AI Article Synopsis
- The study focused on synthesizing new biphenyl derivatives and evaluating their antiviral activity against specific viruses, particularly coxsackievirus B3 and human rhinoviruses.
- A novel synthesis method using Suzuki coupling reaction was developed, leading to compounds that showed significant antiviral effects, particularly against CVB3 and HRV-2, while being ineffective against HRV-14.
- Overall, the findings suggest that biphenyloxyisoxazole derivatives could be potential treatments for infections caused by HRV-2 and CVB3.
Article Abstract
Objectives: During this study, novel biphenyl derivatives were synthesized and tested for antiviral activity.
Methods: A new method based on the Suzuki coupling reaction has been established for the synthesis of these polysubstituted chain systems. In parallel with cytotoxicity, the antiviral activity of biphenyl derivatives has been determined in cytopathic effect (CPE)-inhibitory assays with the pleconaril-resistant coxsackievirus B3 (CVB3) strain Nancy, human rhinovirus 2 (HRV-2) and 14 (HRV-14) and in plaque reduction assays with the pleconaril-sensitive human isolate CVB3 97-927 in HeLa cells. Based on the results from these investigations the selectivity index (SI) was determined as the ratio of the 50% cytotoxic concentration to the 50% inhibitory concentration.
Results: The new method based on the Suzuki coupling reaction includes the condensation of 2,6-dimethyl-4-bromophenol with pentyne chloride by means of potassium carbonate and potassium iodide in N-methylpyrrolidone-2 and yields 5-bromo-1,3-dimethyl-2-(4-pentynyloxy)benzene. Its condensation with methylacetaldoxime results in 3-methylisoxazole derivatives. The following reaction with different benzeneboronic acids by means of tetrakis(triphenylphosphine)-palladium(0) finally yields the corresponding derivatives. Several of the novel synthesized derivatives demonstrated a good antiviral activity on CVB3 (SI > 2 to > 37.5) and a strong anti-HRV-2 activity (SI > 50 to > 200). In contrast, none of the compounds inhibited the HRV-14-induced CPE.
Conclusions: These results indicate that [(biphenyloxy)propyl]isoxazole derivatives are potential inhibitors of HRV-2 and CVB3 replication, and make them promising agents for the specific treatment of these virus infections.
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Article Synopsis
- The study focused on synthesizing new biphenyl derivatives and evaluating their antiviral activity against specific viruses, particularly coxsackievirus B3 and human rhinoviruses.
- A novel synthesis method using Suzuki coupling reaction was developed, leading to compounds that showed significant antiviral effects, particularly against CVB3 and HRV-2, while being ineffective against HRV-14.
- Overall, the findings suggest that biphenyloxyisoxazole derivatives could be potential treatments for infections caused by HRV-2 and CVB3.
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