GW182 is critical for the stability of GW bodies expressed during the cell cycle and cell proliferation

doi:10.1242/jcs.01477

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JCS ePress online publication date 19 Oct 2004
doi: 10.1242/jcs.01477

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Research Article

GW182 is critical for the stability of GW bodies expressed during the cell cycle and cell proliferation

Zheng Yang, Andrew Jakymiw, Malcolm R. Wood, Theophany Eystathioy, Robert L. Rubin, Marvin J. Fritzler, and Edward K.L. Chan^*
^* Author for correspondence (e-mail: echan{at}ufl.edu)

A novel cytoplasmic compartment referred to as GW bodies wasinitially identified using human autoantibodies to a 182 kDaprotein named GW182. GW bodies are small, generally spherical,cytoplasmic domains that vary in number and size in severalmammalian cell types examined to date. Based on our earlierstudies, GW bodies were proposed to be cytoplasmic sites formRNA storage and/or degradation. In the present study, immunogoldelectron microscopy identified electron dense structures of100-300 nm diameter devoid of a lipid bilayer membrane. Thesestructures appeared to comprise clusters of electron dense strandsof 8-10 nm in diameter. By costaining with CENP-F and PCNA,and employing a double-thymidine block to synchronize HeLa cells,GW bodies were observed to be small in early S phase and largerduring late S and G2 phases of the cell cycle. The majorityof GW bodies disassembled prior to mitosis and small GW bodiesreassembled in early G1. The analysis of GW bodies in two experimentalmodels of cell proliferation using reversal of 3T3/serum-starvationand concanavalin A stimulation of mouse splenocytes and T cells,revealed that proliferating cells contained larger, brighter,and more numerous GW bodies as well as up to a fivefold moretotal GW182 protein than quiescent cells. In vitro gene knockdownof GW182 led to the disappearance of GW bodies demonstratingthat GW182 is a critical component of GW bodies. The incrementalexpression of the GW182 protein in cells induced to proliferateand the cyclic formation and breakdown of GW bodies during mitosisare intriguing in view of the notion that GW bodies are specializedcenters involved in maintaining stability and/or controllingdegradation of mRNA.

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