Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting

Hirokazu Matsushita; Matthew D. Vesely; Daniel C. Koboldt; Charles G. Rickert; Ravindra Uppaluri; Vincent J. Magrini; Cora D. Arthur; J. Michael White; Yee Shiuan Chen; Lauren K. Shea; Jasreet Hundal; Michael C. Wendl; Ryan Demeter; Todd Wylie; James P. Allison; Mark J. Smyth; Lloyd J. Old; Elaine R. Mardis; Robert D. Schreiber

doi:10.1038/nature10755

Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting

Hirokazu Matsushita, Matthew D. Vesely, Daniel C. Koboldt, Charles G. Rickert, Ravindra Uppaluri, Vincent J. Magrini, Cora D. Arthur, J. Michael White, Yee Shiuan Chen, Lauren K. Shea, Jasreet Hundal, Michael C. Wendl, Ryan Demeter, Todd Wylie, James P. Allison, Mark J. Smyth, Lloyd J. Old, Elaine R. Mardis, Robert D. Schreiber

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

984 Scopus citations

Abstract

Cancer immunoediting, the process by which the immune system controls tumour outgrowth and shapes tumour immunogenicity, is comprised of three phases: elimination, equilibrium and escape. Although many immune components that participate in this process are known, its underlying mechanisms remain poorly defined. A central tenet of cancer immunoediting is that T-cell recognition of tumour antigens drives the immunological destruction or sculpting of a developing cancer. However, our current understanding of tumour antigens comes largely from analyses of cancers that develop in immunocompetent hosts and thus may have already been edited. Little is known about the antigens expressed in nascent tumour cells, whether they are sufficient to induce protective antitumour immune responses or whether their expression is modulated by the immune system. Here, using massively parallel sequencing, we characterize expressed mutations in highly immunogenic methylcholanthrene-induced sarcomas derived from immunodeficient Rag2 ^-/- mice that phenotypically resemble nascent primary tumour cells. Using class I prediction algorithms, we identify mutant spectrin-β2 as a potential rejection antigen of the d42m1 sarcoma and validate this prediction by conventional antigen expression cloning and detection. We also demonstrate that cancer immunoediting of d42m1 occurs via a T-cell-dependent immunoselection process that promotes outgrowth of pre-existing tumour cell clones lacking highly antigenic mutant spectrin-β2 and other potential strong antigens. These results demonstrate that the strong immunogenicity of an unedited tumour can be ascribed to expression of highly antigenic mutant proteins and show that outgrowth of tumour cells that lack these strong antigens via a T-cell-dependent immunoselection process represents one mechanism of cancer immunoediting.

Original language	English (US)
Pages (from-to)	400-404
Number of pages	5
Journal	Nature
Volume	482
Issue number	7385
DOIs	https://doi.org/10.1038/nature10755
State	Published - Feb 16 2012
Externally published	Yes

ASJC Scopus subject areas

General

Access to Document

10.1038/nature10755

Cite this

Matsushita, H., Vesely, M. D., Koboldt, D. C., Rickert, C. G., Uppaluri, R., Magrini, V. J., Arthur, C. D., White, J. M., Chen, Y. S., Shea, L. K., Hundal, J., Wendl, M. C., Demeter, R., Wylie, T., Allison, J. P., Smyth, M. J., Old, L. J., Mardis, E. R., & Schreiber, R. D. (2012). Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting. Nature, 482(7385), 400-404. https://doi.org/10.1038/nature10755

Matsushita, H, Vesely, MD, Koboldt, DC, Rickert, CG, Uppaluri, R, Magrini, VJ, Arthur, CD, White, JM, Chen, YS, Shea, LK, Hundal, J, Wendl, MC, Demeter, R, Wylie, T, Allison, JP, Smyth, MJ, Old, LJ, Mardis, ER & Schreiber, RD 2012, 'Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting', Nature, vol. 482, no. 7385, pp. 400-404. https://doi.org/10.1038/nature10755

@article{0745ba11d1d84a6f8e48e0f092daea56,

title = "Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting",

abstract = "Cancer immunoediting, the process by which the immune system controls tumour outgrowth and shapes tumour immunogenicity, is comprised of three phases: elimination, equilibrium and escape. Although many immune components that participate in this process are known, its underlying mechanisms remain poorly defined. A central tenet of cancer immunoediting is that T-cell recognition of tumour antigens drives the immunological destruction or sculpting of a developing cancer. However, our current understanding of tumour antigens comes largely from analyses of cancers that develop in immunocompetent hosts and thus may have already been edited. Little is known about the antigens expressed in nascent tumour cells, whether they are sufficient to induce protective antitumour immune responses or whether their expression is modulated by the immune system. Here, using massively parallel sequencing, we characterize expressed mutations in highly immunogenic methylcholanthrene-induced sarcomas derived from immunodeficient Rag2 -/- mice that phenotypically resemble nascent primary tumour cells. Using class I prediction algorithms, we identify mutant spectrin-β2 as a potential rejection antigen of the d42m1 sarcoma and validate this prediction by conventional antigen expression cloning and detection. We also demonstrate that cancer immunoediting of d42m1 occurs via a T-cell-dependent immunoselection process that promotes outgrowth of pre-existing tumour cell clones lacking highly antigenic mutant spectrin-β2 and other potential strong antigens. These results demonstrate that the strong immunogenicity of an unedited tumour can be ascribed to expression of highly antigenic mutant proteins and show that outgrowth of tumour cells that lack these strong antigens via a T-cell-dependent immunoselection process represents one mechanism of cancer immunoediting.",

author = "Hirokazu Matsushita and Vesely, {Matthew D.} and Koboldt, {Daniel C.} and Rickert, {Charles G.} and Ravindra Uppaluri and Magrini, {Vincent J.} and Arthur, {Cora D.} and White, {J. Michael} and Chen, {Yee Shiuan} and Shea, {Lauren K.} and Jasreet Hundal and Wendl, {Michael C.} and Ryan Demeter and Todd Wylie and Allison, {James P.} and Smyth, {Mark J.} and Old, {Lloyd J.} and Mardis, {Elaine R.} and Schreiber, {Robert D.}",

note = "Funding Information: Acknowledgements We are grateful to J. Archambault for expert technical assistance, T. H. Hansen (Washington University) for providing MHC class I antibodies, S. Horvath and P. M. Allen (Washington University) for synthesizing MHC class I peptides, the National Institutes of Health (NIH) Tetramer Core Facility for producing MHC class I tetramers, and T. S. Stappenbeck (Washington University) for technical help in recovering frozen tumour samples. We also thank E. Unanue, P. M. Allen and J. Bui for criticisms and comments, all members of the Schreiber laboratory for discussions, and the many members of The Genome Institute at Washington University School of Medicine, especially L. Ding for her insights into our analytical approaches. This work was supported by grants to R.D.S. from the National Cancer Institute, the Ludwig Institute for Cancer Research, the Cancer Research Institute, and the WWWW Foundation; and to E.R.M. from the NationalHuman Genome Research Institute. M.D.V. is supported by a pre-doctoral fellowship from the Cancer Research Institute. J.P.A. is supported by the Howard Hughes Medical Institute and the Ludwig Center for Cancer Immunotherapy; M.J.S. by the National Health and Medical Research Council of Australia (NH&MRC) and from the Association for International Cancer Research; and L.J.O. by the Ludwig Institute for Cancer Research and the Cancer Research Institute.",

year = "2012",

month = feb,

day = "16",

doi = "10.1038/nature10755",

language = "English (US)",

volume = "482",

pages = "400--404",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Publishing Group",

number = "7385",

}

TY - JOUR

T1 - Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting

AU - Matsushita, Hirokazu

AU - Vesely, Matthew D.

AU - Koboldt, Daniel C.

AU - Rickert, Charles G.

AU - Uppaluri, Ravindra

AU - Magrini, Vincent J.

AU - Arthur, Cora D.

AU - White, J. Michael

AU - Chen, Yee Shiuan

AU - Shea, Lauren K.

AU - Hundal, Jasreet

AU - Wendl, Michael C.

AU - Demeter, Ryan

AU - Wylie, Todd

AU - Allison, James P.

AU - Smyth, Mark J.

AU - Old, Lloyd J.

AU - Mardis, Elaine R.

AU - Schreiber, Robert D.

N1 - Funding Information: Acknowledgements We are grateful to J. Archambault for expert technical assistance, T. H. Hansen (Washington University) for providing MHC class I antibodies, S. Horvath and P. M. Allen (Washington University) for synthesizing MHC class I peptides, the National Institutes of Health (NIH) Tetramer Core Facility for producing MHC class I tetramers, and T. S. Stappenbeck (Washington University) for technical help in recovering frozen tumour samples. We also thank E. Unanue, P. M. Allen and J. Bui for criticisms and comments, all members of the Schreiber laboratory for discussions, and the many members of The Genome Institute at Washington University School of Medicine, especially L. Ding for her insights into our analytical approaches. This work was supported by grants to R.D.S. from the National Cancer Institute, the Ludwig Institute for Cancer Research, the Cancer Research Institute, and the WWWW Foundation; and to E.R.M. from the NationalHuman Genome Research Institute. M.D.V. is supported by a pre-doctoral fellowship from the Cancer Research Institute. J.P.A. is supported by the Howard Hughes Medical Institute and the Ludwig Center for Cancer Immunotherapy; M.J.S. by the National Health and Medical Research Council of Australia (NH&MRC) and from the Association for International Cancer Research; and L.J.O. by the Ludwig Institute for Cancer Research and the Cancer Research Institute.

PY - 2012/2/16

Y1 - 2012/2/16

N2 - Cancer immunoediting, the process by which the immune system controls tumour outgrowth and shapes tumour immunogenicity, is comprised of three phases: elimination, equilibrium and escape. Although many immune components that participate in this process are known, its underlying mechanisms remain poorly defined. A central tenet of cancer immunoediting is that T-cell recognition of tumour antigens drives the immunological destruction or sculpting of a developing cancer. However, our current understanding of tumour antigens comes largely from analyses of cancers that develop in immunocompetent hosts and thus may have already been edited. Little is known about the antigens expressed in nascent tumour cells, whether they are sufficient to induce protective antitumour immune responses or whether their expression is modulated by the immune system. Here, using massively parallel sequencing, we characterize expressed mutations in highly immunogenic methylcholanthrene-induced sarcomas derived from immunodeficient Rag2 -/- mice that phenotypically resemble nascent primary tumour cells. Using class I prediction algorithms, we identify mutant spectrin-β2 as a potential rejection antigen of the d42m1 sarcoma and validate this prediction by conventional antigen expression cloning and detection. We also demonstrate that cancer immunoediting of d42m1 occurs via a T-cell-dependent immunoselection process that promotes outgrowth of pre-existing tumour cell clones lacking highly antigenic mutant spectrin-β2 and other potential strong antigens. These results demonstrate that the strong immunogenicity of an unedited tumour can be ascribed to expression of highly antigenic mutant proteins and show that outgrowth of tumour cells that lack these strong antigens via a T-cell-dependent immunoselection process represents one mechanism of cancer immunoediting.

AB - Cancer immunoediting, the process by which the immune system controls tumour outgrowth and shapes tumour immunogenicity, is comprised of three phases: elimination, equilibrium and escape. Although many immune components that participate in this process are known, its underlying mechanisms remain poorly defined. A central tenet of cancer immunoediting is that T-cell recognition of tumour antigens drives the immunological destruction or sculpting of a developing cancer. However, our current understanding of tumour antigens comes largely from analyses of cancers that develop in immunocompetent hosts and thus may have already been edited. Little is known about the antigens expressed in nascent tumour cells, whether they are sufficient to induce protective antitumour immune responses or whether their expression is modulated by the immune system. Here, using massively parallel sequencing, we characterize expressed mutations in highly immunogenic methylcholanthrene-induced sarcomas derived from immunodeficient Rag2 -/- mice that phenotypically resemble nascent primary tumour cells. Using class I prediction algorithms, we identify mutant spectrin-β2 as a potential rejection antigen of the d42m1 sarcoma and validate this prediction by conventional antigen expression cloning and detection. We also demonstrate that cancer immunoediting of d42m1 occurs via a T-cell-dependent immunoselection process that promotes outgrowth of pre-existing tumour cell clones lacking highly antigenic mutant spectrin-β2 and other potential strong antigens. These results demonstrate that the strong immunogenicity of an unedited tumour can be ascribed to expression of highly antigenic mutant proteins and show that outgrowth of tumour cells that lack these strong antigens via a T-cell-dependent immunoselection process represents one mechanism of cancer immunoediting.

UR - http://www.scopus.com/inward/record.url?scp=84862776855&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84862776855&partnerID=8YFLogxK

U2 - 10.1038/nature10755

DO - 10.1038/nature10755

M3 - Article

C2 - 22318521

AN - SCOPUS:84862776855

SN - 0028-0836

VL - 482

SP - 400

EP - 404

JO - Nature

JF - Nature

IS - 7385

ER -

Cancer exome analysis reveals a T-cell-dependent mechanism of cancer immunoediting

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this