NANOGP1, a tandem duplicate of NANOG, exhibits partial functional conservation in human naïve pluripotent stem cells

Author:

Maskalenka Katsiaryna1,Alagöz Gökberk2,Krueger Felix3,Wright Joshua1,Rostovskaya Maria1,Nakhuda Asif4,Bendall Adam1,Krueger Christel1,Walker Simon5,Scally Aylwyn2,Rugg-Gunn Peter J.167ORCID

Affiliation:

1. Babraham Institute 1 Epigenetics Programme , , Cambridge CB22 3AT, UK

2. University of Cambridge 2 Department of Genetics , , Cambridge CB2 3EH, UK

3. Babraham Institute 3 Bioinformatics Group , , Cambridge CB22 3AT, UK

4. Babraham Institute 4 Gene Targeting Facility , , Cambridge CB22 3AT, UK

5. Babraham Institute 5 Imaging Facility , , Cambridge CB22 3AT, UK

6. Wellcome-MRC Cambridge Stem Cell Institute 6 , Cambridge CB2 0AW, UK

7. Centre for Trophoblast Research, University of Cambridge 7 , Cambridge CB2 3EG, UK

Abstract

ABSTRACT Gene duplication events can drive evolution by providing genetic material for new gene functions, and they create opportunities for diverse developmental strategies to emerge between species. To study the contribution of duplicated genes to human early development, we examined the evolution and function of NANOGP1, a tandem duplicate of the transcription factor NANOG. We found that NANOGP1 and NANOG have overlapping but distinct expression profiles, with high NANOGP1 expression restricted to early epiblast cells and naïve-state pluripotent stem cells. Sequence analysis and epitope-tagging revealed that NANOGP1 is protein coding with an intact homeobox domain. The duplication that created NANOGP1 occurred earlier in primate evolution than previously thought and has been retained only in great apes, whereas Old World monkeys have disabled the gene in different ways, including homeodomain point mutations. NANOGP1 is a strong inducer of naïve pluripotency; however, unlike NANOG, it is not required to maintain the undifferentiated status of human naïve pluripotent cells. By retaining expression, sequence and partial functional conservation with its ancestral copy, NANOGP1 exemplifies how gene duplication and subfunctionalisation can contribute to transcription factor activity in human pluripotency and development.

Funder

Biotechnology and Biological Sciences Research Council

Medical Research Council

Wellcome Trust

Darwin Trust

Cambridge Commonwealth, European and International Trust

Erasmus+

Babraham Institute

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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