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Publication : Cx31 and Cx43 double-deficient mice reveal independent functions in murine placental and skin development.

First Author  Kibschull M Year  2005
Journal  Dev Dyn Volume  233
Issue  3 Pages  853-63
PubMed ID  15895417 Mgi Jnum  J:98807
Mgi Id  MGI:3579961 Doi  10.1002/dvdy.20424
Citation  Kibschull M, et al. (2005) Cx31 and Cx43 double-deficient mice reveal independent functions in murine placental and skin development. Dev Dyn 233(3):853-863
abstractText  The overlapping expression of gap junctional connexins in tissues has indicated that the channels may compensate for each other. During development, Cx31 and Cx43 are coexpressed in preimplantation embryos, in the spongiotrophoblast of the placenta and in the epidermis. This study shows that Cx31/Cx43 double-deficient mice exhibit the known phenotypes of the single-knockout strains but no combined effects. Thus, Cx43, coexpressed with Cx31 at midgestation in the spongiotrophoblast of the placenta, cannot be responsible for a partial rescue of the lethal Cx31 knockout phenotype, as assumed before (Plum et al. [ 2001] Dev Biol 231:334-337). It follows that both connexins have unique functions in placental development. Despite an altered expression of other epidermal connexin mRNAs, epidermal differentiation and physiology was unaltered by the absence of Cx31 and Cx43. Therefore, in epidermal and preimplantation development, gap junctional communication can probably be compensated by other isoforms coexpressed with Cx31 and Cx43. Developmental Dynamics 233:853-863, 2005. (c) 2005 Wiley-Liss, Inc.
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