Microcalorimetric assessment of gyrase-inhibitors

Nalidixic acid inhibits the expression of those cysteine genes which are regulated by the cysB product, it has no affect, however, on the constitutively expressed eysE gene. The expression of cysteine genes in a strain carrying a mutation in the nalA locus is resistant to this drug. Novobiocin affec

The number and strength of the acid sites of a variety of NaHZSM-5 zeolites were measured as a function of the exchange level using NH, adsorption monitored by microcalorimetry. While the number of acid sites increased quasi linearly with the exchange level, the acid strength remained almost consta

The design, synthesis and in vitro biological evaluation of isothiochroman 2,2-dioxide and 1,2-benzooxathiin 2,2-dioxide analogues of coumarin inhibitors of gyrase B are described. Compared to coumarin derivatives, compounds of the 1,2-benzooxathiin 2,2-dioxide series display improved inhibitory pot

## Abstract A series of 4‐quinazolone‐5‐carboxylic acids were designed as bacterial DNA gyrase inhibitors. The syntheses of the target compounds were accomplished by reacting 3‐aminophthalimide with aroyl chlorides followed by rearrangement of the resulting 3‐acylaminophthalimides under basic condi

AbstractÐThe synthesis and biological pro®le in vitro of a series of coumarin inhibitors of gyrase B bearing a N-propargyloxycarbamate at C-3 H of noviose is presented. Replacement of the 5-methylpyrrole-2-carboxylate of coumarin drugs with an N-propargyloxycarbamate bioisostere leads to analogues w