ATP synthase F1 subunits recruited to centromeres by CENP-A are required for male meiosis

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Caitríona M. Collins
Beatrice Malacrida
Colin Burke
Patrick A. Kiely
Elaine M. Dunleavy
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[1] National University of Ireland Galway,Centre for Chromosome Biology, Biomedical Sciences
[2] University of Limerick,Graduate Entry Medical School and Health Research Institute
[3] Queen’s University,undefined
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The histone H3 variant CENP-A epigenetically defines the centromere and is critical for chromosome segregation. Here we report an interaction between CENP-A and subunits of the mitochondrial ATP synthase complex in the germline of male Drosophila. Furthermore, we report that knockdown of CENP-A, as well as subunits ATPsyn-α, -βlike (a testis-specific paralogue of ATPsyn-β) and -γ disrupts sister centromere cohesion in meiotic prophase I. We find that this disruption is likely independent of reduced ATP levels. We identify that ATPsyn-α and -βlike localise to meiotic centromeres and that this localisation is dependent on the presence of CENP-A. We show that ATPsyn-α directly interacts with the N-terminus of CENP-A in vitro and that truncation of its N terminus perturbs sister centromere cohesion in prophase I. We propose that the CENP-A N-terminus recruits ATPsyn-α and -βlike to centromeres to promote sister centromere cohesion in a nuclear function that is independent of oxidative phosphorylation.
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