[
WormBook,
2005]
Cell-division control affects many aspects of development. Caenorhabditis elegans cell-cycle genes have been identified over the past decade, including at least two distinct Cyclin-Dependent Kinases (CDKs), their cyclin partners, positive and negative regulators, and downstream targets. The balance between CDK activation and inactivation determines whether cells proceed through G 1 into S phase, and from G 2 to M, through regulatory mechanisms that are conserved in more complex eukaryotes. The challenge is to expand our understanding of the basic cell cycle into a comprehensive regulatory network that incorporates environmental factors and coordinates cell division with growth, differentiation and tissue formation during development. Results from several studies indicate a critical role for CKI-1 , a CDK inhibitor of the Cip/Kip family, in the temporal control of cell division, potentially acting downstream of heterochronic genes and dauer regulatory pathways.
[
1982]
Caenorhabditis elegans is a free-living, nonparasitic nematode. It is a self-fertilizing hermaphrodite. Males arise spontaneously by nondisjunction of X-chromosomes. Of all eukaryotic organisms C. elegans has probably been most extensively studied at the cellular level. Within 12 hours the fertilized egg develops into a young larva with 558 nuclei (560 in the male). During postembryonic development the animal proceeds through four larval stages increasing its number of nuclei to 959 (1,031 in the male) plus some 2,000 germ cells (about 1,000 in the male). The cell lineages from fertilization to adulthood have been completely analyzed in living embryos and animals. This and its well-established genetics (more than 300 genes have been mapped on the six linkage groups) make it a suitable model organism to study problems of gene action and development. Various techniques have been used to interfere with normal development (including laser-induced cell ablations) and to analyze development on the subcellular level (including recombinant DNA technology). The characteristic features of rigidly determined development, the low cell number, and the knowledge of cellular events should make it possible to identify molecular action in situ and relate it to the structure and
[
WormBook,
2006]
There are two sexes in C. elegans, hermaphrodite and male. While there are many sex-specific differences between males and hermaphrodites that affect most tissues, the basic body plan and many of its structures are identical. However, most structures required for mating or reproduction are sexually dimorphic and are generated by sex-specific cell lineages. Thus to understand cell fate specification in hermaphrodites, one must consider how the body plan, which is specified during embryogenesis, influences the fates individual cells. One possible mechanism may involve the asymmetric distribution of POP-1 /Tcf, the sole C. elegans Tcf homolog, to anterior-posterior sister cells. Another mechanism that functions to specify cell fates along the anterior-posterior body axis in both hermaphrodites and males are the Hox genes. Since most of the cell fate specifications that occur in hermaphrodites also occur in males, the focus of this chapter will be on those that only occur in hermaphrodites. This will include the cell fate decisions that affect the HSN neurons, ventral hypodermal P cells, lateral hypodermal cells V5 , V6 , and T ; as well as the mesodermal M, Z1 , and Z4 cells and the intestinal cells. Both cell lineage-based and cell-signaling mechanisms of cell fate specification will be discussed. Only two direct targets of the sex determination pathway that influence cell fate specification to produce hermaphrodite-specific cell fates have been identified. Thus a major challenge will be to learn additional mechanisms by which the sex determination pathway interacts with signaling pathways and other cell fate specification genes to generate hermaphrodite-specific cell fates.