Literature DB >> 24571987

A murine uterine transcriptome, responsive to steroid receptor coactivator-2, reveals transcription factor 23 as essential for decidualization of human endometrial stromal cells.

Ramakrishna Kommagani1, Maria M Szwarc, Ertug Kovanci, Chad J Creighton, Bert W O'Malley, Francesco J Demayo, John P Lydon.   

Abstract

Recent data from human and mouse studies strongly support an indispensable role for steroid receptor coactivator-2 (SRC-2)-a member of the p160/SRC family of coregulators-in progesterone-dependent endometrial stromal cell decidualization, an essential cellular transformation process that regulates invasion of the developing embryo into the maternal compartment. To identify the key progesterone-induced transcriptional changes that are dependent on SRC-2 and required for endometrial decidualization, we performed comparative genome-wide transcriptional profiling of endometrial tissue RNA from ovariectomized SRC-2(flox/flox) (SRC-2(f/f) [control]) and PR(cre/+)/SRC-2(flox/flox) (SRC-2(d/d) [SRC-2-depleted]) mice, acutely treated with vehicle or progesterone. Although data mining revealed that only a small subset of the total progesterone-dependent transcriptional changes is dependent on SRC-2 (∼13%), key genes previously reported to mediate progesterone-driven endometrial stromal cell decidualization are present within this subset. Along with providing a more detailed molecular portrait of the decidual transcriptional program governed by SRC-2, the degree of functional diversity of these progesterone mediators underscores the pleiotropic regulatory role of SRC-2 in this tissue. To showcase the utility of this powerful informational resource to uncover novel signaling paradigms, we stratified the total SRC-2-dependent subset of progesterone-induced transcriptional changes in terms of novel gene expression and identified transcription factor 23 (Tcf23), a basic-helix-loop-helix transcription factor, as a new progesterone-induced target gene that requires SRC-2 for full induction. Importantly, using primary human endometrial stromal cells in culture, we demonstrate that TCF23 function is essential for progesterone-dependent decidualization, providing crucial translational support for this transcription factor as a new decidual mediator of progesterone action.

Entities:  

Keywords:  decidualization; endometrium; human; microarray; mouse; progesterone; steroid receptor coactivator-2; transcription factor 23

Mesh:

Substances:

Year:  2014        PMID: 24571987      PMCID: PMC4076383          DOI: 10.1095/biolreprod.114.117531

Source DB:  PubMed          Journal:  Biol Reprod        ISSN: 0006-3363            Impact factor:   4.285


  50 in total

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5.  Genomic organization and chromosomal mapping of the basic helix-loop-helix factor OUT (Tcf23/TCF23).

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Journal:  Cytogenet Cell Genet       Date:  2001

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Review 7.  Normal and cancer-related functions of the p160 steroid receptor co-activator (SRC) family.

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Review 8.  Decidualization of the human endometrium: mechanisms, functions, and clinical perspectives.

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10.  Amphiregulin is an implantation-specific and progesterone-regulated gene in the mouse uterus.

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3.  Neonatal Progesterone Programs Adult Uterine Responses to Progesterone and Susceptibility to Uterine Dysfunction.

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4.  The Flavonoid Baicalein Negatively Regulates Progesterone Target Genes in the Uterus in Vivo.

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5.  Uterine function in the mouse requires speckle-type poz protein.

Authors:  Lan Hai; Maria M Szwarc; Bin He; David M Lonard; Ramakrishna Kommagani; Francesco J DeMayo; John P Lydon
Journal:  Biol Reprod       Date:  2018-06-01       Impact factor: 4.285

Review 6.  Emerging roles of steroid receptor coactivators in stromal cell responses.

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7.  Deletion of Arid1a in Reproductive Tract Mesenchymal Cells Reduces Fertility in Female Mice.

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8.  The Promyelocytic Leukemia Zinc Finger Transcription Factor Is Critical for Human Endometrial Stromal Cell Decidualization.

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  9 in total

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