Literature DB >> 12058055

Centrosome reorientation in wound-edge cells is cell type specific.

Anne-Marie C Yvon1, Jonathan W Walker, Barbara Danowski, Carey Fagerstrom, Alexey Khodjakov, Patricia Wadsworth.   

Abstract

The reorientation of the microtubule organizing center during cell migration into a wound in the monolayer was directly observed in living wound-edge cells expressing gamma-tubulin tagged with green fluorescent protein. Our results demonstrate that in CHO cells, the centrosome reorients to a position in front of the nucleus, toward the wound edge, whereas in PtK cells, the centrosome lags behind the nucleus during migration into the wound. In CHO cells, the average rate of centrosome motion was faster than that of the nucleus; the converse was true in PtK cells. In both cell lines, centrosome motion was stochastic, with periods of rapid motion interspersed with periods of slower motion. Centrosome reorientation in CHO cells required dynamic microtubules and cytoplasmic dynein/dynactin activity and could be prevented by altering cell-to-cell or cell-to-substrate adhesion. Microtubule marking experiments using photoactivation of caged tubulin demonstrate that microtubules are transported in the direction of cell motility in both cell lines but that in PtK cells, microtubules move individually, whereas their movement is more coherent in CHO cells. Our data demonstrate that centrosome reorientation is not required for directed migration and that diverse cells use distinct mechanisms for remodeling the microtubule array during directed migration.

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Year:  2002        PMID: 12058055      PMCID: PMC117610          DOI: 10.1091/mbc.01-11-0539

Source DB:  PubMed          Journal:  Mol Biol Cell        ISSN: 1059-1524            Impact factor:   4.138


  52 in total

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5.  Centrosome behavior in motile HGF-treated PtK2 cells expressing GFP-gamma tubulin.

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8.  Mechanism of centrosome positioning during the wound response in BSC-1 cells.

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10.  Actions of cytochalasins on the organization of actin filaments and microtubules in a neuronal growth cone.

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  39 in total

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4.  Tropomyosin isoform expression regulates the transition of adhesions to determine cell speed and direction.

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5.  Cellular polarity in aging: role of redox regulation and nutrition.

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Review 6.  Orientation and function of the nuclear-centrosomal axis during cell migration.

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7.  Orientation and polarity in collectively migrating cell structures: statics and dynamics.

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8.  Control of endothelial cell polarity and sprouting angiogenesis by non-centrosomal microtubules.

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Review 9.  The Golgi and the centrosome: building a functional partnership.

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10.  The centrosome neither persistently leads migration nor determines the site of axonogenesis in migrating neurons in vivo.

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