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Biocell - Antiviral and immunomodulatory activities of synthetic stigmastane analogs

Congress

Authorship
ALCHE, LAURA EDITH
Date
2012
Publishing House and Editing Place
Instituto de Histología y Embriología "Dr. Mario H. Burgos" (IHEM-CONICET). Facultad de Cs. Médicas, U.N. Cuyo, Mendoza
ISSN
0327-9545
Summary Information provided by the agent in SIGEVA
The stigmastane analog (22S,23S)-22,23-dihydroxystigmast-4-en-3-one (compound 1) displays antiviral activity in vitro against Herpes Simplex Virus Type 1 (HSV-1). The compound also significantly diminishes proinflammatory cytokines production in inflammatory cells. The 3-keto group and the double bond in 4 in the steroid A ring provide the molecule with structural similarities to that of corticosteroids. In order to improve the immunomodulatory activity of this molecule, we designed new... The stigmastane analog (22S,23S)-22,23-dihydroxystigmast-4-en-3-one (compound 1) displays antiviral activity in vitro against Herpes Simplex Virus Type 1 (HSV-1). The compound also significantly diminishes proinflammatory cytokines production in inflammatory cells. The 3-keto group and the double bond in 4 in the steroid A ring provide the molecule with structural similarities to that of corticosteroids. In order to improve the immunomodulatory activity of this molecule, we designed new stigmastane analogs, keeping the (22S,23S)-22,23-dihydroxylated side chain of the steroidal structure, responsible of the antiviral activity, and introducing an additional double bond in 1 and/or a fluorine atom in the molecule, structural features known to improve the anti-inflammatory activity of steroidal drugs. The presence of the 1-4 ceto in the stigmastane structure reduced anti HSV-1 activity and did not improve the immunomodulatory effect of the compound. However, a fluorine atom in C6 enhanced both antiviral and immunosuppressive activities of the new compounds, since they were more effective than compound 1 to reduce virus yields in epithelial cells infected with HSV-1 and cytokine production in inflammatory cells, as determined by virus yield reduction assays and ELISA, respectively. Radioligand binding assays and reporter gene induction assays showed that the stigmastane analogs did not exhibit affinity for the glucocorticoids and mineralocorticoid receptors. The compounds would be exerting their effect through a mechanism of action different from that of commercial anti-inflammatory steroidal drugs.
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Key Words
HSV-1STIGMASTANE ANALOGSIMMUNOMODULATORYANTIVIRAL