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DOI: 10.1055/s-0042-1753032
Synthesis of Versatile Enantiopure Morpholine Fragments from Chiral-Pool Starting Materials
Key words
morpholines - cyclic sulfamidates - chiral pool - building blocks - bioisosterism - asymmetric synthesis
Significance
The favorable physicochemical properties of morpholines make them attractive motifs for incorporation into bioactive molecules, often as bioisosteric replacements for piperidines; this is a common strategy owing, not only to the lower basicity of the nitrogen, but also because the CYP-mediated degradation of the morpholine ring often leads to nontoxic metabolites. The current report describes methods for synthesizing enantiopure functionalized morpholine fragments, with the 3-hydroxymethylmorpholines 5–8 featuring two nucleophilic groups, whereas the corresponding sulfamidates 1–4 can be viewed as aziridine equivalents and used in annulation reactions for the introduction of morpholine moieties.
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Comment
The integral stereochemistry of the desired building blocks is imparted through appropriate selection of readily available enantiopure starting materials specifically derived from Boc-protected serine (e.g., 9) or 1,2-propanediol (e.g., 12). Optimization studies involving the selection of a suitable base–solvent combination were carried out for the critical ring opening of the cyclic sulfamidate 11 with diol 12; aqueous citric acid was used to cleave the resulting sulfamate intermediate. Sulfamidates 1–3 were synthesized in ~10% yield over seven steps (three chromatographic purifications) whereas the dimethyl-substituted derivative 4 was obtained in a similar yield, also in seven steps, but with four chromatographic purifications; a double-Grignard addition to a readily available lactam served as the key step in this synthesis.
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Publication History
Article published online:
18 October 2022
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