Literature DB >> 15496142

Identification and characterization of the human ARD1-NATH protein acetyltransferase complex.

Thomas Arnesen1, Dave Anderson, Christian Baldersheim, Michel Lanotte, Jan E Varhaug, Johan R Lillehaug.   

Abstract

Protein acetyltransferases and deacetylases have been implicated in oncogenesis, apoptosis and cell cycle regulation. Most of the protein acetyltransferases described acetylate epsilon-amino groups of lysine residues within proteins. Mouse ARD1 (homologue of yeast Ard1p, where Ard1p stands for arrest defective 1 protein) is the only known protein acetyltransferase catalysing acetylation of proteins at both alpha-(N-terminus) and epsilon-amino groups. Yeast Ard1p interacts with Nat1p (N-acetyltransferase 1 protein) to form a functional NAT (N-acetyltransferase). We now describe the human homologue of Nat1p, NATH (NAT human), as the partner of the hARD1 (human ARD1) protein. Included in the characterization of the NATH and hARD1 proteins is the following: (i) endogenous NATH and hARD1 proteins are expressed in human epithelial, glioma and promyelocytic cell lines; (ii) NATH and hARD1 form a stable complex, as investigated by reciprocal immunoprecipitations followed by MS analysis; (iii) NATH-hARD1 complex expresses N-terminal acetylation activity; (iv) NATH and hARD1 interact with ribosomal subunits, indicating a co-translational acetyltransferase function; (v) NATH is localized in the cytoplasm, whereas hARD1 localizes both to the cytoplasm and nucleus; (vi) hARD1 partially co-localizes in nuclear spots with the transcription factor HIF-1alpha (hypoxia-inducible factor 1alpha), a known epsilon-amino substrate of ARD1; (vii) NATH and hARD1 are cleaved during apoptosis, resulting in a decreased NAT activity. This study identifies the human homologues of the yeast Ard1p and Nat1p proteins and presents new aspects of the NATH and hARD1 proteins relative to their yeast homologues.

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Year:  2005        PMID: 15496142      PMCID: PMC1134861          DOI: 10.1042/BJ20041071

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  43 in total

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Journal:  J Bacteriol       Date:  1989-11       Impact factor: 3.490

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7.  Composition and biological significance of the human Nalpha-terminal acetyltransferases.

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Journal:  BMC Proc       Date:  2009-08-04

8.  A synopsis of eukaryotic Nalpha-terminal acetyltransferases: nomenclature, subunits and substrates.

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10.  Arrest defective-1 controls tumor cell behavior by acetylating myosin light chain kinase.

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