Mutational and putative neoantigen load predict clinical benefit of adoptive T cell therapy in melanoma

Lauss, Martin; Donia, Marco; Harbst, Katja; Andersen, Rikke; Mitra, Shamik; Rosengren, Frida; Salim, Maryem; Vallon‐Christersson, Johan; Törngren, Therese; Kvist, Anders; Ringnér, Markus; Svane, Inge Marie; Jönsson, Göran

doi:10.1038/s41467-017-01460-0

Cited by 357 publications

(329 citation statements)

References 60 publications

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“…Filtering algorithms and cutoffs for putative germline variants, variant allele frequency (VAF), and FFPE‐induced deamination artefacts vary between assays and can be affected by biological and preanalytical factors. For example, VAF cutoffs can vary from 0.5 to 10%, with lower thresholds increasing the risk of including false‐positives arising from contamination or sequencing artefacts …”

Section: Variation In Tmb Assessment and Factors That Impact Tmb Outputmentioning

confidence: 99%

“…For example, VAF cutoffs can vary from 0.5 to 10%, with lower thresholds increasing the risk of including false-positives arising from contamination or sequencing artefacts. 4,24,36,48,[72][73][74] For calculation of the TMB denominator, genome coverage and bioinformatic parameters must be considered. Most studies have reported a TMB value in mut/Mb, whereas others have reported total mutations per tumor (WES studies); this makes it difficult to compare TMB values across patients and studies.…”

Section: Variation In Tmb Assessment and Factors That Impact Tmb Oumentioning

confidence: 99%

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Tumor mutational burden standardization initiatives: Recommendations for consistent tumor mutational burden assessment in clinical samples to guide immunotherapy treatment decisions

Stenzinger

Allen

Maas³

et al. 2019

Genes Chromosomes & Cancer

183

161

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Characterization of tumors utilizing next‐generation sequencing methods, including assessment of the number of somatic mutations (tumor mutational burden [TMB]), is currently at the forefront of the field of personalized medicine. Recent clinical studies have associated high TMB with improved patient response rates and survival benefit from immune checkpoint inhibitors; hence, TMB is emerging as a biomarker of response for these immunotherapy agents. However, variability in current methods for TMB estimation and reporting is evident, demonstrating a need for standardization and harmonization of TMB assessment methodology across assays and centers. Two uniquely placed organizations, Friends of Cancer Research (Friends) and the Quality Assurance Initiative Pathology (QuIP), have collaborated to coordinate efforts for international multistakeholder initiatives to address this need. Friends and QuIP, who have partnered with several academic centers, pharmaceutical organizations, and diagnostic companies, have adopted complementary, multidisciplinary approaches toward the goal of proposing evidence‐based recommendations for achieving consistent TMB estimation and reporting in clinical samples across assays and centers. Many factors influence TMB assessment, including preanalytical factors, choice of assay, and methods of reporting. Preliminary analyses highlight the importance of targeted gene panel size and composition, and bioinformatic parameters for reliable TMB estimation. Herein, Friends and QuIP propose recommendations toward consistent TMB estimation and reporting methods in clinical samples across assays and centers. These recommendations should be followed to minimize variability in TMB estimation and reporting, which will ensure reliable and reproducible identification of patients who are likely to benefit from immune checkpoint inhibitors.

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Section: Variation In Tmb Assessment and Factors That Impact Tmb Outputmentioning

confidence: 99%

Section: Variation In Tmb Assessment and Factors That Impact Tmb Oumentioning

confidence: 99%

Tumor mutational burden standardization initiatives: Recommendations for consistent tumor mutational burden assessment in clinical samples to guide immunotherapy treatment decisions

Stenzinger

Allen

Maas³

et al. 2019

Genes Chromosomes & Cancer

183

161

View full text Add to dashboard Cite

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“…Indeed, ACT with tumor infiltrating lymphocytes (TIL) harboring NeoAg specificities has induced tumor regression in patients with metastatic breast cancer and melanoma 31,32 . Furthermore, patients with higher mutational burden malignancies (and therefore a greater diversity of NeoAg targets) experience a greater response rate to both TIL ACT and ICB 33–35 . NeoAg‐specific T cells have also been identified as effectors of antitumor immunity in mouse models 36–38 .…”

Section: Which Antigens Do T Cells Recognize In Cancer?mentioning

confidence: 99%

“…31,32 Furthermore, patients with higher mutational burden malignancies (and therefore a greater diversity of NeoAg targets) experience a greater response rate to both TIL ACT and ICB. [33][34][35] NeoAg-specific T cells have also been identified as effectors of antitumor immunity in mouse models. [36][37][38] Specifically, NeoAg-specific T cell populations increased in frequency and a greater percentage produced effector cytokines in mice bearing MCA-induced sarcomas receiving ICB.…”

Section: Which Antigens Do T Cells Recognize In Cancer?mentioning

confidence: 99%

Harnessing neoantigen specific CD4 T cells for cancer immunotherapy

Brightman

Naradikian

Miller

et al. 2020

Journal of Leukocyte Biology

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The goal of precision immunotherapy is to direct a patient's T cell response against the immunogenic mutations expressed on their tumors. Most immunotherapy approaches to‐date have focused on MHC class I‐restricted peptide epitopes by which cytotoxic CD8+ T lymphocytes (CTL) can directly recognize tumor cells. This strategy largely overlooks the critical role of MHC class II‐restricted CD4+ T cells as both positive regulators of CTL and other effector cell types, and as direct effectors of antitumor immunity. In this review, we will discuss the role of neoantigen specific CD4+ T cells in cancer immunotherapy and how existing treatment modalities may be leveraged to engage this important T cell subset.

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“…Balachandran et al 2017; Brown et al 2014; Gros et al 2016; Hodges et al 2017; Lauss et al 2017; Linnemann et al 2015; Luksza et al 2017; Matsushita et al 2012; McGranahan et al 2016; Ock et al 2017; Pritchard et al 2015a; Rizvi et al 2015; Robbins et al 2013; Snyder et al 2014; Tran et al 2016; Van Allen et al 2015; van Rooij et al 2013; Verdegaal et al 2016). While these various tools have an important role to play in the prediction of immunogenic antigens, the majority of the identified epitopes do not initiate an immune response (e.g.…”

Section: Identification Of Neoantigensmentioning

confidence: 99%

Identifying neoantigens for use in immunotherapy

Hutchison

Pritchard

2018

Mamm Genome

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This review focuses on the types of cancer antigens that can be recognised by the immune system and form due to alterations in the cancer genome, including cancer testis, overexpressed and neoantigens. Specifically, neoantigens can form when cancer cell-specific mutations occur that result in alterations of the protein from 'self'. This type of antigen can result in an immune response sufficient to clear tumour cells when activated. Furthermore, studies have reported that the likelihood of successful immunotherapeutic targeting of cancer by many different methods was reliant on immune response to neoantigens. The recent resurgence of interest in the immune response to tumour cells, in conjunction with technological advances, has resulted in a large increase in the predicted, identified and functionally confirmed neoantigens. This growth in identified neoantigen sequences has increased the contents of training sets for algorithms, which in turn improves the prediction of which genetic mutations may form neoantigens. Additionally, algorithms predicting how proteins will be processed into peptide epitopes by the proteasome and which peptides bind to the transporter complex are also improving with this research. Now that large screens of all the tumour-specific protein altering mutations are possible, the emerging data from assessment of the immunogenicity of neoantigens suggest that only a minority of variants will form targetable epitopes. The potential for immunotherapeutic targeting of neoantigens will therefore be greater in cancers with a higher frequency of protein altering somatic variants. There is considerable potential in the use of neoantigens to treat patients, either alone or in combination with other immunotherapies and with continued advancements, these potentials will be realised.

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Mutational and putative neoantigen load predict clinical benefit of adoptive T cell therapy in melanoma

Cited by 357 publications

References 60 publications

Tumor mutational burden standardization initiatives: Recommendations for consistent tumor mutational burden assessment in clinical samples to guide immunotherapy treatment decisions

Tumor mutational burden standardization initiatives: Recommendations for consistent tumor mutational burden assessment in clinical samples to guide immunotherapy treatment decisions

Harnessing neoantigen specific CD4 T cells for cancer immunotherapy

Identifying neoantigens for use in immunotherapy

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