Total Synthesis of the Antitumor
Antibiotic (±)-Streptonigrin:
First- and Second-Generation Routes for de Novo Pyridine Formation
Using Ring-Closing Metathesis
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Abstract
The total synthesis of (±)-streptonigrin,
a potent tetracyclic
aminoquinoline-5,8-dione antitumor antibiotic that reached phase II
clinical trials in the 1970s, is described. Two routes to construct
a key pentasubstituted pyridine fragment are depicted, both relying
on ring-closing metathesis but differing in the substitution and complexity
of the precursor to cyclization. Both routes are short and high yielding,
with the second-generation approach ultimately furnishing (±)-streptonigrin
in 14 linear steps and 11% overall yield from inexpensive ethyl glyoxalate.
This synthesis will allow for the design and creation of druglike
late-stage natural product analogues to address pharmacological limitations.
Furthermore, assessment of a number of chiral ligands in a challenging
asymmetric Suzuki–Miyaura cross-coupling reaction has enabled
enantioenriched (up to 42% ee) synthetic streptonigrin intermediates
to be prepared for the first time