Tilapia, a good model for studying reproductive endocrinology

Minghui Li; Lina Sun; Linyan Zhou; Deshou Wang

doi:10.1016/j.ygcen.2023.114395

Tilapia, a good model for studying reproductive endocrinology

Gen Comp Endocrinol. 2024 Jan 1:345:114395. doi: 10.1016/j.ygcen.2023.114395. Epub 2023 Oct 23.

Authors

Minghui Li¹, Lina Sun¹, Linyan Zhou¹, Deshou Wang²

Affiliations

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, China.
² 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, China. Electronic address: wdeshou@swu.edu.cn.

PMID: 37879418
DOI: 10.1016/j.ygcen.2023.114395

Abstract

The Nile tilapia (Oreochromis niloticus), with a system of XX/XY sex determination, is a worldwide farmed fish with a shorter sexual maturation time than that of most cultured fish. Tilapia show a spawning cycle of approximately 14 days and can be artificially propagated in the laboratory all year round to obtain genetically all female (XX) and all male (XY) fry. Its genome sequence has been opened, and a perfect gene editing platform has been established. With a moderate body size, it is convenient for taking enough blood to measure hormone level. In recent years, using tilapia as animal model, we have confirmed that estrogen is crucial for female development because 1) mutation of star2, cyp17a1 or cyp19a1a (encoding aromatase, the key enzyme for estrogen synthesis) results in sex reversal (SR) due to estrogen deficiency in XX tilapia, while mutation of star1, cyp11a1, cyp17a2, cyp19a1b or cyp11c1 affects fertility due to abnormal androgen, cortisol and DHP levels in XY tilapia; 2) when the estrogen receptors (esr2a/esr2b) are mutated, the sex is reversed from female to male, while when the androgen receptors are mutated, the sex cannot be reversed; 3) the differentiated ovary can be transdifferentiated into functional testis by inhibition of estrogen synthesis, and the differentiated testis can be transdifferentiated into ovary by simultaneous addition of exogenous estrogen and androgen synthase inhibitor; 4) loss of male pathway genes amhy, dmrt1, gsdf causes SR with upregulation of cyp19a1a in XY tilapia. Disruption of estrogen synthesis rescues the male to female SR of amhy and gsdf but not dmrt1 mutants; 5) mutation of female pathway genes foxl2 and sf-1 causes SR with downregulation of cyp19a1a in XX tilapia; 6) the germ cell SR of foxl3 mutants fails to be rescued by estrogen treatment, indicating that estrogen determines female germ cell fate through foxl3. This review also summarized the effects of deficiency of other steroid hormones, such as androgen, DHP and cortisol, on fish reproduction. Overall, these studies demonstrate that tilapia is an excellent animal model for studying reproductive endocrinology of fish.

Keywords: Estrogen; Reproductive endocrinology; Sex determination; Sexual plasticity; Tilapia.

Publication types

Review

MeSH terms

Androgens
Animals
Cichlids* / metabolism
Estrogens / metabolism
Female
Hydrocortisone
Male
Sex Differentiation / genetics
Tilapia* / genetics
Tilapia* / metabolism

Substances

Androgens
Hydrocortisone
Estrogens