Evolution of an Aurora Kinase A Inhibitor from an Essential tRNA Synthetase

James Julian Ross
Polina Tikanova
Andreas Hagmüller
Daniel Krogull
Keyu Xiao
Casper van Bavel
Till Balla
Tianhua Liao
Kolin Angelo Echano
Joseph Gokcezade
Peter Duchek
Danny Nedialkova
Rob Jelier
Gang Dong
Alejandro Burga

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Abstract

Gene duplication is a major driver of evolution, yet how it generates fundamentally new molecular functions remains poorly understood. Here, we show how such novelty arose in KLMT-1, a selfish toxin that causes genetic incompatibilities in Caenorhabditis tropicalis . KLMT-1 evolved via duplication of an essential tRNA synthetase but, strikingly, lost its ancestral role in tRNA biology and translation. Instead, KLMT-1 localizes to centrosomes, where it targets Aurora kinase A (AIR-1). This innovation is mediated by a three–amino acid insertion that extends a β-hairpin loop, enabling electrostatic interaction with a regulatory interface on the kinase. Our results demonstrate how changes in selective pressure, combined with minimal modifications in neutrally evolving regions, allow duplicated proteins to access new functional space and evolve entirely new molecular activities.

Version published to 10.64898/2026.05.15.725417 on bioRxiv
May 16, 2026

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