Multiply Attenuated, Self-Inactivating Lentiviral Vectors Efficiently Deliver and Express Genes for Extended Periods of Time in Adult Rat Cardiomyocytes In Vivo

doi:10.1161/01.CIR.0000065598.46411.EF

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Circulation. 2003;107:2375-2382
Published online before print April 14, 2003, doi: 10.1161/01.CIR.0000065598.46411.EF

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(Circulation. 2003;107:2375.)
© 2003 American Heart Association, Inc.

Basic Science Reports

Multiply Attenuated, Self-Inactivating Lentiviral Vectors Efficiently Deliver and Express Genes for Extended Periods of Time in Adult Rat Cardiomyocytes In Vivo

Sylvain Fleury, PhD; Eleonora Simeoni, PhD; Christian Zuppinger, PhD; Nicole Déglon, PhD; Ludwig K. von Segesser, MD; Lukas Kappenberger, MD; Giuseppe Vassalli, MD

From the Division of Cardiology (S.F., E.S., L.K., G.V.), Division of Experimental Surgery (S.F., E.S., G.V.), and Department of Cardiovascular Surgery (L.K.v.S.), University of Lausanne; the Neurosciences Institute (N.D.), Swiss Federal School of Technology, Lausanne; and the Division of Cardiology (C.Z.), University of Berne, Switzerland.

Correspondence to Giuseppe Vassalli, MD, CHUV-BH10, 1011 Lausanne, Switzerland. E-mail giuseppe.vassalli{at}chuv.hospvd.ch

Background— Among retroviral vectors, lentiviral vectorsare unique in that they transduce genes into both dividing andnondividing cells. However, their ability to provide sustainedmyocardial transgene expression has not been evaluated.

Methods and Results— Multiply attenuated, self-inactivatinglentivectors based on human immunodeficiency virus-1 containedthe enhanced green fluorescent protein (EGFP) gene under thetranscriptional control of either the cytomegalovirus (CMV)immediate-early enhancer/promoter, the elongation factor-1 ${alpha}$ (EF-1 ${alpha}$ )promoter, or the phosphoglycerate-kinase (PGK) promoter. Lentivectorstransduced adult rat cardiomyocytes in a dose-dependent manner(transduction rates, >90%; multiplicity of infection, ${approx}$ 5).The CMV promoter achieved higher EGFP expression levels thanthe EF-1 ${alpha}$ and PGK promoters. Insertion of the central polypurinetract pol sequence improved gene transfer efficiency by ${approx}$ 2-fold.In vivo gene transfer kinetics was studied by measuring thecopy number of integrated lentivirus DNA and EGFP concentrationsin cardiac extracts by real-time polymerase chain reaction andELISA, respectively. With CMV promoter-containing lentivectors,vector DNA peaked at day 3, declined by ${approx}$ 4-fold at day 14, butthen remained stable up to week 10. Similarly, EGFP expressionpeaked at day 7, decreased by ${approx}$ 7-fold at day 14, but was essentiallystable thereafter. In contrast, vector DNA and EGFP expressiondeclined rapidly with EF-1 ${alpha}$ promoter–containing lentivectors.Peak EGFP expression with titer-matched adenovectors was ${approx}$ 35%higher than with CMV lentivectors but was lost rapidly overtime.

Conclusions— Lentivectors efficiently transduce and expressgenes for extended periods of time in cardiomyocytes in vivo.Lentivectors provide a useful tool for studying myocardial biologyand a potential system for gene heart therapy.

Key Words: gene therapy • myocardium • viruses

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