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Gadd45g is required for timely Sry expression independently of RSPO1 activity

Abstract:: Sex determination in mammals is controlled by the dominance of either pro-testis (SRY-SOX9-FGF9) or pro-ovary (RSPO1-WNT4-FOXL2) genetic pathways during early gonad development in XY and XX embryos, respectively. We have previously shown that early, robust expression of mouse Sry is dependent on the nuclear protein GADD45g. In the absence of GADD45g, XY gonadal sex reversal occurs, associated with a major reduction of Sry levels at 11.5 dpc. Here, we probe the relationship between Gadd45g and Sry further, using gain- and loss-of-function genetics. First, we show that transgenic Gadd45g overexpression can elevate Sry expression levels at 11.5 dpc in the B6.YPOS model of sex reversal, resulting in phenotypic rescue. We then show that the zygosity of pro-ovarian Rspo1 is critical for the degree of gonadal sex reversal observed in both B6.YPOS and Gadd45g-deficient XY gonads, in contrast to that of Foxl2. Phenotypic rescue of sex reversal is observed in XY gonads lacking both Gadd45g and Rspo1, but this is not associated with rescue of Sry expression levels at 11.5 dpc. Instead, Sox9 levels are rescued by around 12.5 dpc. We conclude that Gadd45g is absolutely required for timely expression of Sry in XY gonads, independently of RSPO1-mediated WNT signalling, and discuss these data in light of our understanding of antagonistic interactions between the pro-testis and pro-ovary pathways.

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Warr, N., Siggers, P., May, J., Chalon, N., Pope, M., Wells, S., Chaboissier, M.-C., & Greenfield, A. (2022). Gadd45g is required for timely Sry expression independently of RSPO1 activity. Reproduction, 163(6), 333–340.

MLA Style

Warr, N, et al. “Gadd45g Is Required for Timely Sry Expression Independently of RSPO1 Activity.” Reproduction, vol. 163, no. 6, 2022, pp. 333–40.

Chicago Style

Warr, N, P Siggers, J May, et al. 2022. “Gadd45g Is Required for Timely Sry Expression Independently of RSPO1 Activity.” Reproduction 163 (6): 333–40.
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Files:: Warr_et_al_2022_Gadd45g_is_required.pdf

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Publisher copy:: 10.1530/rep-21-0443

Authors

+ Warr, N More by this author

Role:: Author

+ Siggers, P More by this author

Role:: Author

+ May, J More by this author

Role:: Author

+ Chalon, N More by this author

Role:: Author

+ Pope, M More by this author

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+ Medical Research Council More from this funder

Funder identifier:: https://ror.org/03x94j517
Grant:: MC_UP_2201/1

Publisher:: BioScientifica
Journal:: Reproduction More from this journal
Volume:: 163
Issue:: 6
Pages:: 333-340
Place of publication:: England
Publication date:: 2022-04-22
Acceptance date:: 2022-03-22
DOI:: 10.1530/rep-21-0443
EISSN:: 1741-7899
ISSN:: 1470-1626
Pmid:: 35315790

Language:: English
Keywords:: mammals

sex differentiation

mice

gonads

gene expression regulation

developmental

thrombospondins

testis

sox9 transcription factor

sex determination processes

ovary

wnt signaling pathway

sex-determining region y protein
Pubs id:: 2077806
Local pid:: pubs:2077806
Deposit date:: 2025-02-25
ARK identifier:: ark:/29072/ora_bcc2700511fe4d71ba19a0f89ba76d7d

Terms of use

Copyright holder:: Warr et al
Copyright date:: 2022
Rights statement:: © 2022 The Authors. This work is licensed under a Creative Commons Attribution 4.0 International License.

Licence:: CC Attribution (CC BY)

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