Margaret E. Ginn‐Pease scite author profile

Although phosphatase and tensin homologue deleted on chromosome 10 (PTEN) localization in the nucleus and cytoplasm is established, the mechanism is unknown. PTEN is a tumor suppressor phosphatase that causes cell cycle arrest and/or apoptosis. Nuclear-cytoplasmic compartmentalization may be a novel mechanism in regulating these events. PTEN does not contain a traditional nuclear localization sequence (NLS); however, we identified putative NLS-like sequences, which we analyzed by site-directed mutagenesis and localization studies in MCF-7 cells. Two double site mutations exhibited nuclear localization defects. Furthermore, unlike wild-type PTEN, double NLS mutant PTEN did not interact with major vault protein (MVP), a previously hypothesized nuclear-cytoplasmic transport protein. We conclude that these two NLS-like sequences are required for PTEN nuclear import that is mediated by MVP. Further, we show that this MVP-mediated nuclear import is independent of PTEN phosphorylation and of the lipid and protein phosphatase activities of PTEN. (Cancer Res 2005; 65(10): 4108-16)

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Pediatric head injuries: Can clinical factors reliably predict an abnormality on computed tomography?

Dietrich

Bowman

Ginn‐Pease

et al. 1993

Annals of Emergency Medicine

145

116

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Redox Signals and NF-κB Activation in T Cells

Ginn‐Pease

Whisler

1998

Free Radical Biology and Medicine

205

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Pulmonary function is compromised in children with mediastinal lymphoma

King

Patrick

Ginn‐Pease

et al. 1997

Journal of Pediatric Surgery

145

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