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Dive into the research topics where P. Dan Cook is active.

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Featured researches published by P. Dan Cook.


Biochemical Pharmacology | 1985

Biochemical and antitumor activity of tiazofurin and its selenium analog (2-β-D-ribofuranosyl-4-selenazolecarboxamide)

Theodore J. Boritzki; David A. Berry; Judith A. Besserer; P. Dan Cook; David W. Fry; Wilbur R. Leopold; Robert C. Jackson

2-beta-D-Ribofuranosyl-4-selenazolecarboxamide (selenazofurin, CI-935), the selenium analog of tiazofurin (CI-909), was 3- to 10-fold more cytotoxic to murine or human tumor cells in vitro than tiazofurin and was also more active against P388 mouse leukemia in vivo. In vitro cytotoxicity could be reversed by guanosine or guanine but not by other purine nucleosides or bases. Three human tumor cell lines selected for selenazofurin or tiazofurin resistance showed cross resistance between selenazofurin and tiazofurin. Treatment with tiazofurin, selenazofurin, or mycophenolic acid decreased guanylate pools and caused an accumulation of IMP in WIL2 human lymphoma cells. The decrease in guanylate pools was accompanied by inhibition of RNA and DNA synthesis. The NAD analogs of tiazofurin and selenazofurin were inhibitors of L1210 IMP dehydrogenase (IMP:NAD oxidoreductase, EC 1.2.1.14), and both showed uncompetitive inhibition with respect to NAD having Kii values of 5.7 X 10(-8)M and 3.3 X 10(-8)M respectively.


Antiviral Research | 1986

Effect of selenazofurin on influenza A and B virus infections of mice

Robert W. Sidwell; John H. Huffman; Evan W. Call; Hassan A. Alaghamandan; P. Dan Cook; Roland K. Robins

The inhibitory effects of selenazofurin and ribavirin on influenza A and B virus infections in mice were compared. Both compounds, when administered intraperitoneally (i.p.), reduced lung consolidation and prolonged mean day of death, but ribavirin more effectively increased survivor number and lowered lung viral hemagglutinin (HA) titers. Lung HA titers often increased in selenazofurin-treated animals. To determine the most appropriate i.p. treatment schedule, influenza A virus-infected mice were treated once, twice or thrice daily for 7-9 days, or once only. Treatment once daily for 9 days beginning 4 h pre-virus exposure, for 3 days beginning 24 h post-virus exposure, or once only 48 h post-virus exposure was most effective. Body temperature, which usually declined during infection, increased to near-normal levels in animals treated with selenazofurin, especially in animals treated a single time or for 3 days with high dose levels. Selenazofurin was well tolerated at a dose of 50 mg/kg administered twice daily, and at 400 mg/kg administered once only. Rectal temperatures temporarily declined following every other day treatment with 400 mg/kg.


Antiviral Research | 1982

Evaluation of the anti-herpesvirus drug combinations: Virazole plus arabinofuranosylhypoxanthine and Virazole plus arabinofuranosyladenine

Lois B. Allen; Linda K. Vanderslice; Christina M. Fingal; Florah McCright; Elizabeth F. Harris; P. Dan Cook

Combinations of Virazole plus arabinofuranosylhypoxanthine (ara-Hx) and Virazole plus arabinofuranosyladenine (ara-A) were investigated in KB or BHK cells infected with types 1 or 2 herpes viruses. Combinations of Virazole and ara-Hx exhibited significant synergy as evaluated graphically (isobolograms) or by fractional inhibitory concentration (FIC) indices. Optimal ratios for the combination were 1:1 to 1:10 for Virazole to ara-Hx. At these ratios, FIC indices in the range of 0.5-0.2 were commonly observed. Combinations of Virazole and ara-A were antagonistic when observed in the presence of pentostatin, an adenosine deaminase inhibitor. In the absence of pentostatin, the minimum inhibitory concentration (MIC) of ara-A and degree of synergy with Virazole were variable.


Advances in Enzyme Regulation | 1989

Biochemical pharmacology and antitumor properties of 4-amino-8-[β--ribofuranosylamino]pyrimido-[5,4-d]pyrimidine

Robert C. Jackson; Theodore J. Boritzki; P. Dan Cook; Kenneth E. Hook; Wilbur R. Leopold; David W. Fry

Abstract 1. 1. APP is activated by adenosine kinase to its 5′-phosphate (APP-MP). 2. 2. APP-MP inhibits PRPP synthetase, and depletes cellular PRPP and purine and pyrimidine nucleotides. 3. 3. APP inhibits synthesis of DNA and RNA, and blocks cells in G1 phase of the cell cycle. 4. 4. APP retains full activity against MDR cells. 5. 5. APP is equally active against quiescent and proliferating CHO cells. 6. 6. APP has only weak activity against L1210 leukemia in vivo , but has substantial activity against mammary carcinoma 16/c. 7. 7. In vitro , APP has a relatively high ratio of solid tumor: leukemia activity.


Journal of Medicinal Chemistry | 1986

Synthesis, antimalarial activity, and quantitative structure-activity relationships of tebuquine and a series of related 5-[(7-chloro-4-quinolinyl)amino]-3-[(alkylamino)methyl] [1,1'-biphenyl]-2-ols and N omega-oxides.

Leslie M. Werbel; P. Dan Cook; Edward F. Elslager; Jocelyn Hung; Judith L. Johnson; Stephen J. Kesten; Dennis Joseph Mcnamara; Daniel F. Ortwine; Donald F. Worth


Journal of Heterocyclic Chemistry | 1986

A synthesis of 2-β-D-ribofuranosyl-4-selenazolecarboxamide (selenazofurin) and certain N-substituted amide derivatives suitable for large scale syntheses

P. Dan Cook; Dennis Joseph Mcnamara


Journal of Medicinal Chemistry | 1990

Synthesis, antitumor activity, and antiviral activity of 3-substituted 3-deazacytidines and 3-substituted 3-deazauridines

Dennis Joseph Mcnamara; P. Dan Cook; Lois B. Allen; Mary Jo Kehoe; Carolyn S. Holland; Annette G. Teepe


Journal of Medicinal Chemistry | 1987

Synthesis and antitumor activity of fluorine-substituted 4-amino-2(1H)-pyridinones and their nucleosides. 3-Deazacytosines.

Dennis Joseph Mcnamara; P. Dan Cook


Journal of Heterocyclic Chemistry | 1976

The synthesis of some pyrrolo[1,5‐b:2,3‐c′]dipyridazines

Fred V. Wells; Raymond N. Castle; P. Dan Cook


Antiviral Research | 1987

Inhibition of herpes simplex virus DNA replication by ara-tubercidin

Steven R. Turk; P. Dan Cook; C.Michael Reinke; John C. Drach

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Florah McCright

University of North Texas

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Fred V. Wells

Brigham Young University

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