D.1,Brevig T.2,Falborg L.1,Gee A.1,Gillings N. M.1,Hansen S. B.1,Hermansen F.1,Johansen J.3,Johansen T. E.3,Dahl-Jørgensen A.2,Jørgensen H. A.4,Meyer M.2,Munk O.1,Pedersen E. B.2,Poulsen P. H.15,Rodell A. B.1,Sakoh M.1,Simonsen C. Z.6,Smith D. F.7,Sørensen J. C.52,Østergård L.6,Zimmer J.2,Gjedde A.1,Møller A.3

Affiliation:

1. PET-Center, University Hospital, Denmark

2. Department Anatomy and Neurobiology, University of Southern Denmark-University of Odense, Denmark

3. Neuro Search, Glostrup, Denmark

4. Department of Neuroanaesthesia at Aarhus University Hospital, Denmark

5. Department of Neurosurgery, University Hospital, Denmark

6. Department of Neuroradiology, University Hospital, Denmark

7. Department of Biological Psychiatry, Aarhus University Psychiatric Hospital, Denmark

Abstract

A multicenter study is under way to investigate the efficacy of allografting of embryonic mesencephalic neurons in a pig model of Parkinson's disease. We have first established that a stable parkinsonian syndrome can be established by 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) intoxication of adult male Göttingen minipigs. We are now using positron emission tomography (PET) methods for testing the physiological responses to MPTP intoxication and the time course of the response to several treatment strategies. We now report preliminary results obtained in 11 pigs employed in the initial phase of the study; the completed study shall ultimately include 30 pigs. Animals were randomly assigned to one of five groups: 1) Control, 2) MPTP intoxication, 3) MPTP intoxication followed by allograft, 4) MPTP intoxication followed by allograft with immunosuppression, and 5) MPTP intoxication followed by allograft with immunosuppression and co-grafting of immortalized HiB5 cells, which had been manipulated to secrete glia cell line-derived neurotrophic factor (GDNF) (≈2 ng GDNF/h/105 cells). MPTP was administered (1 mg/kg/day, SC) for 7–10 days until the pigs had developed mild parkinsonian symptoms of muscle rigidity, hypokinesia, and impaired coordination, especially of the hind limbs. Approximately 2 weeks after the last MPTP dose, animals received a T1-weighted magnetic resonance imaging (MRI) scan, and a series of dynamic PET recordings. After the first series of PET scans, four grafts of porcine embryonic mesencephalic tissue (E28 days) were placed in each striatum of some MPTP-intoxicated pigs, using MRI-based stereotactic techniques. Immunosuppression of some animals with cyclosporin and prednisolone began just prior to surgery. Two more series of PET scans were performed at 4-month intervals after surgery. After the last scans, pigs were killed and the brains were perfused for unbiased stereological examination of cytological and histochemical markers in striatum and substantial nigra. The behavioral impairment of the animals (the “Parkinson's score”) had been evaluated throughout the 8-month period. Kinetic analysis of the first set of PET scans has indicated that the rate constant for the decarboxylation of FDOPA in catecholamine fibers was reduced by 33% in striatum of the mildly parkinsonian pigs. The rate of association of [11C]NS-2214 to catecholamine uptake sites was reduced by 62% in the same groups of pigs. No significant difference was found in the binding potential of [11C]raclopride to the dopamine D2-like receptors in striatum of the MPTP-intoxicated versus control pigs. These preliminary results are suggestive that the activity of DOPA decarboxylase may be upregulated in the partially denervated pig striatum.

Publisher

SAGE Publications

Subject

Transplantation,Cell Biology,Biomedical Engineering

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