Sensitive, high-throughput HLA-I and HLA-II immunopeptidomics using parallel accumulation-serial fragmentation mass spectrometry

Phulphagar, Kshiti; Ctortecka, Claudia; Vaca, Sebastian; Klaeger, Susan; Verzani, Eva K; Hernandez, Gabrielle M.; Udeshi, Namrata D.; Clauser, Karl R.; Abelin, Jennifer G.; Carr, Steven A.

doi:10.1101/2023.03.10.532106

Cited by 10 publications

(20 citation statements)

References 37 publications

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“…To enable the detection of rare and clinically relevant antigens from a limited cell input, Phulphagar et al 30 developed a high-throughput single-shot MS-based immunopeptidomics workflow using the timsTOF single-cell proteomics system (SCP). This workflow was applied to sample inputs ranging from 1 million to 40 million A-375 cell equivalents, a melanoma cell line which expresses the following HLA-I genes: A*01:01, A*02:02, B*57:01, B*44:03, C*16:02, and C*06:02.…”

Section: Resultsmentioning

confidence: 99%

“…To investigate whether low input samples benefit from PSM rescoring, we rescored a timsTOF SCP dataset. For detailed information on data acquisition, please refer to the original publication by Phulphagar et al 30 . In brief, HLA-I peptides were directly enriched from 1 million to 40 million A-375 cell equivalents by single shot injections on timsTOF SCP.…”

Section: Re-analysis Of An Immunopeptidomics Dataset Measured On Tims...mentioning

confidence: 99%

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Fragment ion intensity prediction improves the identification rate of non-tryptic peptides in timsTOF

Adams

Gabriel

Laukens

et al. 2023

Preprint

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Immunopeptidomics plays a crucial role in identifying targets for immunotherapy and vaccine development. Because the generation of immunopeptides from their parent proteins does not adhere to clear-cut rules, rather than being able to use known digestion patterns, every possible protein subsequence within HLA class-specific length restrictions needs to be considered. This leads to an inflation of the search space and results in lower spectrum annotation rates. Rescoring is a powerful enhancement of standard sequence database searching that boosts the spectrum annotation performance. In the field of immunopeptidomics low abundant peptides often occur, which is why the highly sensitive timsTOF instruments are increasingly gaining popularity. To improve rescoring for immunopeptides measured using timsTOF instruments, we trained a deep learning-based fragment ion intensity prediction model. Over 300,000 synthesized non-tryptic peptides from the ProteomeTools project were analyzed on a timsTOF-Pro to generate a dataset that was used to fine-tune an existing Prosit model. By applying our fragment ion intensity prediction model, we demonstrate up to 3-fold improvement in the identification of immunopeptides. Furthermore, our approach increased detection of immunopeptides even from low input samples.

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Section: Resultsmentioning

confidence: 99%

Section: Re-analysis Of An Immunopeptidomics Dataset Measured On Tims...mentioning

confidence: 99%

Fragment ion intensity prediction improves the identification rate of non-tryptic peptides in timsTOF

Adams

Gabriel

Laukens

et al. 2023

Preprint

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“…Application of DeepNovo Peptidome to expand the reference HLA Ligand Atlas of benign human tissues As neoantigens mostly arise from non-canonical sources which are challenging for standard database search approaches, we built DeepNovo Peptidome, a de novo sequencing-based workflow for HLA peptide identification and neoantigen discovery. We trained the de novo sequencing model 13,14 on a very large, carefully curated dataset from 20 previous MS-based immunopeptidomics studies 5,15,16,[24][25][26][27][28][29][30][31][32][33][34][35][36][37][38][39][40] . The dataset included nearly 3,000 runs on two major MS instruments Orbitrap and timsTOF, >26M PSMs and >1.1M unique HLA peptides, and covering more than 90 alleles for each HLA class.…”

Section: Resultsmentioning

confidence: 99%

A complete mass spectrometry-based immunopeptidomics pipeline for neoantigen identification and validation

Li,

Tran,

Peng

et al. 2023

Preprint

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Here we proposed DeepImmu, a complete pipeline for neoantigen identification and validation that was based solely on mass spectrometry (MS) immunopeptidomics. In particular, a new enrichment kit was developed for HLA peptide purification from a small amount of biopsied tissue as low as 18mg. To identify candidate neoantigens from such a small amount of sample, we built DeepNovo Peptidome, a highly sensitive de novo sequencing-based workflow for HLA peptide identification. Furthermore, we developed DeepSelf, a personalized model for immunogenicity prediction based on the central tolerance of T cells, which could be used to prioritize candidate neoantigens from de novo HLA peptides for in vitro validation. Finally, we presented a new MS-based immunopeptidomics study of native tumor tissues from five patients with cervical cancer. We applied DeepImmu pipeline to identify and prioritize candidate neoantigens from low amounts of tumor tissues, and then performed in vitro validation of autologous neoantigen-specific T cell responses to confirm our results. Our MS-based de novo sequencing approach provides an unbiased solution for neoantigen discovery, because it does not depend on prior knowledge of protein databases, RNA sequencing data, or the source of neoantigens. By reducing the amount of sample to biopsy size, our DeepImmu pipeline can be easily performed in routine clinical applications.

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“…Other IM-MS-based immunopeptidomics methodologies have been acknowledged by other groups as well to show their potential to expand the identification of immunopeptides. [48][49][50][51][52] Not long ago, one of the challenges in immunopeptidomics was reported to be the unfeasibility of analysis from a small amount of sample. 53 However, the situation has been improving due to the advancements of IM, improved sensitivity, and the scan speed by the mass spectrometer.…”

Section: Ion Mobility a New Ion Separation Technology In Msmentioning

confidence: 99%

“…These results indicate the advantage of IM in immunopeptidomics, which requires a sensitive analysis. Other IM‐MS‐based immunopeptidomics methodologies have been acknowledged by other groups as well to show their potential to expand the identification of immunopeptides 48–52 . Not long ago, one of the challenges in immunopeptidomics was reported to be the unfeasibility of analysis from a small amount of sample 53 .…”

Section: Transformative Technologies That Shed Light Upon the Dark Ma...mentioning

confidence: 99%

Emerging potential of immunopeptidomics by mass spectrometry in cancer immunotherapy

Minegishi,

Haga,

Ueda

2024

Cancer Science

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With significant advances in analytical technologies, research in the field of cancer immunotherapy, such as adoptive T cell therapy, cancer vaccine, and immune checkpoint blockade (ICB), is currently gaining tremendous momentum. Since the efficacy of cancer immunotherapy is recognized only by a minority of patients, more potent tumor‐specific antigens (TSAs, also known as neoantigens) and predictive markers for treatment response are of great interest. In cancer immunity, immunopeptides, presented by human leukocyte antigen (HLA) class I, play a role as initiating mediators of immunogenicity. The latest advancement in the interdisciplinary multiomics approach has rapidly enlightened us about the identity of the “dark matter” of cancer and the associated immunopeptides. In this field, mass spectrometry (MS) is a viable option to select because of the naturally processed and actually presented TSA candidates in order to grasp the whole picture of the immunopeptidome. In the past few years the search space has been enlarged by the multiomics approach, the sensitivity of mass spectrometers has been improved, and deep/machine‐learning‐supported peptide search algorithms have taken immunopeptidomics to the next level. In this review, along with the introduction of key technical advancements in immunopeptidomics, the potential and further directions of immunopeptidomics will be reviewed from the perspective of cancer immunotherapy.

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Sensitive, high-throughput HLA-I and HLA-II immunopeptidomics using parallel accumulation-serial fragmentation mass spectrometry

Cited by 10 publications

References 37 publications

Fragment ion intensity prediction improves the identification rate of non-tryptic peptides in timsTOF

Fragment ion intensity prediction improves the identification rate of non-tryptic peptides in timsTOF

A complete mass spectrometry-based immunopeptidomics pipeline for neoantigen identification and validation

Emerging potential of immunopeptidomics by mass spectrometry in cancer immunotherapy

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