Alterations in glycosaminoglycan metabolism in β-aminopropionitrile-treated chick embryos

Author:

Elders M. Joycelyn1,Smith James D.1,Smith W. Grady1,Hughes Edwin R.1

Affiliation:

1. Departments of Pediatrics and Biochemistry, University of Arkansas School of Medicine, Little Rock, Ark. 72205, U.S.A., and West Virginia University School of Medicine, Morgantown, W. Va. 26505, U.S.A.

Abstract

1. Na235SO4, [1-14C]glucosamine and [1-14C]acetate were used as precursors of the sulphated glycosaminoglycans to study the biochemical effect of β-aminopropionitrile in chick embryos. The incorporation of all three precursors was decreased in the treated embryos between days 7 and 10 of embryonic development. No inhibition of incorporation of these precursors occurred between days 16 and 20 of embryonic development at the dosages of β-aminopropionitrile used. 2. β-Aminopropionitrile treatment also decreased the amount of N-acetylhexosamines in the chick embryo and decreased the percentage of the hexosamine esterified by nucleotides. Respiration was decreased by homogenates prepared from treated embryos. Likewise, UDP-xylosyl- and UDP-galactosyl-transferase activities were decreased in treated embryos and cartilage from embryos and growing chicks. 3. The data suggest that β-aminopropionitrile, in addition to the known lathyrogenic activity, either is or gives rise to a potent metabolic poison that interferes with basic cellular metabolism. The results are consistent with a decreased rate of ATP generation as an explanation for the decrease in glycosaminoglycan synthesis.

Publisher

Portland Press Ltd.

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