| Literature DB >> 18481075 |
Nora Prochnow1, Rolf Dermietzel.
Abstract
Recent evidence indicates, that gap junction forming proteins do not only contribute to intercellular communication (Kanno and Saffitz in Cardiovasc Pathol 10:169-177, 2001; Saez et al. in Physiol Rev 83:1359-1400, 2003), ion homeostasis and volume control (Goldberg et al. in J Biol Chem 277:36725-36730, 2002; Saez et al. in Physiol Rev 83:1359-1400, 2003). They also serve biological functions in a mechanical sense, supporting adherent connections between neighbouring cells of epithelial and non-epithelial tissues (Clair et al. in Exp Cell Res 314:1250-1265, 2008; Shaw et al. in Cell 128:547-560, 2007), where they stabilize migratory pathways in the developing central nervous system (Elias et al. in Nature 448:901-907, 2007; Malatesta et al. in Development 127:5253-5263, 2000; Noctor et al. in Nature 409:714-720, 2001; Rakic in Brain Res 33:471-476, 1971; J Comp Neurol 145:61-83 1972; Science 241:170-176, 1988), or mediate polarized movements and directionality of neural crest cells during organogenesis (Kirby and Waldo in Circ Res 77:211-215, 1995; Xu et al. in Development 133:3629-3639, 2006). Since, most data describing adhesive properties of gap junctions delt with connexin 43 (Cx43) (Beardslee et al. in Circ Res 83:629-635, 1998), we will focus our brief review on this isoform.Entities:
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Year: 2008 PMID: 18481075 PMCID: PMC2413113 DOI: 10.1007/s00418-008-0434-7
Source DB: PubMed Journal: Histochem Cell Biol ISSN: 0948-6143 Impact factor: 4.304
Fig. 1General structure of a gap junction plaque. Gap junctions are formed by paired hemichannels (connexons) of two adjacent cells. A single connexon is made by a polymer of six connexins. Only apposed connexons allow intercellular transfer of ions (ionic coupling) and small metabolites (metabolic coupling). Unapposed connexons seem to perform per se functions
Fig. 2a shows cultured cardiomyocytes immunolabelled with an anti-Cx43 antibody (red). Immunolabelling is prevalent in apposed cell membranes, but also in some unapposed domains. Nuclei are counterstained with Hoechst dye. b Immunolabelling of heart tissue with Cx43 antibody. Intercalated discs (red) are intensivley stained. Bar indicates 25 μm
Fig. 3Model for microtubulus mediated delivery of vesicle-bound connexons to adherens junctions (adapted from Shaw et al. 2007). Microtubules bind via their +end to EB1. EB1 in turn binds to P150 (GLUED), a component of the dynein/dynactin complex, which interacts with β-catenin through P120-catenin with the adherens junction. This interaction is understood to tether the microtubule to the junction and to serve as a gateway for connexon delivery