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Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes

The focusing of microtubules into mitotic spindle poles in vertebrate somatic cells has been assumed to be the consequence of their nucleation from centrosomes. Contrary to this simple view, in this article we show that an antibody recognizing the light intermediate chain of cytoplasmic dynein (70.1...

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Detalles Bibliográficos
Autores principales: Gaglio, Tirso, Dionne, Mary A., Compton, Duane A.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1997
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2136753/
https://www.ncbi.nlm.nih.gov/pubmed/9281583
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author Gaglio, Tirso
Dionne, Mary A.
Compton, Duane A.
author_facet Gaglio, Tirso
Dionne, Mary A.
Compton, Duane A.
author_sort Gaglio, Tirso
collection PubMed
description The focusing of microtubules into mitotic spindle poles in vertebrate somatic cells has been assumed to be the consequence of their nucleation from centrosomes. Contrary to this simple view, in this article we show that an antibody recognizing the light intermediate chain of cytoplasmic dynein (70.1) disrupts both the focused organization of microtubule minus ends and the localization of the nuclear mitotic apparatus protein at spindle poles when injected into cultured cells during metaphase, despite the presence of centrosomes. Examination of the effects of this dynein-specific antibody both in vitro using a cell-free system for mitotic aster assembly and in vivo after injection into cultured cells reveals that in addition to its direct effect on cytoplasmic dynein this antibody reduces the efficiency with which dynactin associates with microtubules, indicating that the antibody perturbs the cooperative binding of dynein and dynactin to microtubules during spindle/aster assembly. These results indicate that microtubule minus ends are focused into spindle poles in vertebrate somatic cells through a mechanism that involves contributions from both centrosomes and structural and microtubule motor proteins. Furthermore, these findings, together with the recent observation that cytoplasmic dynein is required for the formation and maintenance of acentrosomal spindle poles in extracts prepared from Xenopus eggs (Heald, R., R. Tournebize, T. Blank, R. Sandaltzopoulos, P. Becker, A. Hyman, and E. Karsenti. 1996. Nature (Lond.). 382: 420–425) demonstrate that there is a common mechanism for focusing free microtubule minus ends in both centrosomal and acentrosomal spindles. We discuss these observations in the context of a search-capture-focus model for spindle assembly.
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spelling pubmed-21367532008-05-01 Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes Gaglio, Tirso Dionne, Mary A. Compton, Duane A. J Cell Biol Article The focusing of microtubules into mitotic spindle poles in vertebrate somatic cells has been assumed to be the consequence of their nucleation from centrosomes. Contrary to this simple view, in this article we show that an antibody recognizing the light intermediate chain of cytoplasmic dynein (70.1) disrupts both the focused organization of microtubule minus ends and the localization of the nuclear mitotic apparatus protein at spindle poles when injected into cultured cells during metaphase, despite the presence of centrosomes. Examination of the effects of this dynein-specific antibody both in vitro using a cell-free system for mitotic aster assembly and in vivo after injection into cultured cells reveals that in addition to its direct effect on cytoplasmic dynein this antibody reduces the efficiency with which dynactin associates with microtubules, indicating that the antibody perturbs the cooperative binding of dynein and dynactin to microtubules during spindle/aster assembly. These results indicate that microtubule minus ends are focused into spindle poles in vertebrate somatic cells through a mechanism that involves contributions from both centrosomes and structural and microtubule motor proteins. Furthermore, these findings, together with the recent observation that cytoplasmic dynein is required for the formation and maintenance of acentrosomal spindle poles in extracts prepared from Xenopus eggs (Heald, R., R. Tournebize, T. Blank, R. Sandaltzopoulos, P. Becker, A. Hyman, and E. Karsenti. 1996. Nature (Lond.). 382: 420–425) demonstrate that there is a common mechanism for focusing free microtubule minus ends in both centrosomal and acentrosomal spindles. We discuss these observations in the context of a search-capture-focus model for spindle assembly. The Rockefeller University Press 1997-09-08 /pmc/articles/PMC2136753/ /pubmed/9281583 Text en This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Gaglio, Tirso
Dionne, Mary A.
Compton, Duane A.
Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes
title Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes
title_full Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes
title_fullStr Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes
title_full_unstemmed Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes
title_short Mitotic Spindle Poles are Organized by Structural and Motor Proteins in Addition to Centrosomes
title_sort mitotic spindle poles are organized by structural and motor proteins in addition to centrosomes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2136753/
https://www.ncbi.nlm.nih.gov/pubmed/9281583
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