Thiazolidine, derivatives, preparation

Because of the structural requirements of the bielectrophile, fully aromatized heterocycles are usually not readily available by this procedure. The dithiocarbamate (159) reacted with oxalyl chloride to give the substituted thiazolidine-4,5-dione (160) (see Chapter 4.19), and the same reagent reacted with iV-alkylbenzamidine (161) at 100-140 °C to give the 1 -alkyl-2-phenylimidazole-4,5-dione (162) (see Chapter 4.08). Iminochlorides of oxalic acid also react with iV,iV-disubstituted thioureas in this case the 2-dialkylaminothiazolidine-2,4-dione bis-imides are obtained. Thiobenzamide generally forms linear adducts, but 2-thiazolines will form under suitable conditions (70TL3781). Phenyliminooxalic acid dichloride, prepared from oxalic acid, phosphorus pentachloride and aniline in benzene, likewise yielded thiazolidine derivatives on reaction with thioureas (71KGS471). 

In 2000, novel thiazolidine derivatives were prepared from L-cysteine by Guan et al, showing good enantioselectivities of up to 90% ee when used as ligands in the addition of ZnEt2 to aldehydes. The results collected in Scheme 3.6 show that the catalytic efficiency of the thiazolidine derivatives was influenced by the different structures of the thiazolidine rings and the bulkiness of the moiety in... 

Cuscutic resinoside A (1 tetradecanoic acid, (115)-[[6-deoxy-3-(9-(6-deoxy-a-L-mannopyranosyl)-4-0-[(2/ ,3R)-3-hydroxy-2-niethyl-l-oxobutyl]-a-L-nianno-pyranosyl]oxy]-intramol. l,2 -ester) was obtained from the ethyl acetate-soluble fraction of a methanol extract prepared from the seeds of Cuscuta chinensis Lam. The purification of this compound employed a combination of column and preparative-scale HPLC. The structure was deduced from spectroscopic evidence and acid hydrolysis 14). The degradative process gave convolvuUnolic acid, nilic acid, and L-rhamnose. The sugar components were identified by GC analysis after being converted to their thiazolidine derivatives. This disaccharide has a unique macrocyclic lactone, which is placed between C-1 and C-2 of the first rhamnose moiety. 

Peptide aldehydes can be synthesized via hydrolysis of thiazolidine precursors with mercury or copper salts (Scheme 10). 56 The Phe-thiazolidine derivative 27 was prepared from reduction of dihydrothiazole ring in 26, which was formed from a (5-hydroxy thioamide cyclization of 25 using the Mitsunobu reaction. N-Terminal Boc and Z groups on thiazolidine pseudopeptides such as Boc-Ala-Phe-thiazolidine and Z-Phe-Tyr-thiazolidine are stable to hydrolysis that affords Boc-Ala-Phe-H and Z-Phe-Tyr-H. 56 ... 

In earlier investigations by the authors (1,2), 2-oxo-l,2,3,4-tetrahydropyrazines, (I), and thiazolidine derivatives, (II), respectively, were prepared, which were effective as chymase inhibitors. 

Peptidyl thiazolidines, (VI), DPP-IV prodrugs prepared by Demuth (6) and dipeptidyl thiazolidine derivatives, (VII), prepared by Ashton (7) were effective as DPP-IV inhibitors and used in the treatment of diabetes mellitus and impaired glucose tolerance disorders. 

The additional peaks in Figure 7 represent thiazolidine derivatives. The content of methyl glyoxal in soy bean paste was considerably lower than that of soy sauce even though they were prepared by similar procedures. This may be due to differences in fermentation time. 

Other Oxazolidine as well as Thiazolidine Derivatives for Branching Amino Acids. The cyclic derivative of alanine and other amino acids employed most frequently for a-allq lation is not (1) but rather the benzaldehyde acetal (5), either with a benzoyl or with a Cbz group on nitrogen. These compounds were used for the preparation of 2-methyl-2-aminobutanoic acid, a-methylphenylalanine, a-methyllysine, 2-methylaspartic acid, and 2-methylglutamic acid. Bicyclic compounds containing oxazolidinone rings such as (6) (from alanine, leucine, and phenylalanine) and (7) (from azetidinecaiboxylic acid, proline, " hydroxyproline, and cysteine ) have also been applied to the synthesis of branched amino acids. 

As illustrated in Scheme 134, both distereoisomers of thiazolidine 535 prepared from commercially available amino acid derivatives 533 and 534 can serve as /3-turn mimetics in the secondary structure of peptides and proteins therefore, they play an important role in many molecular recognition events in biological systems <2002TL1197>. A similar application can be found with thiazoline lactams <1999TL477>. 

The 1,3-dipolar cycloaddition reaction of azomethine ylides with thioketones has been used to prepare 1,3-thiazoIidines. The metallated azomethine ylides 67 were generated in situ by treating a-amino acid ester imines 66 with lithium bromide and DBU. The ylides were then treated with highly reactive thioketones such as thiobenzophenone or fluorene-9-thione, to afford 1,3-thiazolidine derivatives 68 (main isomer) and 69 (minor isomer) in good yield and in diastereoisomeric ratios of between 2 1 and 4 1 <01H(55)691>. 

Imidazolidine and imidazoline derivatives were formed when dialdose derivatives reacted with 2,3-bis(hydroxylamino)-2,3-dimethylbutane (Scheme 60) oxidation of these derivatives afforded stable free radicals that were examined by e.s.r. spectroscopy. Several oxazole and thiazolidine derivatives having C-5 and C-6 of 3-0-benzyl-l,2-0-isopropylidene-jS-L-idofuranose as part of the heterocyclic ring, and a new class of bicyclic thiazolidine derivative (172) have been prepared by the reactions shown in Scheme 61. The bis(l,3,4-oxadia-zole) derivative (173) has been prepared by condensative cyclization of 2,3,4,5-tetra-O-acetylgalactaric acid bis(benzoylhydrazide) with triethyl orthoformate in p-dioxan. Other heterocyclic derivatives are referred to in Chapters 14 and 15. 

Application of the Curtius reaction to the 3-carboxyl of a penicillin has provided intermediates which have been used for the construction of cephem derivatives. As can be seen in Scheme 23, this route allows the selective cleavage of the C(3)—N(4) bond of the thiazolidine ring, thereby allowing a reconstruction of that ring in a different form (72HCA388 and the following three papers). The preparation of a related intermediate is shown in Scheme 24 (76HCA2298). 

Evans et al. reported that the bis(imine)-copper (II) complex 25, prepared from chiral bis(imine) ligand and Cu(OTf)2, is also an effective chiral Lewis acid catalyst [34] (Scheme 1.44, Table 1.18). By tuning the aryl imine moiety, the bis(2,6-dichlor-ophenylimine) derivative was found to be suitable. Although the endojexo selectivity for 3-alkenoyloxazolidinones is low, significant improvement is achieved with the thiazolidine-2-thione analogs, for which both dienophile reactivity and endojexo selectivity are enhanced. 

Reaction of isothiocyanate with amine gives the corresponding thioureas. Many reports are appeared.102 111 The thiourea derivatives have been prepared by reactions of isothiocyanates with arylamines (Scheme 39) and reacted with some substrates to afford heterocyclic compounds, such as 2-amino-4//-ben-zothiazine, 1,3-thiazine, 1,3-thiazinone and l,3-thiazolidin-4-one.112 115... 

Acetaldehyde is oxidized to acetic acid by NAD+-dependent aldehyde dehydrogenases (ALDH) in liver and nasal mucosal preparations. Its administration to rats causes an increase in urinary excretion of sulfur metabolites and it is known to react with cysteine to produce a thiazolidine 4-carboxylic acid derivative that can be A -nitro-sated in vivo upon co-administration of nitrite (lARC, 1985). Many studies have been published subsequently, but these have been mainly in the context of ethanol metabolism. 

Examples of this ring system (263) were prepared by cyclocondensation of anthranilic acid with the 1,3-thiazole derivatives 262 (82MI1 83AP394). Reductive cyclization of the 4-ethylamino-3-(2-nitrobenzyl)thiazolidines (264) was affected by heating with iron filings and acetic acid to give 4//-3,3a-dihydrothiazolo[4,3- >]quinazoline (265) (87JHC107). 

Activated acid derivatives are easily prepared by condensation of a carboxylic acid with thiazolidine-2-thione (608) in the presence of DCC or alternatively, by reaction of an acid... 

Due to the extremely low nucleophilicity of the imino group, 187,188 acylation of thiazolidine-4-carboxylic acid (11) is not a trivial procedure. In fact, N-protected Thz derivatives can be prepared by standard procedures, but strong acylating conditions are required. The related N-Boc derivative is obtained only by prolonged reaction times with Boc-N3 U2,189 or with Boc20. 113 For preparation of the N-Z derivative, silylation of Thz with, for example, chlorotrimethylsilane is recommended prior to the reaction benzyl chloroformate. 200 Due to the stability of thiazolidine-4-carboxylic acid to acids its methyl ester is obtained by HC1 catalyzed reaction with methanol, 190 whereas the amide is formed by reacting Thz N-carboxyanhydride with ammonia.1 89 Derivatives of thiazolidine-4-carboxylic acid are listed in Table 8. 

As mentioned above, thiazolidine-4-carboxylic acid is characterized by an anomalously low basicity and thus difficult acylation in peptide synthesis. 189 Therefore, the incorporation of this amino acid residue into a growing peptide chain is preferentially preformed via dipeptide derivatives. 139 Suitably N-protected amino acids are coupled directly to the thiazolidine-4-carboxylic acid by the acid fluoride 139 or iV-carboxyan hydride 1392111 methods. The resulting dipeptides are used as building blocks without risk of racemization 139 and standard coupling procedures are applied as pentachlorophenyl esters prepared by the mixed anhydride procedure 121 or PyBOP. 171 ... 

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