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@ARTICLE{Drennhaus:885453,
author = {Drennhaus, Till and Öhler, Laura and Djalali, Saveh and
Höfmann, Svenja and Müller, Clemens and Pietruszka, Jörg
and Worgull, Dennis},
title = {{E}nantioselective {A}mmonium {Y}lide {M}ediated
{O}ne‐{P}ot {S}ynthesis of {H}ighly {S}ubstituted γ
‐{B}utyrolactones},
journal = {Advanced synthesis $\&$ catalysis},
volume = {362},
number = {12},
issn = {1615-4169},
address = {Weinheim},
publisher = {Wiley-VCH},
reportid = {FZJ-2020-03836},
pages = {2385 - 2396},
year = {2020},
abstract = {An ammonium ylide mediated access towards
trans‐β,γ‐disubstituted,
all‐trans‐α,β,γ‐trisubstituted, and
α,α,β,γ‐tetrasubstituted γ‐butyrolactones bearing a
broad variety of functionalities was developed. Starting
from widely accessible benzylidene Meldrum's acid
derivatives and α‐bromo carbonyl compounds,
γ‐butyrolactones were obtained in yields between
$32–99\%$ with up to excellent diastereoselectivities
(>95:5) via a DABCO‐mediated [2+1] annulation. Utilization
of enantiomerically pure cinchona alkaloid derivatives
enables the first asymmetric ammonium ylide mediated method
to provide (3R, 4R)‐β,γ‐disubstituted and (2R, 3R,
4R)‐α,β,γ‐trisubstituted γ‐butyrolactones in
moderate to good yields with up to very good enantiomeric
ratios (97:3). The scalability of the transformation was
proven while determining the absolute configuration.},
cin = {IBOC / IBG-1},
ddc = {660},
cid = {I:(DE-Juel1)IBOC-20090406 / I:(DE-Juel1)IBG-1-20101118},
pnm = {581 - Biotechnology (POF3-581)},
pid = {G:(DE-HGF)POF3-581},
typ = {PUB:(DE-HGF)16},
UT = {WOS:000540092500012},
doi = {10.1002/adsc.202000039},
url = {https://juser.fz-juelich.de/record/885453},
}
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