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D-aspartate regulates melanocortin formation and function: behavioral alterations in D-aspartate oxidase-deficient mice.


ABSTRACT: D-aspartate, an abundant D-amino acid enriched in neuroendocrine tissues, can be degraded by D-aspartate oxidase (Ddo). To elucidate the function of D-aspartate, we generated mice with targeted deletion of Ddo (Ddo(-/-)) and observe massive but selective augmentations of D-aspartate in various tissues. The pituitary intermediate lobe, normally devoid of D-aspartate from endogenous Ddo expression, manifests pronounced increases of immunoreactive D-aspartate in Ddo(-/-) mice. Ddo(-/-) mice show markedly diminished synthesis and levels of pituitary proopiomelanocortin/alpha-MSH, associated with decreased melanocortin-dependent behaviors. Therefore, Ddo is the endogenous enzyme that degrades D-aspartate, and Ddo-enriched organs, low in D-aspartate, may represent areas of high turnover where D-aspartate may be physiologically important.

SUBMITTER: Huang AS 

PROVIDER: S-EPMC6675153 | biostudies-literature | 2006 Mar

REPOSITORIES: biostudies-literature

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D-aspartate regulates melanocortin formation and function: behavioral alterations in D-aspartate oxidase-deficient mice.

Huang Alex S AS   Beigneux Anne A   Weil Zachary M ZM   Kim Paul M PM   Molliver Mark E ME   Blackshaw Seth S   Nelson Randy J RJ   Young Stephen G SG   Snyder Solomon H SH  

The Journal of neuroscience : the official journal of the Society for Neuroscience 20060301 10


D-aspartate, an abundant D-amino acid enriched in neuroendocrine tissues, can be degraded by D-aspartate oxidase (Ddo). To elucidate the function of D-aspartate, we generated mice with targeted deletion of Ddo (Ddo(-/-)) and observe massive but selective augmentations of D-aspartate in various tissues. The pituitary intermediate lobe, normally devoid of D-aspartate from endogenous Ddo expression, manifests pronounced increases of immunoreactive D-aspartate in Ddo(-/-) mice. Ddo(-/-) mice show ma  ...[more]

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