Early Intermediates of mariner Transposition: Catalysis without Synapsis of the Transposon Ends Suggests a Novel Architecture of the Synaptic Complex

doi:10.1128/MCB.24.18.8301-8311.2004

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Molecular and Cellular Biology, September 2004, p. 8301-8311, Vol. 24, No. 18
0270-7306/04/$08.00+0 DOI: 10.1128/MCB.24.18.8301-8311.2004
Copyright © 2004, American Society for Microbiology. All Rights Reserved.

Early Intermediates of mariner Transposition: Catalysis without Synapsis of the Transposon Ends Suggests a Novel Architecture of the Synaptic Complex

Karen Lipkow ,¹^,^, Nicolas Buisine,¹^, David J. Lampe,² and Ronald Chalmers¹^*

Department of Biochemistry, University of Oxford, Oxford, United Kingdom,¹ Department of Biological Sciences, Duquesne University, Pittsburgh, Pennsylvania²

Received 2 February 2004/ Returned for modification 3 March 2004/ Accepted 9 June 2004

The mariner family is probably the most widely distributed familyof transposons in nature. Although these transposons are relatedto the well-studied bacterial insertion elements, there is evidencefor major differences in their reaction mechanisms. We reportthe identification and characterization of complexes that containthe Himar1 transposase bound to a single transposon end. Titrationsand mixing experiments with the native transposase and transposasefusions suggested that they contain different numbers of transposasemonomers. However, the DNA protection footprints of the twomost abundant single-end complexes are identical. This indicatesthat some transposase monomers may be bound to the transposonend solely by protein-protein interactions. This would meanthat the Himar1 transposase can dimerize independently of thesecond transposon end and that the architecture of the synapticcomplex has more in common with V(D)J recombination than withbacterial insertion elements. Like V(D)J recombination and incontrast to the case for bacterial elements, Himar1 catalysisdoes not appear to depend on synapsis of the transposon ends,and the single-end complexes are active for nicking and probablyfor cleavage. We discuss the role of this single-end activityin generating the mutations that inactivate the vast majorityof mariner elements in eukaryotes.

* Corresponding author. Mailing address: Department of Biochemistry, University of Oxford, South Parks Rd., Oxford OX1 3QU, United Kingdom. Phone and fax: 44-1865 275307. E-mail: chalmers{at}bioch.ox.ac.uk.

K.L. and N.B. contributed equally to this work.

Present address: Department of Anatomy, University of Cambridge,Cambridge CB2 3DY, United Kingdom.

Molecular and Cellular Biology, September 2004, p. 8301-8311, Vol. 24, No. 18
0022-538X/04/$08.00+0 DOI: 10.1128/MCB.24.18.8301-8311.2004
Copyright © 2004, American Society for Microbiology. All Rights Reserved.

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