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Nucleic Acids Research, 1992, Vol. 20, No. 2 307-314
© 1992


MOLECULAR BIOLOGY

In vivo stability and kinetics of absorption and disposition of 3' phosphopropyl amine oligonucleotides

Joseph G. Zendegui*, Karen M. Vasquez1, John H. Tinsley1, Donald J. Kessler1 and Michael E. Hogan1

Triplex Pharmaceutical Corporation The Woodlands, TX 77380 1Center for Biotechnology, Baylor College of Medicine The Woodlands, TX 77381, USA

*To whom correspondence should be addressed

Received September 6, 1991. Revised December 16, 1991. Accepted December 16, 1991.

Development of oligonucleotide derivatives as therapeutic agents requires an understanding of their pharmacokinetic behavior. The in vivo disposition and stability of a prototype of such compounds are reported here. The compound studied, a relatively G-rich 38 base 3' phosphopropyl amine oligonucleotide (TFO-1), was cleared from the circulation with a half-life of approximately 10 minutes, displaying distribution kinetics consistent with a two compartment model. TFO-1 was also readily absorbed into circulation from the peritoneal cavity. All tissues examined except brain accumulated the compound reaching concentrations calculated to be in the micromolar range. TFO-1 was found to be stable in circulation and in tissues in that a large fraction of intact material was detected 8 hours after injection, as assessed by gel electrophoresis. Approximately 20–30% of the injected dose was excreted in the urine over an 8 hour period. These results suggest that G-rich oligonucleotides, minimally modified at the 3' end, are relatively stable in vivo and have distribution kinetics favorable to use as therapeutic agents.


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