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Scalable De Novo Synthesis of Aldgarose and Total Synthesis of Aldgamycin N
Author(s) -
Späth Georg,
Fürstner Alois
Publication year - 2021
Publication title -
angewandte chemie
Language(s) - English
Resource type - Journals
eISSN - 1521-3757
pISSN - 0044-8249
DOI - 10.1002/ange.202016477
Subject(s) - aglycone , total synthesis , chemistry , combinatorial chemistry , ruthenium , glycoside , stereochemistry , alcohol , orthoester , catalysis , organic chemistry
Since the accompanying study had shown that the introduction of the eponymous aldgarose sugar to the C5‐OH group of the macrocyclic aglycone of aldgamycin N is most difficult, if not even impossible, the synthesis route was revised and the glycosidation performed at an earlier stage. To mitigate the “cost” of this strategic amendment, a practical and scalable de novo synthesis of this branched octose was developed. The glycoside formation required mild conditions; it commenced with the reaction of the aglycone with the trichloroacetimidate donor to give a transient orthoester, which slowly rearranged to the desired aldgaropyranoside. The presence of the polar peripheral groups in the product did not impede the selective late‐stage functionalization of the macrolide ring itself: the contained propargylic alcohol entity was readily transformed into the characteristic acyloin motif of the target by a ruthenium‐catalyzed trans ‐hydrostannation followed by a modified Chan‐Lam‐type coupling.