Identification of monoclonal nonspecific suppressor factor beta (mNSFβ) as one of the genes differentially expressed at implantation sites compared to interimplantation sites in the mouse uterus
Identifieur interne : 003736 ( Main/Exploration ); précédent : 003735; suivant : 003737Identification of monoclonal nonspecific suppressor factor beta (mNSFβ) as one of the genes differentially expressed at implantation sites compared to interimplantation sites in the mouse uterus
Auteurs : Gui-Ying Nie [Australie] ; Ying Li [Australie] ; Anne L. Hampton [Australie] ; Lois A. Salamonsen [Australie] ; Judith A. Clements [Australie] ; Jock K. Findlay [Australie]Source :
- Molecular Reproduction and Development [ 1040-452X ] ; 2000-04.
English descriptors
- Teeft :
- Additional animals, Blastocyst, Boehringer mannheim, Candidate bands, Cdna, Cdna fragment, Cdna library, Cdna sequence, Cdna sequences, Cell immunol nakamura, Clone, Cytokine, Ddpcr, Ddpcr analysis, Desmin, Differential display, Differentially, Early pregnancy, Embryo, False positives, Gapdh, Gapdh probe, Immune, Immune response, Immune system, Immunol, Implantation, Implantation sites, Interimplantation, Interimplantation sites, Liang, Lower panel, Mnsf, Monoclonal, Monoclonal suppressor factor, Monoclonal suppressor factor beta, Mouse, Mouse mnsf, Mouse uterus, Mrna, Mrna expression, Mrna level, Nakamura, Nonpregnant, Nonpregnant mice, Nonpregnant uterus, Northern analysis, Northern blot analysis, Nucleotide, Pardee, Pregnancy, Pregnant mice, Pregnant uterus, Primer, Primer pair combinations, Receptive state, Receptor, Same membrane, Serial sections, Suppressor, Suppressor factor beta, Tanigawa, Uterine, Uterine tissue, Uterus, Whole uterus.
Abstract
Successful implantation requires synchronous development of and active dialogue between the maternal endometrium and the implanting blastocyst. While it is well established that appropriate maternal steroid hormones are essential for endometrial preparation for implantation, the molecular events at the actual site of implantation are still little understood. The aims of our studies were to identify genes explicitly expressed or repressed at the sites of implantation by utilising RNA differential display (DDPCR), and to establish the roles of these genes in the implantation process in a mouse model. Ten bands unique in implantation sites compared to interimplantation sites were identified by DDPCR and subsequently confirmed by Northern blotting. One of these bands contained a cDNA fragment that was highly homologous to mouse monoclonal nonspecific suppressor factor beta (MNSFβ) or Fau. The full cDNA sequence of this gene, obtained by screening a λgt11 cDNA library, was essentially the same as MNSFβ, except that it had much longer 5′ untranslated region. Interestingly, both Northern and immunohistochemical analysis showed that the expression of this gene was much lower in implantation sites compared to interimplantation sites on day 4.5 of pregnancy, when embryos first attach to the uterus and initiate implantation, and on day 5.5, when implantation has advanced. These results suggest a role for MNSF during implantation and early pregnancy, possibly through regulating the proliferation and/or differentiation of uterine stromal cells. It may also be involved in the selective production of TH2‐type cytokines in implantation sites to regulate the immune system at the maternal‐fetal interface. Mol. Reprod. Dev. 55:351–363, 2000. © 2000 Wiley‐Liss, Inc.
Url:
DOI: 10.1002/(SICI)1098-2795(200004)55:4<351::AID-MRD1>3.0.CO;2-L
Affiliations:
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While it is well established that appropriate maternal steroid hormones are essential for endometrial preparation for implantation, the molecular events at the actual site of implantation are still little understood. The aims of our studies were to identify genes explicitly expressed or repressed at the sites of implantation by utilising RNA differential display (DDPCR), and to establish the roles of these genes in the implantation process in a mouse model. Ten bands unique in implantation sites compared to interimplantation sites were identified by DDPCR and subsequently confirmed by Northern blotting. One of these bands contained a cDNA fragment that was highly homologous to mouse monoclonal nonspecific suppressor factor beta (MNSFβ) or Fau. The full cDNA sequence of this gene, obtained by screening a λgt11 cDNA library, was essentially the same as MNSFβ, except that it had much longer 5′ untranslated region. Interestingly, both Northern and immunohistochemical analysis showed that the expression of this gene was much lower in implantation sites compared to interimplantation sites on day 4.5 of pregnancy, when embryos first attach to the uterus and initiate implantation, and on day 5.5, when implantation has advanced. These results suggest a role for MNSF during implantation and early pregnancy, possibly through regulating the proliferation and/or differentiation of uterine stromal cells. It may also be involved in the selective production of TH2‐type cytokines in implantation sites to regulate the immune system at the maternal‐fetal interface. Mol. Reprod. Dev. 55:351–363, 2000. © 2000 Wiley‐Liss, Inc.</div></front></TEI><affiliations><list><country><li>Australie</li></country></list><tree><country name="Australie"><noRegion><name sortKey="Nie, Gui Ing" sort="Nie, Gui Ing" uniqKey="Nie G" first="Gui-Ying" last="Nie">Gui-Ying Nie</name></noRegion><name sortKey="Clements, Judith A" sort="Clements, Judith A" uniqKey="Clements J" first="Judith A." last="Clements">Judith A. Clements</name><name sortKey="Clements, Judith A" sort="Clements, Judith A" uniqKey="Clements J" first="Judith A." last="Clements">Judith A. Clements</name><name sortKey="Findlay, Jock K" sort="Findlay, Jock K" uniqKey="Findlay J" first="Jock K." last="Findlay">Jock K. Findlay</name><name sortKey="Hampton, Anne L" sort="Hampton, Anne L" uniqKey="Hampton A" first="Anne L." last="Hampton">Anne L. Hampton</name><name sortKey="Li, Ying" sort="Li, Ying" uniqKey="Li Y" first="Ying" last="Li">Ying Li</name><name sortKey="Nie, Gui Ing" sort="Nie, Gui Ing" uniqKey="Nie G" first="Gui-Ying" last="Nie">Gui-Ying Nie</name><name sortKey="Nie, Gui Ing" sort="Nie, Gui Ing" uniqKey="Nie G" first="Gui-Ying" last="Nie">Gui-Ying Nie</name><name sortKey="Salamonsen, Lois A" sort="Salamonsen, Lois A" uniqKey="Salamonsen L" first="Lois A." last="Salamonsen">Lois A. Salamonsen</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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