Functional Divergence of the Nuclear Receptor NR2C1 as a Modulator of Pluripotentiality During Hominid Evolution.
Jennifer L BakerKatherine A DunnJoseph MingroneBernard A WoodBeverly A KarpinskiChet C SherwoodDerek E WildmanThomas M MaynardJoseph P BielawskiPublished in: Genetics (2016)
Genes encoding nuclear receptors (NRs) are attractive as candidates for investigating the evolution of gene regulation because they (1) have a direct effect on gene expression and (2) modulate many cellular processes that underlie development. We employed a three-phase investigation linking NR molecular evolution among primates with direct experimental assessment of NR function. Phase 1 was an analysis of NR domain evolution and the results were used to guide the design of phase 2, a codon-model-based survey for alterations of natural selection within the hominids. By using a series of reliability and robustness analyses we selected a single gene, NR2C1, as the best candidate for experimental assessment. We carried out assays to determine whether changes between the ancestral and extant NR2C1s could have impacted stem cell pluripotency (phase 3). We evaluated human, chimpanzee, and ancestral NR2C1 for transcriptional modulation of Oct4 and Nanog (key regulators of pluripotency and cell lineage commitment), promoter activity for Pepck (a proxy for differentiation in numerous cell types), and average size of embryological stem cell colonies (a proxy for the self-renewal capacity of pluripotent cells). Results supported the signal for alteration of natural selection identified in phase 2. We suggest that adaptive evolution of gene regulation has impacted several aspects of pluripotentiality within primates. Our study illustrates that the combination of targeted evolutionary surveys and experimental analysis is an effective strategy for investigating the evolution of gene regulation with respect to developmental phenotypes.
Keyphrases
- gene expression
- stem cells
- single cell
- dna methylation
- genome wide
- transcription factor
- cell therapy
- endothelial cells
- induced apoptosis
- cross sectional
- cell proliferation
- embryonic stem cells
- high throughput
- cell fate
- genome wide identification
- mesenchymal stem cells
- oxidative stress
- bone marrow
- cancer therapy
- copy number
- endoplasmic reticulum stress