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[
1977]
The workshop on nematodes presented current research from four laboratories on the development and physiology of C. elegans.
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[
1983]
More than 100 years ago, early European embryologists had posed the two central questions of animal development: First, how is the sameness of cells and organisms maintained during development and reproduction, and what factors transmit this hereditary information? Second, how do the cells of an embryo become different; what factors dictate that a particular cell at a particular time and position becomes committed to a particular developmental pathway? In the intervening century, we have largely answered the first question, acquiring extensive information about the genetic machinery and how it works. By contrast, we have gained little new understanding of the epigenetic process responsible for temporal and positional control of cell determination in embryos. How this process operates remains a central problem of contemporary
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[
1984]
Developmental fates of blastomeres in early C. elegans embryos appear to be governed by internally segregating, cell-autonomous determinants. To ascertain whether previously described gut-lineage dterminants are nuclear or cytoplasmic, laser microsurgery was used to show that exposing the nucleus of a non-gut-precursor cell to gut-precursor cytoplasm can cause the progeny of the resulting hybrid cell to express gut-specific differentiation markers, supporting the view that the determinants are cytoplasmic. In attempts to obtain molecular probes for such determinants, a library of monoclonal antibodies to early embryonic antigens was generated and screened by immunofluorescence microscopy for antibodies reacting with lineage-specific components. Three of the antibodies react with cytoplasmic granules (P granules) that segregate specifically with the germ line in early cleavages and are found uniquely in germ-line cells throughout the life cycle. Experiments on unfertilized eggs, on mutant embryos with defects in early cleavage, and on normal embryos treated with various cytoskeletal inhibitors indicate that P-granule segregation depends upon fertilization and requires the function of actin microfilaments, but is independent of spindle and microtubule functions. Work on the biochemical nature and function of the P granules is in progress.
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[
1987]
Work in our laboratory over the past several years has focused on the nature of early determinative decisions in embryos of the free-living nematode Caenorhabditis elegans. Two of these decisions regard determination of sex and determination of the level of X-chromosome expression. C. elegans has two sexes, self-fertilizing hermaphrodites and males. Hermaphrodites normally have two X chromosomes, and males have only one (there is no Y chromosome). Genetic and molecular evidence suggest that C. elegans compensates for this difference in X dosage, not by X inactivation as in mammals, but rather by global regulation of the X chromosome as in Drosophila; that is, X-linked genes are expressed at a higher level per chromosome in 1X than 2X animals, so that levels of X expression are similar in the two sexes. Also as in Drosophila, the primary signal that dictates both sex determination and level of X expression in C. elegans is the ration of the number of X chromosomes to the number of sets of autosomes (X/A ratio) rather than the absolute number of X chromosomes.|
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[
Methods Cell Biol,
1995]
Caenorhabditis elegans is in all likelihood the first metazoan animal whose entire genome will be determined. In addition, a very detailed description of the animal's morphology, development, and physiology is available (see elsewhere in this book, and Wood, 1988). Thus, the complete phenotype and genotype of an animal will be known. What is not known is how genotype determines phenotype; to study this, one needs to establish connections between genome sequence and phenotypes. Much has been done by classic or forward genetics: mutagenesis experiments have identified loci involved in a specific trait. Many of these loci have already been defined at the molecular level, and the genome sequence will certainly aid in the identification of many more. The opposite approach, reverse genetics, becomes naturally more important when more of the genome sequence is determined: Given the sequence of a gene of which nothing else is know, how can the function of that gene be determined? Reverse genetics is more than targeted inactivation. One can study a gene's function by several approaches...|
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Programmed cell death is a common cell fate in most if not all multicellular organisms. Apoptosis, which will be used as a synonym for programmed cell death throughout this chapter, occurs extensively during development as well as during later life. The development of the nematode worm Caenorhabditis elegans provides a good example of the extensive use of programmed cell death.
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[
WormBook,
2007]
The intestine is one of the major organs in C. elegans and is largely responsible for food digestion and assimilation as well as the synthesis and storage of macromolecules. In addition, the intestine is emerging as a powerful experimental system in which to study such universal biological phenomena as vesicular trafficking, biochemical clocks, stress responses and aging. The present chapter describes some of these many and varied properties of the C. elegans intestine: the embryonic cell lineage, intestine morphogenesis, structure and physiology of the intestinal cell and, finally, the transcription factor network controlling intestine development and function.
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[
WormBook,
2005]
Nematodes are the most abundant type of animal on earth, and live in hot springs, polar ice, soil, fresh and salt water, and as parasites of plants, vertebrates, insects, and other nematodes. This extraordinary ability to adapt, which hints at an underlying genetic plasticity, has long fascinated biologists. The fully sequenced genomes of Caenorhabditis elegans and Caenorhabditis briggsae, and ongoing sequencing projects for eight other nematodes, provide an exciting opportunity to investigate the genomic changes that have enabled nematodes to invade many different habitats. Analyses of the C. elegans and C. briggsae genomes suggest that these include major changes in gene content; as well as in chromosome number, structure and size. Here I discuss how the data set of ten genomes will be ideal for tackling questions about nematode evolution, as well as questions relevant to all eukaryotes.
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[
1990]
The free-living nematode Caenorhabditis elegans is a small and unpretentious organism. It may thrive unnoticed in the cabbage patch in your backyard or the flower pot on your balcony. In their natural habitat soil nematodes live in a thin film of water. In the laboratory C. elegans dwells on Petri dishes in the liquid film on the top of an agar layer, but can also be grown in liquid culture. As in other nematodes the liquid-filled body cavity (pseudocoelom) functions as a hydroskeleton. When the worm dries out, the hydroskeleton collapses and the animal inevitably dies. In a loose sense C. elegans may therefore be considered as a kind of aquatic animal. Because of this and because C. elegans is particularly well suited to the study of certain aspects of development, the following chapter is included in this book on Experimental Embryology of Aquatic Organisms. The intention of this contribution is to serve as an introduction and as a reference source rather than as a complete summary of present knowledge in the field. As indicated by the title, the review will focus on embryonic cell lineages, pattern formation in the embryo and the analysis of mutants affecting early
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[
Methods Cell Biol,
1995]
Genetic balancers are genetic constructs or chromosomal rearrangements that allow lethal or sterile mutations to be stably maintained in heterozygotes. In this chapter we use the term balancer primarily to refer to chromosomal duplications or rearrangements that suppress crossing over. In addition, we define lethal as any mutation that blocks survival or reproduction. Phenotypes associated with lethal mutations in Caenorhabditis elegans range from egg or larval lethality to adult sterility and maternal effect lethality, and can include conditional effects such as temperature sensitivity. The number of essential genes in C. elegans (those identified by lethal mutations) may range as high as 7000 according to genetic estimates. Thus, lethal mutations constitute a rich source of information about basic biological processes in this nematode.