Mouse Sox17 haploinsufficiency leads to female subfertility due to impaired implantation

Hirate, Yoshikazu; Suzuki, Hitomi; Kawasumi, Miyuri; Takase, Hinako M.; Igarashi, Hitomi; Naquet, Philippe; Kanai, Yoshikatsu; Kanai‐Azuma, Masami

doi:10.1038/srep24171

Cited by 45 publications

(40 citation statements)

References 38 publications

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“…Similarly, motifs of Sex Determining Region Y Box (SOX) factors are also enriched in the uterine, but not the HPC7 cell GATA2 cistrome (Table S4). It is worthy to note that, SOX17 is also expressed in the uterine epithelial cells (Rubel et al, 2012b), where GATA2 is expressed, and functions in the process of embryo implantation (Hirate et al, 2016). These findings revealed a uterine-specific GATA2 occupancy pattern that is associated with the presence of binding motifs of transcription factors, such as PGR, and SOX17 that have been known to regulate uterine function.…”

Section: Resultsmentioning

confidence: 99%

“…6B) that consists of GATA2, PGR and SOX17 transcription factors (Guimaraes-Young et al, 2016; Hirate et al, 2016; Rubel et al, 2012a; Rubel et al, 2012b). To investigate this network in human endometrial samples, we performed path analyses on the GSE58144 dataset using a structural equation modeling (Xiong et al, 2004).…”

Section: Resultsmentioning

confidence: 99%

“…In this group, the binding motif for Forkhead box (FOX) proteins is enriched in the GATA2 occupying sites, which bears a resemblance of co-occupancy of GATA2 and FOXA1 in genomic loci of AR target genes in prostate cancer (Wu et al, 2014). Furthermore, the enrichment of SOX (Sex Determining Region Y Box) factor binding motifs also implicates a potential interaction between GATA2 and other uterine transcription regulators such as SOX17 (Garcia et al, 2007; Guimaraes-Young et al, 2016; Hirate et al, 2016). These results indicate future investigations on potential mechanisms by which GATA2 and PGR work independently with other transcription regulators to direct gene expression in the uterus.…”

Section: Discussionmentioning

confidence: 99%

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A Gata2-Dependent Transcription Network Regulates Uterine Progesterone Responsiveness and Endometrial Function

et al. 2016

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SUMMARY Altered progesterone responsiveness leads to female infertility and cancer, but underlying mechanisms remain unclear. Mice with uterine-specific ablation of Gata2 are infertile showing failures in embryo implantation, endometrial decidualization and uninhibited estrogen signaling. Gata2 deficiency results in reduced progesterone receptor (PGR) expression and attenuated progesterone signaling, as evidenced by genome-wide expression profiling and chromatin immunoprecipitation. GATA2 not only occupies at and promotes expression of Pgr, but also regulates downstream progesterone responsive genes in conjunction with the PGR. Additionally, Gata2 knockout uteri exhibit abnormal luminal epithelia with ectopic TRP63 expressing squamous cells and a cancer related molecular profile in a progesterone independent manner. Lastly, we found a conserved GATA2-PGR regulatory network in both human and mouse, based on gene signature and path analyses using gene expression profiles of human endometrial tissues. In conclusion, uterine Gata2 regulates a key regulatory network of gene expression for progesterone signaling at the early pregnancy stage.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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A Gata2-Dependent Transcription Network Regulates Uterine Progesterone Responsiveness and Endometrial Function

et al. 2016

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“…Notably, many mouse models of implantation or early pregnancy failure require study in the immediate post-implantation time frame, beginning at 5.5 d.p.c. [7, 21–23]. In studies described here, the ability to accurately detect implantation site number, location, and growth from 5.5 d.p.c onwards in both 2-D and 3-D visual reconstruction in the pregnant mouse provides clear advantages over earlier studies that were limited to mid-pregnancy and used only 2-D imaging [14, 15].…”

Section: Discussionmentioning

confidence: 97%

Three-Dimensional High-Frequency Ultrasonography for Early Detection and Characterization of Embryo Implantation Site Development in the Mouse

et al. 2017

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Ultrasonography is a powerful tool to non-invasively monitor in real time the development of the human fetus in utero. Although genetically engineered mice have served as valuable in vivo models to study both embryo implantation and pregnancy progression, such studies usually require sacrifice of parous mice for subsequent phenotypic analysis. To address this issue, we used three-dimensional (3-D) reconstruction in silico of high-frequency ultrasound (HFUS) imaging data for early detection and characterization of murine embryo implantation sites and their development in utero. With HFUS imaging followed by 3-D reconstruction, we were able to precisely quantify embryo implantation site number and embryonic developmental progression in pregnant C57BL6J/129S mice from as early as 5.5 days post coitus (d.p.c.) through to 9.5 d.p.c. using a VisualSonics Vevo 2100 (MS550S) transducer. In addition to measurements of implantation site number, location, volume and spacing, embryo viability via cardiac activity monitoring was also achieved. A total of 12 dams were imaged with HFUS with approximately 100 embryos examined per embryonic day. For the post-implantation period (5.5 to 8.5 d.p.c.), 3-D reconstruction of the gravid uterus in mesh or solid overlay format enabled visual representation in silico of implantation site location, number, spacing distances, and site volume within each uterine horn. Therefore, this short technical report describes the feasibility of using 3-D HFUS imaging for early detection and analysis of post-implantation events in the pregnant mouse with the ability to longitudinally monitor the development of these early pregnancy events in a non-invasive manner. As genetically engineered mice continue to be used to characterize female reproductive phenotypes, we believe this reliable and non-invasive method to detect, quantify, and characterize early implantation events will prove to be an invaluable investigative tool for the study of female infertility and subfertility phenotypes based on a defective uterus.

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“…Recently, new gene editing technology, such as CRISPR/Cas9 system has opened a new era for the generation of transgenic animal models in a more efficient and economical way that can help further identify uterine-specific enhancer or promoter regions of these PGR-associated genes. For example, PGR and GATA2 both occupy at putative enhancers of the Sox17 and Ihh genes [45] that have pivotal uterine functions [54, 91, 92]. While results from in vitro assays suggest a cooperation of PGR and GATA2 in the regulation of enhancers for the Sox17 and Ihh genes, the in vivo function of such enhancers remains to be demonstrated, perhaps by CRISPR technology.…”

Section: Discussionmentioning

confidence: 99%

Hormone dependent uterine epithelial-stromal communication for pregnancy support

Wang

DeMayo

2017

Placenta

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Human fertility is a relatively inefficient process. Despite the presence of visibly healthy embryos, 30% of pregnancies generated by assisted reproductive technology (ART) fail before the second trimester. The uterine microenvironment plays a critical role in establishing and maintaining a successful pregnancy that requires coordinated communication between the epithelial and stromal cells of the endometrium. The epithelial cells must cease proliferation and become permissive for the conceptus (embryo and associated extraembryonic membranes), while the stromal cells undergoes mesenchymal-to-epithelioid transformation to form the decidua in support of subsequent embryo development. The ovarian steroids Estrogen (E2) and Progesterone (P4) are the major hormones governing these processes. These hormones act via their nuclear receptors, the estrogen receptor, ESR1, and progesterone receptor, PGR, to direct the transcription of genes that orchestrate epithelial and stromal cell communication. This review will discuss the molecular mechanisms utilized by steroid hormones that regulate uterine receptivity, as well, establish and maintain pregnancy.

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Mouse Sox17 haploinsufficiency leads to female subfertility due to impaired implantation

Cited by 45 publications

References 38 publications

A Gata2-Dependent Transcription Network Regulates Uterine Progesterone Responsiveness and Endometrial Function

A Gata2-Dependent Transcription Network Regulates Uterine Progesterone Responsiveness and Endometrial Function

Three-Dimensional High-Frequency Ultrasonography for Early Detection and Characterization of Embryo Implantation Site Development in the Mouse

Hormone dependent uterine epithelial-stromal communication for pregnancy support

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