(Patho)physiologic pathways to drug targeting: artificial viral envelopes

Journal of Molecular Recognition : JMR
H SchreierR Chander

Abstract

The goal of this study was to exploit molecular recognition of cell surface receptors by viral surface glycoproteins as a means for the selective intracellular delivery of macromolecules. To accomplish this, artificial viral envelopes (AVE) resembling the human immunodeficiency virus-1 (HIV-1) were designed as a model system. Recombinant HIV-1 surface glycoprotein gp160 (HIV-1 rgp160) was inserted in the artificial envelope by a two-step detergent dialysis process. The artificial HIV-1 envelope recognized the CD4 cell surface receptor. FITC-dextran and ricin A were employed as model macromolecules as they cannot passively diffuse across cell membranes. Selective transfer of FITC-dextran encapsulated in HIV-1 rgp160 AVE into a CD4-positive cell line (REX-1B) versus a CD4-negative cell line (KG-1) was demonstrated. Ricin A at concentrations as low as 2 ng/ml arrested cell growth of CD4-positive MOLT-4 cells, whereas 8 ng/ml ricin A in solution had no effect on cell growth. The arrest of cell growth was reverted in the presence of excess anti-gp120 monoclonal antibody. Naked envelopes (without HIV-1 rgp160 inserted) were also found to interact with cells and transfer material, although less efficiently and in a non-specific manner...Continue Reading

References

Jun 1, 1978·Proceedings of the National Academy of Sciences of the United States of America·C R AlvingW L Hanson
Feb 1, 1988·Proceedings of the National Academy of Sciences of the United States of America·R C AloiaL M Gordon
Jul 11, 1985·Biochimica Et Biophysica Acta·L D MayerA S Janoff

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Citations

Sep 1, 2000·Advanced Drug Delivery Reviews·S P Vyas, V Sihorkar
Dec 4, 2003·Journal of Oral Rehabilitation·P DionysopoulosK Tolidis

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