© 1998 American Heart Association, Inc.
Original Contributions |
Flow-Mediated Regulation of G-Protein Expression in Cocultured Vascular Smooth Muscle and Endothelial Cells
From the Georgetown University Medical Center, Department of Surgery, Washington, DC.
Abstract—G-proteins have been
implicated in the transduction of a number of flow-induced responses.
We determined whether flow can modulate vascular
endothelial or smooth muscle cell G-protein signaling.
By use of a perfused transcapillary coculture system that
permits the chronic exposure of cultured endothelial
cells (ECs) and smooth muscle cells (SMCs) to
physiological shear stresses, cocultures were
exposed to stepwise increases in flow up to (1) 2 mL/min (low flow: 0.5
dyne/cm2), or (2) 44 mL/min (high flow: 15
dyne/cm2) and maintained for 72 hours before SMCs and ECs
were harvested separately. Using Western blot analysis, EC
Gi
3 expression was significantly increased (41±2.9%)
by high-flow conditions compared with low-flow. The changes in
G-protein expression were associated with a significant increase in
endothelial nitric oxide synthase (eNOS) activity,
elevated prostacyclin levels in the perfusing media, increased
pertussis toxin–catalyzed ADP ribosylation of Gi substrates, and
enhanced agonist-stimulated GTPase activity in cocultured ECs. In
contrast, high flow induced a significant decrease in
Gi1–2 expression (57±5%) in SMCs cocultured with ECs,
an effect that was endothelium dependent, inhibited by
indomethacin, and correlated with a decrease in
pertussis toxin–catalyzed ADP ribosylation of Gi substrates,
reduced agonist-stimulated GTPase activity, and enhanced basal and
G-protein–stimulated adenylyl cyclase activity. These data demonstrate
that flow mediates selective changes in EC and SMC G-protein expression
concomitant with changes in G-protein functionality and cellular
signaling capacity. Moreover, flow-induced changes in SMC G-protein
signaling capacity are endothelium dependent and
require a cyclooxygenase product. G-protein
modulation may thus represent an important mechanism whereby
hemodynamic forces regulate vessel wall function.
Key Words: shear stress • flow • vascular endothelial cells • vascular smooth muscle • G-proteins
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