Journal
EXPERIMENTAL CELL RESEARCH
Volume 313, Issue 3, Pages 627-637Publisher
ELSEVIER INC
DOI: 10.1016/j.yexcr.2006.11.004
Keywords
DNA topoisomerase II; nuclear import; nuclear export; CRM1; importin alpha; nuclear localization; nucleocytoplasmic shuttling
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Resistance to anticancer drugs that target DNA topoisomerase II (topo II) isoforms alpha and/or beta is associated with decreased nuclear and increased cytoplasmic topo II alpha. Earlier studies have confirmed that functional nuclear localization and export signal sequences (NLS and NES) are present in both isoforms. in this study, we show that topo II alpha and beta bind and are imported into the nucleus by importin alpha 1, alpha 3, and alpha 5 in conjunction with importin beta. Topo II alpha also binds exportin/CRM1 in vitro. However, wild-type topo II alpha has only been observed in the cytoplasm of cells that are entering plateau phase growth. This suggests that topo II alpha may shuttle between the nucleus and the cytoplasm with the equilibrium towards the nucleus in proliferating cells but towards the cytoplasm in plateau phase cells. The CRM1 inhibitor Leptomycin B increases the nuclear localization of GFP-tagged topo II alpha with a mutant NLS, suggesting that its export is being inhibited. However, homokaryon shuttling experiments indicate that fluorescence-tagged wild-type topo II alpha and beta proteins do not shuttle in proliferating Cos-1 or HeLa cells. We conclude that topo II alpha and beta nuclear export is inhibited in proliferating cells so that these proteins do not shuttle. (c) 2006 Elsevier Inc. All rights reserved.
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