Antibodies specifically targeting a locally misfolded region of tumor associated EGFR

Thomas P.J. Garrett; Antony W. Burgess; Hui K. Gan; Rod B. Luwor; Glenn Cartwright; Francesca Walker; Suzanne G. Orchard; Andrew H.A. Clayton; Edouard C. Nice; Julie Rothacker; Bruno Catimel; Webster K. Cavenee; Lloyd J. Old; Elisabeth Stockert; Gerd Ritter; Timothy E. Adams; Peter A. Hoyne; Dane Wittrup; Ginger Chao; Jennifer R. Cochran; Cindy Luo; Mezhen Lou; Trevor Huyton; Yibin Xu; W. Douglas Fairlie; Shenggen Yao; Andrew M. Scott; Terrance G. Johns

doi:10.1073/pnas.0811559106

Antibodies specifically targeting a locally misfolded region of tumor associated EGFR

Thomas P.J. Garrett
, Antony W. Burgess
, Hui K. Gan
, Rod B. Luwor
, Glenn Cartwright
, Francesca Walker
, Suzanne G. Orchard
, Andrew H.A. Clayton
, Edouard C. Nice
, Julie Rothacker
, Bruno Catimel
, Webster K. Cavenee
, Lloyd J. Old
, Elisabeth Stockert
, Gerd Ritter
, Timothy E. Adams
, Peter A. Hoyne
, Dane Wittrup
, Ginger Chao
, Jennifer R. Cochran

Cindy Luo, Mezhen Lou, Trevor Huyton, Yibin Xu, W. Douglas Fairlie, Shenggen Yao, Andrew M. Scott, Terrance G. Johns

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

71 Citations (Scopus)

Abstract

Epidermal Growth Factor Receptor (EGFR) is involved in stimulating the growth of many human tumors, but the success of therapeutic agents has been limited in part by interference from the EGFR on normal tissues. Previously, we reported an antibody (mab806) against a truncated form of EGFR found commonly in gliomas. Remarkably, it also recognizes full-length EGFR on tumor cells but not on normal cells. However, the mechanism for this activity was unclear. Crystallographic structures for Fab:EGFR_287-302 complexes of mAb806 (and a second, related antibody, mAb175) show that this peptide epitope adopts conformations similar to those found in the wtEGFR. However, in both conformations observed for wtEGFR, tethered and untethered, antibody binding would be prohibited by significant steric clashes with the CR1 domain. Thus, these antibodies must recognize a cryptic epitope in EGFR. Structurally, it appeared that breaking the disulfide bond preceding the epitope might allow the CR1 domain to open up sufficiently for antibody binding. The EGFR _C271A/C283A mutant not only binds mAb806, but binds with 1:1 stoichiometry, which is significantly greater than wtEGFR binding. Although mAb806 and mAb175 decrease tumor growth in xenografts displaying mutant, overexpressed, or autocrine stimulated EGFR, neither antibody inhibits the in vitro growth of cells expressing wtEGFR. In contrast, mAb806 completely inhibits the ligand-associated stimulation of cells expressing EGFR _C271A/C283A. Clearly, the binding of mAb806 and mAb175 to the wtEGFR requires the epitope to be exposed either during receptor activation, mutation, or overexpression. This mechanism suggests the possibility of generating antibodies to target other wild-type receptors on tumor cells.

Original language	English
Pages (from-to)	5082-5087
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	106
Issue number	13
DOIs	https://doi.org/10.1073/pnas.0811559106
Publication status	Published - 31 Mar 2009
Externally published	Yes

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10.1073/pnas.0811559106

Cite this

Garrett, T. P. J., Burgess, A. W., Gan, H. K., Luwor, R. B., Cartwright, G., Walker, F., Orchard, S. G., Clayton, A. H. A., Nice, E. C., Rothacker, J., Catimel, B., Cavenee, W. K., Old, L. J., Stockert, E., Ritter, G., Adams, T. E., Hoyne, P. A., Wittrup, D., Chao, G., ... Johns, T. G. (2009). Antibodies specifically targeting a locally misfolded region of tumor associated EGFR. Proceedings of the National Academy of Sciences of the United States of America, 106(13), 5082-5087. https://doi.org/10.1073/pnas.0811559106

@article{defecc4bd2b541dfadd68d851357229f,

title = "Antibodies specifically targeting a locally misfolded region of tumor associated EGFR",

abstract = "Epidermal Growth Factor Receptor (EGFR) is involved in stimulating the growth of many human tumors, but the success of therapeutic agents has been limited in part by interference from the EGFR on normal tissues. Previously, we reported an antibody (mab806) against a truncated form of EGFR found commonly in gliomas. Remarkably, it also recognizes full-length EGFR on tumor cells but not on normal cells. However, the mechanism for this activity was unclear. Crystallographic structures for Fab:EGFR287-302 complexes of mAb806 (and a second, related antibody, mAb175) show that this peptide epitope adopts conformations similar to those found in the wtEGFR. However, in both conformations observed for wtEGFR, tethered and untethered, antibody binding would be prohibited by significant steric clashes with the CR1 domain. Thus, these antibodies must recognize a cryptic epitope in EGFR. Structurally, it appeared that breaking the disulfide bond preceding the epitope might allow the CR1 domain to open up sufficiently for antibody binding. The EGFR C271A/C283A mutant not only binds mAb806, but binds with 1:1 stoichiometry, which is significantly greater than wtEGFR binding. Although mAb806 and mAb175 decrease tumor growth in xenografts displaying mutant, overexpressed, or autocrine stimulated EGFR, neither antibody inhibits the in vitro growth of cells expressing wtEGFR. In contrast, mAb806 completely inhibits the ligand-associated stimulation of cells expressing EGFR C271A/C283A. Clearly, the binding of mAb806 and mAb175 to the wtEGFR requires the epitope to be exposed either during receptor activation, mutation, or overexpression. This mechanism suggests the possibility of generating antibodies to target other wild-type receptors on tumor cells.",

keywords = "Cancer, Cryptic, Epitope, Structure, Therapeutic antibody",

author = "Garrett, \{Thomas P.J.\} and Burgess, \{Antony W.\} and Gan, \{Hui K.\} and Luwor, \{Rod B.\} and Glenn Cartwright and Francesca Walker and Orchard, \{Suzanne G.\} and Clayton, \{Andrew H.A.\} and Nice, \{Edouard C.\} and Julie Rothacker and Bruno Catimel and Cavenee, \{Webster K.\} and Old, \{Lloyd J.\} and Elisabeth Stockert and Gerd Ritter and Adams, \{Timothy E.\} and Hoyne, \{Peter A.\} and Dane Wittrup and Ginger Chao and Cochran, \{Jennifer R.\} and Cindy Luo and Mezhen Lou and Trevor Huyton and Yibin Xu and Fairlie, \{W. Douglas\} and Shenggen Yao and Scott, \{Andrew M.\} and Johns, \{Terrance G.\}",

year = "2009",

month = mar,

day = "31",

doi = "10.1073/pnas.0811559106",

language = "English",

volume = "106",

pages = "5082--5087",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

issn = "0027-8424",

publisher = "National Academy of Sciences",

number = "13",

}

Garrett, TPJ, Burgess, AW, Gan, HK, Luwor, RB, Cartwright, G, Walker, F, Orchard, SG, Clayton, AHA, Nice, EC, Rothacker, J, Catimel, B, Cavenee, WK, Old, LJ, Stockert, E, Ritter, G, Adams, TE, Hoyne, PA, Wittrup, D, Chao, G, Cochran, JR, Luo, C, Lou, M, Huyton, T, Xu, Y, Fairlie, WD, Yao, S, Scott, AM & Johns, TG 2009, 'Antibodies specifically targeting a locally misfolded region of tumor associated EGFR', Proceedings of the National Academy of Sciences of the United States of America, vol. 106, no. 13, pp. 5082-5087. https://doi.org/10.1073/pnas.0811559106

TY - JOUR

T1 - Antibodies specifically targeting a locally misfolded region of tumor associated EGFR

AU - Garrett, Thomas P.J.

AU - Burgess, Antony W.

AU - Gan, Hui K.

AU - Luwor, Rod B.

AU - Cartwright, Glenn

AU - Walker, Francesca

AU - Orchard, Suzanne G.

AU - Clayton, Andrew H.A.

AU - Nice, Edouard C.

AU - Rothacker, Julie

AU - Catimel, Bruno

AU - Cavenee, Webster K.

AU - Old, Lloyd J.

AU - Stockert, Elisabeth

AU - Ritter, Gerd

AU - Adams, Timothy E.

AU - Hoyne, Peter A.

AU - Wittrup, Dane

AU - Chao, Ginger

AU - Cochran, Jennifer R.

AU - Luo, Cindy

AU - Lou, Mezhen

AU - Huyton, Trevor

AU - Xu, Yibin

AU - Fairlie, W. Douglas

AU - Yao, Shenggen

AU - Scott, Andrew M.

AU - Johns, Terrance G.

PY - 2009/3/31

Y1 - 2009/3/31

N2 - Epidermal Growth Factor Receptor (EGFR) is involved in stimulating the growth of many human tumors, but the success of therapeutic agents has been limited in part by interference from the EGFR on normal tissues. Previously, we reported an antibody (mab806) against a truncated form of EGFR found commonly in gliomas. Remarkably, it also recognizes full-length EGFR on tumor cells but not on normal cells. However, the mechanism for this activity was unclear. Crystallographic structures for Fab:EGFR287-302 complexes of mAb806 (and a second, related antibody, mAb175) show that this peptide epitope adopts conformations similar to those found in the wtEGFR. However, in both conformations observed for wtEGFR, tethered and untethered, antibody binding would be prohibited by significant steric clashes with the CR1 domain. Thus, these antibodies must recognize a cryptic epitope in EGFR. Structurally, it appeared that breaking the disulfide bond preceding the epitope might allow the CR1 domain to open up sufficiently for antibody binding. The EGFR C271A/C283A mutant not only binds mAb806, but binds with 1:1 stoichiometry, which is significantly greater than wtEGFR binding. Although mAb806 and mAb175 decrease tumor growth in xenografts displaying mutant, overexpressed, or autocrine stimulated EGFR, neither antibody inhibits the in vitro growth of cells expressing wtEGFR. In contrast, mAb806 completely inhibits the ligand-associated stimulation of cells expressing EGFR C271A/C283A. Clearly, the binding of mAb806 and mAb175 to the wtEGFR requires the epitope to be exposed either during receptor activation, mutation, or overexpression. This mechanism suggests the possibility of generating antibodies to target other wild-type receptors on tumor cells.

AB - Epidermal Growth Factor Receptor (EGFR) is involved in stimulating the growth of many human tumors, but the success of therapeutic agents has been limited in part by interference from the EGFR on normal tissues. Previously, we reported an antibody (mab806) against a truncated form of EGFR found commonly in gliomas. Remarkably, it also recognizes full-length EGFR on tumor cells but not on normal cells. However, the mechanism for this activity was unclear. Crystallographic structures for Fab:EGFR287-302 complexes of mAb806 (and a second, related antibody, mAb175) show that this peptide epitope adopts conformations similar to those found in the wtEGFR. However, in both conformations observed for wtEGFR, tethered and untethered, antibody binding would be prohibited by significant steric clashes with the CR1 domain. Thus, these antibodies must recognize a cryptic epitope in EGFR. Structurally, it appeared that breaking the disulfide bond preceding the epitope might allow the CR1 domain to open up sufficiently for antibody binding. The EGFR C271A/C283A mutant not only binds mAb806, but binds with 1:1 stoichiometry, which is significantly greater than wtEGFR binding. Although mAb806 and mAb175 decrease tumor growth in xenografts displaying mutant, overexpressed, or autocrine stimulated EGFR, neither antibody inhibits the in vitro growth of cells expressing wtEGFR. In contrast, mAb806 completely inhibits the ligand-associated stimulation of cells expressing EGFR C271A/C283A. Clearly, the binding of mAb806 and mAb175 to the wtEGFR requires the epitope to be exposed either during receptor activation, mutation, or overexpression. This mechanism suggests the possibility of generating antibodies to target other wild-type receptors on tumor cells.

KW - Cancer

KW - Cryptic

KW - Epitope

KW - Structure

KW - Therapeutic antibody

UR - https://www.scopus.com/pages/publications/65249179550

U2 - 10.1073/pnas.0811559106

DO - 10.1073/pnas.0811559106

M3 - Article

C2 - 19289842

AN - SCOPUS:65249179550

SN - 0027-8424

VL - 106

SP - 5082

EP - 5087

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 13

ER -

Antibodies specifically targeting a locally misfolded region of tumor associated EGFR

Abstract

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