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Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages

In motile cells, the activities of the different Rho family GTPases are spatially segregated within the cell, and during cytokinesis there is evidence that this may also be the case. But while Rho’s role as the central organizer for contractile ring assembly is well established, the role of Rac and...

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Autores principales: Pal, Debadrita, Ellis, Andrea, Sepúlveda-Ramírez, Silvia P., Salgado, Torey, Terrazas, Isabella, Reyes, Gabriela, De La Rosa, Richard, Henson, John H., Shuster, Charles B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7705106/
https://www.ncbi.nlm.nih.gov/pubmed/33282870
http://dx.doi.org/10.3389/fcell.2020.591141
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author Pal, Debadrita
Ellis, Andrea
Sepúlveda-Ramírez, Silvia P.
Salgado, Torey
Terrazas, Isabella
Reyes, Gabriela
De La Rosa, Richard
Henson, John H.
Shuster, Charles B.
author_facet Pal, Debadrita
Ellis, Andrea
Sepúlveda-Ramírez, Silvia P.
Salgado, Torey
Terrazas, Isabella
Reyes, Gabriela
De La Rosa, Richard
Henson, John H.
Shuster, Charles B.
author_sort Pal, Debadrita
collection PubMed
description In motile cells, the activities of the different Rho family GTPases are spatially segregated within the cell, and during cytokinesis there is evidence that this may also be the case. But while Rho’s role as the central organizer for contractile ring assembly is well established, the role of Rac and the branched actin networks it promotes is less well understood. To characterize the contributions of these proteins during cytokinesis, we manipulated Rac and Arp2/3 activity during mitosis and meiosis in sea urchin embryos and sea star oocytes. While neither Rac nor Arp2/3 were essential for early embryonic divisions, loss of either Rac or Arp2/3 activity resulted in polar body defects. Expression of activated Rac resulted in cytokinesis failure as early as the first division, and in oocytes, activated Rac suppressed both the Rho wave that traverses the oocyte prior to polar body extrusion as well as polar body formation itself. However, the inhibitory effect of Rac on cytokinesis, polar body formation and the Rho wave could be suppressed by effector-binding mutations or direct inhibition of Arp2/3. Together, these results suggest that Rac- and Arp2/3 mediated actin networks may directly antagonize Rho signaling, thus providing a potential mechanism to explain why Arp2/3-nucleated branched actin networks must be suppressed at the cell equator for successful cytokinesis.
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spelling pubmed-77051062020-12-03 Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages Pal, Debadrita Ellis, Andrea Sepúlveda-Ramírez, Silvia P. Salgado, Torey Terrazas, Isabella Reyes, Gabriela De La Rosa, Richard Henson, John H. Shuster, Charles B. Front Cell Dev Biol Cell and Developmental Biology In motile cells, the activities of the different Rho family GTPases are spatially segregated within the cell, and during cytokinesis there is evidence that this may also be the case. But while Rho’s role as the central organizer for contractile ring assembly is well established, the role of Rac and the branched actin networks it promotes is less well understood. To characterize the contributions of these proteins during cytokinesis, we manipulated Rac and Arp2/3 activity during mitosis and meiosis in sea urchin embryos and sea star oocytes. While neither Rac nor Arp2/3 were essential for early embryonic divisions, loss of either Rac or Arp2/3 activity resulted in polar body defects. Expression of activated Rac resulted in cytokinesis failure as early as the first division, and in oocytes, activated Rac suppressed both the Rho wave that traverses the oocyte prior to polar body extrusion as well as polar body formation itself. However, the inhibitory effect of Rac on cytokinesis, polar body formation and the Rho wave could be suppressed by effector-binding mutations or direct inhibition of Arp2/3. Together, these results suggest that Rac- and Arp2/3 mediated actin networks may directly antagonize Rho signaling, thus providing a potential mechanism to explain why Arp2/3-nucleated branched actin networks must be suppressed at the cell equator for successful cytokinesis. Frontiers Media S.A. 2020-11-17 /pmc/articles/PMC7705106/ /pubmed/33282870 http://dx.doi.org/10.3389/fcell.2020.591141 Text en Copyright © 2020 Pal, Ellis, Sepúlveda-Ramírez, Salgado, Terrazas, Reyes, De La Rosa, Henson and Shuster. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cell and Developmental Biology
Pal, Debadrita
Ellis, Andrea
Sepúlveda-Ramírez, Silvia P.
Salgado, Torey
Terrazas, Isabella
Reyes, Gabriela
De La Rosa, Richard
Henson, John H.
Shuster, Charles B.
Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages
title Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages
title_full Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages
title_fullStr Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages
title_full_unstemmed Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages
title_short Rac and Arp2/3-Nucleated Actin Networks Antagonize Rho During Mitotic and Meiotic Cleavages
title_sort rac and arp2/3-nucleated actin networks antagonize rho during mitotic and meiotic cleavages
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7705106/
https://www.ncbi.nlm.nih.gov/pubmed/33282870
http://dx.doi.org/10.3389/fcell.2020.591141
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