Conditional Deletion of MSX Homeobox Genes in the Uterus Inhibits Blastocyst Implantation by Altering Uterine Receptivity

Daikoku, Takiko; Cha, Jeeyeon; Sun, Xiaofei; Tranguch, Susanne; Xie, Hua; Fujita, Tomoko; Hirota, Yasushi; Lydon, John P.; DeMayo, Francesco J.; Maxson, Robert E.; Dey, Sudhansu K.

doi:10.1016/j.devcel.2011.09.010

Cited by 186 publications

(270 citation statements)

References 86 publications

(94 reference statements)

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“…48,49 This timely remodeling of junction complexes under the control of ovarian steroid hormones represents a decreased epithelial apicalbasal polarity during uterine receptivity establishment. 9,11,45 In fact, previous studies have demonstrated a lack of transition of the luminal epithelium from a high to a less apical-basal polar state in the absence of uterine Msx1 and 2 genes hampers blastocyst implantation. 9 As a small GTPase, Rac1 has been found crucial in regulating cell shape and epithelial polarity.…”

Section: Discussionmentioning

confidence: 99%

“…9,11,45 In fact, previous studies have demonstrated a lack of transition of the luminal epithelium from a high to a less apical-basal polar state in the absence of uterine Msx1 and 2 genes hampers blastocyst implantation. 9 As a small GTPase, Rac1 has been found crucial in regulating cell shape and epithelial polarity. For example, Rac1 mutant lens placode cells are shorter and more apically restricted than the control cells.…”

Section: Discussionmentioning

confidence: 99%

“…For example, on day 4 morning in mice, luminal epithelial cells cease proliferation under the dominance of increasing levels of ovarian progesterone and preimplantation estrogen. Meanwhile, the epithelial cells undergo differentiation, accompanied with a dynamic junction complex remodeling and membrane maturation, leading to a decrease of epithelial polarity approaching implantation and a cell-shape transition from columnar to cubical configuration, 9 thus gradually achieving the capacity for blastocyst attachment on day 4 evening. 10 Therefore, a timely regulated epithelial membrane maturation and precisely maintained epithelial integrity is critical for embryo implantation.…”

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confidence: 99%

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Uterine RAC1 via Pak1-ERM signaling directs normal luminal epithelial integrity conducive to on-time embryo implantation in mice

Wang

Cui

et al. 2015

Cell Death Differ

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Successful embryo implantation requires functional luminal epithelia to establish uterine receptivity and blastocyst-uterine adhesion. During the configuration of uterine receptivity from prereceptive phase, the luminal epithelium undergoes dynamic membrane reorganization and depolarization. This timely regulated epithelial membrane maturation and precisely maintained epithelial integrity are critical for embryo implantation in both humans and mice. However, it remained largely unexplored with respect to potential signaling cascades governing this functional epithelial transformation prior to implantation. Using multiple genetic and cellular approaches combined with uterine conditional Rac1 deletion mouse model, we demonstrated herein that Rac1, a small GTPase, is spatiotemporally expressed in the periimplantation uterus, and uterine depletion of Rac1 induces premature decrease of epithelial apical-basal polarity and defective junction remodeling, leading to disrupted uterine receptivity and implantation failure. Further investigations identified Pak1-ERM as a downstream signaling cascade upon Rac1 activation in the luminal epithelium necessary for uterine receptivity. In addition, we also demonstrated that Rac1 via P38 MAPK signaling ensures timely epithelial apoptotic death at postimplantation. Besides uncovering a potentially important molecule machinery governing uterine luminal integrity for embryo implantation, our finding has high clinical relevance, because Rac1 is essential for normal endometrial functions in women. The implantation of the blastocyst into the maternal uterus is a crucial step in establishing pregnancy and thus ensuring further embryonic development. 1-3 Similar to many developmental processes, implantation involves an intricate succession of molecular and cellular interactions which must be executed within an optimal time frame. During this period, the acquisition of blastocyst implantation competency is synchronized with the establishment of uterine receptivity. [4][5][6] On the basis of previous findings, uterine sensitivity to implantationcompetent blastocysts is classically divided into three stages: pre-receptive, receptive and refractory phases. 7 In mice, prior to day 4 of pregnancy, the uterus is conventionally considered as the pre-receptive phase. On day 4 and beyond, the uterus becomes fully receptive following the priming actions of ovarian progesterone and preimplantation estrogen; whereas by late day 5, the uterus becomes refractory to initiate the implantation. 2,4,8 Upon entering the receptive phase, uterine luminal epithelium undergoes dynamic transformation. For example, on day 4 morning in mice, luminal epithelial cells cease proliferation under the dominance of increasing levels of ovarian progesterone and preimplantation estrogen. Meanwhile, the epithelial cells undergo differentiation, accompanied with a dynamic junction complex remodeling and membrane maturation, leading to a decrease of epithelial polarity approaching implantation and a cell-shape transition from...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Uterine RAC1 via Pak1-ERM signaling directs normal luminal epithelial integrity conducive to on-time embryo implantation in mice

Wang

Cui

et al. 2015

Cell Death Differ

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“…Recently, MSX homeobox genes are reported to be essential transcriptional regulators which morphologically modulate luminal epithelium and control normal implantation in mice [17]. Uterine deletion of both Msx1 and Msx2 completely inhibits blastocyst implantation [17].…”

Section: Leukemia Inhibitory Factormentioning

confidence: 99%

“…Uterine deletion of both Msx1 and Msx2 completely inhibits blastocyst implantation [17]. LIF reduces uterine Msx1 expression and deficiency of Msx1/2 reduces LIF expression [17].…”

Section: Leukemia Inhibitory Factormentioning

confidence: 99%

Uterine receptivity and embryo–uterine interactions in embryo implantation: lessons from mice

Egashira

Hirota

2013

Reprod Medicine & Biology

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Implantation is a process of the first fetomaternal encounter in the uterus. A competent blastocyst and a receptive uterus are critical for successful implantation. For an acquisition of uterine receptivity, the following conditions need to be satisfied in the uterine environments: the endometrial preparation with stromal proliferation and epithelial differentiation in the prereceptive phase and proper interactions between the uterus and blastocyst later in the phase. Focusing on these points and primarily referring to the mouse in vivo evidence, this review article has shown detailed molecular mechanisms for successful implantation.

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Homeobox genes for embryo implantation: From mouse to human

Kong

et al. 2018

Anim Models and Exp Med

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The proper development of uterus to a state of receptivity and the attainment of implantation competency for blastocyst are 2 indispensable aspects for implantation, which is considered to be a critical event for successful pregnancy. Like many developmental processes, a large number of transcription factors, such as homeobox genes, have been shown to orchestrate this complicated but highly organized physiological process during implantation. In this review, we focus on progress in studies Homeobox genes are a family of regulatory genes coding for specific nuclear proteins that act as transcription factors.6,7 They are characterized by sharing a homeobox sequence, a highly conserved 183-nucleotide sequence that encodes a 61-amino-acid domain, termed the homeodomain (HD), which is responsible for the recognition and binding of sequence-specific DNA motifs.8,9

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Conditional Deletion of MSX Homeobox Genes in the Uterus Inhibits Blastocyst Implantation by Altering Uterine Receptivity

Cited by 186 publications

References 86 publications

Uterine RAC1 via Pak1-ERM signaling directs normal luminal epithelial integrity conducive to on-time embryo implantation in mice

Uterine RAC1 via Pak1-ERM signaling directs normal luminal epithelial integrity conducive to on-time embryo implantation in mice

Uterine receptivity and embryo–uterine interactions in embryo implantation: lessons from mice

Homeobox genes for embryo implantation: From mouse to human

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