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  • 1
    ISSN: 1432-0878
    Keywords: Key words Adhering junctions ; Desmosomes ; Endothelial junctions ; Plaque proteins ; Desmoplakin ; Cadherins ; Protein ZO-1 ; Rat ; cell culture
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology , Medicine
    Notes: Abstract  Two major types of plaque-bearing adhering junctions are commonly distinguished: the actin microfilament-anchoring adhaerens junctions (AJs) and the desmosomes anchoring intermediate-sized filaments (IFs). Both types of junction usually possess the common plaque protein, plakoglobin, whereas the other plaque proteins and the transmembrane cadherins are mutually exclusive. For example, AJs contain E-, N-, or P-cadherin in combination with α- and β-catenin, vinculin and α-actinin, whereas in desmosomes, desmogleins and desmocollins are associated with desmoplakin and one or several of the plakophilins (PP1–3). Here we describe a novel type of adhering junction comprising proteins of both AJs and desmosomes and the tight junction (TJ) plaque protein, ZO-1, in a newly established, liver-derived tumorigenic rat cell line (RMEC-1). By immunofluorescence microscopy, cell-cell contacts are characterized by mostly continuous-appearing lines which are usually resolved by electron microscopy as extended arrays of closely spaced small plaque subunits. These plaque-covered regions are positive for plakoglobin, α- and β-catenin, the arm-repeat protein p120, vinculin, desmoplakin and protein ZO-1. They are positive for E-cadherin in cultures early on in passaging, but tend to turn negative for all known cadherins in densely grown cultures. On immunoblotting SDS-PAGE-separated proteins from dense-grown cell monolayers, “pan-cadherin” antibodies have reacted with a band at ∼140 kDa, identified as N-cadherin by peptide fingerprinting of the immunoprecipitated protein, which for reasons not yet clear is modified or masked in immunolocalization experiments. The exact histological derivation of RMEC-1 cells is not known. However, the observations of several endothelial markers and the fact that all cells are rich in IFs containing vimentin and/or desmin, while only subpopulations also reveal IFs containing CKs 8 and 18, is suggestive of a mesenchymal, probably endothelial origin. We discuss the molecular relationship of this novel type of extended junction with other types of adhering junctions.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 0016-7835
    Keywords: Key words Variscan fold belt ; Armorica ; Avalonia ; Palaeomagnetism ; Palaeogeography
    Source: Springer Online Journal Archives 1860-2000
    Topics: Geosciences
    Notes: Abstract  The Variscan fold belt of Europe resulted from the collision of Africa, Baltica, Laurentia and the intervening microplates in early Paleozoic times. Over the past few years, many geological, palaeobiogeographic and palaeomagnetic studies have led to significant improvements in our understanding of this orogenic belt. Whereas it is now fairly well established that Avalonia drifted from the northern margin of Gondwana in Early Ordovician times and collided with Baltica in the late Ordovician/early Silurian, the nature of the Gondwana derived Armorican microplate is more enigmatic. Geological and new palaeomagnetic data suggest Armorica comprises an assemblage of terranes or microblocks. Palaeobiogeographic data indicate that these terranes had similar drift histories, and the Rheic Ocean separating Avalonia from the Armorican Terrane Assemblage closed in late Silurian/early Devonian times. An early to mid Devonian phase of extensional tectonics along this suture zone resulted in formation of the relatively narrow Rhenohercynian basin which closed progressively between the late Devonian and early Carboniferous. In this contribution, we review the constraints provided by palaeomagnetic data, compare these with geological and palaeobiogeographic evidence, and present a sequence of palaeogeographic reconstructions for these circum-Atlantic plates and microplates from Ordovician through to Devonian times.
    Type of Medium: Electronic Resource
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