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Dive into the research topics where James B. Springer is active.

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Featured researches published by James B. Springer.


Cancer Chemotherapy and Pharmacology | 2000

Evidence for a role of chloroethylaziridine in the cytotoxicity of cyclophosphamide

James L. Flowers; Susan M. Ludeman; Michael P. Gamcsik; O. Michael Colvin; Kai-Liu Shao; Jila H. Boal; James B. Springer; David J. Adams

Abstract A number of investigators have observed that the use of 4-hydroperoxycyclophosphamide (4-HC) in multiwell plate cytotoxicity assays can be associated with toxicity to cells in wells that contain no drug. Previous reports have implicated diffusion of 4-HC decomposition products, and acrolein in particular, as the active species. Purpose: The purpose of this study was to elucidate the species responsible for the airborne cytotoxicity of 4-HC, and to devise ways to minimize such effects in chemosensitivity assays. Methods: To this end, analogues of 4-HC were synthesized to identify the contributions of individual cyclophosphamide metabolites to cytotoxicity. The analogues were then tested for activity against three human breast tumor cell lines (including a line resistant to 4-HC), and one non-small-cell lung carcinoma line. Cytotoxicity was evaluated by assays that quantitate cellular metabolism and nucleic acid content. Results: Didechloro-4-hydroperoxycyclophosphamide, a compound that generates acrolein and a nontoxic analogue of phosphoramide mustard, gave no cross-well toxicity. In contrast, a significant neighboring well effect was observed with phenylketophosphamide, a compound that generates phosphoramide mustard but not acrolein. Addition of authentic chloroethylaziridine reproduced the airborne toxicity patterns generated by 4-HC and phenylketophosphamide. Increasing the buffering capacity of the growth medium and sealing the microtiter plates prevented airborne cytotoxicity. Conclusions: Since it is unlikely that phosphoramide mustard is volatile, these findings implicate chloroethylaziridine rather than acrolein as the volatile metabolite of 4-HC that is responsible for airborne cytotoxicity. The fact that chloroethylaziridine is generated in amounts sufficient to volatilize, diffuse across wells and cause cytotoxicity indicates that it is an important component in the overall cytotoxicity of 4-HC in vitro. Furthermore, these findings suggest that chloroethylaziridine may also contribute to the toxicity of cyclophosphamide in vivo.


Journal of Organic Chemistry | 1998

Isophosphoramide Mustard and Its Mechanism of Bisalkylation.

James B. Springer; Michael E. Colvin; and O. Michael Colvin; Susan M. Ludeman


Journal of Organic Chemistry | 1999

PENTADIENYLNITROBENZYL AND PENTADIENYLNITROPIPERONYL PHOTOCHEMICALLY REMOVABLE PROTECTING GROUPS

Michael C. Pirrung; Yong Rok Lee; Kaapjoo Park; James B. Springer


Journal of Organic Chemistry | 1996

Synthesis and Characterization of In-Plane and Out-of-Plane Enone−Lewis Acid Complexes: Implications for Diels−Alder Reactions1

D. K. Singh; James B. Springer; Patricia A. Goodson; Robert C. Corcoran


Journal of Organic Chemistry | 1996

Reactive Geometries in Lewis Acid-Mediated Diels−Alder Reactions: Insights from Covalently Attached Acids1

James B. Springer; Robert C. Corcoran


Cancer Chemotherapy and Pharmacology | 2003

Selective enhancement of ifosfamide-induced toxicity in Chinese hamster ovary cells.

Sonali M. Smith; Susan M. Ludeman; Lynette R. Wilson; James B. Springer; Mihir C. Gandhi; M. Eileen Dolan


Journal of Labelled Compounds and Radiopharmaceuticals | 2007

Labeled oxazaphosphorines for applications in MS studies. Synthesis of deuterium labeled cyclophosphamides and ifosfamides

James B. Springer; O. Michael Colvin; Susan M. Ludeman


Journal of Pharmaceutical Sciences | 2002

Exposure to a deuterated analogue of phenylbutyrate retards S-phase progression in HT-29 colon cancer cells.

Kevin Clarke; Susan M. Ludeman; James B. Springer; O. Michael Colvin; Michael A. Lea; Lawrence E. Harrison


Archive | 2008

method of treating neuroblastoma

Susan M. Ludeman; Michael P. Gamcsik; Timothy A. Driscoll; James B. Springer; O. Michael Colvin; David J. Adams; Karel Base


Chemical Research in Toxicology | 2004

1,3- vs 1,5-intramolecular alkylation reactions in isophosphoramide and phosphoramide mustards

James B. Springer; Young H. Chang; Kyo I. Koo; O. Michael Colvin; Michael E. Colvin; M. Eileen Dolan; Shannon M. Delaney; James L. Flowers; Susan M. Ludeman

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Michael P. Gamcsik

North Carolina State University

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Michael E. Colvin

Lawrence Livermore National Laboratory

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C. Bryce Johnson

North Carolina State University

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Collin R. Dempsey

Albany College of Pharmacy and Health Sciences

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