Vascular endothelial growth factor-A isoform and (co)receptor expression are differentially regulated by 17β-oestradiol in the ovariectomised mouse uterus

Walter, Lisa M.; Rogers, Peter A. W.; Girling, Jane E.

doi:10.1530/rep-10-0047

Cited by 16 publications

(14 citation statements)

References 49 publications

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“…It is interesting that NRP2 expression was associated with gender difference in our experiment, suggesting that NRP2 expression may be regulated by the sex hormones. Previous studies have demonstrated that NRP2 mRNA was decreased by estrogen in animal models (Walter et al 2010), which was consistent with our observation to some extent and may partially elucidate why male patients had higher NRP2 expression in our experiment. However, the underlying mechanisms of the correlation between NRP2 expression and sex hormone level is still misty.…”

Section: Discussionsupporting

confidence: 93%

Concurrent Expression of VEGF-C and Neuropilin-2 Is Correlated with Poor Prognosis in Glioblastoma

Zhao

Hou

et al. 2016

Tohoku J. Exp. Med.

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Section: Discussionsupporting

confidence: 93%

Concurrent Expression of VEGF-C and Neuropilin-2 Is Correlated with Poor Prognosis in Glioblastoma

Zhao

Hou

et al. 2016

Tohoku J. Exp. Med.

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“…Transgenic mice were slightly older because tghFST315 mice do not demonstrate mating behaviour until ,8 wks of age (Lin et al 2008). Following bilateral ovariectomy, mice were left for a minimum of 7 days to recover and to allow for endometrial regression, before one of two steroid hormone protocols commenced (Heryanto and Rogers 2002;Walter et al 2005Walter et al , 2010Girling et al 2007). Protocol 1 (short-term oestrogen, E): mice were given a single subcutaneous (s.c.) injection of oestradiol-17b (100 ng in 100 mL peanut oil; Sigma-Aldrich, St Louis, MO, USA) or vehicle (100 mL peanut oil) 8 days post-ovariectomy (n ¼ 7-9 per group).…”

Section: Study 1: Examination Of Fst Transgenic Oviducts and Uterimentioning

confidence: 99%

Follistatin is essential for normal postnatal development and function of mouse oviduct and uterus

Holdsworth-Carson

Craythorn

Winnall

et al. 2015

Reprod. Fertil. Dev.

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Abstract. Female mice lacking the follistatin gene but expressing a human follistatin-315 transgene (tghFST315) have reproductive abnormalities (reduced follicles, no corpora lutea and ovarian-uterine inflammation). We hypothesised that the absence of follistatin-288 causes the abnormal reproductive tract via both developmental abnormalities and abnormal ovarian activity. We characterised the morphology of oviducts and uteri in wild type (WT), tghFST315 and follistatinknockout mice expressing human follistatin-288 (tghFST288). The oviducts and uteri were examined in postnatal Day-0 and adult mice (WT and tghFST315 only) using histology and immunohistochemistry. Adult WT and tghFST315 mice were ovariectomised and treated with vehicle, oestradiol-17b (100 ng injection, dissection 24 h later) or progesterone (1 mg Â three daily injections, dissection 24 h later). No differences were observed in the oviducts or uteri at birth, but abnormalities developed by adulthood. Oviducts of tghFST315 mice failed to coil, the myometrium was disorganised, endometrial gland number was reduced and oviducts and uteri contained abundant leukocytes. After ovariectomy, tghFST315 mice had altered uterine cell proliferation, and inflammation was maintained and exacerbated by oestrogen. These studies show that follistatin is crucial to postnatal oviductal-uterine development and function. Further studies differentiating the role of ovarian versus oviductal-uterine follistatin in reproductive tract function at different developmental stages are warranted.

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“…Estrogen regulates several angiogenic factors in the mouse uterus, including Angiopoietin-2 and VEGF (Walter et al 2010;Guo et al 2012). Furthermore, similar to human decidual cells (Gibson et al 2013), mouse decidual cells are able to synthesize estrogen during pregnancy, which is critical for endometrial angiogenesis.…”

Section: Discussionmentioning

confidence: 99%

Mapping of estradiol binding sites through receptor micro-autoradiography in the endometrial stroma of early pregnant mice

Zorn

Favaro

Soto-Suazo

et al. 2017

Histochem Cell Biol

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Estradiol triggers key biological responses in the endometrium, which rely on the presence and levels of its cognate receptors on target cells. Employing the receptor micro-autoradiography (RMAR) technique, we aimed to provide a temporal and spatial map of the functional binding sites for estradiol in the mouse endometrial stroma during early pregnancy. Uterine samples from days 1.5 to 7.5 of pregnancy were collected 1 h after tritiated- (3H-) estradiol administration and prepared for RMAR analysis. Autoradiographic incorporation of 3H-thymidine (after 1-h pulse) was evaluated over the same gestational interval. Combined RMAR with either histochemistry with Dolichus biflorus (DBA) lectin or immunohistochemistry for detection of the desmin further characterized 3H-estradiol binding pattern in uterine Natural Killer (uNK) and decidual cells, respectively. 3H-estradiol binding levels oscillated in the pregnant endometrial stroma between the mesometrial and antimesometrial regions as well as the superficial and deep domains. Although most of the endometrial stromal cells retained the hormone, a sub-population of them, as well as endothelial and uNK cells, were unable to do so. Rises in the levels of 3H-estradiol binding preceded endometrial stromal cell proliferation. 3H-estradiol binding and 3H-thymidine incorporation progressively decreased along the development of the antimesometrial decidua. Endothelial proliferation occurred regardless of 3H-estradiol binding, whereas pericytes proliferation was associated with high levels of hormone binding. Endometrial cell populations autonomously control their levels of 3H-estradiol binding and retention, a process associated with their proliferative competence. Collectively, our results illustrate the intricate regulatory dynamic of nuclear estrogen receptors in the pregnant mouse endometrium.

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Vascular endothelial growth factor-A isoform and (co)receptor expression are differentially regulated by 17β-oestradiol in the ovariectomised mouse uterus

Cited by 16 publications

References 49 publications

Concurrent Expression of VEGF-C and Neuropilin-2 Is Correlated with Poor Prognosis in Glioblastoma

Concurrent Expression of VEGF-C and Neuropilin-2 Is Correlated with Poor Prognosis in Glioblastoma

Follistatin is essential for normal postnatal development and function of mouse oviduct and uterus

Mapping of estradiol binding sites through receptor micro-autoradiography in the endometrial stroma of early pregnant mice

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