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2006Zhou Longhu; Thakur Chandar S; Molinaro Ross J; Paranjape Jayashree M; Hoppes Rieuwert; Jeang Kuan-Teh; Silverman Robert H; Torrence Paul F
Delivery of 2-5A cargo into living cells using the Tat cell penetrating peptide: 2-5A-tat.
Bioorganic & medicinal chemistry 2006;14(23):7862-74.
2',5'-Oligoadenylate tetramer (2-5A) has been chemically conjugated to short HIV-1 Tat peptides to provide 2-5A-tat chimeras. Two different convergent synthetic approaches have been employed to provide such 2-5A-tat bioconjugates. One involved generation of a bioconjugate through reaction of a cysteine terminated Tat peptide with a alpha-chloroacetyl derivative of 2-5A. The second synthetic strategy was based upon a cycloaddition reaction of an azide derivative of 2-5A with a Tat peptide bearing an alkyne function. Either bioconjugate of 2-5A-tat was able to activate human RNase L. The union of 2-5A and Tat peptide provided an RNase L-active chimeric nucleopeptide with the ability to be taken up by cells by virtue of the Tat peptide and to activate RNase L in intact cells. This strategy provides a valuable vehicle for the entry of the charged 2-5A molecule into cells and may provide a means for targeted destruction of HIV RNA in vivo.

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