Inactivation of maternal Hif-1α at mid-pregnancy causes placental defects and deficits in oxygen delivery to the fetal organs under hypoxic stress

Kenchegowda, Doreswamy; Natale, Bryony V.; Lemus, Maria A.; Natale, David R.C.; Fisher, Steven A.

doi:10.1016/j.ydbio.2016.12.013

Cited by 35 publications

(38 citation statements)

References 51 publications

(83 reference statements)

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“…Hif-1α results in a decrease in the number of uNK cells and impaired oxygen delivery to the fetus at E13.5-15.5 (Kenchegowda et al, 2017). Overall, this analysis indicates that disruption of Prl7d1 has a profound effect on signaling in the female placenta.…”

Section: Tissue Expression Enrichment Analysismentioning

confidence: 62%

“…Further, Wnt2‐ deficient mice exhibit decreased numbers of fetal capillaries and fibrinoid deposition in the placenta, and as a result, approximately 50% of pups die perinatally (Monkley, Delaney, Pennisi, Christiansen, & Wainwright, ). Inactivation of maternal Hif‐1α results in a decrease in the number of uNK cells and impaired oxygen delivery to the fetus at E13.5–15.5 (Kenchegowda et al, ). Overall, this analysis indicates that disruption of Prl7d1 has a profound effect on signaling in the female placenta.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, the placenta itself also synthesizes a variety of hormones, enzymes, and cytokines, which are mostly encoded by placenta‐specific genes, to adjust placental physiology and mediate gas exchange, nutrient uptake, and waste elimination between the mother and fetus (Bu, Alam, Dhakal, Vivian, & Soares, ; Burton & Fowden, ; Naruse et al, ; Simmons, Rawn, Davies, Hughes, & Cross, ). Emerging evidence suggests that some internal or external factors can target certain placenta‐specific genes, and therefore may impair placenta formation and function, ultimately contributing to the etiology of many pregnancy‐related diseases such as pre‐eclampsia, intrauterine growth restriction, and abortion; this can have consequences for the long‐term health of the individual (Huynh, Dawson, Roberts, & Bentley‐Lewis, ; Kenchegowda, Natale, Lemus, Natale, & Fisher, ; Sones et al, ). Thus, decoding the functions of these placental genes will help to elucidate placental physiology and pregnancy‐related diseases.…”

Section: Introductionmentioning

confidence: 99%

“…the long-term health of the individual (Huynh, Dawson, Roberts, & Bentley-Lewis, 2015;Kenchegowda, Natale, Lemus, Natale, & Fisher, 2017;Sones et al, 2018). Thus, decoding the functions of these placental genes will help to elucidate placental physiology and pregnancy-related diseases.…”

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confidence: 99%

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Deletion of Prl7d1 causes placental defects at mid‐pregnancy in mice

Zhang

Hao

2019

Molecular Reproduction Devel

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Prolactin family 7, subfamily d, member 1 (Prl7d1), a member of the expanding prolactin family, is mainly expressed in the placental junctional zone (including trophoblast giant cells and spongiotrophoblast cells) with peak expression observed at 12 days postcoitum (dpc) in mice. Previous studies have shown that PRL7D1 is a key mediator of angiogenesis in vitro; however, its physiological roles in placental development in vivo have not been characterized. To address this issue, we deleted Prl7d1 in mice and demonstrated that its absence results in reduced litter size and fertility. Histologically, Prl7d1 mutants exhibited striking placental abnormalities at 12.5 dpc, including a reduction in the proportion of labyrinth layers and a significant increase in decidual natural killer cells, glycogen trophoblasts, and trophoblast giant cells in the junctional zone. Moreover, placentas from Prl7d1‐null mice displayed a thickened decidual spiral artery. Notably, these negative effects were more pronounced in male fetuses. Further RNA‐sequencing analysis showed that Prl7d1 deletion results in significant differences in the placental transcriptome profile between the two sexes of fetuses. Together, this study demonstrates that Prl7d1 possesses antiangiogenic properties in deciduas and inhibits the development of junctional zone, which potentially alters the functional capacity of the placenta to support optimal fetal growth. Moreover, of note, the role of Prl7d1 in the placenta is regulated in a fetal sex‐specific manner.

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Section: Tissue Expression Enrichment Analysismentioning

confidence: 62%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

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Deletion of Prl7d1 causes placental defects at mid‐pregnancy in mice

Zhang

Hao

2019

Molecular Reproduction Devel

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“…Using the promoter from a specific gene or a chimeric DNA construct to direct Cre expression in specific cells is the key component of the Cre/loxP system. Although several promoters have been used to target transgene expression in trophoblast lineages, to our knowledge very few studies have been conducted using inducible Cre/loxP specifically for placental research . Furthermore, in both of these models, broadly expressed Cre transgenic animals were utilized, complicating the interpretation of the results.…”

Section: Introductionmentioning

confidence: 99%

The platelet‐derived growth factor receptor alpha promoter‐directed expression of cre recombinase in mouse placenta

Wattez

Qiao

Lee

et al. 2019

Developmental Dynamics

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Background Numerous pathologies of pregnancy originate from placental dysfunction. It is essential to understand the functions of key genes in the placenta in order to discern the etiology of placental pathologies. A paucity of animal models that allow conditional and inducible expression of a target gene in the placenta is a major limitation for studying placental development and function. Results To study the platelet‐derived growth factor receptor alpha ( PDGFRα )‐directed and tamoxifen‐induced Cre recombinase expression in the placenta, PDGFRα‐CreER mice were crossed with mT/mG dual‐fluorescent reporter mice. The expression of endogenous membrane‐localized enhanced green fluorescent protein (mEGFP) and/or dTomato in the placenta was examined to identify PDGFRα promoter‐directed Cre expression. Pregnant PDGFRα‐CreER ;mT/mG mice were treated with tamoxifen at various gestational ages. Upon tamoxifen treatment, reporter protein mEGFP was observed in the junctional zone (JZ) and chorionic plate (CP). Furthermore, a single dose of tamoxifen was sufficient to induce the recombination. Conclusions PDGFRα‐CreER expression is restricted to the JZ and CP of mouse placentas. PDGFRα‐CreER mice provide a useful tool to conditionally knock out or overexpress a target gene in these regions of the mouse placenta.

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Hypoxia and Placental Development

Soares

Iqbal

Kozai

2017

Birth Defects Research

102

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Hemochorial placentation is orchestrated through highly regulated temporal and spatial decisions governing the fate of trophoblast stem/progenitor cells. Trophoblast cell acquisition of specializations facilitating invasion and uterine spiral artery remodeling is a labile process, sensitive to the environment, and represents a process that is vulnerable to dysmorphogenesis in pathologic states. Hypoxia is a signal guiding placental development, and molecular mechanisms directing cellular adaptations to low oxygen tension are integral to trophoblast cell differentiation and placentation. Hypoxia can also be used as an experimental tool to investigate regulatory processes controlling hemochorial placentation. These developmental processes are conserved in mouse, rat, and human placentation. Consequently, elements of these developmental events can be modeled and hypotheses tested in trophoblast stem cells and in genetically-manipulated rodents. Hypoxia is also a consequence of a failed placenta, yielding pathologies that can adversely affect maternal adjustments to pregnancy, fetal health, and susceptibility to adult disease. The capacity of the placenta for adaptation to environmental challenges highlights the importance of its plasticity in safeguarding a healthy pregnancy.

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Inactivation of maternal Hif-1α at mid-pregnancy causes placental defects and deficits in oxygen delivery to the fetal organs under hypoxic stress

Cited by 35 publications

References 51 publications

Deletion of Prl7d1 causes placental defects at mid‐pregnancy in mice

Deletion of Prl7d1 causes placental defects at mid‐pregnancy in mice

The platelet‐derived growth factor receptor alpha promoter‐directed expression of cre recombinase in mouse placenta

Hypoxia and Placental Development

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