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Dive into the research topics where Mi-Young Chae is active.

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Featured researches published by Mi-Young Chae.


Biochemical Pharmacology | 1998

O6-Alkylguanine-DNA Alkyltransferase Inactivation by Ester Prodrugs of O6-Benzylguanine Derivatives and their Rate of Hydrolysis by Cellular Esterases

M. Eileen Dolan; Sandip K. Roy; Bonnie J. Garbiras; Paul Helft; Phil Paras; Mi-Young Chae; Robert C. Moschel; Anthony E. Pegg

To modulate the bioavailability and perhaps improve the tumor cell selectivity of O6-alkylguanine-DNA alkyltransferase (AGT) inactivators, pivaloyloxymethyl ester derivatives of O6-benzylguanine (BG) were synthesized and tested as AGT inactivators and as substrates for cellular esterases. The potential prodrugs examined were the 7- and 9-pivaloyloxymethyl derivatives of O6-benzylguanine (7- and 9-esterBG), and of 8-aza-O6-benzylguanine (8-aza-7-esterBG and 8-aza-9-esterBG) and the 9-pivaloyloxymethyl derivative of 8-bromo-O6-benzylguanine (8-bromo-9-esterBG). The benzylated purines were all potent inactivators of the pure AGT and of the AGT activity in HT29 cells and cell extracts. Each ester was at least 75 times less potent than the corresponding benzylated purine against the pure human AGT. In contrast, the activities of esters and their respective benzylated purine were similar in crude cell extracts and in intact cells. The increase in potency of esters in cellular extracts could be explained by a conversion of the respective prodrug to the more potent benzylated purine in the presence of cellular esterases. The apparent catalytic activity (Vmax/Km) of liver microsomal esterase for 8-azaBG ester prodrugs was 70-130 times greater than for BG prodrugs and 10-20 times greater than for 8-bromo-9-esterBG. Tumor cell hydrolysis of the esters varied considerably as a function of cell type and prodrug structure. These data suggest that these or related prodrugs may be advantageous for selective AGT inactivation in certain tumor types.


Journal of Medicinal Chemistry | 1995

8-Substituted O6-benzylguanine, substituted 6(4)-(benzyloxy)pyrimidine, and related derivatives as inactivators of human O6-alkylguanine-DNA alkyltransferase.

Mi-Young Chae; K. Swenn; Sreenivas Kanugula; Dolan Me; Anthony E. Pegg; R. C. Moschel


Journal of Medicinal Chemistry | 1994

Substituted O6-benzylguanine derivatives and their inactivation of human O6-alkylguanine-DNA alkyltransferase.

Mi-Young Chae; McDougall Mg; Dolan Me; K. Swenn; Anthony E. Pegg; R. C. Moschel


Cancer Research | 1994

Metabolism of O6-Benzylguanine, an Inactivator of O6-Alkylguanine-DNA Alkyltransferase

Dolan Me; Mi-Young Chae; Anthony E. Pegg; J. H. Mullen; Henry S. Friedman; R. C. Moschel


Archive | 1999

Substituted o6 -benzylguanines

Robert C. Moschel; Anthony E. Pegg; M. Eileen Dolan; Mi-Young Chae


Cancer Research | 1995

Specific Labeling of O6-Alkylguanine-DNA Alkyltransferase by Reaction with O6-(p-Hydroxy[3H]methylbenzyl)guanine

Gina M. Ciocco; Robert C. Moschel; Mi-Young Chae; Patricia J. McLaughlin; Ian S. Zagon; Anthony E. Pegg


Archive | 1995

Substituted 6(4)-benzyloxypyrimidines

Robert C. Moschel; Anthony E. Pegg; Eilleen M. Dolan; Mi-Young Chae


Archive | 1995

Substituted o6-benzylguanines and use thereof

Robert C. Moschel; Anthony E. Pegg; M. Eileen Dolan; Mi-Young Chae


Archive | 1995

6(4)-BENCILOXIPIRIMIDINAS SUSTITUIDAS.

Mi-Young Chae; Eilleen M. Dolan; Robert C. Moschel; Anthony E. Pegg


Archive | 1995

O6-benzylguanines substituees et 6(4)benzyloxypyrimidines substituees

Robert C. Moschel; Anthony E. Pegg; M. Eileen Dolan; Mi-Young Chae

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Anthony E. Pegg

United States Department of Commerce

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Robert C. Moschel

National Institutes of Health

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M. Eileen Dolan

National Institutes of Health

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Dolan Me

Pennsylvania State University

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Eilleen M. Dolan

National Institutes of Health

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R. C. Moschel

Pennsylvania State University

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Ian S. Zagon

Pennsylvania State University

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