Autologous transplants of Adipose-Derived Adult Stromal (ADAS) cells afford dopaminergic neuroprotection in a model of Parkinson's disease

Melissa K. McCoy; Terina N. Martinez; Kelly A. Ruhn; Philip C. Wrage; Edward W. Keefer; Barry R. Botterman; Keith E. Tansey; Malú G. Tansey

doi:10.1016/j.expneurol.2007.10.011

Autologous transplants of Adipose-Derived Adult Stromal (ADAS) cells afford dopaminergic neuroprotection in a model of Parkinson's disease

Melissa K. McCoy, Terina N. Martinez, Kelly A. Ruhn, Philip C. Wrage, Edward W. Keefer, Barry R. Botterman, Keith E. Tansey, Malú G. Tansey

Research output: Contribution to journal › Article › peer-review

91 Scopus citations

Abstract

Adult adipose contains stromal progenitor cells with neurogenic potential. However, the stability of neuronal phenotypes adopted by Adipose-Derived Adult Stromal (ADAS) cells and whether terminal neuronal differentiation is required for their consideration as alternatives in cell replacement strategies to treat neurological disorders is largely unknown. We investigated whether in vitro neural induction of ADAS cells determined their ability to neuroprotect or restore function in a lesioned dopaminergic pathway. In vitro-expanded naïve or differentiated ADAS cells were autologously transplanted into substantia nigra 1 week after an intrastriatal 6-hydroxydopamine injection. Neurochemical and behavioral measures demonstrated neuroprotective effects of both ADAS grafts against 6-hydroxydopamine-induced dopaminergic neuron death, suggesting that pre-transplantation differentiation of the cells does not determine their ability to survive or neuroprotect in vivo. Therefore, we investigated whether equivalent protection by naïve and neurally-induced ADAS grafts resulted from robust in situ differentiation of both graft types into dopaminergic fates. Immunohistological analyses revealed that ADAS cells did not adopt dopaminergic cell fates in situ, consistent with the limited ability of these cells to undergo terminal differentiation into electrically active neurons in vitro. Moreover, re-exposure of neurally-differentiated ADAS cells to serum-containing medium in vitro confirmed ADAS cell phenotypic instability (plasticity). Lastly, given that gene expression analyses of in vitro-expanded ADAS cells revealed that both naïve and differentiated ADAS cells express potent dopaminergic survival factors, ADAS transplants may have exerted neuroprotective effects by production of trophic factors at the lesion site. ADAS cells may be ideal for ex vivo gene transfer therapies in Parkinson's disease treatment.

Original language	English (US)
Pages (from-to)	14-29
Number of pages	16
Journal	Experimental Neurology
Volume	210
Issue number	1
DOIs	https://doi.org/10.1016/j.expneurol.2007.10.011
State	Published - Mar 2008

Keywords

6-Hydroxydopamine
Autologous transplantation
Dopaminergic
Neural differentiation
Neuroprotection
Parkinson's disease
Stromal adipose
Tyrosine hydroxylase

ASJC Scopus subject areas

Neurology
Developmental Neuroscience

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10.1016/j.expneurol.2007.10.011

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@article{c9252bda53e3457ba48549ef09b73f6e,

title = "Autologous transplants of Adipose-Derived Adult Stromal (ADAS) cells afford dopaminergic neuroprotection in a model of Parkinson's disease",

abstract = "Adult adipose contains stromal progenitor cells with neurogenic potential. However, the stability of neuronal phenotypes adopted by Adipose-Derived Adult Stromal (ADAS) cells and whether terminal neuronal differentiation is required for their consideration as alternatives in cell replacement strategies to treat neurological disorders is largely unknown. We investigated whether in vitro neural induction of ADAS cells determined their ability to neuroprotect or restore function in a lesioned dopaminergic pathway. In vitro-expanded na{\"i}ve or differentiated ADAS cells were autologously transplanted into substantia nigra 1 week after an intrastriatal 6-hydroxydopamine injection. Neurochemical and behavioral measures demonstrated neuroprotective effects of both ADAS grafts against 6-hydroxydopamine-induced dopaminergic neuron death, suggesting that pre-transplantation differentiation of the cells does not determine their ability to survive or neuroprotect in vivo. Therefore, we investigated whether equivalent protection by na{\"i}ve and neurally-induced ADAS grafts resulted from robust in situ differentiation of both graft types into dopaminergic fates. Immunohistological analyses revealed that ADAS cells did not adopt dopaminergic cell fates in situ, consistent with the limited ability of these cells to undergo terminal differentiation into electrically active neurons in vitro. Moreover, re-exposure of neurally-differentiated ADAS cells to serum-containing medium in vitro confirmed ADAS cell phenotypic instability (plasticity). Lastly, given that gene expression analyses of in vitro-expanded ADAS cells revealed that both na{\"i}ve and differentiated ADAS cells express potent dopaminergic survival factors, ADAS transplants may have exerted neuroprotective effects by production of trophic factors at the lesion site. ADAS cells may be ideal for ex vivo gene transfer therapies in Parkinson's disease treatment.",

keywords = "6-Hydroxydopamine, Autologous transplantation, Dopaminergic, Neural differentiation, Neuroprotection, Parkinson's disease, Stromal adipose, Tyrosine hydroxylase",

author = "McCoy, {Melissa K.} and Martinez, {Terina N.} and Ruhn, {Kelly A.} and Wrage, {Philip C.} and Keefer, {Edward W.} and Botterman, {Barry R.} and Tansey, {Keith E.} and Tansey, {Mal{\'u} G.}",

note = "Funding Information: This work was supported by grants from the National Parkinson Foundation (MGT), the National Institute of Neurological Disorders and Stroke, National Institutes of Health (R21 NS051526-02, MGT and KET), and a National Institutes of Health Predoctoral Training Grant GM007062 (PCW). We would like to thank Sabrina P. Martinez for assistance with tissue culture in the earliest stages of the project, John Hong for technical help with immunocytochemistry, Christine Smith for help with surgery and animal care, and members of the Tansey labs for helpful discussions. We would also like to thank Dr. Don Cooper in the Department of Psychiatry at UT Southwestern for access to his StereoInvestigator system. ",

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T1 - Autologous transplants of Adipose-Derived Adult Stromal (ADAS) cells afford dopaminergic neuroprotection in a model of Parkinson's disease

AU - McCoy, Melissa K.

AU - Martinez, Terina N.

AU - Ruhn, Kelly A.

AU - Wrage, Philip C.

AU - Keefer, Edward W.

AU - Botterman, Barry R.

AU - Tansey, Keith E.

AU - Tansey, Malú G.

N1 - Funding Information: This work was supported by grants from the National Parkinson Foundation (MGT), the National Institute of Neurological Disorders and Stroke, National Institutes of Health (R21 NS051526-02, MGT and KET), and a National Institutes of Health Predoctoral Training Grant GM007062 (PCW). We would like to thank Sabrina P. Martinez for assistance with tissue culture in the earliest stages of the project, John Hong for technical help with immunocytochemistry, Christine Smith for help with surgery and animal care, and members of the Tansey labs for helpful discussions. We would also like to thank Dr. Don Cooper in the Department of Psychiatry at UT Southwestern for access to his StereoInvestigator system.

PY - 2008/3

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N2 - Adult adipose contains stromal progenitor cells with neurogenic potential. However, the stability of neuronal phenotypes adopted by Adipose-Derived Adult Stromal (ADAS) cells and whether terminal neuronal differentiation is required for their consideration as alternatives in cell replacement strategies to treat neurological disorders is largely unknown. We investigated whether in vitro neural induction of ADAS cells determined their ability to neuroprotect or restore function in a lesioned dopaminergic pathway. In vitro-expanded naïve or differentiated ADAS cells were autologously transplanted into substantia nigra 1 week after an intrastriatal 6-hydroxydopamine injection. Neurochemical and behavioral measures demonstrated neuroprotective effects of both ADAS grafts against 6-hydroxydopamine-induced dopaminergic neuron death, suggesting that pre-transplantation differentiation of the cells does not determine their ability to survive or neuroprotect in vivo. Therefore, we investigated whether equivalent protection by naïve and neurally-induced ADAS grafts resulted from robust in situ differentiation of both graft types into dopaminergic fates. Immunohistological analyses revealed that ADAS cells did not adopt dopaminergic cell fates in situ, consistent with the limited ability of these cells to undergo terminal differentiation into electrically active neurons in vitro. Moreover, re-exposure of neurally-differentiated ADAS cells to serum-containing medium in vitro confirmed ADAS cell phenotypic instability (plasticity). Lastly, given that gene expression analyses of in vitro-expanded ADAS cells revealed that both naïve and differentiated ADAS cells express potent dopaminergic survival factors, ADAS transplants may have exerted neuroprotective effects by production of trophic factors at the lesion site. ADAS cells may be ideal for ex vivo gene transfer therapies in Parkinson's disease treatment.

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KW - Tyrosine hydroxylase

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Autologous transplants of Adipose-Derived Adult Stromal (ADAS) cells afford dopaminergic neuroprotection in a model of Parkinson's disease

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Keywords

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