Integrase Mediates Nuclear Localization of Ty3

doi:10.1128/MCB.21.22.7826-7838.2001

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Molecular and Cellular Biology, November 2001, p. 7826-7838, Vol. 21, No. 22
0270-7306/01/$04.00+0 DOI: 10.1128/MCB.21.22.7826-7838.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

Integrase Mediates Nuclear Localization of Ty3

Sophia S. Lin, M. Henrietta Nymark-McMahon, Lynn Yieh, and Suzanne B. Sandmeyer^*

Department of Biological Chemistry, University of California, Irvine, California 92697

Received 15 June 2001/Returned for modification 19 July 2001/Accepted 9 August 2001

Retroviruses in nondividing cells and yeast retrotransposons must transit the nuclear membrane in order for integration tooccur. Mutations in a bipartite basic motif in the carboxyl-terminaldomain of the Ty3 integrase (IN) protein were previously shownto block transposition at a step subsequent to 3'-end processingof Ty3 extrachromosomal DNA. In this work, the Ty3 IN was shownto be sufficient to target green fluorescent protein to the nucleolus.Mutations in the bipartite basic motif abrogated this localization.The region containing the motif was shown to be sufficient fornuclear but not subnuclear localization of a heterologous protein.Viruslike particles (VLPs) from cells expressing a Ty3 elementdefective for nuclear localization were inactive in an in vitrointegration assay, suggesting that nuclear entry is required toform active VLPs or that this motif is required for post-nuclearentry steps. Ty3 inserts at transcription initiation sites ofgenomic tRNA genes and plasmid-borne 5S and U6 RNA genes transcribedby RNA polymerase III. In situ hybridization with Ty3- and Ty3long terminal repeat-specific probes showed that these elementswhich are associated with tRNA genes do not colocalize with theribosomal DNA (rDNA). However, a PCR assay of cells undergoingtransposition showed that Ty3 insertion does occur into the 5Sgenes, which, in yeast, are interspersed with the rDNA and therefore,like Ty3 IN, associated with thenucleolus.

^* Corresponding author. Mailing address: Department of Biological Chemistry, College of Medicine, University of California,Irvine, Irvine, CA 92697-1700. Phone: (949) 824-7571. Fax: (949)824-2688. E-mail: sbsandme{at}uci.edu.

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