4.7 Article

Evolution of a transcriptional regulator from a transmembrane nucleoporin

Journal

GENES & DEVELOPMENT
Volume 30, Issue 10, Pages 1155-1171

Publisher

COLD SPRING HARBOR LAB PRESS, PUBLICATIONS DEPT
DOI: 10.1101/gad.280941.116

Keywords

evolution; hominoid; Pom121; Nup98; transcription; nuclear pore complex (NPC)

Funding

  1. American Cancer Society [PF-11-142-01-DMC, P30CA014195]
  2. National Institutes of Health [R01GM098749]
  3. Glenn Aging Foundation
  4. National Institute of Health [P50 GM107632]
  5. Helmsley Charitable Fund
  6. Mathers Foundation
  7. JPB Foundation

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Nuclear pore complexes (NPCs) emerged as nuclear transport channels in eukaryotic cells similar to 1.5 billion years ago. While the primary role of NPCs is to regulate nucleo-cytoplasmic transport, recent research suggests that certain NPC proteins have additionally acquired the role of affecting gene expression at the nuclear periphery and in the nucleoplasm in metazoans. Here we identify a widely expressed variant of the transmembrane nucleoporin (Nup) Pom121 (named sPom121, for soluble Pom121) that arose by genomic rearrangement before the divergence of hominoids. sPom121lacks the nuclear membrane-anchoring domain and thus does not localize to the NPC. Instead, sPom121 colocalizes and interacts with nucleoplasmic Nup98, a previously identified transcriptional regulator, at gene promoters to control transcription of its target genes in human cells. Interestingly, sPom121 transcripts appear independently in several mammalian species, suggesting convergent innovation of Nup-mediated transcription regulation during mammalian evolution. Our findings implicate alternate transcription initiation as a mechanism to increase the functional diversity of NPC components.

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