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Pharmacological targeting of the pseudokinase Her3

Authors
Xie, TingLim, Sang MinWestover, Kenneth D.Dodge, Michael E.Ercan, DaliaFicarro, Scott B.Udayakumar, DurgaGurbani, DeepakTae, Hyun SeopRiddle, Steven M.Sim, TaeboMarto, Jarrod A.Jaenne, Pasi A.Crews, Craig M.Gray, Nathanael S.
Issue Date
12월-2014
Publisher
NATURE PUBLISHING GROUP
Citation
NATURE CHEMICAL BIOLOGY, v.10, no.12, pp.1006 - +
Indexed
SCIE
SCOPUS
Journal Title
NATURE CHEMICAL BIOLOGY
Volume
10
Number
12
Start Page
1006
End Page
+
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/96612
DOI
10.1038/nchembio.1658
ISSN
1552-4450
Abstract
Her3 (also known as ErbB3) belongs to the epidermal growth factor receptor tyrosine kinases and is well credentialed as an anti-cancer target but is thought to be 'undruggable' using ATP-competitive small molecules because it lacks appreciable kinase activity. Here we report what is to our knowledge the first selective Her3 ligand, TX1-85-1, that forms a covalent bond with Cys721 located in the ATP-binding site of Her3. We demonstrate that covalent modification of Her3 inhibits Her3 signaling but not proliferation in some Her3-dependent cancer cell lines. Subsequent derivatization with a hydrophobic adamantane moiety demonstrates that the resultant bivalent ligand (TX2-121-1) enhances inhibition of Her3-dependent signaling. Treatment of cells with TX2-121-1 results in partial degradation of Her3 and serendipitously interferes with productive heterodimerization between Her3 with either Her2 or c-Met. These results suggest that small molecules will be capable of perturbing the biological function of Her3 and -60 other pseudokinases found in human cells.
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