Publications by authors named "O Tabarrini"

Article Synopsis
  • * Researchers developed a compound, derivative 33, from a quinolone library that showed anti-ovarian cancer activity and worked well alongside cisplatin in resistant cancer cells.
  • * Derivative 33 binds to TRBP, influencing miRNA maturation, and has a stronger effect against ovarian cancer cells compared to the previously known modulator, enoxacin, suggesting it could lead to new treatments.
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Influenza viruses (IV) are single-stranded RNA viruses with a negative-sense genome and have the potential to cause pandemics. While vaccines exist for influenza, their protection is only partial. Additionally, there is only a limited number of approved anti-IV drugs, which are associated to emergence of drug resistance.

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In search of novel therapeutic options to treat influenza virus (IV) infections, we previously identified a series of inhibitors that act by disrupting the interactions between the PA and PB1 subunits of the viral RNA polymerase. These compounds showed broad-spectrum antiviral activity against human influenza A and B viruses and a high barrier to the induction of drug resistance in vitro. In this short communication, we investigated the effects of combinations of the PA-PB1 interaction inhibitor 54 with oseltamivir carboxylate (OSC), zanamivir (ZA), favipiravir (FPV), and baloxavir marboxil (BXM) on the inhibition of influenza A and B virus replication in vitro.

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Article Synopsis
  • Respiratory syncytial virus (RSV) is the leading cause of infant hospitalizations worldwide and the second-highest contributor to infant mortality after malaria.
  • While three vaccines have been approved for older adults and pregnant women, there is no effective antiviral treatment available for RSV infections in general.
  • This overview discusses recent advancements in developing small molecule antivirals targeting RSV's fusion and polymerase proteins, alongside insights from research on HCV and HIV, highlighting the importance of the newly approved vaccines.
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Nontuberculous mycobacteria (NTM), which include the Mycobacterium avium complex, are classified as difficult-to-treat pathogens due to their ability to quickly develop drug resistance against the most common antibiotics used to treat NTM infections. The overexpression of efflux pumps (EPs) was demonstrated to be a key mechanism of clarithromycin (CLA) resistance in NTM. Therefore, in this work, 24 compounds from an in-house library, characterized by chemical diversity, were tested as potential NTM EP inhibitors (EPIs) against Mycobacterium smegmatis mc155 and M.

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