| Literature DB >> 29396292 |
Susanne Höing1, Ting-Yu Yeh2, Matthias Baumann3, Nancy E Martinez4, Peter Habenberger3, Lea Kremer5, Hannes C A Drexler6, Philipp Küchler4, Peter Reinhardt7, Axel Choidas3, Mia-Lisa Zischinsky3, Gunther Zischinsky3, Swaran Nandini8, Aaron P Ledray8, Stephanie A Ketcham2, Lydia Reinhardt7, Masin Abo-Rady9, Michael Glatza7, Stephen J King8, Peter Nussbaumer3, Slava Ziegler4, Bert Klebl3, Trina A Schroer10, Hans R Schöler11, Herbert Waldmann12, Jared Sterneckert13.
Abstract
Aberrant hedgehog (Hh) signaling contributes to the pathogenesis of multiple cancers. Available inhibitors target Smoothened (Smo), which can acquire mutations causing drug resistance. Thus, compounds that inhibit Hh signaling downstream of Smo are urgently needed. We identified dynarrestin, a novel inhibitor of cytoplasmic dyneins 1 and 2. Dynarrestin acts reversibly to inhibit cytoplasmic dynein 1-dependent microtubule binding and motility in vitro without affecting ATP hydrolysis. It rapidly and reversibly inhibits endosome movement in living cells and perturbs mitosis by inducing spindle misorientation and pseudoprometaphase delay. Dynarrestin reversibly inhibits cytoplasmic dynein 2-dependent intraflagellar transport (IFT) of the cargo IFT88 and flux of Smo within cilia without interfering with ciliogenesis and suppresses Hh-dependent proliferation of neuronal precursors and tumor cells. As such, dynarrestin is a valuable tool for probing cytoplasmic dynein-dependent cellular processes and a promising compound for medicinal chemistry programs aimed at development of anti-cancer drugs.Entities:
Keywords: ciliary transport; ciliobrevin; dynein; glioblastoma; hedgehog; intraflagellar transport; phenotypic screening; stem cell-based phenotypic screening; vismodegib
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Year: 2018 PMID: 29396292 DOI: 10.1016/j.chembiol.2017.12.014
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116