Teleost fish are the most diverse group of vertebrates and provide opportunities to study the evolution of sex determination (SD) systems. Using genomic and functional analyses, we identified a male-specific duplication of
anti-Müllerian hormone
(
amh
) gene as the male master sex-determining (MSD) gene in
Sebastes schlegelii
. By resequencing 10 males and 10 females, we characterized a 5 kb-long fragment in HiC_Scaffold_12 as a male-specific region, which contained an
amh
gene (named
amhy
). We then demonstrated that
amhy
is a duplication of autosomal
amh
that was later translocated to the ancestral Y chromosome.
amha
and
amhy
shared high-nucleotide identity with the most significant difference being two insertions in intron 4 of
amhy
. Furthermore,
amhy
overexpression triggered female-to-male sex reversal in
S. schlegelii
, displaying its fundamental role in driving testis differentiation. We developed a PCR assay which successfully identified sexes in two species of northwest Pacific rockfish related to
S. schlegelii
. However, the PCR assay failed to distinguish the sexes in a separate clade of northeast Pacific rockfish. Our study provides new examples of
amh
as the MSD in fish and sheds light on the convergent evolution of
amh
duplication as the driving force of sex determination in different fish taxa.
Here, we describe the first mitochondrial genome of the angelshark,
Squatina squatina.
The genome is 16,689 bp in length with 13 protein-coding genes, 22 tRNA genes, 2 rRNA genes, and a non-coding control region. Base composition of the mitogenome has an A + T bias (62.9%), seen commonly in other elasmobranchs. This genome provides a key resource for future investigations of the population genetic dynamics and evolution of this Critically Endangered shark.
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