97073291999051920131121
1058-838821241998AugDevelopmental dynamics : an official publication of the American Association of AnatomistsDev DynAnterior structural defects by misexpression of Xgbx-2 in early Xenopus embryos are associated with altered expression of cell adhesion molecules.563579563-79The RNA of the noncluster homeobox gene, Xgbx-2, is localized during neurulation to a narrow band of tissue at the midbrain hindbrain boundary (anterior hindbrain). The localized expression of Xgbx-2 within the nervous system prompted us to assess its function during early development by injection of synthetic Xgbx-2 RNA into the animal pole region of both dorsal blastomeres at the four-cell stage. Injection of Xgbx-2 RNA leads to dose-dependent alterations in anterior dorsal structures. These defects include abnormal eye development including reduced and missing eyes, reduced or missing cement glands, and abnormal brain development. Additionally, coinjection with lineage label (either beta-galactosidase or green fluorescent protein) shows there is a dose-dependent misplacement of cells. These misplaced cells can be found in such locations as the blastocoele, gastrocoele, or ventricles in the brain. In some spawnings, misplaced cells are expelled from the embryo into the periviteline space. In general, the phenotype of Xgbx-2 RNA-injected embryos is strikingly similar to the phenotypes observed when dominant-negative RNA constructs of Ca2+-dependent cell-adhesion molecules are injected into similar regions of early embryos. Xgbx-2 misexpression enhanced the dissociation of animal hemisphere cells, and inhibited Ca2+-dependent cell adhesion in dissociated animal hemisphere cells in vitro. Additionally, when the expression of various calcium-dependent cadherins was tested, it was shown that misexpression of Xgbx-2 prevents N-cadherin expression during early neurulation. These observations suggest that the transcription factor, Xgbx-2, functions normally in the regionalization of the neural tube (specifically the anterior hindbrain) by regulating differential cell adhesion and subsequently cell identity.KingM WMWDepartment of Biochemistry and Molecular Biology, Terre Haute Center for Medical Education, Indiana University School of Medicine, 47809, USA. memwk@thcme.indstate.eduNdiemaMMNeffA WAWengJournal ArticleResearch Support, Non-U.S. Gov't
United StatesDev Dyn92019271058-83880Cadherins0Cell Adhesion Molecules0Gbx2 protein, Xenopus0Homeodomain Proteins0Xenopus Proteins63231-63-0RNASY7Q814VUPCalciumIMAnimalsBlastocystdrug effectsBrainabnormalitiesdrug effectsembryologyCadherinsbiosynthesisdrug effectsCalciummetabolismCell Adhesion Moleculesbiosynthesisdrug effectsEye AbnormalitiesembryologyGastruladrug effectsGene Expression Regulation, Developmentaldrug effectsphysiologyHomeodomain Proteinsbiosynthesisdrug effectsNervous Systemdrug effectsPhenotypeRNApharmacologyXenopus ProteinsXenopus laevisembryologygenetics199882621620006221001998826216ppublish970732910.1002/(SICI)1097-0177(199808)212:4<563::AID-AJA9>3.0.CO;2-F10.1002/(SICI)1097-0177(199808)212:4<563::AID-AJA9>3.0.CO;2-F