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Tyrosinase deficiency impairs social novelty preference in mice

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Objective Tyrosinase is a rate-limiting enzyme for the biosynthesis of melanin pigment in peripheral tissues, such as skin and the retina. We recently reported the expression and enzymatic activity of tyrosinase as well as its protective effects against oxidative stress-induced protein damage in the mouse brain. The functional role of tyrosinase in the central nervous system, however, remains largely unknown. In the present study, we investigated the involvement of tyrosinase in social behavior in mice. Methods Pigmented C57BL/10JMsHir (B10) and tyrosinase-deficient albino B10.C-Tyrc /Hir (B10-c) mice were subjected to the three-chamber sociability test to assess sociability and social novelty preference. In addition, we measured the mRNA expression of genes involved in catecholamine metabolism in the hippocampus by real-time quantitative PCR analysis. Results The results obtained showed that tyrosinase deficiency impaired social novelty preference, but not sociability in mice. We also found that the hippocampal expression of genes involved in catecholamine metabolism, such as monoamine oxidase A and catechol-O-methyltransferase, were significantly decreased in tyrosinase-deficient B10-c mice. Conclusion These results suggest that tyrosinase activity is functionally involved in the phenotypic expression of social behavior, particularly social novelty preference, in mice. The present study will advance our understanding of the functional role of tyrosinase in the central nervous system.
Ovid Technologies (Wolters Kluwer Health)
Title: Tyrosinase deficiency impairs social novelty preference in mice
Description:
Objective Tyrosinase is a rate-limiting enzyme for the biosynthesis of melanin pigment in peripheral tissues, such as skin and the retina.
We recently reported the expression and enzymatic activity of tyrosinase as well as its protective effects against oxidative stress-induced protein damage in the mouse brain.
The functional role of tyrosinase in the central nervous system, however, remains largely unknown.
In the present study, we investigated the involvement of tyrosinase in social behavior in mice.
Methods Pigmented C57BL/10JMsHir (B10) and tyrosinase-deficient albino B10.
C-Tyrc /Hir (B10-c) mice were subjected to the three-chamber sociability test to assess sociability and social novelty preference.
In addition, we measured the mRNA expression of genes involved in catecholamine metabolism in the hippocampus by real-time quantitative PCR analysis.
Results The results obtained showed that tyrosinase deficiency impaired social novelty preference, but not sociability in mice.
We also found that the hippocampal expression of genes involved in catecholamine metabolism, such as monoamine oxidase A and catechol-O-methyltransferase, were significantly decreased in tyrosinase-deficient B10-c mice.
Conclusion These results suggest that tyrosinase activity is functionally involved in the phenotypic expression of social behavior, particularly social novelty preference, in mice.
The present study will advance our understanding of the functional role of tyrosinase in the central nervous system.

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