Vigilant Vector: Heart-Specific Promoter in an Adeno-Associated Virus Vector for Cardioprotection

doi:10.1161/hy0202.103472

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Hypertension. 2002;39:651-655
doi: 10.1161/hy0202.103472

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(Hypertension. 2002;39:651.)
© 2002 American Heart Association, Inc.

Scientific Contributions

Vigilant Vector: Heart-Specific Promoter in an Adeno-Associated Virus Vector for Cardioprotection

M. Ian Phillips; Yi Tang; Kai Schmidt-Ott; Keping Qian; Shuntaro Kagiyama

From the Department of Physiology and Functional Genomics, University of Florida, Gainesville, FL.

Correspondence to Dr M. Ian Phillips, Physiology and Functional Genomics, University of Florida, College of Medicine, Box 100274, Gainesville, FL 32610-0274. E-mail MIP{at}ufl.edu

Repeated bouts of ischemia in the heart lead to fibrosis andeventually to heart failure. Although certain genes, such asSOD or hemoxygenase and antisense to AT₁R, ACE, and (ß₁-ARcan provide short-term protection of the heart from ischemia,there is no known mechanism for constantly responding to repeatedincidences of ischemia. We hypothesized that a "vigilant vector,"designed to be expressed specifically in the heart and switchon therapeutic genes only during hypoxia, would provide cardioprotection.To attain cardiac specificity, we inserted an MLC2v promoterinto an adeno-associated virus (AAV) designed to deliver ASto AT₁R and gfp. In in vitro experiments in cardiomyocytes (H9C2cells), the MLC2v-AAV-gfp drove gene expression in all cellsat levels comparable to a cytomegalovirus (CMV) promoter. Inin vivo experiments, the rAAV-MLC2v-gfp was injected intravenouslyinto mice or rats. Green fluoresence protein (GFP) DNA was locatedin kidney, heart (right and left ventricle), lung, adrenal andspleen. GFP mRNA, however, was expressed only in the heart andabsent in other tissues. To switch on the rAAV transgene duringischemia, we inserted a hypoxia response element (HRE). Thisupregulates transcription when O₂ levels are low. Thus, thereare 4 components to the vigilant vector; a gene switch (HRE),a heart-specific promoter (MLC2v), a therapeutic gene (AS-AT₁R)and a reporter gene (gfp). To silence or lower basal level ofexpression while retaining specificity, we have reduced thelength of the MLC2v promoter from 3 kb to 1775 bp or 281 bp.The truncated promoter is equally effective in heart specificexpression. Preliminary studies with the rAAV-HRE-gfp in vitroshow an increased expression in 1% O₂ in 4 to 6 hours. By addingadditional hypoxia-inducible factor (HIF ${alpha}$ ) (5 µg), theMLC2v-gfp expression is increased by 4-fold in 1% O₂. Furtheramplification of the gene to 400-fold in 1% O₂ can be achievedwith a double plasmid. The construct may serve as a prototype"vigilant vector" to switch on therapeutic genes in specifictissue with physiological signals.

Key Words: ischemia • cardiac function • hypoxia • myosin • gene therapy • adeno-associated virus

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