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serotonylation of vascular proteins important to contractionserotonylation收缩血管蛋白的重要
Serotonylation of Vascular Proteins Important to
Contraction
Stephanie W. Watts*, Jessica R. C. Priestley, Janice M. Thompson
Department of Pharmacology and Toxicology, Michigan State University, East Lansing, Michigan, United States of America
Abstract
Background: Serotonin (5-hydroxytryptamine, 5-HT) was named for its source (sero-) and ability to modify smooth muscle
tone (tonin). The biological effects of 5-HT are believed to be carried out by stimulation of serotonin receptors at the plasma
membrane. Serotonin has recently been shown to be synthesized in vascular smooth muscle and taken up from external
sources, placing 5-HT inside the cell. The enzyme transglutaminase uses primary amines such as 5-HT to covalently modify
proteins on glutamine residues. We tested the hypothesis that 5-HT is a substrate for transglutaminase in arterial vascular
smooth muscle, with protein serotonylation having physiological function.
Methodology/Principal Findings: The model was the rat aorta and cultured aortic smooth muscle cells. Western analysis
demonstrated that transglutaminase II was present in vascular tissue, and transglutaminase activity was observed as a
cystamine-inhibitable incorporation of the free amine pentylamine-biotin into arterial proteins. Serotonin-biotin was
incorporated into a -actin, b-actin, c-actin, myosin heavy chain and filamin A as shown through tandem mass spectrometry.
Using antibodies directed against biotin or 5-HT, immunoprecipitation and immunocytochemistry confirmed serotonylation
of smooth muscle a–actin. Importantly, the a-actin-dependent process of arterial isometric contraction to 5-HT was reduced
by cystamine.
Conclusions: 5-HT covalently modifies proteins integral to contractility and the cytoskeleton. These findings suggest new
mechanisms of action for 5-HT in vascular smooth muscle and con
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