Directing Cell Division During Development

3 November 1989

journal article
review article
Published by American Association for the Advancement of Science (AAAS) in Science

Vol. 246 (4930) , 635-640
https://doi.org/10.1126/science.2683080

Abstract

Several evolutionarily conserved proteins constitute a universal mitotic trigger that is precisely controlled during the orderly cell divisions of embryogenesis. As development progresses, the mechanisms controlling this trigger change. Early divisions are executed by maternally synthesized gene products, and in Xenopus they are timed by the accumulation and periodic degradation of cyclin, a trigger component. Later, the zygotic genome assumes control, and in Drosophila, zygotic transcription is required for production of another trigger protein, the product of string. After this transition to zygotic control, pulses of string transcription define the timing of highly patterned embryonic cell divisions and cyclin accumulation is not rate limiting.

Keywords

This publication has 49 references indexed in Scilit:

Accurate measurements of dynamics and reproducibility in small genetic networks
Molecular Systems Biology, 2013
The role of cyclin B in meiosis I.
The Journal of cell biology, 1989
Transcripts of one of two Drosophila cyclin genes become localized in pole cells during embryogenesis
Nature, 1989
Cyclin in fission yeast
Cell, 1988
The molecular genetics of embryonic pattern formation in Drosophila
Nature, 1988
Cell cycle control by the nucleo-cytoplasmic ratio in early Drosophila development
Cell, 1986
A major developmental transition in early xenopus embryos: II. control of the onset of transcription
Cell, 1982
A major developmental transition in early xenopus embryos: I. characterization and timing of cellular changes at the midblastula stage
Cell, 1982
The translational control phase of early development
Bioscience Reports, 1982
Mutations affecting segment number and polarity in Drosophila
Nature, 1980