Biochemical Characterisation of the Short Isoform of Histone N-Terminal Acetyltransferase NAA40

Author:

Klavaris Ariel1,Kouma Maria1,Ozdemir Cem2ORCID,Nicolaidou Vicky3ORCID,Miller Kyle M.2ORCID,Koufaris Costas14ORCID,Kirmizis Antonis1ORCID

Affiliation:

1. Epigenetics and Gene Regulation Laboratory, Department of Biological Sciences, University of Cyprus, Nicosia 2109, Cyprus

2. Department of Molecular Biosciences, The University of Texas at Austin, Austin, TX 78712, USA

3. Department of Life Sciences, University of Nicosia, Nicosia 2417, Cyprus

4. Cyprus Cancer Research Institute, Nicosia 2109, Cyprus

Abstract

N-alpha-acetyltransferase 40 (NAA40) is an evolutionarily conserved N-terminal acetyltransferase (NAT) linked to oncogenesis and chemoresistance. A recent study reported the generation of a second, shorter NAA40 isoform (NAA40S) through alternative translation, which we proceeded to further characterise. Notably, recombinant NAA40S had a greater in vitro enzymatic activity and affinity towards its histone H2A/H4 substrates compared to full-length NAA40 (NAA40L). Within cells, NAA40S was enzymatically active, based on its ability to suppress the H2A/H4S1Ph antagonistic mark in CRISPR-generated NAA40 knockout cells. Finally, we show that in addition to alternative translation, the NAA40S isoform could be derived from a primate and testis-specific transcript, which may align with the “out-of-testis” origin of recently evolved genes and isoforms. To summarise, our data reveal an even greater functional divergence between the two NAA40 isoforms than had been previously recognised.

Funder

European Regional Development Fund and the Republic of Cyprus

Cyprus Cancer Research Institute’s (C.C.R.I) Bridges in research excellence grant

Cancer Prevention and Research Institute of Texas

Publisher

MDPI AG

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