Recurrent Sites for New Centromere Seeding

Mario Ventura(Istituto Nazionale di Fisica Nucleare, Sezione di Bari), Stefania Weigl(University of California, Santa Cruz), Lucia Carbone(University of California, Santa Cruz), Maria Francesca Cardone(University of California, Santa Cruz), Doriana Misceo(University of California, Santa Cruz), Mariagrazia Teti(University of California, Santa Cruz), Pietro D’Addabbo(University of California, Santa Cruz), Annelise Wandall(University of Copenhagen), Erik Björck(Karolinska Institutet), Pieter J. de Jong(University of California, Santa Cruz), Xinwei She(University of California, Santa Cruz), Evan E. Eichler(University of California, Santa Cruz), Nicoletta Archidiacono(University of California, Santa Cruz), Mariano Rocchi(University of California, Santa Cruz)
Genome Research
September 1, 2004
Cited by 152Open Access
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Abstract

Using comparative FISH and genomics, we have studied and compared the evolution of chromosome 3 in primates and two human neocentromere cases on the long arm of this chromosome. Our results show that one of the human neocentromere cases maps to the same 3q26 chromosomal region where a new centromere emerged in a common ancestor of the Old World monkeys approximately 25-40 million years ago. Similarly, the locus in which a new centromere was seeded in the great apes' ancestor was orthologous to the site in which a new centromere emerged in the New World monkeys' ancestor. These data suggest the recurrent use of longstanding latent centromeres and that there is an inherent potential of these regions to form centromeres. The second human neocentromere case (3q24) revealed unprecedented features. The neocentromere emergence was not accompanied by any chromosomal rearrangement that usually triggers these events. Instead, it involved the functional inactivation of the normal centromere, and was present in an otherwise phenotypically normal individual who transmitted this unusual chromosome to the next generation. We propose that the formation of neocentromeres in humans and the emergence of new centromeres during the course of evolution share a common mechanism.


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