Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC

Dgp71WD/Nedd1 proteins are essential for mitotic spindle formation. In human cells, Nedd1 targets γ-tubulin to both centrosomes and spindles, but in other organisms the function of Dgp71WD/Nedd1 is less clear. In Drosophila cells, Dgp71WD plays a major part in targeting γ-tubulin to spindles, but no...

Descripción completa

Detalles Bibliográficos
Autores principales: Reschen, Richard F., Colombie, Nathalie, Wheatley, Lucy, Dobbelaere, Jeroen, St Johnston, Daniel, Ohkura, Hiro, Raff, Jordan W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3507215/
https://www.ncbi.nlm.nih.gov/pubmed/23213433
http://dx.doi.org/10.1242/bio.2012596
_version_ 1782251041178255360
author Reschen, Richard F.
Colombie, Nathalie
Wheatley, Lucy
Dobbelaere, Jeroen
St Johnston, Daniel
Ohkura, Hiro
Raff, Jordan W.
author_facet Reschen, Richard F.
Colombie, Nathalie
Wheatley, Lucy
Dobbelaere, Jeroen
St Johnston, Daniel
Ohkura, Hiro
Raff, Jordan W.
author_sort Reschen, Richard F.
collection PubMed
description Dgp71WD/Nedd1 proteins are essential for mitotic spindle formation. In human cells, Nedd1 targets γ-tubulin to both centrosomes and spindles, but in other organisms the function of Dgp71WD/Nedd1 is less clear. In Drosophila cells, Dgp71WD plays a major part in targeting γ-tubulin to spindles, but not centrosomes, while in Xenopus egg extracts, Nedd1 acts as a more general microtubule (MT) organiser that can function independently of γ-tubulin. The interpretation of these studies, however, is complicated by the fact that some residual Dgp71WD/Nedd1 is likely present in the cells/extracts analysed. Here we generate a Dgp71WD null mutant lacking all but the last 12 nucleotides of coding sequence. The complete loss of Dgp71WD has no quantifiable effect on γ-tubulin or Centrosomin recruitment to the centrosome in larval brain cells. The recruitment of γ-tubulin to spindle MTs, however, is severely impaired, and spindle MT density is reduced in a manner that is indistinguishable from cells lacking Augmin or γ-TuRC function. In contrast, the absence of Dgp71WD leads to defects in the assembly of the acentrosomal female Meiosis I spindle that are more severe than those seen in Augmin or γ-TuRC mutants, indicating that Dgp71WD has additional functions that are independent of these complexes in oocytes. Moreover, the localisation of bicoid RNA during oogenesis, which requires γ-TuRC function, is unperturbed in Dgp71WD(120) mutants. Thus, Dgp71WD is not simply a general cofactor required for γ-TuRC and/or Augmin targeting, and it appears to have a crucial role independent of these complexes in the acentrosomal Meiosis I spindle.
format Online
Article
Text
id pubmed-3507215
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher The Company of Biologists
record_format MEDLINE/PubMed
spelling pubmed-35072152012-12-04 Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC Reschen, Richard F. Colombie, Nathalie Wheatley, Lucy Dobbelaere, Jeroen St Johnston, Daniel Ohkura, Hiro Raff, Jordan W. Biol Open Research Article Dgp71WD/Nedd1 proteins are essential for mitotic spindle formation. In human cells, Nedd1 targets γ-tubulin to both centrosomes and spindles, but in other organisms the function of Dgp71WD/Nedd1 is less clear. In Drosophila cells, Dgp71WD plays a major part in targeting γ-tubulin to spindles, but not centrosomes, while in Xenopus egg extracts, Nedd1 acts as a more general microtubule (MT) organiser that can function independently of γ-tubulin. The interpretation of these studies, however, is complicated by the fact that some residual Dgp71WD/Nedd1 is likely present in the cells/extracts analysed. Here we generate a Dgp71WD null mutant lacking all but the last 12 nucleotides of coding sequence. The complete loss of Dgp71WD has no quantifiable effect on γ-tubulin or Centrosomin recruitment to the centrosome in larval brain cells. The recruitment of γ-tubulin to spindle MTs, however, is severely impaired, and spindle MT density is reduced in a manner that is indistinguishable from cells lacking Augmin or γ-TuRC function. In contrast, the absence of Dgp71WD leads to defects in the assembly of the acentrosomal female Meiosis I spindle that are more severe than those seen in Augmin or γ-TuRC mutants, indicating that Dgp71WD has additional functions that are independent of these complexes in oocytes. Moreover, the localisation of bicoid RNA during oogenesis, which requires γ-TuRC function, is unperturbed in Dgp71WD(120) mutants. Thus, Dgp71WD is not simply a general cofactor required for γ-TuRC and/or Augmin targeting, and it appears to have a crucial role independent of these complexes in the acentrosomal Meiosis I spindle. The Company of Biologists 2012-03-06 /pmc/articles/PMC3507215/ /pubmed/23213433 http://dx.doi.org/10.1242/bio.2012596 Text en © 2012. Published by The Company of Biologists Ltd http://creativecommons.org/licenses/by-nc-sa/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial Share Alike License (http://creativecommons.org/licenses/by-nc-sa/3.0/).
spellingShingle Research Article
Reschen, Richard F.
Colombie, Nathalie
Wheatley, Lucy
Dobbelaere, Jeroen
St Johnston, Daniel
Ohkura, Hiro
Raff, Jordan W.
Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC
title Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC
title_full Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC
title_fullStr Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC
title_full_unstemmed Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC
title_short Dgp71WD is required for the assembly of the acentrosomal Meiosis I spindle, and is not a general targeting factor for the γ-TuRC
title_sort dgp71wd is required for the assembly of the acentrosomal meiosis i spindle, and is not a general targeting factor for the γ-turc
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3507215/
https://www.ncbi.nlm.nih.gov/pubmed/23213433
http://dx.doi.org/10.1242/bio.2012596
work_keys_str_mv AT reschenrichardf dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc
AT colombienathalie dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc
AT wheatleylucy dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc
AT dobbelaerejeroen dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc
AT stjohnstondaniel dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc
AT ohkurahiro dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc
AT raffjordanw dgp71wdisrequiredfortheassemblyoftheacentrosomalmeiosisispindleandisnotageneraltargetingfactorforthegturc

Ejemplares similares