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Cell type-specific recruitment of Drosophila Lin-7 to distinct MAGUK-based protein complexes defines novel roles for Sdt and Dlg-S97
| Autor | dc.contributor.author | Bachmann, André | |
| Autor | dc.contributor.author | Timmer, Marco | es_CL |
| Autor | dc.contributor.author | Sierralta Jara, Jimena | es_CL |
| Autor | dc.contributor.author | Pietrini, Grazia | es_CL |
| Autor | dc.contributor.author | Gundelfinger, Eckart D. | es_CL |
| Autor | dc.contributor.author | Knust, Elisabeth | es_CL |
| Autor | dc.contributor.author | Thomas, Ulrich | es_CL |
| Fecha ingreso | dc.date.accessioned | 2007-04-18T13:24:06Z | |
| Fecha disponible | dc.date.available | 2007-04-18T13:24:06Z | |
| Fecha de publicación | dc.date.issued | 2004-04-15 | |
| Cita de ítem | dc.identifier.citation | JOURNAL OF CELL SCIENCE 117 (10): 1899-1909 APR 15 2004 | en |
| Identificador | dc.identifier.issn | 0021-9533 | |
| Identificador | dc.identifier.uri | https://repositorio.uchile.cl/handle/2250/127086 | |
| Resumen | dc.description.abstract | Stardust (Sdt) and Discs-Large (Dig) are membrane-associated guanylate kinases (MAGUKs) involved in the organization of supramolecular protein complexes at distinct epithelial membrane compartments in Drosophila. Loss of either Sdt or Dig affects epithelial development with severe effects on apico-basal polarity. Moreover, Dig is required for the structural and functional integrity of synaptic junctions. Recent biochemical and cell culture studies have revealed that various mammalian MAGUKs can interact with mLin-7/Veli/MALS, a small PDZ-domain protein. To substantiate these findings for their in vivo significance with regard to Sdt- and Dlg-based protein complexes, we analyzed the subcellular distribution of Drosophila Lin-7 (DLin-7) and performed genetic and biochemical assays to characterize its interaction with either of the two MAGUKs. In epithelia, Sdt mediates the recruitment of DLin-7 to the subapical region, while at larval neuromuscular junctions, a particular isoform of Dig, Dlg-S97, is required for postsynaptic localization of DLin-7. Ectopic expression of Dlg-S97 in epithelia, however, was not sufficient to induce a redistribution of DLin-7. These results imply that the recruitment of DLin7 to MAGUK-based protein complexes is defined by cell-type specific mechanisms and that DLin-7 acts downstream of Sdt in epithelia and downstream of Dig at synapses. | en |
| Idioma | dc.language.iso | en | en |
| Publicador | dc.publisher | COMPANY OF BIOLOGISTS LTD | en |
| Palabras claves | dc.subject | TUMOR-SUPPRESSOR PROTEIN | en |
| Título | dc.title | Cell type-specific recruitment of Drosophila Lin-7 to distinct MAGUK-based protein complexes defines novel roles for Sdt and Dlg-S97 | en |
| Tipo de documento | dc.type | Artículo de revista |
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