Hydroxamic acid derivatives carboxylic acids

Cyclocondensation of malonyl derived O-acyl hydroxamic acid derivatives 6, in the presence of phosphazene super base P2-r-Bu 7, gave rise to isoxazolone carboxylic esters 8 <03TL7763>. 

Rearrangement of O-acyl hydroxamic acid derivatives with base or heat to amines or urea derivatives (via isocyanates), or rearrangement of carboxylic acids via their hydroxamic acids to amines (see 1st edition). 

The phosphazene bases BTPP and Bu-P2 mediate the rearrangement of unactivated A -alkyl-(9-benzoyl hydroxamic acid derivatives to give 2-benzoyl amides. The rate of reaction was found to be dependent upon the steric nature of the A -alkyl substituent [39a]. Treatment of malonyl derived (9-acyUiydroxamic acid derivatives with the phosphazene superbase Bu-P2 gives 2,3-dihydro-4-isoxazole carboxylic ester derivatives. The rate and yield of the reaction depend upon the (9-acyl substituent [36b] (Scheme 5.21). 

Clark, A.J., Al-Faiyz, Y.S.S., Patel, D. and Broadhurst, M.J. (2001) Rearrangement of unactivated A-alkyl-O-benzoyl hydroxamic acid derivatives with phosphazene bases. Tetrahedron Letters, 42, 2007-2009 Clark, A.J., Patel, D. and Broadhurst, M.J. (2003) Base-mediated reaction of A-alkyl-O-acyl hydroxamic acids synthesis of 3-oxo-2,3-dihydro-4-isoxazole carboxylic ester derivatives. Tetrahedron Letters, 44, 7763-7765. 

Benzo-hydroxamic acid derivatives inhibited the scale formation less effectively (10-22%) than phosphonic and/or carboxylic acids. 

Indirect detection of an intermediate. The overall reaction of hydroxylamine with a carboxylic acid derivative yields a hydroxamic acid as the product, Eq. (3-176). 

In 2000, an efficient three-step procedure for the synthesis of 5-substituted 3-isoxazolols (without formation of undesired 5-isoxazolone byproduct) was published. The method uses an activated carboxylic acid derivative to acylate Meldrum s acid, which is treated with A,0-bis(ten-butoxycarbonyl)hydroxylamine to provide the N,0-di-Boc-protected P-keto hydroxamic acids 14. Cyclization to the corresponding 5-substituted 3-isoxazolols 15 occurs upon treatment with hydrochloric acid in 76-99% yield. 

In general, a hydroxamic acid function results from the condensation of a hydroxylamine group with a carboxylic acid derivative. If these two groups are positioned suitably in the same molecule, spontaneous cyclization can occur. The most usual technique involves... 

Some hydroxamic acids of the isoxazole series also display a marked antituberculosis activity. The penicillin derivatives, acylated with isoxazole carboxylic acids possess an antibacterial activity similar to that of penicillin, against resistant species.Among other isoxazole derivatives possessing activity one should especially mention the sulfonamides of this series, and 4-hydroxyiminoisoxazol-5-... 

Complexation of metal ions by hydroxamic acids is the starting point of a number of analytical determinations . All hydroxamic acids, in acid solutions, react with ferric chloride to give rust brown complex salts 89 (Scheme 47). These colored complexes form the basis for the sensitive qualitative and quantitative determination of carboxylic acids and their derivatives too. 

In 2001, De Luca and GiacomeUi " reported a new simple and high-yielding one-flask synthesis of Weinreb amides from carboxylic acids and A-protected amino acids that uses different 1,3,5-triazine derivatives (such as 236) as the coupling agents (Scheme 104). The method allows the preparation of Weinreb amides 237 and hydroxamates as O-benzyl and 0-silyl hydroxamates that can be easily transformed into hydroxamic acids. 

As befits the euhauced uucleophilicity of hydroxylamiues (cf. the a effect), the reactiou of hydroxylamiue itself with esters, aud a variety of other carboxylic acid derivatives, readily produce the correspoudiug hydroxamic acid (equatiou 4),... 

Peptide a-oxo acids, a-oxo esters, and a-oxoamides are also potent inhibitors of cysteine and serine proteases. Oxidation of peptide a-substituted carboxylic acid derivatives provides a general route to these compounds (Section 15.1.5). Peptide hydroxamic acids have been shown to be inhibitors of metalloproteinase and some have been reported to have antibiotic, anticarcinogenic, and antiviral activities. Peptide hydroxamic adds may be prepared by solution and solid-phase methods using a variety of resins (Section 15.1.6). a-Aminoboronic acids may be prepared by several routes and are reported to be inhibitors of aminopepti-dases. Procedures have been developed for their incorporation into peptides (Section 15.1.7). 

Carboxylic acid derivatives of thiazepine were obtained by cyclization of D-penicillamine. The ester derivative 107a was transformed to the carboxylic acid 107b and hydroxamic acid 107c. The latter compound is a matrix metalloproteinase (MMP) inhibitor (Figure 13) <1999JME4547>. 

The simpler examples are readily hydrolysed in aqueous solution, and therefore react with sodium hydrogen carbonate and also give the ester test they may be confirmed by applying the hydroxamic ester test (Section 9.5.3, p. 1222). Carbonyl adsorption is apparent in the infrared spectrum at about 1820 cm-1 and at about 1760cm-1. It should be noted that aromatic anhydrides and higher aliphatic anhydrides are not readily hydrolysed with water and are therefore effectively neutral (Section 9.5.3, p. 1218). The final characterisation of the acid anhydride is achieved by conversion into a crystalline carboxylic acid derivative as for add halides. 

In search for potent and systemically available inhibitors of the matrix metalloproteinase MMP-8 (Matter et al. 1999 Matter et al. 2002) following oral administration, a local ADME model was derived to support lead optimization. For an internal series of inhibitors on the tetrahydroisoquinoline scaffold, hydroxamic acids for zinc ion binding in 3-position are essential for MMP affinity in first generation inhibitors. However, those compounds are characterized by insufficient pharmacokinetic properties and low systemic exposure following oral administration. Driven by X-ray and 3D-QSAR studies (CoMFA), alternative Zn2+ binding groups like carboxylates were... 

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