Synthesis of 6-thiatetracycline, a highly active analogue of the antibiotic tetracycline

Kirchlechner, R.; Rogalski, Werner

doi:10.1016/s0040-4039(00)71180-4

Cited by 17 publications

(6 citation statements)

References 9 publications

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“…It is noteworthy that the condensation (2b+3) occurs with a catalytic quantity of the exceedingly weak base, basic lead acetate (Pb(OAc) 2 .Pb(OH) 2 ). 5,8,9 This supports the case for the relatively enhanced aromaticity of Ib. The mild conditions are particularly suited for aliphatic aldehydes, several of which afford the expected products 5 in excellent yields ( Table 1).…”

Section: Introductionsupporting

confidence: 67%

“…[5][6][7] The reaction mixture was treated with an aldehyde (3) and a catalytic amount of basic lead acetate over 20 min. 5,8,9 Minimal work-up and chromatographic purification led to the isolation of the 4-alkylidene or 4-arylidene thioazlactone derivative 5, in generally excellent yields (Table 1). These results indicate that the thiazolin-5-one (2b) generated in situ with DCC, 7 has condensed with the aldehyde (3).…”

Section: Introductionmentioning

confidence: 99%

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The Erlenmeyer synthesis with a thioazlactone

Chandrasekhar¹,

Srimannarayana²

2009

Arkivoc

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2-Phenylthiazolin-5-one (2b) was generated in situ and condensed with various aldehydes in CH 2 Cl 2 (r.t./20 min.), to obtain the corresponding 4-alkylidene or arylidene products in good yields (68-81%). The reaction is catalyzed by basic lead acetate, and is equally successful with both aliphatic and aromatic aldehydes. This mild version of the classical Erlenmeyer azlactone synthesis is apparently enabled by the enhanced aromaticity of the thioazlactone anion intermediate.

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Section: Introductionsupporting

confidence: 67%

Section: Introductionmentioning

confidence: 99%

The Erlenmeyer synthesis with a thioazlactone

Chandrasekhar¹,

Srimannarayana²

2009

Arkivoc

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“…There follows a short description of the synthesis of 6-thiatetracycline (327) (Fig.40), the simplest basic structure in this series, which is also exemplary for all other compounds (KIRCHLECHNER and ROGALSKI 1980). The synthesis starts from 2-chloro-4-aminothiophenol (313).…”

Section: A) Chemistrymentioning

confidence: 99%

Chemical Modification of the Tetracyclines

Rogalski¹

1985

The Tetracyclines

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“…The Woodward, Shemyakin, and Muxfeldt groups reported remarkable advances for their time with their successful constructions of sancycline (25 synthetic steps, 0.002 % yield), tetracycline (yield not reported), and oxytetracycline (22 steps, 0.06 % yield), respectively, but these routes were lengthy and impractical to scale (though it should be noted that the Muxfeldt approach was for a time adapted by researchers at Merck in Germany for the preparation of fully synthetic 6-thiatetracycline, an antibiotic candidate that was abandoned during clinical development due to liver toxicity). [123] Interestingly, each group had employed a "left-to-right" or D!A mode of construction, which was not ideal from the standpoint of drug discovery, since substitution of the D ring proves to be remarkably fruitful for the development of novel antibiotics, especially those with improved activities against tetracyclineresistant microorganisms, whereas most substitutions of the A ring diminish or abolish antibiotic activity.…”

Section: A Fully Synthetic Platform For the Discovery And Developmentmentioning

confidence: 99%

The Evolving Role of Chemical Synthesis in Antibacterial Drug Discovery

2014

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The discovery and implementation of antibiotics in the early twentieth century transformed human health and wellbeing. Chemical synthesis enabled the development of the first antibacterial substances, organoarsenicals and sulfa drugs, but these were soon outshone by a host of more powerful and vastly more complex antibiotics from nature: penicillin, streptomycin, tetracycline, and erythromycin, among others. These primary defences are now significantly less effective as an unavoidable consequence of rapid evolution of resistance within pathogenic bacteria, made worse by widespread misuse of antibiotics. For decades medicinal chemists replenished the arsenal of antibiotics by semisynthetic and to a lesser degree fully synthetic routes, but economic factors have led to a subsidence of this effort, which places society on the precipice of a disaster. We believe that the strategic application of modern chemical synthesis to antibacterial drug discovery must play a critical role if a crisis of global proportions is to be averted.

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Synthesis of 6-thiatetracycline, a highly active analogue of the antibiotic tetracycline

Cited by 17 publications

References 9 publications

The Erlenmeyer synthesis with a thioazlactone

The Erlenmeyer synthesis with a thioazlactone

Chemical Modification of the Tetracyclines

The Evolving Role of Chemical Synthesis in Antibacterial Drug Discovery

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