Note to users. If you're seeing this message, it means that your browser cannot find this page's style/presentation instructions -- or possibly that you are using a browser that does not support current Web standards. Find out more about why this message is appearing, and what you can do to make your experience of our site the best it can be.
Sci. Signal., 30 June 2009
Vol. 2, Issue 77, p. ra31
[DOI: 10.1126/scisignal.2000352]
RESEARCH ARTICLES
Therapeutically Targeting ErbB3: A Key Node in Ligand-Induced Activation of the ErbB Receptor–PI3K Axis
Birgit Schoeberl*,
Emily A. Pace*,
Jonathan B. Fitzgerald*,
Brian D. Harms,
Lihui Xu,
Lin Nie,
Bryan Linggi,
Ashish Kalra,
Violette Paragas,
Raghida Bukhalid,
Viara Grantcharova,
Neeraj Kohli,
Kip A. West,
Magdalena Leszczyniecka,
Michael J. Feldhaus,
Arthur J. Kudla, and
Ulrik B. Nielsen
Merrimack Pharmaceuticals, One Kendall Square, Building 700, Cambridge, MA 02139, USA.
* These authors contributed equally to this work.
Abstract:
The signaling network downstream of the ErbB family of receptors has been extensively targeted by cancer therapeutics; however, understanding the relative importance of the different components of the ErbB network is nontrivial. To explore the optimal way to therapeutically inhibit combinatorial, ligand-induced activation of the ErbB–phosphatidylinositol 3-kinase (PI3K) axis, we built a computational model of the ErbB signaling network that describes the most effective ErbB ligands, as well as known and previously unidentified ErbB inhibitors. Sensitivity analysis identified ErbB3 as the key node in response to ligands that can bind either ErbB3 or EGFR (epidermal growth factor receptor). We describe MM-121, a human monoclonal antibody that halts the growth of tumor xenografts in mice and, consistent with model-simulated inhibitor data, potently inhibits ErbB3 phosphorylation in a manner distinct from that of other ErbB-targeted therapies. MM-121, a previously unidentified anticancer therapeutic designed using a systems approach, promises to benefit patients with combinatorial, ligand-induced activation of the ErbB signaling network that are not effectively treated by current therapies targeting overexpressed or mutated oncogenes.
To whom correspondence should be addressed. E-mail: unielsen{at}merrimackpharma.com
Citation: B. Schoeberl, E. A. Pace, J. B. Fitzgerald, B. D. Harms, L. Xu, L. Nie, B. Linggi, A. Kalra, V. Paragas, R. Bukhalid, V. Grantcharova, N. Kohli, K. A. West, M. Leszczyniecka, M. J. Feldhaus, A. J. Kudla, U. B. Nielsen, Therapeutically Targeting ErbB3: A Key Node in Ligand-Induced Activation of the ErbB Receptor–PI3K Axis. Sci. Signal.2, ra31 (2009).
The editors suggest the following Related Resources on Science sites:
In Science Signaling
EDITORIAL GUIDES
Nancy R. Gough (6 September 2011) Sci. Signal.4 (189), eg8.
[DOI: 10.1126/scisignal.2002478] |Abstract »|Full Text »|PDF »
EDITORIAL GUIDES
Elizabeth M. Adler and Nancy R. Gough (29 March 2011) Sci. Signal.4 (166), eg3.
[DOI: 10.1126/scisignal.2002014] |Abstract »|Full Text »|PDF »
EDITORS' CHOICE
Nancy R. Gough (7 December 2010) Sci. Signal.3 (151), ec373.
[DOI: 10.1126/scisignal.3151ec373] |Abstract »
EDITORS' CHOICE
Nancy R. Gough (19 October 2010) Sci. Signal.3 (144), ec322.
[DOI: 10.1126/scisignal.3144ec322] |Abstract »
RESEARCH ARTICLES
Igor Astsaturov, Vladimir Ratushny, Anna Sukhanova, Margret B. Einarson, Tetyana Bagnyukova, Yan Zhou, Karthik Devarajan, Joshua S. Silverman, Nadezhda Tikhmyanova, Natalya Skobeleva, Anna Pecherskaya, Rochelle E. Nasto, Catherine Sharma, Sandra A. Jablonski, Ilya G. Serebriiskii, Louis M. Weiner, and Erica A. Golemis (21 September 2010) Sci. Signal.3 (140), ra67.
[DOI: 10.1126/scisignal.2001083] |Editor's Summary »|Abstract »|Full Text »|PDF »|Supplementary Materials »
EDITORS' CHOICE
Annalisa M. VanHook (4 May 2010) Sci. Signal.3 (120), ec133.
[DOI: 10.1126/scisignal.3120ec133] |Abstract »
EDITORIAL GUIDES
Elizabeth M. Adler (5 January 2010) Sci. Signal.3 (103), eg1.
[DOI: 10.1126/scisignal.3103eg1] |Abstract »|Full Text »|PDF »
PODCASTS
Michael B. Yaffe and Annalisa M. VanHook (5 January 2010) Sci. Signal.3 (103), pc1.
[DOI: 10.1126/scisignal.3103pc1] |Abstract »|Full Text »|Podcast »
EDITORS' CHOICE
Nancy R. Gough (15 September 2009) Sci. Signal.2 (88), ec304.
[DOI: 10.1126/scisignal.288ec304] |Abstract »
PODCASTS
Ulrik B. Nielsen and Annalisa M. VanHook (30 June 2009) Sci. Signal.2 (77), pc12.
[DOI: 10.1126/scisignal.277pc12] |Abstract »|Full Text »|Podcast »
In Science Magazine
EDITORS' CHOICE: HIGHLIGHTS OF THE RECENT LITERATURE
L. Bryan Ray (24 July 2009) Science325 (5939), 369-b.
[DOI: 10.1126/science.325_369b] |Full Text »|PDF »
THIS ARTICLE HAS BEEN CITED BY OTHER ARTICLES:
Using Partial Least Squares Regression to Analyze Cellular Response Data.
Antitumor Activity of a Novel Bispecific Antibody That Targets the ErbB2/ErbB3 Oncogenic Unit and Inhibits Heregulin-Induced Activation of ErbB3.
C. F. McDonagh, A. Huhalov, B. D. Harms, S. Adams, V. Paragas, S. Oyama, B. Zhang, L. Luus, R. Overland, S. Nguyen, et al. (2012)
Mol. Cancer Ther.
11, 582-593
|Abstract »|Full Text »|PDF »
Reduction of Complex Signaling Networks to a Representative Kernel.
J.-R. Kim, J. Kim, Y.-K. Kwon, H.-Y. Lee, P. Heslop-Harrison, and K.-H. Cho (2011)
Science Signaling
4, ra35
|Abstract »|Full Text »|PDF »
Combining phage and staphylococcal surface display for generation of ErbB3-specific Affibody molecules.
N. Kronqvist, M. Malm, L. Gostring, E. Gunneriusson, M. Nilsson, I. Hoiden Guthenberg, L. Gedda, F. Y. Frejd, S. Stahl, and J. Lofblom (2011)
Protein Eng. Des. Sel.
24, 385-396
|Abstract »|Full Text »|PDF »
Receptor Tyrosine Kinase Coactivation Networks in Cancer.
An ErbB3 Antibody, MM-121, Is Active in Cancers with Ligand-Dependent Activation.
B. Schoeberl, A. C. Faber, D. Li, M.-C. Liang, K. Crosby, M. Onsum, O. Burenkova, E. Pace, Z. Walton, L. Nie, et al. (2010)
Cancer Res.
70, 2485-2494
|Abstract »|Full Text »|PDF »
