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The experimental power of FR900359 to study Gq-regulated biological processes.

Authors :
Schrage R
Schmitz AL
Gaffal E
Annala S
Kehraus S
Wenzel D
Büllesbach KM
Bald T
Inoue A
Shinjo Y
Galandrin S
Shridhar N
Hesse M
Grundmann M
Merten N
Charpentier TH
Martz M
Butcher AJ
Slodczyk T
Armando S
Effern M
Namkung Y
Jenkins L
Horn V
Stößel A
Dargatz H
Tietze D
Imhof D
Galés C
Drewke C
Müller CE
Hölzel M
Milligan G
Tobin AB
Gomeza J
Dohlman HG
Sondek J
Harden TK
Bouvier M
Laporte SA
Aoki J
Fleischmann BK
Mohr K
König GM
Tüting T
Kostenis E
Source :
Nature communications [Nat Commun] 2015 Dec 14; Vol. 6, pp. 10156. Date of Electronic Publication: 2015 Dec 14.
Publication Year :
2015

Abstract

Despite the discovery of heterotrimeric αβγ G proteins ∼25 years ago, their selective perturbation by cell-permeable inhibitors remains a fundamental challenge. Here we report that the plant-derived depsipeptide FR900359 (FR) is ideally suited to this task. Using a multifaceted approach we systematically characterize FR as a selective inhibitor of Gq/11/14 over all other mammalian Gα isoforms and elaborate its molecular mechanism of action. We also use FR to investigate whether inhibition of Gq proteins is an effective post-receptor strategy to target oncogenic signalling, using melanoma as a model system. FR suppresses many of the hallmark features that are central to the malignancy of melanoma cells, thereby providing new opportunities for therapeutic intervention. Just as pertussis toxin is used extensively to probe and inhibit the signalling of Gi/o proteins, we anticipate that FR will at least be its equivalent for investigating the biological relevance of Gq.

Details

Language :
English
ISSN :
2041-1723
Volume :
6
Database :
MEDLINE
Journal :
Nature communications
Publication Type :
Academic Journal
Accession number :
26658454
Full Text :
https://doi.org/10.1038/ncomms10156