Affiliation:
1. Department of Biochemistry and Molecular Biology, University of Miami School of Medicine, Miami, Florida 33101
Abstract
ABSTRACT
Although
the role of macromolecular interactions in cell function has attracted
considerable attention, important questions about the organization of
cells remain. To help clarify this situation, we used a simple protocol
that measures macromolecule release after gentle permeabilization for
the examination of the status of endogenous macromolecules. Treatment
of Chinese hamster ovary cells with saponin under carefully controlled
conditions allowed entry of molecules of at least 800 kDa; however,
there were minimal effects on internal cellular architecture and
protein synthesis remained at levels comparable to those seen with
intact cells. Most importantly, total cellular protein and RNA were
released from these cells extremely slowly. The release of
actin-binding proteins and a variety of individual cytoplasmic proteins
mirrored that of total protein, while marker proteins from subcellular
compartments were not released. In contrast, glycolytic enzymes leaked
rapidly, indicating that cells contain at least two distinct
populations of cytoplasmic proteins. Addition of
microfilament-disrupting agents led to rapid and extensive release of
cytoplasmic macromolecules and a dramatic reduction in protein
synthesis. These observations support the conclusion that
mammalian cells behave as highly organized, macromolecular assemblies
(dependent on the actin cytoskeleton) in which endogenous
macromolecules normally are not free to diffuse over large
distances.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
Cited by
69 articles.
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