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PABA/NO as an anticancer lead: Analogue synthesis, structure revision, solution chemistry, reactivity toward glutathione, and in vitro activity

  1. Author:
    Saavedra, J. E.
    Srinivasan, A.
    Buzard, G. S.
    Davies, K. M.
    Waterhouse, D. J.
    Inami, K.
    Wilde, T. C.
    Citro, M. L.
    Cuellar, M.
    Deschamps, J. R.
    Parrish, D.
    Shami, P. J.
    Findlay, V. J.
    Townsend, D. M.
    Tew, K. D.
    Singh, S.
    Jia, L.
    Ji, X. H.
    Keefer, L. K.

  2. Author Address

    Natl Canc Inst, Basi Res Program, SAIC Frederick, Chem Sect,Lab Comparat Carcinogenesis, Ft Detrick, MD 21702 USA. Natl Canc Inst, Biomol Struct Sect, Macromol Crystallog Lab, Ft Detrick, MD 21702 USA. George Mason Univ, Dept Chem, Fairfax, VA 22030 USA. USN, Res Lab, Struct Matter Lab, Washington, DC 20375 USA. Univ Utah, Dept Internal Med, Div Med Oncol, Salt Lake City, UT 84112 USA. Med Univ S Carolina, Dept Cell & Mol Pharmacol & Expt Therapeut, Charleston, SC 29425 USA. Univ Pittsburgh, Inst Canc, Dept Pharmacol, Pittsburgh, PA 15213 USA. NCI, Dev Therapeut Program, Bethesda, MD 20892 USA Keefer, LK, Natl Canc Inst, Basi Res Program, SAIC Frederick, Chem Sect,Lab Comparat Carcinogenesis, Ft Detrick, MD 21702 USA
    1. Year: 2006
    2. Date: FEB 9
  2. Journal: Journal of Medicinal Chemistry
    1. 49
    2. 3
    3. Pages: 1157-1164
  4. Type of Article: Article
  1. Abstract:

    PABA/NO is a diazeniumdiolate of structure Me2NN(O)=NOAr (where Ar is a 5-substituted-2,4-dinitrophenyl ring whose 5-substituent is N-methyl-p-aminobenzoic acid). It has shown activity against human ovarian cancer xenografts in mice rivaling that of cisplatin, but it is poorly soluble and relatively unstable in water. Here we report structure-based optimization efforts resulting in three analogues with improved solubility and stability in aqueous solution. We sought to explain PABA/NO's physicochemical uniqueness among these four compounds, whose aminobenzoic acid precursors differ structurally only in the presence or absence of the N-methyl group and/or the position of the carboxyl moiety (meta or para). Studies revealed that PABA/NO's N-methyl-p-aminobenzoic acid substituent is bound to the dinitrobenzene ring via its carboxyl oxygen while the other three are linked through the aniline nitrogen. This constitutes a revision of the previously published PABA/NO structure. All four analogues reacted with GSH to produce bioactive nitric oxide (NO), but PABA/NO was the most reactive. Consistent with PABA/NO's potent suppression of A2780 human ovarian cancer xenograft growth in mice, it was the most potent of the four in the OVCAR-3 cell line

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  2. WOS: 000235826300033

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