Antiviral Activity of N-Phenyl-N′-arylthiourea Derivatives against some Rhinoviruses

Galabov, Angel S.; Velichkova, E; Vassilev, G. N.

doi:10.1159/000221975

Cited by 13 publications

(3 citation statements)

References 17 publications

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“…The search for effective antirhinovirus agents has yielded a wealth of compounds belonging to widely varying chemical classes: thiosemicarbazones (20), isoquinolines (35,43), triazinoindoles (27), guanidines (5), benzoates (30), furanyls (2), benzimidazoles (12), thiourea (18), diketones (14,16,17), flavans (3,32), flavones (25), chalcones (24), nitrobenzenes (34,41), and isoxazoles (15,31). The most recently developed antirhinovirus compounds (3,15,24,31) reach their MICs within the range of 0.001 to 0.01 ,ug/ml.…”

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confidence: 99%

Antirhinovirus activity of purine nucleoside analogs

Clercq¹,

Bernaerts²,

Bergstrom³

et al. 1986

Antimicrob Agents Chemother

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A wide variety of purine nucleoside (mainly tubercidin and adenosine) analogs, which had previously been shown to inhibit the replication of a broad spectrum of RNA viruses, were evaluated for their antirhinovirus activity in human diploid (WI-38) fibroblasts. Tubercidin, 5-(l-hydroxyethyl)tubercidin, 5-(2-buten-lyl)tubercidin, toyocamycin, and sangivamycin emerged as the most potent inhibitors. These compounds inhibited the replication of rhinovirus types 1A, 1B, and 9 at an MIC well below 1 ,ug/ml. However, these compounds proved cytotoxic for the uninfected host cells at concentrations which were only slightly higher (3-to 10-fold, on the average) than those required for inhibition of rhinovirus replication. The most selective inhibitor of rhinovirus replication was 3-deazaguanine, with a selectivity index of 50. None of the carbocyclic and acyclic analogs of adenosine tested exhibited a potent or selective antirhinovirus activity.The search for effective antirhinovirus agents has yielded a wealth of compounds belonging to widely varying chemical classes: thiosemicarbazones

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mentioning

confidence: 99%

Antirhinovirus activity of purine nucleoside analogs

Clercq¹,

Bernaerts²,

Bergstrom³

et al. 1986

Antimicrob Agents Chemother

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“…36) are inhibitors of coxsackie virus, poliovirus, FMDV and rhinoviruses. Drug concentrations of approximately 2/~g/mL of N-phenyl-N'-3hydroxyphenyl-thiourea (PTU-23) reduced rhinovirus growth by one-log (Galabov et al, 1977). The potency and antiviral index of N-phenyl-N'-arylthiourea are rather low and probably these compounds block an early step of rhinovirus replication after adsorption (Galabov et al, 1977;Galabov, 1979).…”

Section: Tenuazonic Acidmentioning

confidence: 99%

“…Drug concentrations of approximately 2/~g/mL of N-phenyl-N'-3hydroxyphenyl-thiourea (PTU-23) reduced rhinovirus growth by one-log (Galabov et al, 1977). The potency and antiviral index of N-phenyl-N'-arylthiourea are rather low and probably these compounds block an early step of rhinovirus replication after adsorption (Galabov et al, 1977;Galabov, 1979). PTU-23 had activity against coxsackie infection in mice, whereas another derivative (PTU-24) was active against FMDV in mice and guinea pigs (Galabov, 1979).…”

Section: Tenuazonic Acidmentioning

confidence: 99%

Picornavirus inhibitors

Carrasco

1994

Pharmacology & Therapeutics

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Picornaviruses are among the best understood animal viruses in molecular terms. A number of important human and animal pathogens are members of the Picornaviridae family. The genome organization, the different steps of picornavirus growth and numerous compounds that have been reported as inhibitors of picornavirus functions are reviewed. The picornavirus particles and several agents that interact with them have been solved at atomic resolution, leading to computer-assisted drug design. Picornavirus inhibitors are useful in aiding a better understanding of picornavirus biology. In addition, some of them are promising therapeutic agents. Clinical efficacy of agents that bind to picornavirus particles has already been demonstrated.

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Synthesis of n-glycosylthioureas, N-glycosylrhodanines, and N-glycosyl-2-aminothiazoles and their Antimicrobial Activity

Foye

1981

Journal of Pharmaceutical Sciences

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Antiviral Activity of N-Phenyl-N′-arylthiourea Derivatives against some Rhinoviruses

Cited by 13 publications

References 17 publications

Antirhinovirus activity of purine nucleoside analogs

Antirhinovirus activity of purine nucleoside analogs

Picornavirus inhibitors

Synthesis of n-glycosylthioureas, N-glycosylrhodanines, and N-glycosyl-2-aminothiazoles and their Antimicrobial Activity

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