ESR1 mediates estrogen-induced feminization of genetic male Chinese soft-shelled turtle

Author:

Li Pan12,Guo Yin12,Jin Lin12,Liang Xiao3,Chen Gaoan1,Sun Wei12,Xiao Ling12,Qian Guoying2,Ge Chutian12

Affiliation:

1. Institute of Animal Sex and Development, Zhejiang Wanli University , Ningbo, China

2. College of Biological and Environmental Sciences, Zhejiang Wanli University , Ningbo, China

3. College of Fisheries and Life Sciences, Shanghai Ocean University , Shanghai, China

Abstract

Abstract Exogenous estrogen have shown their feminization abilities during the specific sex differentiation period in several reptiles. However, the specific regulatory mechanism and downstream regulatory genes of estrogen remain elusive. In the present study, 17β-estradiol (E2), as well as drugs of specific antagonists and/or agonists of estrogen receptors, were employed to figure out the molecular pathway involved in the E2-induced feminization in Chinese soft-shelled turtles, an important aquaculture species in China. E2 treatment led to typical female characteristics in the gonads of ZZ individuals, including thickened outer cortex containing a number of germ cells and degenerated medullary cords, as well as the disappearance of male marker SOX9, and the ectopic expression of ovarian regulator FOXL2 at the embryonic developmental stage 27 and 1 month after hatching. The specific ESR1 antagonist or a combination of three estrogen receptor antagonists could block the sex reversal of ZZ individuals induced by estrogen. In addition, specific activation of ESR1 by agonist also led to the feminization of ZZ gonads, which was similar to the effect of estrogen treatment. Furthermore, transcriptome data showed that the expression level of FOXL2 was significantly upregulated, whereas mRNA levels of DMRT1, SOX9, and AMH were downregulated after estrogen treatment. Taken together, our results indicated that E2 induced the feminization of ZZ Chinese soft-shelled turtles via ESR1, and decrease of male genes DMRT1, SOX9, and AMH and increase of ovarian development regulator FOXL2 might be responsible for the initiation of E2-induced feminization.

Funder

National Key Research and Development Program

National Natural Science Foundation of China

Natural Science Foundation of Zhejiang Province for Distinguished Young Scholars

Key Scientific and Technological Grant of Zhejiang for Breeding New Agricultural Varieties

Basic Public Welfare Research Projects of Zhejiang Province

Key Technology Research and Development Projects in Ningbo

Key Agricultural Project of Ningbo

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,General Medicine,Reproductive Medicine

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