| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1314449 | Journal of Fluorine Chemistry | 2009 | 5 Pages |
Enantioselective α-sulfenylation of α-fluoro-β-ketoesters 4 with phenylsulfenyl chloride catalyzed by DBFOX–Ph/Ni(II) complex afforded the corresponding α-fluoro-α-sulfenyl-β-ketoesters 2 in moderate to good yields with excellent enantiomeric excesses up to 93% ee. α-Fluoro-α-sulfenyl-β-ketoesters can be effectively converted to tri-fluorinated α-sulfenylcarboxylates by the use of DAST, which should be useful intermediates for the synthesis of non-racemized fluorinated isosteres of pharmaceutically attractive SM32. The enantioselective α-phenylsulfenylation as well as α-pentafluoro-phenylsulfenylation of non-fluorinated β-ketoesters 5 were also carried out under the same catalyst conditions affording up to 95% ee of the products 6–8.
Graphical abstractEnantioselective α-sulfenylation of α-fluoro-β-ketoesters 4 with phenylsulfenyl chloride catalyzed by DBFOX–Ph/Ni(II) complex afforded the corresponding α-fluoro-α-sulfenyl-β-ketoesters 2 in moderate to good yields with excellent enantiomeric excesses up to 93% ee. α-Fluoro-α-sulfenyl-β-ketoesters can be effectively converted to tri-fluorinated α-sulfenylcarboxylates by the use of DAST, which should be useful intermediates for the synthesis of non-racemized fluorinated isosteres of pharmaceutically attractive SM32. The enantioselective α-phenylsulfenylation as well as α-pentafluoro-phenylsulfenylation of non-fluorinated β-ketoesters 5 were also carried out under the same catalyst conditions affording up to 95% ee of the products 6–8.Figure optionsDownload full-size imageDownload as PowerPoint slide
