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Loss of Cell Cycle Checkpoint Control in Drosophila Rfc4 Mutants

Krause, Sue A.; Loupart, Marie-Louise; Vass, Sharron; Schoenfelder, Stefan; Harrison, Steve; Heck, Margaret M. S.

Authors

Sue A. Krause

Marie-Louise Loupart

Stefan Schoenfelder

Steve Harrison

Margaret M. S. Heck



Abstract

Two alleles of the Drosophila melanogaster Rfc4(DmRfc4) gene, which encodes subunit 4 of the replication factor C (RFC) complex, cause striking defects in mitotic chromosome cohesion and condensation. These mutations produce larval phenotypes consistent with a role in DNA replication but also result in mitotic chromosomal defects appearing either as premature chromosome condensation-like or precocious sister chromatid separation figures. Though the DmRFC4 protein localizes to all replicating nuclei, it is dispersed from chromatin in mitosis. Thus the mitotic defects appear not to be the result of a direct role for RFC4 in chromosome structure. We also show that the mitotic defects in these twoDmRfc4 alleles are the result of aberrant checkpoint control in response to DNA replication inhibition or damage to chromosomes. Not all surveillance function is compromised in these mutants, as the kinetochore attachment checkpoint is operative. Intriguingly, metaphase delay is frequently observed with the more severe of the two alleles, indicating that subsequent chromosome segregation may be inhibited. This is the first demonstration that subunit 4 of RFC functions in checkpoint control in any organism, and our findings additionally emphasize the conserved nature of RFC's involvement in checkpoint control in multicellular eukaryotes.

Citation

Krause, S. A., Loupart, M.-L., Vass, S., Schoenfelder, S., Harrison, S., & Heck, M. M. S. (2001). Loss of Cell Cycle Checkpoint Control in Drosophila Rfc4 Mutants. Molecular and Cellular Biology, 21(15), 5156-5168. https://doi.org/10.1128/mcb.21.15.5156-5168.2001

Journal Article Type Article
Acceptance Date Apr 26, 2001
Publication Date Aug 1, 2001
Deposit Date Sep 21, 2016
Journal Molecular and Cellular Biology
Print ISSN 0270-7306
Electronic ISSN 1098-5549
Publisher American Society for Microbiology
Peer Reviewed Peer Reviewed
Volume 21
Issue 15
Pages 5156-5168
DOI https://doi.org/10.1128/mcb.21.15.5156-5168.2001
Keywords Cell Biology; Molecular Biology
Public URL http://researchrepository.napier.ac.uk/Output/369998