427 research outputs found

    Quality design, construction and development enterprises: Exploring the model and marketing strategies for integration

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    Quality Design Construction and Development (QDCD) firms, provide an alternative to the outsourcing trends in construction - competing on the added value derived from producing high-quality design - which is reinforced by the ability to further enhance value across the integrated activities. A QDCD enterprise model is developed, drawing upon several sources, including QDCD origins and scope, design-led organisational issues (structure, culture, processes), systems integration, marketing (investigating the 6 markets framework and relationship against transactional approaches). Six case studies, highlight QDCD as an advantageous market niche, where competition is minimised on the basis that all tangible and intangible routines across DCD will be coordinated to conform to the value proposition, enhancing the prospect of customer identification through design. The Key Account Manager (KAM) role can ensure coordination across DCD activities, by building on the emerging hierarchy/adhocracy cultural pattern to make strategies and routines more explicit internally. KAMs can also activate the tacit RM practices becoming more explicit, by reinforcing the relationship between the internal and external organisational interfaces, namely the organisation and the 6 markets. Finally, branding emerges as a comprehensive solution to marketing QDCDs. Then, branding and the contribution of KAMs in embedding it in the organisational context are further explored

    Regulation of Motility of Myogenic Cells in Filling Limb Muscle Anlagen by Pitx2

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    Cells of the ventrolateral dermomyotome delaminate and migrate into the limb buds where they give rise to all muscles of the limbs. The migratory cells proliferate and form myoblasts, which withdraw from the cell cycle to become terminally differentiated myocytes. The myogenic lineage colonizes pre-patterned regions to form muscle anlagen as muscle fibers are assembled. The regulatory mechanisms that control the later steps of this myogenic program are not well understood. The homeodomain transcription factor Pitx2 is expressed specifically in the muscle lineage from the migration of precursors to adult muscle. Ablation of Pitx2 results in distortion, rather than loss, of limb muscle anlagen, suggesting that its function becomes critical during the colonization of, and/or fiber assembly in, the anlagen. Microarrays were used to identify changes in gene expression in flow-sorted migratory muscle precursors, labeled by Lbx1EGFP/+, which resulted from the loss of Pitx2. Very few genes showed changes in expression. Many small-fold, yet significant, changes were observed in genes encoding cytoskeletal and adhesion proteins which play a role in cell motility. Myogenic cells from genetically-tagged mice were cultured and subjected to live cell-tracking analysis using time-lapse imaging. Myogenic cells lacking Pitx2 were smaller, more symmetrical, and had more actin bundling. They also migrated about half of the total distance and velocity. Decreased motility may prevent myogenic cells from filling pre-patterned regions of the limb bud in a timely manner. Altered shape may prevent proper assembly of higher-order fibers within anlagen. Pitx2 therefore appears to regulate muscle anlagen development by appropriately balancing expression of cytoskeletal and adhesion molecules

    Differential induction of Pax genes by NGF and BDNF in cerebellar primary cultures.

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    Wnt/Lef1 signaling acts via Pitx2 to regulate somite myogenesis

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    AbstractWnt signaling has been implicated in somite, limb, and branchial arch myogenesis but the mechanisms and roles are not clear. We now show that Wnt signaling via Lef1 acts to regulate the number of premyogenic cells in somites but does not regulate myogenic initiation in the limb bud or maintenance in the first or second branchial arch. We have also analysed the function and regulation of a putative downstream transcriptional target of canonical Wnt signaling, Pitx2. We show that loss-of-function of Pitx2 decreases the number of myogenic cells in the somite, whereas overexpression increases myocyte number particularly in the epaxial region of the myotome. Increased numbers of mitotic cells were observed following overexpression of Pitx2 or an activated form of Lef1, suggesting an effect on cell proliferation. In addition, we show that Pitx2 expression is regulated by canonical Wnt signaling in the epaxial somite and second branchial arch, but not in the limb or the first branchial arch. These results suggest that Wnt/Lef1 signaling regulates epaxial myogenesis via Pitx2 but that this link is uncoupled in other regions of the body, emphasizing the unique molecular networks that control the development of various muscles in vertebrates
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