Abstract
BackgroundNASP is an essential protein in mammals that functions in histone transport pathways and maintenance of a soluble reservoir of histones H3/H4. NASP has been studied exclusively in Opisthokonta lineages where some functional diversity has been reported. In humans, growing evidence implicates NASP miss-regulation in the development of a variety of cancers. Although a comprehensive phylogenetic analysis is lacking, NASP-family proteins that possess four TPR motifs are thought to be widely distributed across eukaryotes.ResultsWe characterize the molecular evolution of NASP by systematically identifying putative NASP orthologs across diverse eukaryotic lineages ranging from excavata to those of the crown group. We detect extensive silent divergence at the nucleotide level suggesting the presence of strong purifying selection acting at the protein level. We also observe a selection bias for high frequencies of acidic residues which we hypothesize is a consequence of their critical function(s), further indicating the role of functional constraints operating on NASP evolution. Our data indicate that TPR1 and TPR4 constitute the most rapidly evolving functional units of NASP and may account for the functional diversity observed among well characterized family members. We also show that NASP paralogs in ray-finned fish have different genomic environments with clear differences in their GC content and have undergone significant changes at the protein level suggesting functional diversification.ConclusionWe draw four main conclusions from this study. First, wide distribution of NASP throughout eukaryotes suggests that it was likely present in the last eukaryotic common ancestor (LECA) possibly as an important innovation in the transport of H3/H4. Second, strong purifying selection operating at the protein level has influenced the nucleotide composition of NASP genes. Further, we show that selection has acted to maintain a high frequency of functionally relevant acidic amino acids in the region that interrupts TPR2. Third, functional diversity reported among several well characterized NASP family members can be explained in terms of quickly evolving TPR1 and TPR4 motifs. Fourth, NASP fish specific paralogs have significantly diverged at the protein level with NASP2 acquiring a NNR domain.
Highlights
nuclear autoantigenic sperm protein (NASP) is an essential protein in mammals that functions in histone transport pathways and maintenance of a soluble reservoir of histones H3/H4
Our analysis indicates that NASP is conserved across all of the major eukaryotic lineages ranging from the excavata to the crown group suggesting that the NASP histone chaperone was most likely present in the last eukaryotic common ancestor (LECA)
NASP is highly conserved in eukaryotes We used PSI-BLAST searches with default parameters to identify putative NASP orthologs across a wide range of eukaryotic lineages including those of the crown group, the Guillardia nucleomorph, chromalveolates, and excavatas
Summary
NASP is an essential protein in mammals that functions in histone transport pathways and maintenance of a soluble reservoir of histones H3/H4. Newly synthesized histones H3.1/H4 are thought to successively pass through at least four distinct cytosolic complexes [10,12]. In this context, NASP has been shown to be involved in accepting the histones from heat shock proteins, in the Hat1-dependent acetylation of H4, and subsequently handing over these histones to another histone chaperone, anti-silencing factor 1 (Asf1) through a physical interaction that has been shown to exist in humans and Saccharomyces cerevisiae [10,12,13]
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