Complex formation among the RNA export proteins Nup98, Rae1/Gle2, and TAP - PubMed (original) (raw)
. 2003 Jun 6;278(23):20979-88.
doi: 10.1074/jbc.M302061200. Epub 2003 Mar 13.
Affiliations
- PMID: 12637516
- DOI: 10.1074/jbc.M302061200
Free article
Complex formation among the RNA export proteins Nup98, Rae1/Gle2, and TAP
Melanie B Blevins et al. J Biol Chem. 2003.
Free article
Abstract
Most nucleocytoplasmic traffic through the nuclear pore complex is mediated by soluble receptors of the importin/exportin or karyopherin family. mRNA export is unique in that no receptor of this family has been implicated in trafficking of the bulk of mRNAs. Instead, many diverse proteins have been linked to mRNA export, but an all-encompassing model remains elusive. Understanding how these proteins interact with each other is central to the development of such a model. Here, we have focused on the interactions between three proteins implicated in mRNA export, Nup98, Rae1/Gle2, and TAP. We have defined the binary complexes that form among these proteins. We find that Gle2 requires two sites within TAP for stable interaction. Strikingly, rather than a general affinity for all nucleoporin FG repeats, TAP has highest affinity for a specific region within the GLFG domain of Nup98, indicating that not all repeats are identical in function. We have established that the ternary complex can form through simultaneous binding of both Gle2 and TAP to adjacent sites on Nup98. In contrast, Nup98 competes with TAP for Gle2 binding; when bound to Nup98, Gle2 no longer interacts directly with TAP. From these interactions, we propose that Gle2 may act to deliver TAP to Nup98 and that this may represent the first in a series of interactions between an export complex and a nucleoporin.
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