Differential Regulation of Hyaluronic Acid Synthase Isoforms in Human Saphenous Vein Smooth Muscle Cells. Possible Implications for Vein Graft Stenosis

doi:10.1161/01.RES.0000199263.67107.c0

Circulation Research. 2005
Published online before print December 8, 2005, doi: 10.1161/01.RES.0000199263.67107.c0

A more recent version of this article appeared on January 6, 2006

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Submitted on May 9, 2005
Revised on September 12, 2005
Accepted on November 23, 2005

Differential Regulation of Hyaluronic Acid Synthase Isoforms in Human Saphenous Vein Smooth Muscle Cells. Possible Implications for Vein Graft Stenosis

M. van den Boom ; M. Sarbia ; K. von Wnuck Lipinski ; P. Mann ; J. Meyer-Kirchrath ; B. H. Rauch ; K. Grabitz ; B. Levkau ; K. Schrör ; and J. W. Fischer ^*

From the Molekulare Pharmakologie (M.v.d.B., P.M., J.M.-K., B.H.R., K.S., J.W.F.), Institut für Pharmakologie und Klinische Pharmakologie, Heinrich Heine Universität, Düsseldorf; Institut für Allgemeine Pathologie der Technischen Universität München (M.S.); Institut für Pathophysiologie (K.v.W.L., B.L.), Universitätsklinikum Essen; and Klinik für Gefäßchirurgie und Nierentransplantation (K.G.), Universitätsklinikum Düsseldorf, Germany.

^* To whom correspondence should be addressed. E-mail: jens.fischer{at}uni-duesseldorf.de.

Autologous saphenous vein bypass grafts (SVG) are frequentlycompromised by neointimal thickening and subsequent atherosclerosiseventually leading to graft failure. Hyaluronic acid (HA) generatedby smooth muscle cells (SMC) is thought to augment the progressionof atherosclerosis. The aim of the present study was (1) toinvestigate HA accumulation in native and explanted arterializedSVG, (2) to identify factors that regulate HA synthase (HAS)expression and HA synthesis, and (3) to study the function ofthe HAS2 isoform. In native SVG, expression of all 3 HAS isoformswas detected by RT-PCR. Histochemistry revealed that nativeand arterialized human saphenous vein segments were characterizedby marked deposition of HA in association with SMC. Interestingly,in contrast to native SVG, cyclooxygenase (COX)-2 expressionby SMC and macrophages was detected only in arterialized SVG.In vitro in human venous SMC HAS isoforms were found to be differentiallyregulated. HAS2, HAS1, and HA synthesis were strongly inducedby vasodilatory prostaglandins via G_s-coupled prostaglandinreceptors. In addition, thrombin induced HAS2 via activationof PAR1 and interleukin 1 ${beta}$ was the only factor that induced HAS3.By small interfering RNA against HAS2, it was shown that HAS2mediated HA synthesis is critically involved in cell cycle progressionthrough G₁/S phase and SMC proliferation. In conclusion, thepresent study shows that HA-rich extracellular matrix is maintainedafter arterialization of vein grafts and might contribute tograft failure because of its proproliferative function in venousSMC. Furthermore, COX-2-dependent prostaglandins may play akey role in the regulation of HA synthesis in arterialized veingrafts.

Key words: hyaluronic acid • extracellular matrix • cyclooxygenase-2 • vein graft stenosis

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