Targeted Disruption of TGF-{beta}-Smad3 Signaling Leads to Enhanced Neointimal Hyperplasia With Diminished Matrix Deposition in Response to Vascular Injury

doi:10.1161/01.RES.0000163980.55495.44

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Circulation Research. 2005;96:904-912
Published online before print March 24, 2005, doi: 10.1161/01.RES.0000163980.55495.44

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(Circulation Research. 2005;96:904.)
© 2005 American Heart Association, Inc.

Integrative Physiology

Targeted Disruption of TGF-ß–Smad3 Signaling Leads to Enhanced Neointimal Hyperplasia With Diminished Matrix Deposition in Response to Vascular Injury

Kazuki Kobayashi, Koutaro Yokote, Masaki Fujimoto, Kimihiro Yamashita, Akemi Sakamoto, Masaki Kitahara, Harukiyo Kawamura, Yoshiro Maezawa, Sunao Asaumi, Takeshi Tokuhisa, Seijiro Mori, Yasushi Saito

From the Department of Clinical Cell Biology (K.K., K.Y., M.F., H.K., Y.M., S.A., S.M., Y.S.), Chiba University Graduate School of Medicine; Division of Endocrinology and Metabolism (K.Y., Y.S.), Department of Internal Medicine, Chiba University Hospital; Department of Developmental Genetics (K.Y., A.S., T.T.), Chiba University Graduate School of Medicine, Chiba, Japan; and Shiraoka Research Station of Biological Science (M.K.), Nissan Chemical Industries, Ltd, Saitama, Japan.

Correspondence to Koutaro Yokote, MD, PhD, DMSci, Division of Endocrinology and Metabolism, Department of Internal Medicine, Chiba University Hospital, 1-8-1 Inohana, Chuo-ku, Chiba 260-8670, Japan. E-mail kyokote-cib{at}umin.ac.jp

The role of transforming growth factor (TGF)-ß andits signal in atherogenesis is not fully understood. Here, weexamined mice lacking Smad3, a major downstream mediator ofTGF-ß, to clarify the precise role of Smad3-dependentsignaling in vascular response to injury. Femoral arteries wereinjured in wild-type and Smad3-null (null) male mice on C57Bl/6background. Histopathological evaluation of the arteries 1 to3 weeks after the injury revealed significant enhancement ofneointimal hyperplasia in null compared with wild-type mice.Transplantation of null bone marrow to wild-type mice did notenhance neointimal thickening, suggesting that vascular cellsin situ play a major role in the response. Null intima containedmore proliferating smooth muscle cells (SMC) with less amountof collagen compared with wild-type intima. TGF-ßcaused significant inhibition of cellular proliferation in wild-typeaortic SMC, whereas the growth of null SMC was only weakly inhibitedby TGF-ß in vitro, indicating a crucial role of Smad3in the growth inhibitory function. On the other hand, Smad3-deficiencydid not attenuate chemotaxis of SMC toward TGF-ß.TGF-ß increased transcript level of ${alpha}$ 2 type I collagenand tissue inhibitor of metalloproteinases-1, and suppressedexpression and activity of matrix metalloproteinases in wild-typeSMC. However, these effects of TGF-ß were diminishedin null SMC. Our findings altogether show that the loss of Smad3pathway causes enhanced neointimal hyperplasia on injury throughmodulation of growth and matrix regulation in vascular SMC.These results indicate a vasculoprotective role of endogenousSmad3 in response to injury.

Key Words: transforming growth factor-ß • Smad3 • atherosclerosis • neointimal hyperplasia • smooth muscle cells

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