The Polysaccharide Releasing Phenomenon and Cell Envelope of the Inositol-Exacting Yeast in Inositol-Deficiency

Inositol-deficiency abnormalized the cell envelope, wall and membrane, and the polysaccharides were released out of the cells in a greater amount in inositol-deficiency than in inositol-sufficiency. This release was most notable in the absence of inositol under the tested conditions. The released amount decreased when the culture was provided with inositol or phospholipids, or deprived of all growth-promoting vitamins. Gel filtration of released polysaccharides showed that the lower molecular fraction increased in inositol-deficiency than in sufficiency. DEAE-Sephadex chromatography of released polysaccharides showed the presence of fractions specific for inositol-deficiency which contained mannan and phosphates. Inositol-deficiency also caused enlarging of the pore size of the cell-wall. The relationship between the release of polysaccharides and the syntheses of cell-wall polysaccharides was investigated and discussed.     

Effects of dimethylsulfoxide on sphingomyelinase activities in normal and Niemann-Pick type A, B and C fibroblasts

The effects of dimethylsulfoxide (DMSO) on sphingomyelinase activity measured at pH range 3.5-8.0 were examined in normal and Niemann-Pick disease type A, B and C fibroblasts culture. In normal cells, a minor activity was observed at pH 7.5, which was 3- to 4-fold lower than a major one at pH 5.0. Both activities at pH 5.0 and 7.5 were Mg2+-independent and localized to lysosomes. Niemann-Pick type C cells had 30-50% residual sphingomyelinase activity at both pH 5.0 and 7.5, as compared to normal control cells, whereas type A and B cells exhibited virtually no activity over the entire pH range examined. Treatment with 2% DMSO caused a marked increase in sphingomyelinase activities at pH 5.0 and 7.5 in normal and Niemann-Pick disease type C cells, while in type A and B cells, both activities remained virtually unchanged after DMSO treatment. The increase in sphingomyelinase activity at pH 5.0 induced in normal cells by DMSO resulted in an increase in the Vmax without a substantial change in the Km and was inhibited by the simultaneous addition of 10 micrograms/ml of cycloheximide. By comparison, a less than 2-fold increase in other lysosomal hydrolase activities was observed after DMSO treatment in all cell lines examined.     

The Autonomously Replicating Sequence (ARS) of the Yeast Saccharomyces exiguus Yp74L-3

Fragments containing ARSes were cloned from the genomic DNA of the yeast Saccharomyces exiguus Yp74L-3, and the essential regions for ARSes were restricted for these fragments. Mapping studies of ARS-acting sequences in one of these fragments suggested that S. exiguus recognizes a sequence as an ARS that is different from that recognized by Saccharomyces cerevisiae. Two ARS essential regions of S. exiguus were sequenced, and an ARS core consensus sequence of S. exiguus was deduced to be MATTAMWAWWTK. This sequence differs significantly from that of S. cerevisiae in two positions, suggesting that these nucleotide substitutions cause the difference in the ARS-recognition modes between S. exiguus and S. cerevisiae. Received: 3 August 1998 / Accepted: 18 September 1998