PUBLICATION

A maternal-to-zygotic-transition gene block on the zebrafish sex chromosome

Authors
Wilson, C.A., Postlethwait, J.H.
ID
ZDB-PUB-240312-3
Date
2024
Source
G3 (Bethesda)   14(5): (Journal)
Registered Authors
Postlethwait, John H.
Keywords
Danio rerio, RNA-seq, Sex determination, gonad, heterochromatin, sex chromosome, transposable elements, zebrafish, zygotic genome activation
MeSH Terms
  • Animals
  • Female
  • Gene Expression Profiling
  • Male
  • Sex Chromosomes*/genetics
  • Sex Determination Processes/genetics
  • Testis/metabolism
  • Transcriptome
  • Zebrafish*/genetics
  • Zygote/metabolism
PubMed
38466753 Full text @ G3 (Bethesda)
Abstract
Wild zebrafish (Danio rerio) have a ZZ/ZW chromosomal sex determination system with the major sex locus on the right arm of chromosome-4 (Chr4R) near the largest heterochromatic block in the genome, suggesting that Chr4R transcriptomics might differ from the rest of the genome. To test this hypothesis, we conducted an RNA-seq analysis of adult ZW ovaries and ZZ testes in the Nadia strain and identified four regions of Chr4 with different gene expression profiles. Unique in the genome, protein-coding genes in a 41.7 Mb section (Region-2) were expressed in testis but silent in ovary. The AB lab strain, which lacks sex chromosomes, verified this result, showing that testis-biased gene expression in Region-2 depends on gonad biology, not on sex-determining mechanism. RNA-seq analyses in female and male brain and liver validated reduced transcripts from Region-2 in somatic cells, but without sex-specificity. Region-2 corresponds to the heterochromatic portion of Chr4R and its content of genes and repetitive elements distinguishes it from the rest of the genome. Region-2 lacks protein-coding genes with human orthologs; has zinc finger genes expressed early in zygotic genome activation; has maternal 5S rRNA genes, maternal spliceosome genes, a concentration of tRNA genes, and a distinct set of repetitive elements. The colocalization of 1) genes silenced in ovaries but not in testes that are 2) expressed in embryos briefly at the onset of zygotic genome activation; 3) maternal-specific genes for translation machinery; 4) maternal-specific spliceosome components; and 4) adjacent genes encoding miR-430, which mediates maternal transcript degradation, suggest that this is a Maternal-to-Zygotic-Transition Gene Regulatory Block.
Genes / Markers
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Expression
Phenotype
Mutations / Transgenics
Human Disease / Model
Sequence Targeting Reagents
Fish
Antibodies
Orthology
Engineered Foreign Genes
Mapping