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Featured researches published by Joseph Sam.


Journal of Biological Chemistry | 1998

Sequence-specific Changes in the Metal Site of Ferric Bleomycin Induced by the Binding of DNA

Joseph Sam; Satoshi Takahashi; Istvan Lippai; Jack Peisach; Denis L. Rousseau

The binding of the iron complex of the antineoplastic glycopeptide bleomycin A2(Fe-BLM) to calf thymus DNA and the self-complementary oligonucleotides d(CGCGCG) and d(ATATAT) has been studied using optical, EPR, and resonance Raman spectroscopies. An increase in the intensity of the bands at 365 and 384 nm is observed in the optical spectrum of Fe(III)-BLM when the drug binds to either oligonucleotide. However, in the presence of phosphate, this increase is observed only with d(CGCGCG) and not with d(ATATAT). In addition, the gmax feature in the EPR spectrum of low spin Fe(III)-BLM is narrowed in a way suggesting a reduction of possible conformers that the drug can achieve when it is bound to d(CGCGCG) or to calf thymus DNA but not when bound to d(ATATAT). When Fe(III)-BLM is bound to d(CGCGCG), changes in the resonance Raman spectrum of the metal drug complex suggest conformational changes in three of the ligands to iron: the β-hydroxyhistidyl amide, the pyrimidine, and the axial hydroxide. In addition, the Fe-OH band undergoes narrowing, again consistent, with the reduction of conformers of the drug. No such resonance Raman changes are observed upon binding to d(ATATAT). The changes in the pyrimidine modes upon binding d(CGCGCG) to the drug are consistent with a recently proposed model (Wu, W., Vanderwall, D. E., Turner, C. J., Kozarich, J. W., and Stubbe, J. (1996) J. Am. Chem. Soc. 118, 1281–1294) of DNA recognition by activated bleomycin, HOO-Fe(III)-BLM, in which the pyrimidine moiety of the drug is important for the preferential cleavage of 5′-GpPy-3′ sequences.


Journal of the American Chemical Society | 1994

Electrospray Mass Spectrometry of Iron Bleomycin: Demonstration That Activated Bleomycin Is a Ferric Peroxide Complex

Joseph Sam; Xue-Jun Tang; Jack Peisach


Journal of the American Chemical Society | 1995

Electrospray Mass Spectrometry of Iron Bleomycin II: Investigation of the Reaction of Fe(III)-Bleomycin with Iodosylbenzene

Joseph Sam; Xue-Jun Tang; Richard S. Magliozzo; Jack Peisach


Journal of Pharmaceutical Sciences | 1964

Benzoxazoles: Potent Skeletal Muscle Relaxants

Joseph Sam; James N. Plampin


Journal of the American Chemical Society | 1994

STRUCTURAL CHARACTERIZATION OF IRON-BLEOMYCIN BY RESONANCE RAMAN SPECTROSCOPY

Satoshi Takahashi; Joseph Sam; Jack Peisach; Denis L. Rousseau


Journal of the American Chemical Society | 1960

Hypotensive Basic Ethers in the Indan Series1

Joseph Sam; James N. Plampin


Journal of Medicinal Chemistry | 1973

2-Aminoindans of pharmacological interest.

Everett Solomons; Joseph Sam


Biochemistry | 1993

EPR spectroscopic investigation of the lability of oxygen in activated bleomycin: implications for the mechanism of bleomycin-mediated DNA degradation.

Joseph Sam; Jack Peisach


Journal of Medicinal Chemistry | 1969

Epimeric 2-hydroxy-2-phenylquinolizidines

Joseph Sam; James Don England; Davis L Temple


Journal of the American Chemical Society | 1951

A Thiophene Isostere of 2-Methyl-1-indanone

J. H. Burckhalter; Joseph Sam

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Jack Peisach

Albert Einstein College of Medicine

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Davis L Temple

University of Mississippi

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Denis L. Rousseau

Albert Einstein College of Medicine

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A.J. Bej

University of Rhode Island

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C.W. Richmond

University of Mississippi

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Dorothy M. Nobles

North Dakota State University

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Istvan Lippai

Albert Einstein College of Medicine

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