Tyrosinase exacerbates dopamine toxicity but is not genetically associated with Parkinson's disease

Elisa Greggio; Elisabetta Bergantino; Donald Carter; Rili Ahmad; Gertrude-Emilia Costin; Vincent J Hearing; Jordi Clarimon; Andrew Singleton; Johanna Eerola-Rautio; Olli Hellström; Pentti J Tienari; David W Miller; Alexandra Beilina; Luigi Bubacco; Mark R Cookson

doi:10.1111/j.1471-4159.2005.03019.x

Tyrosinase exacerbates dopamine toxicity but is not genetically associated with Parkinson's disease

Elisa Greggio, Elisabetta Bergantino, Donald Carter, Rili Ahmad, Gertrude-Emilia Costin, Vincent J Hearing, Jordi Clarimon, Andrew Singleton, Johanna Eerola-Rautio, Olli Hellström, Pentti J Tienari, David W Miller, Alexandra Beilina, Luigi Bubacco, Mark R Cookson

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

Abstract

"Tyrosinase is a key enzyme in the synthesis of melanin in skin and hair and has also been proposed to contribute to the formation of neuromelanin (NM). The presence of NM, which is biochemically similar to melanin in peripheral tissues, identifies groups of neurons susceptible in Parkinson's disease (PD). Whether tyrosinase is beneficial or detrimental to neurons is unclear; whilst the enzyme activity of tyrosinase generates dopamine-quinones and other oxidizing compounds, NM may form a sink for such radical species. In the present study, we demonstrated that tyrosinase is expressed at low levels in the human brain. We found that mRNA, protein and enzyme activity are all present but at barely detectable levels. In cell culture systems, expression of tyrosinase increases neuronal susceptibility to oxidizing conditions, including dopamine itself. We related these in vitro observations to the human disease by assessing whether there was any genetic association between the gene encoding tyrosinase and idiopathic PD. We found neither genotypic or haplotypic association with three polymorphic markers of the gene. This argues against a strong genetic association between tyrosinase and PD, although the observed contribution to cellular toxicity suggests that a biochemical association is likely."

Original language	English
Journal	Journal of Neurochemistry
Volume	93
Pages (from-to)	246-256
Number of pages	11
ISSN	0022-3042
DOIs	https://doi.org/10.1111/j.1471-4159.2005.03019.x
Publication status	Published - 2005
MoE publication type	A1 Journal article-refereed

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10.1111/j.1471-4159.2005.03019.x

Cite this

Greggio, E., Bergantino, E., Carter, D., Ahmad, R., Costin, G.-E., Hearing, V. J., Clarimon, J., Singleton, A., Eerola-Rautio, J., Hellström, O., Tienari, P. J., Miller, D. W., Beilina, A., Bubacco, L., & Cookson, M. R. (2005). Tyrosinase exacerbates dopamine toxicity but is not genetically associated with Parkinson's disease. Journal of Neurochemistry, 93, 246-256. https://doi.org/10.1111/j.1471-4159.2005.03019.x

@article{dba2eab9573a4269aac369dc9a3614aa,

title = "Tyrosinase exacerbates dopamine toxicity but is not genetically associated with Parkinson's disease",

abstract = "{"}Tyrosinase is a key enzyme in the synthesis of melanin in skin and hair and has also been proposed to contribute to the formation of neuromelanin (NM). The presence of NM, which is biochemically similar to melanin in peripheral tissues, identifies groups of neurons susceptible in Parkinson's disease (PD). Whether tyrosinase is beneficial or detrimental to neurons is unclear; whilst the enzyme activity of tyrosinase generates dopamine-quinones and other oxidizing compounds, NM may form a sink for such radical species. In the present study, we demonstrated that tyrosinase is expressed at low levels in the human brain. We found that mRNA, protein and enzyme activity are all present but at barely detectable levels. In cell culture systems, expression of tyrosinase increases neuronal susceptibility to oxidizing conditions, including dopamine itself. We related these in vitro observations to the human disease by assessing whether there was any genetic association between the gene encoding tyrosinase and idiopathic PD. We found neither genotypic or haplotypic association with three polymorphic markers of the gene. This argues against a strong genetic association between tyrosinase and PD, although the observed contribution to cellular toxicity suggests that a biochemical association is likely.{"}",

author = "Elisa Greggio and Elisabetta Bergantino and Donald Carter and Rili Ahmad and Gertrude-Emilia Costin and Hearing, {Vincent J} and Jordi Clarimon and Andrew Singleton and Johanna Eerola-Rautio and Olli Hellstr{\"o}m and Tienari, {Pentti J} and Miller, {David W} and Alexandra Beilina and Luigi Bubacco and Cookson, {Mark R}",

year = "2005",

doi = "10.1111/j.1471-4159.2005.03019.x",

language = "English",

volume = "93",

pages = "246--256",

journal = "Journal of Neurochemistry",

issn = "0022-3042",

publisher = "John Wiley and Sons Inc",

}

Greggio, E, Bergantino, E, Carter, D, Ahmad, R, Costin, G-E, Hearing, VJ, Clarimon, J, Singleton, A, Eerola-Rautio, J, Hellström, O, Tienari, PJ, Miller, DW, Beilina, A, Bubacco, L & Cookson, MR 2005, 'Tyrosinase exacerbates dopamine toxicity but is not genetically associated with Parkinson's disease', Journal of Neurochemistry, vol. 93, pp. 246-256. https://doi.org/10.1111/j.1471-4159.2005.03019.x

TY - JOUR

T1 - Tyrosinase exacerbates dopamine toxicity but is not genetically associated with Parkinson's disease

AU - Greggio, Elisa

AU - Bergantino, Elisabetta

AU - Carter, Donald

AU - Ahmad, Rili

AU - Costin, Gertrude-Emilia

AU - Hearing, Vincent J

AU - Clarimon, Jordi

AU - Singleton, Andrew

AU - Eerola-Rautio, Johanna

AU - Hellström, Olli

AU - Tienari, Pentti J

AU - Miller, David W

AU - Beilina, Alexandra

AU - Bubacco, Luigi

AU - Cookson, Mark R

PY - 2005

Y1 - 2005

N2 - "Tyrosinase is a key enzyme in the synthesis of melanin in skin and hair and has also been proposed to contribute to the formation of neuromelanin (NM). The presence of NM, which is biochemically similar to melanin in peripheral tissues, identifies groups of neurons susceptible in Parkinson's disease (PD). Whether tyrosinase is beneficial or detrimental to neurons is unclear; whilst the enzyme activity of tyrosinase generates dopamine-quinones and other oxidizing compounds, NM may form a sink for such radical species. In the present study, we demonstrated that tyrosinase is expressed at low levels in the human brain. We found that mRNA, protein and enzyme activity are all present but at barely detectable levels. In cell culture systems, expression of tyrosinase increases neuronal susceptibility to oxidizing conditions, including dopamine itself. We related these in vitro observations to the human disease by assessing whether there was any genetic association between the gene encoding tyrosinase and idiopathic PD. We found neither genotypic or haplotypic association with three polymorphic markers of the gene. This argues against a strong genetic association between tyrosinase and PD, although the observed contribution to cellular toxicity suggests that a biochemical association is likely."

AB - "Tyrosinase is a key enzyme in the synthesis of melanin in skin and hair and has also been proposed to contribute to the formation of neuromelanin (NM). The presence of NM, which is biochemically similar to melanin in peripheral tissues, identifies groups of neurons susceptible in Parkinson's disease (PD). Whether tyrosinase is beneficial or detrimental to neurons is unclear; whilst the enzyme activity of tyrosinase generates dopamine-quinones and other oxidizing compounds, NM may form a sink for such radical species. In the present study, we demonstrated that tyrosinase is expressed at low levels in the human brain. We found that mRNA, protein and enzyme activity are all present but at barely detectable levels. In cell culture systems, expression of tyrosinase increases neuronal susceptibility to oxidizing conditions, including dopamine itself. We related these in vitro observations to the human disease by assessing whether there was any genetic association between the gene encoding tyrosinase and idiopathic PD. We found neither genotypic or haplotypic association with three polymorphic markers of the gene. This argues against a strong genetic association between tyrosinase and PD, although the observed contribution to cellular toxicity suggests that a biochemical association is likely."

U2 - 10.1111/j.1471-4159.2005.03019.x

DO - 10.1111/j.1471-4159.2005.03019.x

M3 - Article

SN - 0022-3042

VL - 93

SP - 246

EP - 256

JO - Journal of Neurochemistry

JF - Journal of Neurochemistry

ER -