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Literature DB >> 1353982

Expression and modification of Hox 2.1 protein in mouse embryos.

N A Wall¹, C M Jones, B L Hogan, C V Wright.

Abstract

A polyclonal antibody, alpha Hox 2.1a, has been generated and used to immunolocalize Hox 2.1 protein in mouse embryos. Protein is present in nuclei of all tissues previously shown to express Hox 2.1 RNA. In addition, protein is seen in somites and proximal regions of the limb buds, tissues in which Hox 2.1 RNA expression was not clearly detected previously by in situ hybridization. At the 7 somite stage, protein is detectable in the neural tube up to the level of somite 1, but later retracts to a more posterior position. Immunoblot, in vitro translation, and immunoprecipitation experiments were carried out to characterize the Hox 2.1 protein. The results show that the Hox 2.1 gene produces at least two related phosphorylated proteins present in different proportions in different tissues.

Entities: Gene Species

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Year: 1992 PMID： 1353982 DOI： 10.1016/0925-4773(92)90073-s

Source DB: PubMed Journal: Mech Dev ISSN： 0925-4773 Impact factor: 1.882

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Cited

20 in total

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Expression and modification of Hox 2.1 protein in mouse embryos.

1. HoxB5 is an upstream transcriptional switch for differentiation of the vascular endothelium from precursor cells.

Review 2. Hox genes in the lung.

3. Null mutation of mCOUP-TFI results in defects in morphogenesis of the glossopharyngeal ganglion, axonal projection, and arborization.

4. Nav2 is necessary for cranial nerve development and blood pressure regulation.

5. A novel PF/PN motif inhibits nuclear localization and DNA binding activity of the ESX1 homeoprotein.

6. Embryonic gut anomalies in a mouse model of retinoic Acid-induced caudal regression syndrome: delayed gut looping, rudimentary cecum, and anorectal anomalies.

7. Neural crest stem cell multipotency requires Foxd3 to maintain neural potential and repress mesenchymal fates.

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9. Requirement for Foxd3 in the maintenance of neural crest progenitors.

10. Loss of the Sall3 gene leads to palate deficiency, abnormalities in cranial nerves, and perinatal lethality.