A new class of hydrogen sulfide (H 2S)-donating hybrids combined with pharmacologically active compounds is presented in this article. The pharmacological profiles of some hybrid lead compounds in the areas of inflammation, H 2S-donating diclofenac (ACS 15); cardiovascular, H 2S-donating aspirin (ACS 14); urology, H 2S-donating sildenafil (ACS 6); and neurodegenerative, H 2S-donating latanoprost (ACS 67) for glaucoma treatment and H 2S-donating levodopa (ACS 84) for Parkinsons disease, are described. The new H 2S-releasing hybrids demonstrate remarkable improvement in activity and tolerability as compared with the related parent compounds, suggesting an active pharmacological role for H 2S. Finally the mechanism(s) of action of glutathione-dependent and independent, and of gas (H 2S) release (spontaneous or enzymatic) and its implications for clinical pharmacology perspectives will be also discussed.

Therapeutic potential of new hydrogen sulfide-releasing hybrids / A. Sparatore, G. Santus, D. Giustarini, R. Rossi, P. Del Soldato. - In: EXPERT REVIEW OF CLINICAL PHARMACOLOGY. - ISSN 1751-2433. - 4:1(2011 Jan), pp. 109-121. [10.1586/ecp.10.122]

Therapeutic potential of new hydrogen sulfide-releasing hybrids

A. Sparatore;
2011

Abstract

A new class of hydrogen sulfide (H 2S)-donating hybrids combined with pharmacologically active compounds is presented in this article. The pharmacological profiles of some hybrid lead compounds in the areas of inflammation, H 2S-donating diclofenac (ACS 15); cardiovascular, H 2S-donating aspirin (ACS 14); urology, H 2S-donating sildenafil (ACS 6); and neurodegenerative, H 2S-donating latanoprost (ACS 67) for glaucoma treatment and H 2S-donating levodopa (ACS 84) for Parkinsons disease, are described. The new H 2S-releasing hybrids demonstrate remarkable improvement in activity and tolerability as compared with the related parent compounds, suggesting an active pharmacological role for H 2S. Finally the mechanism(s) of action of glutathione-dependent and independent, and of gas (H 2S) release (spontaneous or enzymatic) and its implications for clinical pharmacology perspectives will be also discussed.
biomarker; dithiolethione; gaseous transmitter; glutathione; H 2S-donating hybrids; hydrogen sulfide
Settore CHIM/08 - Chimica Farmaceutica
gen-2011
Article (author)
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/159132
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