Point mutation screening of tumor neoantigens and peptide‑induced specific cytotoxic T lymphocytes using The Cancer Genome Atlas database

Wu, Wanwen; Chen, Ying; Huang, Lan; Li, Wenjian; Tao, Changli; Shen, Han

doi:10.3892/ol.2020.11986

Cited by 2 publications

(2 citation statements)

References 35 publications

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“…Containing amino acid sequences derived from mutations, neoantigens are immunologically considered nonself-antigens that can activate high-affinity T-cells. The cytotoxic effect of CTLs induced by mutant p53 peptides is superior to that of wild-type p53 peptides [27]. Although high immunogenicity is an advantage of neoantigens against conventional TAAs, neoantigens have several issues that need to be addressed in clinical practice.…”

Section: Selecting Tumor Antigens As a Source Of Vaccinesmentioning

confidence: 99%

Antitumor Peptide-Based Vaccine in the Limelight

et al. 2022

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The success of the immune checkpoint blockade has provided a proof of concept that immune cells are capable of attacking tumors in the clinic. However, clinical benefit is only observed in less than 20% of the patients due to the non-specific activation of immune cells by the immune checkpoint blockade. Developing tumor-specific immune responses is a challenging task that can be achieved by targeting tumor antigens to generate tumor-specific T-cell responses. The recent advancements in peptide-based immunotherapy have encouraged clinicians and patients who are struggling with cancer that is otherwise non-treatable with current therapeutics. By selecting appropriate epitopes from tumor antigens with suitable adjuvants, peptides can elicit robust antitumor responses in both mice and humans. Although recent experimental data and clinical trials suggest the potency of tumor reduction by peptide-based vaccines, earlier clinical trials based on the inadequate hypothesis have misled that peptide vaccines are not efficient in eliminating tumor cells. In this review, we highlighted the recent evidence that supports the rationale of peptide-based antitumor vaccines. We also discussed the strategies to select the optimal epitope for vaccines and the mechanism of how adjuvants increase the efficacy of this promising approach to treat cancer.

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Section: Selecting Tumor Antigens As a Source Of Vaccinesmentioning

confidence: 99%

Antitumor Peptide-Based Vaccine in the Limelight

et al. 2022

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“…For example, checkpoint blockade-based treatments have significantly improved cancer survival [ 5 , 6 ]. Other immunotherapy treatments such as adoptive cell transfer therapy and small molecule inhibitors are widely used to treat various cancer types [ 7 , 8 ]. The success of immunotherapy strategies is dependent on presentation of neo-antigens on cancer cell surface.…”

Section: Introductionmentioning

confidence: 99%

A computational workflow for predicting cancer neo-antigens

Kasaragod¹

2022

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Neo-antigens presented on cell surface play a pivotal role in the success of immunotherapies. Peptides derived from mutant proteins are thought to be the primary source of neo-antigens presented on the surface of cancer cells. Mutation data from cancer genome sequencing is often used to predict cancer neo-antigens. However, this strategy is associated with significant false positives as many coding mutations may not be expressed at the protein level. Hence, we describe a computational workflow to integrate genomic and proteomic data to predictpotential neo-antigens.

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Point mutation screening of tumor neoantigens and peptide‑induced specific cytotoxic T lymphocytes using The Cancer Genome Atlas database

Cited by 2 publications

References 35 publications

Antitumor Peptide-Based Vaccine in the Limelight

Antitumor Peptide-Based Vaccine in the Limelight

A computational workflow for predicting cancer neo-antigens

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