TY - JOUR
T1 - Core exosome - Independent roles for Rrp6 in cell cycle progression
AU - Graham, Amy C.
AU - Kiss, Daniel L.
AU - Andrulis, Erik D.
N1 - Copyright:
Copyright 2012 Elsevier B.V., All rights reserved.
PY - 2009/4/15
Y1 - 2009/4/15
N2 - Exosome complexes are 3′ to 5′ exoribonucleases composed of subunits that are critical for numerous distinct RNA metabolic (ribonucleometabolic) pathways. Several studies have implicated the exosome subunits Rrp6 and Dis3 in chromosome segregation and cell division but the functional relevance of these findings remains unclear. Here, we report that, in Drosophila melanogaster S2 tissue culture cells, dRrp6 is required for cell proliferation and error - free mitosis, but the core exosome subunit Rrp40 is not. Micorarray analysis of dRrp6 - depleted cell reveals increased levels of cell cycle - and mitosis - related transcripts. Depletion of dRrp6 elicits a decrease in the frequency of mitotic cells and in the mitotic marker phospho - histone H3 (pH3), with a concomitant increase in defects in chromosome congression, separation, and segregation. Endogenous dRrp6 dynamically redistributes during mitosis, accumulating predominantly but not exclusively on the condensed chromosomes. In contrast, core subunits localize predominantly to MTs throughout cell division. Finally, dRrp6 - depleted cells treated with microtubule poisons exhibit normal kinetochore recruitment of the spindle assembly checkpoint protein BubRl without restoring pH3 levels, suggesting that these cells undergo premature chromosome condensation. Collectively, these data support the idea that dRrp6 has a core exosome - independent role in cell cycle and mitotic progression.
AB - Exosome complexes are 3′ to 5′ exoribonucleases composed of subunits that are critical for numerous distinct RNA metabolic (ribonucleometabolic) pathways. Several studies have implicated the exosome subunits Rrp6 and Dis3 in chromosome segregation and cell division but the functional relevance of these findings remains unclear. Here, we report that, in Drosophila melanogaster S2 tissue culture cells, dRrp6 is required for cell proliferation and error - free mitosis, but the core exosome subunit Rrp40 is not. Micorarray analysis of dRrp6 - depleted cell reveals increased levels of cell cycle - and mitosis - related transcripts. Depletion of dRrp6 elicits a decrease in the frequency of mitotic cells and in the mitotic marker phospho - histone H3 (pH3), with a concomitant increase in defects in chromosome congression, separation, and segregation. Endogenous dRrp6 dynamically redistributes during mitosis, accumulating predominantly but not exclusively on the condensed chromosomes. In contrast, core subunits localize predominantly to MTs throughout cell division. Finally, dRrp6 - depleted cells treated with microtubule poisons exhibit normal kinetochore recruitment of the spindle assembly checkpoint protein BubRl without restoring pH3 levels, suggesting that these cells undergo premature chromosome condensation. Collectively, these data support the idea that dRrp6 has a core exosome - independent role in cell cycle and mitotic progression.
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U2 - 10.1091/mbc.E08-08-0825
DO - 10.1091/mbc.E08-08-0825
M3 - Article
C2 - 19225159
AN - SCOPUS:65349174674
SN - 1059-1524
VL - 20
SP - 2242
EP - 2253
JO - Molecular Biology of the Cell
JF - Molecular Biology of the Cell
IS - 8
ER -