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ATP-dependent Mechanism Protects Spectrin against Glycation in Human Erythrocytes
Authors:Sumie Manno  Narla Mohandas  Yuichi Takakuwa
Institution:From the Department of Biochemistry, Tokyo Women''s Medical University, 8-1 Kawada-Cho, Shinjuku-Ku, Tokyo 162-8666, Japan and ;the §Red Cell Physiology Laboratory, New York Blood Center, New York, New York 10021
Abstract:Human erythrocytes are continuously exposed to glucose, which reacts with the amino terminus of the β-chain of hemoglobin (Hb) to form glycated Hb, HbA1c, levels of which increase with the age of the circulating cell. In contrast to extensive insights into glycation of hemoglobin, little is known about glycation of erythrocyte membrane proteins. In the present study, we explored the conditions under which glucose and ribose can glycate spectrin, both on the intact membrane and in solution and the functional consequences of spectrin glycation. Although purified spectrin could be readily glycated, membrane-associated spectrin could be glycated only after ATP depletion and consequent translocation of phosphatidylserine (PS) from the inner to the outer lipid monolayer. Glycation of membrane-associated spectrin led to a marked decrease in membrane deformability. We further observed that only PS-binding spectrin repeats are glycated. We infer that the absence of glycation in situ is the consequence of the interaction of the target lysine and arginine residues with PS and thus is inaccessible for glycation. The reduced membrane deformability after glycation in the absence of ATP is likely the result of the inability of the glycated spectrin repeats to undergo the obligatory unfolding as a consequence of interhelix cross-links. We thus postulate that through the use of an ATP-driven phospholipid translocase (flippase), erythrocytes have evolved a protective mechanism against spectrin glycation and thus maintain their optimal membrane function during their long circulatory life span.
Keywords:ATP  Erythrocyte  Glucose  Membrane Lipids  Membrane Proteins  Glycation  Pentosidine  Phosphatidylserine  Ribose  Spectrin
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