Clonal neoantigens elicit T cell immunoreactivity and sensitivity to immune checkpoint blockade

doi:10.1126/science.aaf1490

. 2016 Mar 25;351(6280):1463-9.

doi: 10.1126/science.aaf1490. Epub 2016 Mar 3.

Clonal neoantigens elicit T cell immunoreactivity and sensitivity to immune checkpoint blockade

Nicholas McGranahan¹, Andrew J S Furness², Rachel Rosenthal³, Sofie Ramskov⁴, Rikke Lyngaa⁴, Sunil Kumar Saini⁴, Mariam Jamal-Hanjani³, Gareth A Wilson⁵, Nicolai J Birkbak⁵, Crispin T Hiley⁵, Thomas B K Watkins⁵, Seema Shafi³, Nirupa Murugaesu³, Richard Mitter⁶, Ayse U Akarca⁷, Joseph Linares⁷, Teresa Marafioti⁷, Jake Y Henry², Eliezer M Van Allen⁸, Diana Miao⁹, Bastian Schilling¹⁰, Dirk Schadendorf¹⁰, Levi A Garraway⁸, Vladimir Makarov¹¹, Naiyer A Rizvi¹², Alexandra Snyder¹³, Matthew D Hellmann¹³, Taha Merghoub¹⁴, Jedd D Wolchok¹⁵, Sachet A Shukla⁹, Catherine J Wu¹⁶, Karl S Peggs², Timothy A Chan¹¹, Sine R Hadrup⁴, Sergio A Quezada¹⁷, Charles Swanton¹⁸

Affiliations

¹ The Francis Crick Institute, London WC2A 3LY, UK. Centre for Mathematics and Physics in the Life Sciences and Experimental Biology (CoMPLEX), University College London (UCL), London WC1E 6BT, UK. Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK.
² Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK. Cancer Immunology Unit, UCL Cancer Institute, UCL, London WC1E 6BT, UK.
³ Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK.
⁴ Section for Immunology and Vaccinology, National Veterinary Institute, Technical University of Denmark, 1970 Frederiksberg C, Denmark.
⁵ The Francis Crick Institute, London WC2A 3LY, UK. Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK.
⁶ The Francis Crick Institute, London WC2A 3LY, UK.
⁷ Cancer Immunology Unit, UCL Cancer Institute, UCL, London WC1E 6BT, UK. Department of Cellular Pathology, UCL, London WC1E 6BT, UK.
⁸ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA 02215, USA. Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA. Center for Cancer Precision Medicine, Dana-Farber Cancer Institute, Boston, MA 02215, USA.
⁹ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA 02215, USA. Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA.
¹⁰ Department of Dermatology, University Hospital, University Duisburg-Essen, 45147 Essen, Germany. German Cancer Consortium (DKTK), 69121 Heidelberg, Germany.
¹¹ Human Oncology and Pathogenesis Program, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
¹² Hematology/Oncology Division, 177 Fort Washington Avenue, Columbia University, New York, NY 10032, USA.
¹³ Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA. Weill Cornell Medical College, New York, NY 10065, USA.
¹⁴ Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA. Ludwig Collaborative Laboratory, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
¹⁵ Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA. Weill Cornell Medical College, New York, NY 10065, USA. Ludwig Collaborative Laboratory, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
¹⁶ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA 02215, USA. Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA. Department of Medicine, Harvard Medical School, Boston, MA 02115, USA. Department of Internal Medicine, Brigham and Woman's Hospital, Boston, MA 02115, USA.
¹⁷ Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK. Cancer Immunology Unit, UCL Cancer Institute, UCL, London WC1E 6BT, UK. s.quezada@ucl.ac.uk charles.swanton@crick.ac.uk.
¹⁸ The Francis Crick Institute, London WC2A 3LY, UK. Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK. s.quezada@ucl.ac.uk charles.swanton@crick.ac.uk.

PMID: 26940869
PMCID: PMC4984254
DOI: 10.1126/science.aaf1490

Clonal neoantigens elicit T cell immunoreactivity and sensitivity to immune checkpoint blockade

Nicholas McGranahan et al. Science. 2016.

. 2016 Mar 25;351(6280):1463-9.

doi: 10.1126/science.aaf1490. Epub 2016 Mar 3.

Authors

Affiliations

¹ The Francis Crick Institute, London WC2A 3LY, UK. Centre for Mathematics and Physics in the Life Sciences and Experimental Biology (CoMPLEX), University College London (UCL), London WC1E 6BT, UK. Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK.
² Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK. Cancer Immunology Unit, UCL Cancer Institute, UCL, London WC1E 6BT, UK.
³ Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK.
⁴ Section for Immunology and Vaccinology, National Veterinary Institute, Technical University of Denmark, 1970 Frederiksberg C, Denmark.
⁵ The Francis Crick Institute, London WC2A 3LY, UK. Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK.
⁶ The Francis Crick Institute, London WC2A 3LY, UK.
⁷ Cancer Immunology Unit, UCL Cancer Institute, UCL, London WC1E 6BT, UK. Department of Cellular Pathology, UCL, London WC1E 6BT, UK.
⁸ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA 02215, USA. Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA. Center for Cancer Precision Medicine, Dana-Farber Cancer Institute, Boston, MA 02215, USA.
⁹ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA 02215, USA. Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA.
¹⁰ Department of Dermatology, University Hospital, University Duisburg-Essen, 45147 Essen, Germany. German Cancer Consortium (DKTK), 69121 Heidelberg, Germany.
¹¹ Human Oncology and Pathogenesis Program, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
¹² Hematology/Oncology Division, 177 Fort Washington Avenue, Columbia University, New York, NY 10032, USA.
¹³ Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA. Weill Cornell Medical College, New York, NY 10065, USA.
¹⁴ Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA. Ludwig Collaborative Laboratory, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
¹⁵ Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA. Weill Cornell Medical College, New York, NY 10065, USA. Ludwig Collaborative Laboratory, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
¹⁶ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA 02215, USA. Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA. Department of Medicine, Harvard Medical School, Boston, MA 02115, USA. Department of Internal Medicine, Brigham and Woman's Hospital, Boston, MA 02115, USA.
¹⁷ Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK. Cancer Immunology Unit, UCL Cancer Institute, UCL, London WC1E 6BT, UK. s.quezada@ucl.ac.uk charles.swanton@crick.ac.uk.
¹⁸ The Francis Crick Institute, London WC2A 3LY, UK. Cancer Research UK Lung Cancer Centre of Excellence, UCL Cancer Institute, London WC1E 6BT, UK. s.quezada@ucl.ac.uk charles.swanton@crick.ac.uk.

PMID: 26940869
PMCID: PMC4984254
DOI: 10.1126/science.aaf1490

Abstract

As tumors grow, they acquire mutations, some of which create neoantigens that influence the response of patients to immune checkpoint inhibitors. We explored the impact of neoantigen intratumor heterogeneity (ITH) on antitumor immunity. Through integrated analysis of ITH and neoantigen burden, we demonstrate a relationship between clonal neoantigen burden and overall survival in primary lung adenocarcinomas. CD8(+)tumor-infiltrating lymphocytes reactive to clonal neoantigens were identified in early-stage non-small cell lung cancer and expressed high levels of PD-1. Sensitivity to PD-1 and CTLA-4 blockade in patients with advanced NSCLC and melanoma was enhanced in tumors enriched for clonal neoantigens. T cells recognizing clonal neoantigens were detectable in patients with durable clinical benefit. Cytotoxic chemotherapy-induced subclonal neoantigens, contributing to an increased mutational load, were enriched in certain poor responders. These data suggest that neoantigen heterogeneity may influence immune surveillance and support therapeutic developments targeting clonal neoantigens.

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Figures

**Fig. 1. Heterogeneity and prognostic value of neoantigen landscape in primary NSCLC**
(A) Total putative neoantigen burden in multiregion sequenced NSCLC tumors. Proportion of clonal neoantigens, identified ubiquitously in every tumor region, are shown in blue; shared subclonal neoantigens, identified as shared in multiple tumor regions but not all, are shown in yellow; and private subclonal neoantigens, identified in only one tumor region, are in red. (B) Total putative neoantigen burden in TCGA LUAD tumors. Proportion of neoantigens arising from clonal (blue) or subclonal (red) mutations is shown. (C) Schematic illustrating use of different neoantigen ITH thresholds, with bar plot showing separation into the two groups.Without an ITH threshold, samples are simply grouped according to upper quartile of total neoantigen burden. For each ITH threshold, the upper quartile of clonal neoantigens is used to separate tumors with high and low clonal neoantigen burden, and the neoantigen ITH threshold further groups samples. For example, an ITH threshold = 0 involves grouping tumors with high clonal neoantigen burden and zero neoantigen heterogeneity separately from those with low clonal neoantigen burden or any neoantigen heterogeneity. (D) Overall survival curves for samples by using different ITH thresholds. Shown are without an ITH threshold [log-rank, P = 0.025, HR = 0.47 (0.24–0.92)]; ITH threshold = 0 [log-rank, P = 0.019, HR = 0.21 (0.051–0.88)]; ITH threshold = 0.01 [log-rank, P = 0.0096, HR = 0.33 (0.14–0.79)]; and ITH threshold = 0.05 [log-rank, P = 0.021, HR = 0.45 (0.22–0.90)].The number of patients in each group is listed below the survival curves.

**Fig. 2. Prediction and identification of neoantigen-reactive Tcells in NSCLC samples**
(A) Putative neoantigens predicted for all missense mutations in L011. The MTFR2^D326Y neoantigen (FAFQEYDSF) is highlighted. (B) Putative neoantigens predicted for all missense mutations in L012. The CHTF18^L769V neoantigen (LLLDIVAPK) and MYADM^R30W neoantigen (SPMIVGSPW) are indicated. (C) Evolutionary trees for L011 and L012 based on predicted neoantigens. (D and E) MHC-multimer screening of expanded, region-specific, tumor-infiltrating CD8⁺ T lymphocytes and healthy donor (HD) CD8⁺ PBMC controls with candidate neoantigens (L011, n = 288; L012, n = 354) and control HLA-matched viral peptides (L011, n = 10; L012, n = 9). Frequency of CD8⁺ MHC-multimer–positive cells out of total CD3⁺CD8⁺ tumor-infiltrating lymphocyte (TILs) is displayed for (D) and (E), with size of symbol increasing with frequency.

**Fig. 3. Identification and characterization of tumor-infiltrating neoantigen-reactive CD8⁺ T cells in early-stage NSCLC**
(A) MHC-multimer analysis of nonexpanded, tumor-infiltrating CD8⁺ T lymphocytes isolated from tumor regions 1 to 3 and normal lung tissue of patient L011 identifies CD8⁺ TILs reactive to mutant MTFR2 peptide. (B) MHC-multimer analysis of nonexpanded, tumor-infiltrating CD8⁺ T lymphocytes isolated from tumor regions 1 to 3 and normal lung tissue of patient L012 identifies two distinct populations of CD8⁺ TILs reactive to mutant CHTF18 and MYADM peptide. The frequency of CD8⁺ MHC-multimer–positive cells out of total CD3⁺CD8⁺ TILs is displayed for (A) and (B). (C) Multiparametric flow cytometric analysis of tumor-infiltrating T lymphocyte subsets isolated from L011 region 3. Phenotypic data are representative of all tumor regions. Relative expression of iCTLA-4 (intracellular CTLA-4), surface PD-1, and surface LAG-3 by CD4⁺FoxP3⁺ (regulatory Tcell), CD4⁺FoxP3⁻ (CD4 helper Tcell), CD8⁺ multimer–negative, and CD8⁺ multimer–reactive (CD8⁺ MTFR2⁺) Tcells is displayed, plotted against iKi67 (intracellular Ki67). (D) Coexpression of PD-1 and iGzmB (intracellular granzyme B) by tumor-infiltrating T lymphocyte subsets isolated from L011 region 3.

**Fig. 4. Neoantigen clonal architecture and clinical benefit of immune checkpoint blockade**
(A) Samples are grouped according to clinical benefit, with durable clinical benefit on left and no durable benefit on right [defined as in (2)]. Bar plot depicts clonal neoantigens in blue and subclonal neoantigens in red. Mutational signatures identified within each sample, subtype, and expression of PD-L1 are shown below. (B) Progression-free survival in NSCLC (2) cohort treated with antibody to PD1 either without an ITH threshold [HR = 0.29 (0.12−0.69), log-rank P = 0.0032] or with an ITH threshold of 0.01 [HR = 0.20 (0.07−0.60), log-rank P = 0.0017], 0.02 [HR = 0.25 (0.09−0.67), log-rank P = 0.0034], or 0.05 [HR = 0.17 (0.07−0.44), log-rank P=0.000061].(C) Overall survival in melanoma (4) cohort treated with antibody to CTLA-4 either without an ITH threshold [HR = 0.51 (0.23–1.11), P = 0.083] or with an ITH threshold of 0.01 [HR = 0.29 (0.11−0.77), log-rank P = 0.008], 0.02 [HR = 0.34 (0.14−0.81), log-rank P = 0.011], or 0.05 [HR = 0.51 (0.23–1.11), P = 0.083]. An ITH threshold of 0.05 results in the same survival curve as no ITH threshold because no tumors with a high neoantigen burden exhibit >0.05 neoantigen ITH. (D to F) Clonal architecture of (D) CA9903, (E) CR9306, and (F) CR0095, with mutations yielding neoantigens that elicit a Tcell response highlighted. Blue dots represent clonal mutations, with subclonal mutations depicted as red dots. Density plots are shown above.

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Comment in

Immunotherapy: Clonal neoantigens and immune response: a balancing act.
Hutchinson L. Hutchinson L. Nat Rev Clin Oncol. 2016 May;13(5):265. doi: 10.1038/nrclinonc.2016.49. Epub 2016 Mar 31. Nat Rev Clin Oncol. 2016. PMID: 27030076 No abstract available.
Tumor Heterogeneity and Tumor Immunity: A Chicken-and-Egg Problem.
Spranger S. Spranger S. Trends Immunol. 2016 Jun;37(6):349-351. doi: 10.1016/j.it.2016.04.008. Epub 2016 May 8. Trends Immunol. 2016. PMID: 27166403

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[1] Matsushita H, et al. Nature. 2012;482:400–404. - PMC - PubMed

[2] Matsushita H, et al. Nature. 2012;482:400–404. - PMC - PubMed

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Clonal neoantigens elicit T cell immunoreactivity and sensitivity to immune checkpoint blockade

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Clonal neoantigens elicit T cell immunoreactivity and sensitivity to immune checkpoint blockade

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