5- -4 azido-2-hydroxy

Azido hydroxy tetrazole (mercury and silver salts)... 

N-(D-Threo- and racemic erythro-3-amino-2-hydroxy-butanoyl)-2, 3 -dideoxykanamycin A has been prepared using a standard esterification procedure with the corresponding azido-hydroxy-butanoic acid. Glucuronide saponins have been used to furnish paromamine and ribostamycin by means of lead tetraacetate or anodic oxidative decarboxylation procedures. Phase-sensitive 2D COSY spectra... 

It shows that an epoxide ring is opened stereospecifically with NaNs to azido hydroxy cyclohexene, which undergoes ring closure with TPP to give the corresponding aziridine, and is opened again with NaNs to the amino azido cyclohexene derivative with an exactly defined stereochemistry. This azide function remains in the molecule as a masked amine until the second last reaction step. 

When 6-amino-3-chloropyridazine 1-oxide is diazotized in 50% sulfuric acid, 6-hydroxy-3-pyridazinediazonium anhydro salt is formed. An azido group at either position in pyridazine A-oxides can readily be replaced with sodium alkoxides. 

Apparent nucleophilic attack on large, fully unsaturated rings may occur by way of attack on a valence tautomer, such as the reaction of oxepin with azide ion. Attack on the oxanorcaradiene valence tautomer leads to ring opening of the three-membered ring, and formation of 5-azido-6-hydroxy-l,3-cyclohexadiene (Section 5.17.2.2.4). 

Ceroplastol synthesis, 1, 428 Cetyl alcohol synthesis, 1, 478 Chaetoglobasins structures, 4, 376 Chalcone, o -azido-2 -oxy-synthesis, 3, 823 Chalcone, 2-hydroxy-reduction, 3, 751 Chalcone, 2 -hydroxy-mass spectra, 3, 618 Chalcone dibromides flavone synthesis from, 3, 823 Chalcones polymers, 1, 304 Chanoclavine synthesis, 6, 423 Charge density waves in stacks of ions, 1, 351-352 Chartreusin... 

The azidohydrins obtained by azide ion opening of epoxides, except for those possessing a tertiary hydroxy group, can be readily converted to azido mesylates on treatment with pyridine/methanesulfonyl chloride. Reduction and subsequent aziridine formation results upon reaction with hydrazine/ Raney nickel, lithium aluminum hydride, or sodium borohydride/cobalt(II)... 

Attempts to prepare 6-hydroxybenzofuroxan by demethylation of 5-methoxybenzofuroxan, by pyrolysis of 4-azido-3-nitrophenol, and by hypochlorite oxidation of 4-amino-3-nitrophenoD failed. This rather unstable compound was finally prepared by hydrolysis of 5-acetoxybenzofuroxan its tautomeric possibilities are numerous, but from the similarity of its ultraviolet spectrum to that of 5-methoxybenzofuroxan it was considered to be largely in the hydroxy form. It is a fairly strong acid, of pK 6.76 (cf. 5-hydroxybenzo-furazan, pK 7.28). 7-Hydroxy-4,6-dinitrobenzofuroxan has been reported as arising from oxidation and nitration of dinitrosoresorcinol monooxime (tetraoxocyclohexene trioxime). ... 

A variety of methods for the asymmetric syntheses of aziridine-2-carboxylates have been developed. They can be generally classified into eight categories based on the key ring-forming transformation and starting materials employed (i) cyclization of hydroxy amino esters, (ii) cyclization of hydroxy azido esters, (iii) cyclization of a-halo- and ot-sulfonyloxy-(3-amino esters, (iv) aziridination of ot, 3-unsaturated esters, (v) aziridination of imines, (vi) aziridination of aldehydes, (vii) 2-carboxylation of aziridines, and (viii) resolution of racemic aziridine-2-carboxylates. 

A general method for the synthesis of N-unsubstituted aziridine-2-carboxylates involves a triphenylphosphine-mediated reductive cyclization of hydroxy azido esters [17-22]. A recent example involves the treatment of [1-hydroxy-a-azido ester 15 (Scheme 3.6) with PPh3 to give aziridine 16 in 90% yield [19]. a-Hydroxy- 3-azido esters undergo similar reactions to give aziridine-2-carboxylates [20-22],... 

Balli and Felder (1978) and Balli and Ritter (1981) showed that diazo transfer can be applied advantageously to the diazotization of sufficiently nucleophilic heteroaromatic compounds such as 5-hydroxy- and 5-amino-3-methyl-l-phenyl-pyrazole if 3-ethyl-2-azido-benzthiazolium tetrafluoroborate (2.50) is used as diazo transfer reagent (for other applications of this diazo transfer reagent see Zollinger, 1995, Secs. 2.6-2.8). The diazonio group is introduced in the 4-position (2.51). 

CN [/ -(R, / )]-2-azido-Af-[2-hydroxy-l-(hydroxymethyl)-2-(4-nitrophenyl)ethyl]acetamide... 

The DKR of functionalized alcohols such as diols, hydroxy esters, hydroxy aldehydes, azido alcohols and hydroxy nitriles was also taken up as the synthetic uhlity of the products is very high besides such a study will bring out the effect of multifunctional substrates under these reaction conditions to broaden the scope of DKR. Initially, the DKR of diols was achieved with diruthenium catalyst 1... 

The DKRs of (J-azido alcohols and p-hydroxy nitriles were also accomplished hy employing 1 and CALB with PCPA as the acyl donor. The DKRs of p-azido alcohols were performed at 60°C while those of (3-hydroxy nitriles required higher temperature (100°C) primarily to enhance the racemization rate. The optical purities of products were satisfactory in all cases. In the case of p-hydroxy nitriles, dehydrogenation lowered the yield. 

The enhanced reactivity of 5-halogeno-l,2,4-thiadiazoles over 3-halogeno-l,2,4-thiadiazoles has been mentioned before (see Section 5.08.7.1). Nucleophilic substitution at this center is a common route to other 1,2,4-thiadiazoles, including 5-hydroxy, alkoxy, mercapto, alkylthio, amino, sulfonamido, hydrazino, hydroxylamino, and azido derivatives. Halogens in the 3-position of 1,2,4-thiadiazoles are inert toward most nucleophilic reagents, but displacement of the 3-halogen atom can be achieved by reaction with sodium alkoxide in the appropriate alcohol <1996CHEC-II(4)307>. 

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