DC Field
Value
Language
dc.contributor.author
Draskovits, Markus
-
dc.contributor.author
Catorci, Daniele
-
dc.contributor.author
Wimmer, Laurin
-
dc.contributor.author
Rehman, Sabah
-
dc.contributor.author
Siebert, David
-
dc.contributor.author
Ernst, Margot
-
dc.contributor.author
Schnürch, Michael
-
dc.contributor.author
Mihovilovic, Marko D.
-
dc.date.accessioned
2024-01-05T19:12:49Z
-
dc.date.available
2024-01-05T19:12:49Z
-
dc.date.issued
2023
-
dc.identifier.citation
<div class="csl-bib-body"> <div class="csl-entry">Draskovits, M., Catorci, D., Wimmer, L., Rehman, S., Siebert, D., Ernst, M., Schnürch, M., &#38; Mihovilovic, M. D. (2023). Novel synthetic procedures for C2 substituted imidazoquinolines as ligands for the α/β-interface of the GABAA-receptor. <i>Monatshefte Für Chemie - Chemical Monthly</i>, <i>154</i>(12), 1391–1404. https://doi.org/10.1007/s00706-022-02988-8</div> </div>
-
dc.identifier.issn
0026-9247
-
dc.identifier.uri
http://hdl.handle.net/20.500.12708/191135
-
dc.description.abstract
A series of substituted imidazoquinolines, a structurally related chemotype to pyrazoloquinolinones, a well-known class of GABAA ligands, was prepared via two synthetic procedures and the efficiency of these procedures were compared. One method relies on classical heterocyclic synthesis, the other one aims at late-stage decoration of a truncated scaffold via direct C-H functionalization. A pharmacological evaluation disclosed that one of the synthesized derivatives showed interesting activity on a α1β3 containing receptor subtype.
en
dc.description.sponsorship
FWF - Österr. Wissenschaftsfonds
-
dc.description.sponsorship
FWF - Österr. Wissenschaftsfonds
-
dc.language.iso
en
-
dc.publisher
SPRINGER WIEN
-
dc.relation.ispartof
Monatshefte für Chemie - Chemical Monthly
-
dc.rights.uri
http://creativecommons.org/licenses/by/4.0/
-
dc.subject
Direct C–H arylation
en
dc.subject
GABA-induced current modulation
en
dc.subject
Heterocyclic chemistry
en
dc.subject
Medicinal chemistry
en
dc.title
Novel synthetic procedures for C2 substituted imidazoquinolines as ligands for the α/β-interface of the GABAA-receptor
en
dc.type
Article
en
dc.type
Artikel
de
dc.rights.license
Creative Commons Namensnennung 4.0 International
de
dc.rights.license
Creative Commons Attribution 4.0 International
en
dc.identifier.pmid
38020487
-
dc.identifier.scopus
2-s2.0-85141002838
-
dc.identifier.url
https://api.elsevier.com/content/abstract/scopus_id/85141002838
-
dc.contributor.affiliation
TU Wien, Austria
-
dc.contributor.affiliation
Medical University of Vienna, Austria
-
dc.contributor.affiliation
Medical University of Vienna, Austria
-
dc.description.startpage
1391
-
dc.description.endpage
1404
-
dc.relation.grantno
P 27746-B27
-
dc.relation.grantno
DK W1232-B11
-
dc.rights.holder
© The Author(s) 2022
-
dc.type.category
Original Research Article
-
tuw.container.volume
154
-
tuw.container.issue
12
-
tuw.journal.peerreviewed
true
-
tuw.peerreviewed
true
-
tuw.project.title
Liganden für das alpha+/ beta- interface am GABAA Rezeptor
-
tuw.project.title
Doktoratskolleg W 1232-B11
-
tuw.researchinfrastructure
Zentrum für Kernspinresonanzspektroskopie
-
tuw.researchTopic.id
M6
-
tuw.researchTopic.name
Biological and Bioactive Materials
-
tuw.researchTopic.value
100
-
dcterms.isPartOf.title
Monatshefte für Chemie - Chemical Monthly
-
tuw.publication.orgunit
E163 - Institut für Angewandte Synthesechemie
-
tuw.publication.orgunit
E163-03 - Forschungsbereich Organische und Biologische Chemie
-
tuw.publication.orgunit
E163-03-4 - Forschungsgruppe Bioorganische Synthesechemie
-
tuw.publisher.doi
10.1007/s00706-022-02988-8
-
dc.date.onlinefirst
2022-10-29
-
dc.identifier.eissn
1434-4475
-
dc.identifier.libraryid
AC17205330
-
dc.description.numberOfPages
14
-
tuw.author.orcid
0000-0002-9884-5479
-
tuw.author.orcid
0000-0003-2946-9294
-
tuw.author.orcid
0000-0002-5438-8368
-
dc.rights.identifier
CC BY 4.0
de
dc.rights.identifier
CC BY 4.0
en
wb.sci
true
-
wb.sciencebranch
Chemie
-
wb.sciencebranch
Pharmazie, Pharmakologie, Toxikologie
-
wb.sciencebranch.oefos
1040
-
wb.sciencebranch.oefos
3012
-
wb.sciencebranch.value
80
-
wb.sciencebranch.value
20
-
item.fulltext
with Fulltext
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item.openairecristype
http://purl.org/coar/resource_type/c_2df8fbb1
-
item.languageiso639-1
en
-
item.cerifentitytype
Publications
-
item.mimetype
application/pdf
-
item.openaccessfulltext
Open Access
-
item.openairetype
research article
-
item.grantfulltext
mixedopen
-
crisitem.author.dept
E163-03-4 - Forschungsgruppe Bioorganische Synthesechemie
-
crisitem.author.dept
TU Wien
-
crisitem.author.dept
E163 - Institut für Angewandte Synthesechemie
-
crisitem.author.dept
Medical University of Vienna, Austria
-
crisitem.author.dept
E163-03-4 - Forschungsgruppe Bioorganische Synthesechemie
-
crisitem.author.dept
E163 - Institut für Angewandte Synthesechemie
-
crisitem.author.dept
E163-03-4 - Forschungsgruppe Bioorganische Synthesechemie
-
crisitem.author.orcid
0000-0002-9884-5479
-
crisitem.author.orcid
0000-0003-2946-9294
-
crisitem.author.orcid
0000-0002-5438-8368
-
crisitem.author.parentorg
E163-03 - Forschungsbereich Organische und Biologische Chemie
-
crisitem.author.parentorg
E150 - Fakultät für Technische Chemie
-
crisitem.author.parentorg
E163-03 - Forschungsbereich Organische und Biologische Chemie
-
crisitem.author.parentorg
E150 - Fakultät für Technische Chemie
-
crisitem.author.parentorg
E163-03 - Forschungsbereich Organische und Biologische Chemie
-
crisitem.project.funder
FWF - Österr. Wissenschaftsfonds
-
crisitem.project.funder
FWF - Österr. Wissenschaftsfonds
-
crisitem.project.grantno
P 27746-B27
-
crisitem.project.grantno
DK W1232-B11
-
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