[
East Asia C. elegans Meeting,
2006]
Food or nutrition is vital for the life of C. elegans as for other animals, and should affect growth, body size and activity of the worm. In the laboratory, worms usually feed on OP50, a uracil-requiring strain of E. coli, which is a good food for worms in the sense that it supports rapid growth and production of many progeny. However, E. coli is an enteric bacterium that may not be abundant in soil which is said to be the natural habitat of the worm. Avery & Shtonda (2003) identified from soil samples more than 10 bacterial species that supported growth of the worm. Yet, the entire image of the natural food of the worm is not clear. Although the mechanisms of feeding and defecation of E. coli have been extensively studied, much is still to be solved, for example, the mechanisms of food recognition, rate and target of defecation. Furthermore, virtually nothing is known on the mechanisms of digestion of food and absorption of nutrients in the gut of the worm. In mammals, many factors which seem to be involved in digestion or absorption are known, but there is little genetics in any animal. Thus, we have begun studies on some of these, and plan to ask further, as follows. 1) Heat-killed E. coli is not likely to support growth of C. elegans. 2) We are studying whether selected microorganisms are good food or not. For example, yeast S. cerevisiae probably does not support growth to adults. 3) We are trying to identify live or dead microorganisms in the gut of marked worms that were put into a soil sample, by DNA sequencing. 4) Several artificial microspheres of various size or chemical nature are used to get clues to food recognition, feeding and defecation. 5) We are trying to analyze the time course of feeding, digestion and defecation of GFP-marked E. coli. 6) We have found many C. elegans genes possibly involved in digestion or absorption based on amino acid sequence homology with those in mammals. We have obtained KO mutants for some of them from Dr. S. Mitani for reverse genetics. 7) We have begun isolation of mutants on digestion or absorption. The screening at present uses GFP-marked E. coli as food. Two candidate mutants were obtained that retain more GFP fluorescence in the gut without little change in the pumping cycle.