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Article

Mechanisms Directing the Nuclear Localization of the CtBP Family Proteins

, , , , , , & show all
Pages 4882-4894 | Received 16 Dec 2005, Accepted 05 Apr 2006, Published online: 27 Mar 2023
 

Abstract

The C-terminal binding protein (CtBP) family includes four proteins (CtBP1 [CtBP1-L], CtBP3/BARS [CtBP1-S], CtBP2, and RIBEYE) which are implicated both in transcriptional repression and in intracellular trafficking. However, the precise mechanisms by which different CtBP proteins are targeted to different subcellular regions remains unknown. Here, we report that the nuclear import of the various CtBP proteins and splice isoforms is differentially regulated. We show that CtBP2 contains a unique nuclear localization signal (NLS) located within its N-terminal region, which contributes to its nuclear accumulation. Using heterokaryon assays, we show that CtBP2 is capable of shuttling between the nucleus and cytoplasm of the cell. Moreover, CtBP2 can heterodimerize with CtBP1-L and CtBP1-S and direct them to the nucleus. This effect strongly depends on the CtBP2 NLS. PXDLS motif-containing transcription factors, such as BKLF, that bind CtBP proteins can also direct them to the nucleus. We also report the identification of a splice isoform of CtBP2, CtBP2-S, that lacks the N-terminal NLS and localizes to the cytoplasm. Finally, we show that mutation of the CtBP NADH binding site impairs the ability of the proteins to dimerize and to associate with BKLF. This reduces the nuclear accumulation of CtBP1. Our results suggest a model in which the nuclear localization of CtBP proteins is influenced by the CtBP2 NLS, by binding to PXDLS motif partner proteins, and through the effect of NADH on CtBP dimerization.

We thank D. Wotton and F. Schmitz for their generous gifts of reagents. We are indebted to Louise Cole for help with confocal microscopy analyses and Alister Funnell for help with RT-PCR.

This work was supported by an Australian NHMRC grant and a National Institutes of Health grant (HL073443) to M.C. and by grants from AIRC (Italian Association for Cancer Research) and Telethon (Italy) to D.C.

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