AI Article Synopsis

  • A series of C-1 oxazole isosteres of mupirocin with nitroheterocycles were synthesized, revealing notable differences in antibacterial activity and potency compared to mupirocin.
  • Some derivatives showed effectiveness against mupirocin-resistant staphylococci, suggesting they have an additional mechanism of action beyond inhibiting the enzyme isoleucyl-tRNA synthetase.
  • The most effective compound, nitrofuran 3f, is reduced by bacterial enzymes, potentially leading to different cellular targets, proving to be effective in vivo via both subcutaneous and oral administration.

Article Abstract

A series of C-1 oxazole isosteres of pseudomonic acid A (mupirocin) bearing a nitroheterocycle have been synthesized, and significant differences in both spectrum of activity and potency were found between these derivatives and mupirocin. Additionally, the antibacterial potency of two members of this class of compounds against mupirocin-resistant staphylococci could not be accounted for solely by inhibition of the target enzyme isoleucyl-tRNA synthetase (IRS), indicating an additional mode of action. The most potent compound, the nitrofuran 3f (SB 205952), was the most electron affinic derivative prepared and was transformed by NAD(P)H-dependent bacterial reductases at a rate similar to that for nitrofurantoin. The second mode of action of this compound may therefore arise from its reduction to a species with cellular targets other than IRS. In in vivo studies, 3f was shown to be a very effective agent by both the subcutaneous and oral routes of administration.

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http://dx.doi.org/10.1021/jm950882qDOI Listing

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