Pierre Le Ber scite author profile

A series of oligopeptides have been synthesized that are structurally related to the natural agent netropsin. The binding constants to double-stranded polynucleotides as well as the cytostatic activity against both murine human tumor cell lines and the in vitro activity against a range of DNA and RNA viruses have been determined for these novel compounds and some of their synthetic precursors. 1-Methyl-5-nitropyrrole-2-carboxylic acid methyl ester (4), N-[[1-methyl-4-(1-methyl-4-nitropyrrole-2-carboxamido)pyrrol-2- yl]carbonyl]-L-alanine tert-butyl ester (28), and N-[[1-methyl-4-(1-methyl-4-nitropyrrole-2-carboxamido)pyrrol-2- yl]carbonyl]-L-alanyl-L-alanine tert-butyl ester (29) showed modest inhibitory effect on tumor cell proliferation (CD50 = 26-85 micrograms/mL). Of all the compounds that were evaluated, 28 proved the most potent antiviral agent. It was inhibitory to parainfluenza-3 virus and Coxsackie virus B4 in Vero cells at a concentration of 20 micrograms/mL.

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Synthesis of potentially antiviral cyclopropyl nucleosides

Cluet¹,

Haudrechy²,

Ber³

et al. 1994

Synlett

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Spin-labeled oxazolopyridocarbazole as a probe for studying nonintercalating DNA groove binding ligands

Carrier

Ber²,

Auclair³

1990

Biochemistry

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A spin-label (P-OPC) composed of the nitroxide-containing ring proxyl linked at the C1 position of the intercalating fluorescent chromophore oxazolopyridocarbazole (OPC) has been synthesized. The spin-labeled OPC was found to interact with DNA and polynucleotides according to an external minor groove binding mode with association constant values Kapp ranging from 10(5) to 10(6) M-1. External binding was obvious from the inability of P-OPC to increase the length of sonicated DNA upon binding, the low unwinding angle (9.6 degrees) of circular PM2 DNA, and the low energy transfer from DNA bases to bound chromophore. Binding of P-OPC to DNA or polynucleotide results in a strong immobilization of the proxyl moiety, resulting in the appearance of an asymmetric and broad ESR spectrum with a maximal hyperfine splitting of 56.5 G. In the equilibrium conditions, the occurrence of superimposed ESR spectra related to the P-OPC fraction undergoing rapid motion and to the P-OPC fraction immobilized allows the estimation of the concentrations of free and DNA-bound spin-label. The external mode of binding to DNA as well as the characteristics of the ESR spectra make P-OPC suitable for the determination of DNA binding parameters of nonintercalating ligands using competition experiments. The measurement of the binding constants of distamycin A to poly[d(A-T)] and poly[d(G-C)] is taken as an example.

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Synthesis, DNA binding properties and biological evaluation of novel oligo-meta-benzamides related to netropsin

Debart

Gosselin

Rayner

et al. 1991

European Journal of Medicinal Chemistry

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Pierre Le Ber

Bicyclic imidazo derivatives, a new class of highly selective inhibitors for the human immunodeficiency virus type 1

Synthesis, DNA binding and biological evaluation of synthetic precursors and novel analogs of netropsin

Synthesis of potentially antiviral cyclopropyl nucleosides

Spin-labeled oxazolopyridocarbazole as a probe for studying nonintercalating DNA groove binding ligands

Synthesis, DNA binding properties and biological evaluation of novel oligo-meta-benzamides related to netropsin

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