Uterine Msx-1 and Wnt4 Signaling Becomes Aberrant in Mice with the Loss of Leukemia Inhibitory Factor or Hoxa-10: Evidence for a Novel Cytokine-Homeobox-Wnt Signaling in Implantation

Author:

Daikoku Takiko1,Song Haengseok1,Guo Yong1,Riesewijk Anne2,Mosselman Sietse2,Das Sanjoy K.1,Dey Sudhansu K.13

Affiliation:

1. Departments of Pediatrics (T.D., H.S., Y.G., S.K.Da., S.K.De.), Nashville, Tennessee 37232

2. Target Discovery and Department of Pharmacology (A.R., S.M.), NV Organon, 5340 BH Oss, The Netherlands

3. Cell and Developmental Biology and Pharmacology (S.K.De.), Vanderbilt University Medical Center, Nashville, Tennessee 37232

Abstract

AbstractSuccessful implantation absolutely depends on the reciprocal interaction between the implantation-competent blastocyst and the receptive uterus. Expression and gene targeting studies have shown that leukemia inhibitory factor (LIF), a cytokine of the IL-6 family, and Hoxa-10, an abdominalB-like homeobox gene, are crucial to implantation and decidualization in mice. Using these mutant mice, we sought to determine the importance of Msx-1 (another homeobox gene formerly known as Hox-7.1) and of Wnt4 (a ligand of the Wnt family) signaling in implantation because of their reported functions during development. We observed that Msx-1, Wnt4, and a Wnt antagonist sFRP4 are differentially expressed in the mouse uterus during the periimplantation period, suggesting their role in implantation. In addition, we observed an aberrant uterine expression of Msx-1 and sFRP4 in Lif mutant mice, and of Wnt4 and sFRP4 in Hoxa-10 mutant mice, further reinforcing the importance of these signaling pathways in implantation. Collectively, the present results provide evidence for a novel cytokine-homeotic-Wnt signaling network in implantation.

Publisher

The Endocrine Society

Subject

Endocrinology,Molecular Biology,General Medicine

Reference43 articles.

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4. Paracrine induction of stem cell renewal by LIF-deficient cells: a new ES cell regulatory pathway.;Dani;Dev Biol,1998

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