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PLANT PHYSIOLOGY , Vol 107, Issue 1 87-100, Copyright © 1995 by American Society of Plant Biologists
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BIOCHEMISTRY AND ENZYMOLOGY |
Expansin Mode of Action on Cell Walls (Analysis of Wall Hydrolysis, Stress Relaxation, and Binding)
S. J. McQueen-Mason and D. J. Cosgrove
Department of Biology, 208 Mueller Lab, Pennsylvania State University, University Park, Pennsylvania 16802
The biochemical mechanisms underlying cell wall expansion in plants have
long been a matter of conjecture. Previous work in our laboratory
identified two proteins (named "expansins") that catalyze the acid-induced
extension of isolated cucumber cell walls. Here we examine the mechanism of
expansin action with three approaches. First, we report that expansins did
not alter the molecular mass distribution or the viscosity of solutions of
matrix polysaccharides. We conclude that expansins do not hydrolyze the
major pectins or hemicelluloses of the cucumber wall. Second, we
investigated the effects of expansins on stress relaxation of isolated
walls. These studies show that expansins account for the pH-sensitive and
heat-labile components of wall stress relaxation. In addition, these
experiments show that expansins do not cause a progressive weakening of the
walls, as might be expected from the action of a hydrolase. Third, we
studied the binding of expansins to the cell wall and its components. The
binding characteristics are consistent with this being the site of expansin
action. We found that expansins bind weakly to crystalline cellulose but
that this binding is greatly increased upon coating the cellulose with
various hemicelluloses. Xyloglucan, either solubilized or as a coating on
cellulose microfibrils, was not very effective as a binding substrate.
Expansins were present in growing cell walls in low quantities
(approximately 1 part in 5000 on a dry weight basis), suggesting that they
function catalytically. We conclude that expansins bind at the interface
between cellulose microfibrils and matrix polysaccharides in the wall and
induce extension by reversibly disrupting noncovalent bonds within this
polymeric network. Our results suggest that a minor structural component of
the matrix, other than pectin and xyloglucan, plays an important role in
expansin binding to the wall and, presumably, in expansin action.
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