Analysis of two-dimensional protein patterns from mouse embryos with different trisomies.
- 1 June 1983
- journal article
- research article
- Published by Proceedings of the National Academy of Sciences in Proceedings of the National Academy of Sciences
- Vol. 80 (12) , 3753-3757
- https://doi.org/10.1073/pnas.80.12.3753
Abstract
Two-dimensional protein patterns from whole mouse embryos with different trisomies (Ts) (Tsl, -12, -14, -19) and from different organs (normal or malformed) and developmental stages of Ts 12 embryos were analyzed by comparison with control patterns. Quantitatively altered proteins were found, and a portion of these (21/.apprxeq.1000, average) was attributable to the Ts conditions. Most of these variants were found always (regularly) in Ts embryos. They could be divided into 2 groups: group I shows characteristics (chromosome specific, density increased by a factor close to 1.5 .+-. 0.12) compatible with proteins directly affected by the Ts; and group II (chromosome nonspecific, density decreased, seldom increased) results most likely from indirect effects. The incidence of group II variants (about 13/.apprxeq.1000, average) was considerably greater than that of the group I variants (about 3/.apprxeq.1000). The frequency of both types of variants, was far lower than was expected by a rough estimation. Apparently, a relatively small number of changes, rather than a complex, escalating effect, was induced at the protein level by the Ts. This may be due to a stable regulation of protein concentrations. The proportion in which quantitative changes of different types occurred in the protein patterns did not correlate with the degree of developmental impairments (malformation, retardation, early death) of the embryos. The generalized occurrence of protein changes on the cellular level might explain the restricted viability of Ts mouse embryos.This publication has 17 references indexed in Scilit:
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