Pharmacological targeting of the pseudokinase Her3

Ting Xie; Sang M.in Lim; Kenneth D. Westover; Michael E. Dodge; Dalia Ercan; Scott B. Ficarro; Durga Udayakumar; Deepak Gurbani; Hyun S.eop Tae; Steven M. Riddle; Taebo Sim; Jarrod A. Marto; Pasi A. Jänne; Craig M. Crews; Nathanael S. Gray

doi:10.1038/nchembio.1658

Pharmacological targeting of the pseudokinase Her3

Ting Xie
, Sang M.in Lim
, Kenneth D. Westover
, Michael E. Dodge
, Dalia Ercan
, Scott B. Ficarro
, Durga Udayakumar
, Deepak Gurbani
, Hyun S.eop Tae
, Steven M. Riddle
, Taebo Sim
, Jarrod A. Marto
, Pasi A. Jänne
, Craig M. Crews
, Nathanael S. Gray

Research output: Contribution to journal › Article › peer-review

176 Citations (Scopus)

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.

Original language	English
Pages (from-to)	1006-1012
Number of pages	7
Journal	Nature Chemical Biology
Volume	10
Issue number	12
DOIs	https://doi.org/10.1038/nchembio.1658
Publication status	Published - 2014 Dec 1

Bibliographical note

Funding Information:
This work is supported by the Dana Farber Cancer Institute Lander Fellowship (T.X.), Claudia Adams Barr Program Award (N.S.G.), US National Institutes of Health (NIH) grant AI 084140-03 (C.M.C.), Cancer Prevention Research Institute of Texas grant R1207 (K.D.W.), creative/challenging research program of National Research Foundation of Korea NRF-2011-0028676 (T.S.) and NIH grant P01 CA154303 (P.A.J. and N.S.G.).

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1038/nchembio.1658

Cite this

@article{aea8685e476042f0983898ef02a90cfc,

title = "Pharmacological targeting of the pseudokinase Her3",

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. ",

author = "Ting Xie and Lim, \{Sang M.in\} and Westover, \{Kenneth D.\} and Dodge, \{Michael E.\} and Dalia Ercan and Ficarro, \{Scott B.\} and Durga Udayakumar and Deepak Gurbani and Tae, \{Hyun S.eop\} and Riddle, \{Steven M.\} and Taebo Sim and Marto, \{Jarrod A.\} and J{\"a}nne, \{Pasi A.\} and Crews, \{Craig M.\} and Gray, \{Nathanael S.\}",

note = "Funding Information: This work is supported by the Dana Farber Cancer Institute Lander Fellowship (T.X.), Claudia Adams Barr Program Award (N.S.G.), US National Institutes of Health (NIH) grant AI 084140-03 (C.M.C.), Cancer Prevention Research Institute of Texas grant R1207 (K.D.W.), creative/challenging research program of National Research Foundation of Korea NRF-2011-0028676 (T.S.) and NIH grant P01 CA154303 (P.A.J. and N.S.G.).",

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language = "English",

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AU - Xie, Ting

AU - Lim, Sang M.in

AU - Westover, Kenneth D.

AU - Dodge, Michael E.

AU - Ercan, Dalia

AU - Ficarro, Scott B.

AU - Udayakumar, Durga

AU - Gurbani, Deepak

AU - Tae, Hyun S.eop

AU - Riddle, Steven M.

AU - Sim, Taebo

AU - Marto, Jarrod A.

AU - Jänne, Pasi A.

AU - Crews, Craig M.

AU - Gray, Nathanael S.

N1 - Funding Information: This work is supported by the Dana Farber Cancer Institute Lander Fellowship (T.X.), Claudia Adams Barr Program Award (N.S.G.), US National Institutes of Health (NIH) grant AI 084140-03 (C.M.C.), Cancer Prevention Research Institute of Texas grant R1207 (K.D.W.), creative/challenging research program of National Research Foundation of Korea NRF-2011-0028676 (T.S.) and NIH grant P01 CA154303 (P.A.J. and N.S.G.).

PY - 2014/12/1

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N2 - 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.

AB - 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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ER -

Pharmacological targeting of the pseudokinase Her3

Abstract

Bibliographical note

UN SDGs

ASJC Scopus subject areas

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