Neoantigen vaccination induces clinical and immunologic responses in non-small cell lung cancer patients harboring EGFR mutations

Li, Fenge; Deng, Ligang; Jackson, Kyle R.; Talukder, Amjad H.; Katailiha, Arjun; Bradley, Sherille D.; Zou, Qingwei; Chen, Caixia; Huo, Chong; Chiu, Yulun; Stair, Matthew; Feng, Weihong; Bagaev, Aleksander; Kotlov, Nikita; Svekolkin, Viktor; Ataullakhanov, Ravshan; Miheecheva, Natalia; Frenkel, Felix; Wang, Yaling; Zhang, Minying; Hawke, David H.; Han, Leng; Zhou, Shuo; Zhang, Yan; Li, Xiqing; Decker, William K.; Sonnemann, Heather M.; Roszik, Jason; Forget, Marie Andrée; Davies, Michael A.; Bernatchez, Chantale; Yee, Cassian; Bassett, Roland L.; Hwu, Patrick; Du, Xueming; Lizee, Gregory

doi:10.1136/jitc-2021-002531

Cited by 35 publications

(35 citation statements)

References 61 publications

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“…Using this method, we have identified and validated peptides associated with the melanoma differentiation antigen SLC45A2 as shared melanoma-associated tumor targets and have generated TCRs recognizing these peptides. Similarly, we identified VGLL1 as a shared pancreatic and basal breast cancer tumorassociated antigen, for which TCRs showing antitumor activity have been isolated [27][28][29]. TCR-T cell clinical trials targeting these two TAAs are currently in the design stages.…”

Section: Methods For Identifying Tumor-associated Antigensmentioning

confidence: 94%

“…Our group has reported a neoantigen peptide derived from the EGFR-L858R mutation (KITDFGRAK) that is immunogenic and presented by HLA-A*1101. Since EGFR-L858R is found in~40% of EGFR-mutated lung cancers, it constitutes a promising, widely shared NeoAg target for TCR-T therapy of HLA-A*1101/EGFR-L858R lung cancer patients [28]. Our group has generated several promising TCRs specific for this and other EGFR-derived NeoAgs, and we plan to test their efficacy in future clinical trials [28,29]).…”

Section: Discovery Of New Targetsmentioning

confidence: 99%

“…Since EGFR-L858R is found in~40% of EGFR-mutated lung cancers, it constitutes a promising, widely shared NeoAg target for TCR-T therapy of HLA-A*1101/EGFR-L858R lung cancer patients [28]. Our group has generated several promising TCRs specific for this and other EGFR-derived NeoAgs, and we plan to test their efficacy in future clinical trials [28,29]). A number of other studies have also demonstrated the immunogenicity of shared NeoAgs that can be used to generate potentially therapeutic tumor specific TCRs [79][80][81].…”

Section: Discovery Of New Targetsmentioning

confidence: 99%

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Evolution of CD8+ T Cell Receptor (TCR) Engineered Therapies for the Treatment of Cancer

Sun

Sonnemann

et al. 2021

Cells

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Engineered T cell receptor T (TCR-T) cell therapy has facilitated the generation of increasingly reliable tumor antigen-specific adaptable cellular products for the treatment of human cancer. TCR-T cell therapies were initially focused on targeting shared tumor-associated peptide targets, including melanoma differentiation and cancer-testis antigens. With recent technological developments, it has become feasible to target neoantigens derived from tumor somatic mutations, which represents a highly personalized therapy, since most neoantigens are patient-specific and are rarely shared between patients. TCR-T therapies have been tested for clinical efficacy in treating solid tumors in many preclinical studies and clinical trials all over the world. However, the efficacy of TCR-T therapy for the treatment of solid tumors has been limited by a number of factors, including low TCR avidity, off-target toxicities, and target antigen loss leading to tumor escape. In this review, we discuss the process of deriving tumor antigen-specific TCRs, including the identification of appropriate tumor antigen targets, expansion of antigen-specific T cells, and TCR cloning and validation, including techniques and tools for TCR-T cell vector construction and expression. We highlight the achievements of recent clinical trials of engineered TCR-T cell therapies and discuss the current challenges and potential solutions for improving their safety and efficacy, insights that may help guide future TCR-T studies in cancer.

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Section: Methods For Identifying Tumor-associated Antigensmentioning

confidence: 94%

Section: Discovery Of New Targetsmentioning

confidence: 99%

Section: Discovery Of New Targetsmentioning

confidence: 99%

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Evolution of CD8+ T Cell Receptor (TCR) Engineered Therapies for the Treatment of Cancer

Sun

Sonnemann

et al. 2021

Cells

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“…The potential neoantigens can be employed in the development of immunotherapies. So far, several neoantigens have been discovered in preclinical and clinical investigations, some of which are derived from shared mutations in a range of malignancies (30,31,(40)(41)(42)(43)(44)(45)(46)(47) (Table 1).…”

Section: Identification Of Immunogenic Neoantigensmentioning

confidence: 99%

Neoantigens and NK Cells: “Trick or Treat” the Cancers?

Khawar

Liang

et al. 2022

Front. Immunol.

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Immunotherapy has become an important treatment strategy for cancer patients nowadays. Targeting cancer neoantigens presented by major histocompatibility complex (MHC) molecules, which emerge as a result of non-synonymous somatic mutations with high immunogenicity, is one of the most promising cancer immunotherapy strategies. Currently, several therapeutic options based on the personalized or shared neoantigens have been developed, including neoantigen vaccine and adoptive T-cell therapy, both of which are now being tested in clinical trials for various malignancies. The goal of this review is to outline the use of neoantigens as cancer therapy targets, with an emphasis on neoantigen identification, clinical usage of personalized neoantigen-based cancer therapy agents, and the development of off-the-shelf products based on shared neoantigens. In addition, we introduce and discuss the potential impact of the neoantigen–MHC complex on natural killer (NK) cell antitumor function, which could be a novel way to boost immune response-induced cytotoxicity against malignancies.

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“…In mice models bearing the NSCLC tumors, they were able to show that targeted therapy against ACAD8-T105I, BCAR1-G23V, and PLCG1-M245L led to improved immune cell response, demonstrating the feasibility of treatment in vivo . In a stage III/IV NSCLC study with 24 patients, neoantigens-based personalized vaccination was developed based on predictions using a panel of 508 tumor-associated genes from tumor biopsies, with peptides also demonstrating high affinity to HLA class I and II, determined through HLA typing ( 26 ). Researchers were able to demonstrate OS and median PFS of 8.9 and 6 months, respectively.…”

Section: Combination With Cancer Vaccinementioning

confidence: 99%

Immune checkpoint inhibitors for PD-1/PD-L1 axis in combination with other immunotherapies and targeted therapies for non-small cell lung cancer

et al. 2022

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It has been widely acknowledged that the use of immune checkpoint inhibitors (ICI) is an effective therapeutic treatment in many late-stage cancers. However, not all patients could benefit from ICI therapy. Several biomarkers, such as high expression of PD-L1, high mutational burden, and higher number of tumor infiltration lymphocytes have shown to predict clinical benefit from immune checkpoint therapies. One approach using ICI in combination with other immunotherapies and targeted therapies is now being investigated to enhance the efficacy of ICI alone. In this review, we summarized the use of other promising immunotherapies and targeted therapies in combination with ICI in treatment of lung cancers. The results from multiple animals and clinical trials were reviewed. We also briefly discussed the possible outlooks for future treatment.

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Neoantigen vaccination induces clinical and immunologic responses in non-small cell lung cancer patients harboring EGFR mutations

Cited by 35 publications

References 61 publications

Evolution of CD8+ T Cell Receptor (TCR) Engineered Therapies for the Treatment of Cancer

Evolution of CD8+ T Cell Receptor (TCR) Engineered Therapies for the Treatment of Cancer

Neoantigens and NK Cells: “Trick or Treat” the Cancers?

Immune checkpoint inhibitors for PD-1/PD-L1 axis in combination with other immunotherapies and targeted therapies for non-small cell lung cancer

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