In vitro deacetylation of N‐acetylserotonin by arylacetamide deacetylase

Author:

Huang Zheping1ORCID,Li Yu2,Konishi Keigo3,Sakai Yoshiyuki3,Tashiro Kiyomichi3,Fukami Tatsuki34,Borjigin Jimo1

Affiliation:

1. Department of Molecular and Integrative Physiology University of Michigan Medical School Ann Arbor Michigan USA

2. Harbin Center for Disease Control and Prevention, Bacteriologic Laboratory Harbin Center for Disease Control and Prevention Harbin Heilongjiang Province China

3. Faculty of Pharmaceutical Sciences, Drug Metabolism and Toxicology, Faculty of Pharmaceutical Sciences Kanazawa University Kanazawa Kakuma‐machi Japan

4. WPI Nano Life Science Institute (WPI‐Nano LSI) Kanazawa University Kanazawa Kakuma‐machi Japan

Abstract

AbstractArylacetamide deacetylase (AADAC) is a deacetylation enzyme present in the mammalian liver, gastrointestinal tract, and brain. During our search for mammalian enzymes capable of metabolizing N‐acetylserotonin (NAS), AADAC was identified as having the ability to convert NAS to serotonin. Both human and rodent recombinant AADAC proteins can deacetylate NAS in vitro, although the human AADAC shows markedly higher activity compared with rodent enzyme. The AADAC‐mediated deacetylation reaction can be potently inhibited by eserine in vitro. In addition to NAS, recombinant hAADAC can deacetylate melatonin (to form 5‐methoxytryptamine) and N‐acetyltryptamine (NAT) (to form tryptamine). In addition to the in vitro deacetylation of NAS by the recombinant AADAC proteins, liver (mouse and human) and brain (human) extracts were able to deacetylate NAS; these activities were sensitive to eserine. Taken together, these results demonstrate a new role for AADAC and suggest a novel pathway for the AADAC‐mediated metabolism of pineal indoles in mammals.

Funder

U.S. Department of Defense

Publisher

Wiley

Subject

Endocrinology

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