Germline sexual fate is determined by the antagonistic action of dmrt1 and foxl3/foxl2 in tilapia

Author:

Dai Shengfei1ORCID,Qi Shuangshuang1ORCID,Wei Xueyan1ORCID,Liu Xingyong1ORCID,Li Yibing1ORCID,Zhou Xin1ORCID,Xiao Hesheng1ORCID,Lu Baoyue1ORCID,Wang Deshou1ORCID,Li Minghui1ORCID

Affiliation:

1. Key Laboratory of Freshwater Fish Reproduction and Development (Ministry of Education), Key Laboratory of Aquatic Science of Chongqing, School of Life Sciences, Southwest University, Chongqing 400715, China

Abstract

ABSTRACT Germline sexual fate has long been believed to be determined by the somatic environment, but this idea is challenged by recent studies of foxl3 mutants in medaka. Here, we demonstrate that the sexual fate of tilapia germline is determined by the antagonistic interaction of dmrt1 and foxl3, which are transcriptionally repressed in male and female germ cells, respectively. Loss of dmrt1 rescued the germ cell sex reversal in foxl3Δ7/Δ7 XX fish, and loss of foxl3 partially rescued germ cell sex reversal but not somatic cell fate in dmrt1Δ5/Δ5 XY fish. Interestingly, germ cells lost sexual plasticity in dmrt1Δ5/Δ5 XY and foxl3Δ7/Δ7 XX single mutants, as aromatase inhibitor (AI) and estrogen treatment failed to rescue the respective phenotypes. However, recovery of germ cell sexual plasticity was observed in dmrt1/foxl3 double mutants. Importantly, mutation of somatic cell-specific foxl2 resulted in testicular development in foxl3Δ7/Δ7 or dmrt1Δ5/Δ5 mutants. Our findings demonstrate that sexual plasticity of germ cells relies on the presence of both dmrt1 and foxl3. The existence of dmrt1 and foxl3 allows environmental factors to influence the sex fate decision in vertebrates.

Funder

National Natural Science Foundation of China

National Key Research and Development Program of China

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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