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Dive into the research topics where Robert Ian Dowell is active.

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Featured researches published by Robert Ian Dowell.


European Journal of Cancer | 2002

DNA interstrand cross-linking and TP53 status as determinants of tumour cell sensitivity in vitro to the antibody-directed enzyme prodrug therapy ZD2767

Noel R. Monks; David C. Blakey; Simon J. East; Robert Ian Dowell; Joanne A. Calvete; Nicola J. Curtin; Ce Arris; David R. Newell

Cellular determinants of sensitivity to the bifunctional alkylating agent 4-[N,N-bis(2-iodoethyl)amino]phenol (ZD2767D), the active drug produced by ZD2767 antibody-directed enzyme prodrug therapy (ADEPT), were studied. The prodrug 4-[N,N-bis(2-iodoethyl)amino]phenoxycarbonyl L-glutamic acid (ZD2767P)+activating enzyme carboxypeptidase G2 (CPG2) displayed growth inhibitory activity (IC(50) 0.04-2.2 microM) in colorectal tumour and non-small cell lung cancer (NSCLC) cell lines, and was more potent than a monofunctional ZD2767D analogue (colorectal cell lines-IC(50) 18-38 microM), synthesized for the first time. ZD2767P + CPG2 rapidly formed DNA-DNA interstrand cross-links (maximal at 10 min), and semi-quantitative analyses indicate that levels were similar in 3 of 4 cell lines studied (25-75 rad equivalents) at equitoxic (10 x IC(50)/LC(50)) concentrations. In matched HCT116 TP53 functional/non-functional cell lines, there was no significant difference in the sensitivity to ZD2767P+CPG2. Together, these results suggest that cellular sensitivity to ZD2767P+CPG2 is, in part, related to the levels of interstrand crosslinks, but that TP53 status does not markedly effect chemosensitivity.


Journal of Medicinal Chemistry | 1995

Optimization of alkylating agent prodrugs derived from phenol and aniline mustards: a new clinical candidate prodrug (ZD2767) for antibody-directed enzyme prodrug therapy (ADEPT).

Caroline J. Springer; Robert Ian Dowell; Philip J. Burke; Elma Hadley; D. Huw Davies; David C. Blakey; Roger G. Melton; Ion Niculescu-Duvaz


Journal of Medicinal Chemistry | 1992

Methoxytetrahydropyrans. A new series of selective and orally potent 5-lipoxygenase inhibitors

Graham Charles Crawley; Robert Ian Dowell; Philip Neil Edwards; Stephen J. Foster; Rodger M. McMillan; Edward R. H. Walker; David Waterson; T. Geoffrey C. Bird; Pierre Bruneau; Jean Marc Girodeau


Cancer Research | 1996

ZD2767, an Improved System for Antibody-directed Enzyme Prodrug Therapy That Results in Tumor Regressions in Colorectal Tumor Xenografts

David C. Blakey; Philip J. Burke; David H. Davies; Robert Ian Dowell; Simon J. East; Kay Eckersley; John Edward Fitton; John McDaid; Roger G. Melton; Ion Niculescu-Duvaz; Philip E. Pinder; Sk Sharma; Andrew F. Wright; Caroline J. Springer


Journal of Medicinal Chemistry | 1992

Novel inhibitors of prolyl 4-hydroxylase

Robert Ian Dowell; Elizabeth M. Hadley


Journal of Medicinal Chemistry | 1996

New Mustard Prodrugs for Antibody-Directed Enzyme Prodrug Therapy: Alternatives to the Amide Link

Robert Ian Dowell; Caroline J. Springer; Davies Dh; Hadley Em; Philip J. Burke; Boyle Ft; Roger G. Melton; Connors Ta; David C. Blakey; Anthony Mauger


Archive | 1994

Prodrugs for antibody directed enzyme prodrug therapy

Philip J. Burke; Robert Ian Dowell; Anthony Mauger; Caroline Joy Springer


Archive | 1995

Process for antibody directed enzyme prodrug therapy

Philip J. Burke; Robert Ian Dowell; Anthony Mauger


Archive | 1991

Cyclic ether derivatives.

Pierre Bruneau; Robert Ian Dowell; David Waterson


Archive | 1993

Amino acid linked nitrogen mustard derivatives and their use as prodrugs in the treatment of tumours

Philip J. Burke; Robert Ian Dowell; Anthony Mauger; Caroline Joy Springer

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Anthony Mauger

National Institutes of Health

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