A double‐blind controlled trial of bilateral fetal nigral transplantation in Parkinson's disease

Olanow, C. Warren; Goetz, Christopher G.; Kordower, Jeffrey H.; Stoessl, A. Jon; Sossi, Vesna; Brin, Mitchell F.; Shannon, Kathleen M.; Nauert, G. Michael; Perl, Daniel P.; Godbold, James; Freeman, Thomas B.

doi:10.1002/ana.10720

Cited by 1,410 publications

(1,202 citation statements)

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“…Thus, these data suggest that supplementing intrastriatal fetal VM grafts with in vivo injections of viral vector delivering the GDNF gene may decrease the number of VM grafts necessary to re-supply the host striatum with adequate levels of DA. This would be a significant achievement, as the use of eight donors for one human host (Hauser et al, 1999;Olanow et al, 2003) is an obstacle to neural grafting as a treatment option for Parkinson's disease.…”

Section: Discussionmentioning

confidence: 99%

“…Some parkinsonian patients that received fetal VM grafts in recent clinical trials developed off-medication dyskinesias or graft-induced dyskinesias (GID) (Freed et al, 2001;Hagell et al, 2002;Olanow et al, 2003). The proportion of patients in these 3 studies with GID severe enough to constitute clinical therapeutic problems has been estimated to be between 7 and 15% (Hagell and Cenci, 2005).…”

Section: Discussionmentioning

confidence: 99%

“…Animal studies in the rodent (reviewed by Brundin et al, 1994), and in the primate (Annett, 1994;Bankiewicz et al, 1993;Elsworth et al, 1996;Fine et al, 1988;Taylor et al, 1991) have shown that grafts of fetal DA neurons can lead to reversals in biochemical and behavioral indices of DA deficiency. However, in clinical studies the improvements in Parkinsonism have been variable, and generally rather modest (Freed et al, 1992;Freed et al, 2001;Lindvall and Hagell, 2001;Olanow et al, 2003;Redmond, 2002;Spencer et al, 1992;Widner et al, 1992).…”

Section: Introductionmentioning

confidence: 99%

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AAV2-mediated gene transfer of GDNF to the striatum of MPTP monkeys enhances the survival and outgrowth of co-implanted fetal dopamine neurons

Elsworth

Redmond

Léránth

et al. 2008

Experimental Neurology

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Neural transplantation offers the potential of treating Parkinson's disease by grafting fetal dopamine neurons to depleted regions of the brain. However, clinical studies of neural grafting in Parkinson's disease have produced only modest improvements. One of the main reasons for this is the low survival rate of transplanted neurons. The inadequate supply of critical neurotrophic factors in the adult brain is likely to be a major cause of early cell death and restricted outgrowth of fetal grafts placed into the mature striatum. Glial derived neurotrophic factor (GDNF) is a potent neurotrophic factor that is crucial to the survival, outgrowth and maintenance of dopamine neurons, and so is a candidate for protecting grafted fetal dopamine neurons in the adult brain. We found that implantation of adenoassociated virus type 2 encoding GDNF (AAV2-GDNF) in the normal monkey caudate nucleus induced over-expression of GDNF that persisted for at least 6 months after injection. In a 6-month within-animal controlled study, AAV2-GDNF enhanced the survival of fetal dopamine neurons by 4-fold, and increased the outgrowth of grafted fetal dopamine neurons by almost 3-fold in the caudate nucleus of MPTP-treated monkeys, compared with control grafts in the other caudate nucleus. Thus, the addition of GDNF gene therapy to neural transplantation may be a useful strategy to improve treatment for Parkinson's disease.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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AAV2-mediated gene transfer of GDNF to the striatum of MPTP monkeys enhances the survival and outgrowth of co-implanted fetal dopamine neurons

Elsworth

Redmond

Léránth

et al. 2008

Experimental Neurology

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“…Dopaminergic Grafts Can Survive and Become Morphologically Integrated in the PD Patient's Brain Following implantation of postmitotic DA neuroblasts from the ventral mesencephalon of 6-to 9-weekold human fetuses, positron emission tomography (PET) detected increases in 6-L-[ 18 F]-fluorodopa ( 18 F-dopa) uptake ( Fig. 1) [4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19], and histopathological studies have shown long-term, extensive synaptic reinnervation in the striatum [13,[20][21][22][23][24][25][26][27].…”

Section: Can Da Neurons Be Replaced and Neural Grafts Have Functionalmentioning

confidence: 99%

Cell Therapeutics in Parkinson's Disease

Lindvall

Björklund

2011

Neurotherapeutics

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The main pathology underlying motor symptoms in Parkinson's disease (PD) is a rather selective degeneration of nigrostriatal dopamine (DA) neurons. Intrastriatal transplantation of immature DA neurons, which replace those neurons that have died, leads to functional restoration in animal models of PD. Here we describe how far the clinical translation of the DA neuron replacement strategy has advanced. We briefly summarize the lessons learned from the early clinical trials with grafts of human fetal mesencephalic tissue, and discuss recent findings suggesting susceptibility of these grafts to the disease process longterm after implantation. Mechanisms underlying graftinduced dyskinesias, which constitute the only significant adverse event observed after neural transplantation, and how they should be prevented and treated are described. We summarize the attempts to generate DA neurons from stem cells of various sources and patient-specific DA neurons from fully differentiated somatic cells, with particular emphasis on the requirements of these cells to be useful in the clinical setting. The rationale for the new clinical trial with transplantation of fetal mesencephalic tissue is described. Finally, we discuss the scientific and clinical advancements that will be necessary to develop a competitive cell therapy for PD patients.

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“…No hay que olvidar que esta situación se aplica a enfermedades muy prevalentes y con gran impacto social, como el accidente cerebrovascular, la lesión cerebral y medular postraumática, o las enfermedades neurodegenerativas, para las que no existe actualmente alternativa de tratamiento curativo. El aparente fracaso del uso de injertos de células diferenciadas con capacidad de liberar neurotransmisores, fundamentalmente de mesencéfalo fetal en la enfermedad de Parkinson (EP) 45 , ha renovado el interés de la investigación con células troncales neurales (CTN). Aunque no existe evidencia para asegurar que la terapia celular con CTN es superior al uso de neuronas primarias en injertos fetales, su uso puede permitir la disponibilidad de un número elevado de células en distintos grados de diferenciación, y su manipulación in vitro, ambiental o genética, para mejorar su supervivencia, diferenciación, migración e integración 46 .…”

Section: Regeneración Neurológicaunclassified

Medicina regenerativa con células madre adultas

Chávarri

Pascual-Figal

Cardoso

et al. 2005

Revista Clínica Española

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En este trabajo se revisa el estado actual de la medicina regenerativa clínica con células madre de adulto en los campos cardiológico, digestivo, corneal y neurológico. Desde el punto de vista cardiológico existe experiencia clínica con progenitores de médula ósea y células de sangre periférica, así como con mioblastos esqueléticos. En el momento actual las células madre del adulto (hematopoyéticas o mesenquimales de médula ósea) constituyen la mejor opción para la regeneración del tejido cardíaco, mostrando los estudios clínicos resultados favorables, sin problemas éticos ni de seguridad. La mayoría de los estudios con mioblastos esqueléticos también han demostrado que contribuyen significativamente a mejorar la función cardíaca, sobre todo la sistólica, aunque tienen el inconveniente no aclarado totalmente, de inducir arritmias ventriculares malignas. Tanto en uno como en otro caso los estudios clínicos están en la fase inicial y se hace necesario nuevos estudios sobre todo randomizados. En el campo digestivo se presenta la experiencia pionera del Hospital La Paz del uso de células madre procedentes de la grasa abdominal en el tratamiento de la patología fistulosa de pacientes con enfermedad de Crohn. En Oftalmología el trasplante de limbo corneal es una práctica reconocida, usándose células del ojo contralateral cuando el daño es en un solo ojo y células de un donante cuando el daño es bilateral. Por último, en el campo neurológico se han identificado diversas zonas del cerebro de mamíferos adultos donde existen células troncales: el hipocampo, la zona subventricular, el bulbo olfatorio y la zona periependimaria de la médula espinal. Por otra parte, es posible obtener neuronas a partir de células troncales adultas procedentes de otros tejidos, como la médula ósea o el tejido adiposo, lo que supondría una fuente prácticamente inagotable de precursores neurales, bien mediante implante directo tras su selección o bien tras su cultivo in vitro. Aunque hasta la fecha la mayor parte de la experimentación es animal, se están poniendo ya en marcha ensayos clínicos de seguridad en esclerosis lateral amiotrófica.

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A double‐blind controlled trial of bilateral fetal nigral transplantation in Parkinson's disease

Cited by 1,410 publications

References 38 publications

AAV2-mediated gene transfer of GDNF to the striatum of MPTP monkeys enhances the survival and outgrowth of co-implanted fetal dopamine neurons

AAV2-mediated gene transfer of GDNF to the striatum of MPTP monkeys enhances the survival and outgrowth of co-implanted fetal dopamine neurons

Cell Therapeutics in Parkinson's Disease

Medicina regenerativa con células madre adultas

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