6-substituted derivatives of carbovir: Anti-HIV activity

Robert Vince; John Kilama; Phuong T. Pham; Scott A. Beers; Bonnie J. Bowdon; Kathy A. Keith; William B. Parker

doi:10.1080/15257779508009751

6-substituted derivatives of carbovir: Anti-HIV activity

Robert Vince, John Kilama, Phuong T. Pham, Scott A. Beers, Bonnie J. Bowdon, Kathy A. Keith, William B. Parker

Center for Drug Design

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Abstract

A series of 6-alkoxy and 6-alkylamino carbovir derivatives were synthesized in order to evaluate prodrug approaches to increased bioavailability of the anti-HIV agent, carbovir. All of the compounds were active against HIV with the N-alkyl derivatives less active than the corresponding O-alkyl derivatives. The adenosine deaminase inhibitor, EHNA, had no effect on the anti-HIV activity of 6-propoxycarbovir, while the adenylic acid deaminase inhibitor, 2’ -deoxycoformycin, significantly decreased antiviral activity. These observations suggest that the 6-alkoxycarbovirs are metabolized directly to the monophosphates and are subsequently converted to carbovir monophosphate via adenylic acid deaminase.

Original language	English (US)
Pages (from-to)	1703-1708
Number of pages	6
Journal	Nucleosides and Nucleotides
Volume	14
Issue number	8
DOIs	https://doi.org/10.1080/15257779508009751
State	Published - 1995

Bibliographical note

Funding Information:
Acknowledgments. This work was supported by Public Health Service Grant CA23263 from the National Cancer Institute and Grant A129157 from the National Institute of Allergy and Infectious Diseases.

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abstract = "A series of 6-alkoxy and 6-alkylamino carbovir derivatives were synthesized in order to evaluate prodrug approaches to increased bioavailability of the anti-HIV agent, carbovir. All of the compounds were active against HIV with the N-alkyl derivatives less active than the corresponding O-alkyl derivatives. The adenosine deaminase inhibitor, EHNA, had no effect on the anti-HIV activity of 6-propoxycarbovir, while the adenylic acid deaminase inhibitor, 2{\textquoteright} -deoxycoformycin, significantly decreased antiviral activity. These observations suggest that the 6-alkoxycarbovirs are metabolized directly to the monophosphates and are subsequently converted to carbovir monophosphate via adenylic acid deaminase.",

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AU - Kilama, John

AU - Pham, Phuong T.

AU - Beers, Scott A.

AU - Bowdon, Bonnie J.

AU - Keith, Kathy A.

AU - Parker, William B.

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AB - A series of 6-alkoxy and 6-alkylamino carbovir derivatives were synthesized in order to evaluate prodrug approaches to increased bioavailability of the anti-HIV agent, carbovir. All of the compounds were active against HIV with the N-alkyl derivatives less active than the corresponding O-alkyl derivatives. The adenosine deaminase inhibitor, EHNA, had no effect on the anti-HIV activity of 6-propoxycarbovir, while the adenylic acid deaminase inhibitor, 2’ -deoxycoformycin, significantly decreased antiviral activity. These observations suggest that the 6-alkoxycarbovirs are metabolized directly to the monophosphates and are subsequently converted to carbovir monophosphate via adenylic acid deaminase.

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6-substituted derivatives of carbovir: Anti-HIV activity

Abstract

Bibliographical note

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