p53, p21WAF1/CIP1, and MDM2 Involvement in the Proliferation and Apoptosis in an In Vitro Model of Conditionally Immortalized Human Vascular Smooth Muscle Cells

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Arteriosclerosis, Thrombosis, and Vascular Biology. 2000;20:973-981

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Apoptosis

Cell biology/structural biology

Smooth muscle proliferation and differentiation

Mechanism of atherosclerosis/growth factors

Vascular Biology

p53, p21^WAF1/CIP1, and MDM2 Involvement in the Proliferation and Apoptosis in an In Vitro Model of Conditionally Immortalized Human Vascular Smooth Muscle Cells

J.-Kuang Hsieh¹; Dimitris Kletsas¹; Gerard Clunn; Alun D. Hughes; Michael Schachter; Catherine Demoliou-Mason¹

From the Department of Clinical Pharmacology (G.C., A.D.H., M.S., C.D.-M.), National Heart and Lung Institute, Imperial College of Science, Technology, and Medicine, St. Mary’s Hospital, London, UK; the Ludwig Institute (J.-K.H.), St. Mary’s Hospital, London, UK; and the Institute of Biology (D.K.), NCSR "Demokritos," Athens, Greece.

Correspondence to Dr A.D. Hughes, Clinical Pharmacology, National Heart and Lung Institute, Imperial College of Science, Technology, and Medicine, St. Mary’s Hospital, London W2 1NY, UK. E-mail a.hughes{at}ic.ac.uk

Abstract—Using an in vitro model of a conditionally immortalizedcell line, we have investigated how human vascular smooth musclecells (VSMCs) are affected by the expression of simian virus40 (SV40) large T antigen (LT antigen), which binds to cellcycle regulators such as the tumor suppressor protein p53. Cellswere obtained after infection of saphenous vein-derived VSMCswith a nonreplicative retroviral vector containing a temperature-sensitivemutant of SV40 LT antigen and were shown to have maintainedsome characteristics and responses of VSMCs. Under permissive-temperatureconditions (36°C), the increased rate of cell proliferationwas shown to be associated with expression of LT antigen andwith LT antigen binding to and inactivation of p53. p53 inactivationfailed to block apoptosis induced by serum withdrawal or UVirradiation. Downregulation of LT antigen expression at a nonpermissivetemperature (39°C) was shown to be associated with growtharrest, increased expression of the cell cycle inhibitor p21^WAF1/CIP1,increased murine double minute-2 promoter activity, and differentialexpression of murine double minute-2 gene products, suggestingthat p53-induced transcription/transactivation may be involvedin VSMC cycle control but not necessarily in apoptosis. Theestablished SMC line HVTs-SM1 may be a useful model for studyof the processes involved in myointimal hyperplasia and cellularaging, as well as for the study of cell cycle control in general.

Key Words: vascular smooth muscle • SV-40 • p53 • MDM2 • p21^WAF1/CIP1

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