Liposome-CAT complexes induce development of a non-inflammatory neointimal lesion in rabbit carotid arteries

Akiko Iwata; Nicole Campbell; Joy Dalesandro; Ricarda deFries-Hallstrand; Sadahiro Sai; Fieka Wijffels; Gary Koe; Margaret D. Allen

doi:10.1007/BF01616366

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Int J Angiol 2002; 11(2): 67-72
DOI: 10.1007/BF01616366

Original Articles

Liposome-CAT complexes induce development of a non-inflammatory neointimal lesion in rabbit carotid arteries

Akiko Iwata¹ , Nicole Campbell² , Joy Dalesandro³ , Ricarda deFries-Hallstrand⁴ , Sadahiro Sai⁵ , Fieka Wijffels⁶ , Gary Koe⁷ , Margaret D. Allen⁸

¹University of Washington, Seattle, Washington
²Lehman College, Bronx, New York
³University of Minnesota, Minneapolis, Minnesota
⁴Fred Hutchinson Cancer Research Center, Seattle, Washington
⁵Tohoku University, Sendai, Japan
⁶University of Leiden, Leiden, The Netherlands
⁷Valentis Corporation, Burlingame, California
⁸The Hope Heart Institute, Seattle, Washington

This work was performed at the University of Washington, Seattle, WA.This work was supported by the American Heart Association, Grant No. 9650559N.

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Publikationsdatum:
25. April 2011 (online)

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Abstract

Liposomes are attractive vectors for intraarterial cardiovascular applications because they can deliver genes into the quiescent cells of an intact vessel wall. In a model of in vivo intraarterial gene transfer in uninjured rabbit carotid arteries, we found that cationic liposomes complexed to the CAT reporter gene induced formation of an intimal lesion in rabbit arteries. Interestingly, unlike the lesions induced by viral vector gene transfer, this lesion is non-inflammatory, composed only of smooth muscle cells without evidence of leukocyte infiltration. Carotids transfected with liposomes complexed to the plasmid vector alone, liposomes complexed to the eukaryotic gene encoding human endothelial nitric oxide synthase, and sham-operated controls all evidenced only minimal lesions. We postulate that CAT DNA, perhaps through bacterial DNA CpG motifs or, less likely, the CAT protein itself may be inducing smooth muscle cell proliferation in the arterial walls transfected with the CAT-liposome complexes. These observations should be taken into account in other long-term in vivo vascular gene delivery models utilizing CAT as a reporter gene.

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