Antibiotics aminocyclitol, preparation

A Acetylation, O-Phosphorylation, and O-Adenylylation. A/-Acetylation, O-phosphorjiation, and O-adenyljiation provide mechanisms by which therapeutically valuable aminocyclitol antibiotics, eg, kanamycia [8063-07-8] gentamicin [1403-66-3] sisomicin [32385-11-8], streptomycia [57-92-1], neomycin, or spectinomycin are rendered either partially or completely iaactive. Thus, eg, kanamycia B [4696-78-8] (50) can be iaactivated by modification at several sites, as shown. The elucidation of these mechanisms has allowed chemical modification of the sites at which the iaactivation occurs. Several such bioactive analogues, eg, dibekacia and amikacin have been prepared and are not subject to the iaactivation hence, they inhibit those organisms against which the parent antibiotics are iaeffective (96) (see Antibacterial agents, synthetic). 

Alkali metal in ammonia reductions of pyrrolobenzodiazepine-5,11-diones give trans-2-aminocyclohexanecarboxylic acid derivatives (e.g., 4) in enantiomerically pure form.2 3 A method for preparation of cis-2-aminocyclohexanecarboxylic acids related to 4 is based on the enantioselective hydrolysis of symmetrical diesters with pig liver esterase.4 cis-2-Aminocyclohexane derivatives have been used for syntheses of aminocyclitol antibiotics.4 5 6-Alkyl-cis-2-aminocyclohexanecarboxylic acids can be prepared by alkali metal in ammonia reduction of pyrrolobenzodiazepine-5,11-diones followed by olefin hydrogenation the cis-decahydroquinoline alkaloid (+)-pumiliotoxin C has been prepared by this methodology.2... 

A synthesis of spectinomycin together with the preparation of its 5 -n-butyl analog (replacement of the methyl group with n-butyl group) has been described. The 5 -n-butyl derivative (trospectomycin or 6 -n-propylspectinomycin) showed potent antibacterial activity and is the only aminocyclitol antibiotic that is active against anaerobic bacteria [182]. 

This procedure introduced by Ferrier, involving the mercury salt-mediated ring transformation of 6-deoxyhex-5-enopyranosides into deoxyinososes, has provided a route of wide practical utilization in the field of aminocyclitols [42 6] and pseudo-sugar chemistry [47, 48]. This procedure has led to the preparation [49] of the B-A ring system of the antibiotic b-rhodomycin and has extended [50] to thioglycoside analogs of hex-5-enopyranosides (Fig. 8.29). 

Chiral cyclohexanones obtained by the Ferrier carbocyclization reaction are useful precursors for the synthesis of cyclitols and aminocyclitols, some of which are found in clinically important aminoglycoside antibiotics. Additionally, highly substituted cyclohexenones, prepared by the Ferrier carbocyclization followed by (3-elimination, can undergo various further transformations, also making these compounds potential chiral building blocks for the preparation of structurally complex compounds having cyclohexane unit(s). This section provides an overview of the reported synthetic strategies toward various types of natural products based on utilization of the Ferrier carbocyclization reaction. 

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