TY - JOUR T1 - The dynamics of replication licensing in live Caenorhabditis elegans embryos A1 - Sonneville,Remi A1 - Querenet,Matthieu A1 - Craig,Ashley A1 - Gartner,Anton A1 - Blow,J. Julian AU - Sonneville,Remi AU - Querenet,Matthieu AU - Craig,Ashley AU - Gartner,Anton AU - Blow,J. Julian PY - 2012/1/23 Y1 - 2012/1/23 N2 -

Accurate DNA replication requires proper regulation of replication licensing, which entails loading MCM-2-7 onto replication origins. In this paper, we provide the first comprehensive view of replication licensing in vivo, using video microscopy of Caenorhabditis elegans embryos. As expected, MCM-2-7 loading in late M phase depended on the prereplicative complex (pre-RC) proteins: origin recognition complex (ORC), CDC-6, and CDT-1. However, many features we observed have not been described before: GFP-ORC-1 bound chromatin independently of ORC-2-5, and CDC-6 bound chromatin independently of ORC, whereas CDT-1 and MCM-2-7 DNA binding was interdependent. MCM-3 chromatin loading was irreversible, but CDC-6 and ORC turned over rapidly, consistent with ORC/CDC-6 loading multiple MCM-2-7 complexes. MCM-2-7 chromatin loading further reduced ORC and CDC-6 DNA binding. This dynamic behavior creates a feedback loop allowing ORC/CDC-6 to repeatedly load MCM-2-7 and distribute licensed origins along chromosomal DNA. During S phase, ORC and CDC-6 were excluded from nuclei, and DNA was overreplicated in export-defective cells. Thus, nucleocytoplasmic compartmentalization of licensing factors ensures that DNA replication occurs only once.

AB -

Accurate DNA replication requires proper regulation of replication licensing, which entails loading MCM-2-7 onto replication origins. In this paper, we provide the first comprehensive view of replication licensing in vivo, using video microscopy of Caenorhabditis elegans embryos. As expected, MCM-2-7 loading in late M phase depended on the prereplicative complex (pre-RC) proteins: origin recognition complex (ORC), CDC-6, and CDT-1. However, many features we observed have not been described before: GFP-ORC-1 bound chromatin independently of ORC-2-5, and CDC-6 bound chromatin independently of ORC, whereas CDT-1 and MCM-2-7 DNA binding was interdependent. MCM-3 chromatin loading was irreversible, but CDC-6 and ORC turned over rapidly, consistent with ORC/CDC-6 loading multiple MCM-2-7 complexes. MCM-2-7 chromatin loading further reduced ORC and CDC-6 DNA binding. This dynamic behavior creates a feedback loop allowing ORC/CDC-6 to repeatedly load MCM-2-7 and distribute licensed origins along chromosomal DNA. During S phase, ORC and CDC-6 were excluded from nuclei, and DNA was overreplicated in export-defective cells. Thus, nucleocytoplasmic compartmentalization of licensing factors ensures that DNA replication occurs only once.

KW - ORIGIN RECOGNITION COMPLEX KW - EUKARYOTIC DNA-REPLICATION KW - C-ELEGANS KW - CELL-CYCLE KW - MCM2-7 HELICASE KW - GEMININ HOMOLOG KW - ATP-HYDROLYSIS KW - RE-REPLICATION KW - S-PHASE KW - CHROMATIN U2 - 10.1083/jcb.201110080 DO - 10.1083/jcb.201110080 M1 - Article JO - Journal of Cell Biology JF - Journal of Cell Biology SN - 0021-9525 IS - 2 VL - 196 SP - 233 EP - 246 ER -