Abstract:An efficient, step-economical, and scalable synthesis of a diene-bearing AB spiroketal fragment of spongistatin 1, and a demonstration of its efficient coupling to an aldehyde derived from silylformylation of a homopropargyl alcohol to produce the entire complex C(13)–C(17) linker region are described. The scalability of the synthesis of the AB spiroketal fragment was demonstrated by the preparation of 34.5 grams by one chemist in ~60 workdays, and more than 40 grams overall. With this material in hand and hav… Show more
“…We were optimistic that our diamine- and diaminophenol-activated crotyl- and allylsilanes 37 , 38 would, uniquely, be well-suited for the proposed reactions due both to their reliably excellent reactivity and broad generality and to the fact that the requisite crotyl- and allylsilanes 8 and 10 (M = Si) appeared accessible from the simple precursors diene 12 (ref. 39 ) and allylchloride 13 by way of mild, functional group-tolerant, and chemoselective transition metal-catalyzed hydrosilylation and allylic substitution reactions, respectively. Fig.…”
Spongistatin 1 is among the most potent anti-proliferative agents ever discovered rendering it an attractive candidate for development as a payload for antibody–drug conjugates and other targeted delivery approaches. Unfortunately, it is unavailable from natural sources and its size and complex stereostructure render chemical synthesis highly time- and resource-intensive. As a result, the design and synthesis of more acid-stable and linker functional group-equipped analogs that retain the low picomolar potency of the parent natural product requires more efficient and step-economical synthetic access. Using uniquely enabling direct complex fragment coupling crotyl- and alkallylsilylation reactions, we report a 22-step synthesis of a rationally designed D-ring modified analog of spongistatin 1 that is characterized by GI50 values in the low picomolar range, and a proof-of-concept result that the C(15) acetate may be replaced with linker functional group-bearing esters with only minimal reductions in potency.
“…We were optimistic that our diamine- and diaminophenol-activated crotyl- and allylsilanes 37 , 38 would, uniquely, be well-suited for the proposed reactions due both to their reliably excellent reactivity and broad generality and to the fact that the requisite crotyl- and allylsilanes 8 and 10 (M = Si) appeared accessible from the simple precursors diene 12 (ref. 39 ) and allylchloride 13 by way of mild, functional group-tolerant, and chemoselective transition metal-catalyzed hydrosilylation and allylic substitution reactions, respectively. Fig.…”
Spongistatin 1 is among the most potent anti-proliferative agents ever discovered rendering it an attractive candidate for development as a payload for antibody–drug conjugates and other targeted delivery approaches. Unfortunately, it is unavailable from natural sources and its size and complex stereostructure render chemical synthesis highly time- and resource-intensive. As a result, the design and synthesis of more acid-stable and linker functional group-equipped analogs that retain the low picomolar potency of the parent natural product requires more efficient and step-economical synthetic access. Using uniquely enabling direct complex fragment coupling crotyl- and alkallylsilylation reactions, we report a 22-step synthesis of a rationally designed D-ring modified analog of spongistatin 1 that is characterized by GI50 values in the low picomolar range, and a proof-of-concept result that the C(15) acetate may be replaced with linker functional group-bearing esters with only minimal reductions in potency.
“…The IC 50 value for this compound was evaluated at 10 26 M in colon cancer cells and 10 212 M for breast cancer cell lines [82]. Synthetic approaches to the compound have been presented by research groups including Petit and coworkers [83,84].…”
“…An alternative carbonylation-based approach is the tandem intramolecular alkyne silylformylation–crotylation/Tamao oxidation/diastereoselective tautomerization reaction (Figure 1 C). 8 This sequence rapidly assembles stereotriads from simple starting materials, and it seemed plausible that we might adapt it for use in an intermolecular alkyne silylformylation 9 reaction using either propyne or 2-butyne as the starting material (Figure 1 D). Crotylation of the resulting α-methyl-β-silyl-α,β-unsaturated aldehyde (an α-methyl-β-ketoaldehyde or β-dialdehyde in masked form) would be followed by Tamao oxidation 10 with concomitant diastereoselective enol tautomerization to deliver the target stereotriad building blocks.…”
An
efficient, step-economical, and scalable approach to the synthesis
of polypropionate stereotriads has been developed. Either 2-butyne
or propyne is subjected to rhodium-catalyzed silylformylation and
in situ crotylation of the resulting aldehydes. Tamao oxidation under
either “standard” conditions or “aprotic”
conditions then delivers the completed stereotriads in a three-step,
two-pot sequence. In contrast to the classical Roche ester approach,
the α-stereocenter is obtained for “free.”
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