Characterization of T cell repertoire of blood, tumor, and ascites in ovarian cancer patients using next generation sequencing

Jang, Miran; Yew, Poh-Yin; Ikeda, Yuji; Fleming, Gini F.; Nakamura, Yusuke; Park, Jae-Hyun

doi:10.1080/2162402x.2015.1030561

Cited by 55 publications

(42 citation statements)

References 41 publications

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“…In HCC patients, the T‐cell repertoires in tumor and matched adjacent non‐tumor tissues were found to be different (Chen et al, ), suggesting a distinct T‐cell immune microenvironment. Furthermore, in ovarian cancer patients T‐cell repertoire in tumors and ascites was found to be different (Jang et al, ). The T‐cell repertoire in blood and tumor of patients with advanced colorectal cancer were found to be entirely distinct (Tamura et al, ).…”

Section: Discussionmentioning

confidence: 99%

T‐cell receptor diversity as a prognostic biomarker in melanoma patients

Charles

Mouret

Challende

et al. 2020

Pigment Cell Melanoma Res

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There is increasing evidence that T‐cell receptor (TCR) repertoire diversity can be a predictive biomarker of immune responses in cancer patients. However, the characteristics of the T‐cell repertoire together with its prognostic significance in melanoma patients and impact on disease progression remain unknown. We investigated the combinatorial TCR repertoire diversity by semi‐quantitative multi‐N‐plex PCR in peripheral blood samples from 44 melanoma patients together with seven matched metastatic lymph nodes and explored its potential predictive value on clinical prognosis. The diversity was quantified by calculating both richness (number of different specificities) and evenness (relative abundance of the different specificities). Our results revealed that a higher TCR repertoire diversity in blood of patients was associated with a longer PFS, while divpenia (low repertoire diversity) was linked with poor prognosis. The diversity was significantly higher in patients undergoing late relapse and long survival compared to patients who progressed rapidly. Interestingly, the TCR repertoire diversity in tumor may have a potential prognostic value. Thus, our study highlights that the TCR repertoire diversity is a prognostic indicator of clinical outcome in patients with melanoma.

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Section: Discussionmentioning

confidence: 99%

T‐cell receptor diversity as a prognostic biomarker in melanoma patients

Charles

Mouret

Challende

et al. 2020

Pigment Cell Melanoma Res

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“…We established next-generation sequencing-based TCR repertoire analysis using mRNAs and applied our technology for the TCR analysis of various types of tumor. [15][16][17][18][19][20][21] A detailed TCR transcript analysis has provided a new insight into T cell responses in various disease conditions including characterization of the tumor microenvironment.…”

Section: Introductionmentioning

confidence: 99%

TCR sequencing analysis of cancer tissues and tumor draining lymph nodes in colorectal cancer patients

et al. 2019

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Tumor draining lymph nodes (TDLNs) are located in the routes of lymphatic drainage from a primary tumor and have the highest risk of metastasis in various types of solid tumors. TDLNs are also considered as a tissue to activate the antitumor immunity, where antigen-specific effector T cells are generated. However, T cell receptor (TCR) repertoires in TDLNs have not been well characterized. We collected 23 colorectal cancer tumors with 203 lymph nodes with/without metastatic cancer cells (67 were metastasis-positive and the remaining 136 were metastasis-negative) and performed TCR sequencing. Metastasis-positive TDLNs showed a significantly lower TCR diversity and shared TCR clonotypes more frequently with primary tumor tissues compared to metastasis-negative TDLNs. Principal component analysis indicated that TDLNs with metastasis showed similar TCR repertoires. These findings suggest that cancer-reactive T cell clones could be enriched in the metastasis-positive TDLNs. ARTICLE HISTORY

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“…The alpha-and beta-chains of the TCR undergo V(D)J recombination and heterodimerize in the thymus, resulting in a diverse T-cell repertoire that specifically recognizes peptide-MHC complexes. Many studies have analyzed the alpha-and beta-chains of TIL TCRs separately using highthroughput sequencing to describe the diversity of TILs (10)(11)(12)(13). Pairs are readily identified after expansion of T-cell clones, although culture of T cells can lead to substantial skewing of the repertoire (14), which may select for T cells of varied affinity or avidity (15).…”

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confidence: 99%

Identification of shared TCR sequences from T cells in human breast cancer using emulsion RT-PCR

Munson

Egelston

Chiotti

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Infiltration of T cells in breast tumors correlates with improved survival of patients with breast cancer, despite relatively few mutations in these tumors. To determine if T-cell specificity can be harnessed to augment immunotherapies of breast cancer, we sought to identify the alpha-beta paired T-cell receptors (TCRs) of tumor-infiltrating lymphocytes shared between multiple patients. Because TCRs function as heterodimeric proteins, we used an emulsion-based RT-PCR assay to link and amplify TCR pairs. Using this assay on engineered T-cell hybridomas, we observed ∼85% accurate pairing fidelity, although TCR recovery frequency varied. When we applied this technique to patient samples, we found that for any given TCR pair, the dominant alpha-or beta-binding partner comprised ∼90% of the total binding partners. Analysis of TCR sequences from primary tumors showed about fourfold more overlap in tumor-involved relative to tumor-free sentinel lymph nodes. Additionally, comparison of sequences from both tumors of a patient with bilateral breast cancer showed 10% overlap. Finally, we identified a panel of unique TCRs shared between patients' tumors and peripheral blood that were not found in the peripheral blood of controls. These TCRs encoded a range of V, J, and complementarity determining region 3 (CDR3) sequences on the alpha-chain, and displayed restricted V-beta use. The nucleotides encoding these shared TCR CDR3s varied, suggesting immune selection of this response. Harnessing these T cells may provide practical strategies to improve the shared antigen-specific response to breast cancer.T-cell receptors | breast cancer | emulsion RT-PCR | high-throughput sequencing | T-cell repertoire profiling I nfiltration of numerous tumors by CD8 + alpha-beta T cells is associated with better outcomes and longer survival times for patients with breast cancer (1-5). Targeted immune-based therapies hold great promise toward improving breast cancer treatments (6, 7). Studies have examined the immune phenotype of breast cancer tumor-infiltrating lymphocytes (TILs), suggesting that activated nonsuppressive T cells are of most benefit (8). Further assessment of the TIL repertoire has broad implications for breast cancer therapies in antigen discovery, cancer vaccines, and adoptive cell therapies (7).Unique genetic recombination events are required to produce the T-cell receptor (TCR) (reviewed in 9). The alpha-and beta-chains of the TCR undergo V(D)J recombination and heterodimerize in the thymus, resulting in a diverse T-cell repertoire that specifically recognizes peptide-MHC complexes. Many studies have analyzed the alpha-and beta-chains of TIL TCRs separately using highthroughput sequencing to describe the diversity of TILs (10-13). Pairs are readily identified after expansion of T-cell clones, although culture of T cells can lead to substantial skewing of the repertoire (14), which may select for T cells of varied affinity or avidity (15). Single-cell sequencing identifies alpha-beta pairs, but is often laborious and has rela...

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Characterization of T cell repertoire of blood, tumor, and ascites in ovarian cancer patients using next generation sequencing

Cited by 55 publications

References 41 publications

T‐cell receptor diversity as a prognostic biomarker in melanoma patients

T‐cell receptor diversity as a prognostic biomarker in melanoma patients

TCR sequencing analysis of cancer tissues and tumor draining lymph nodes in colorectal cancer patients

Identification of shared TCR sequences from T cells in human breast cancer using emulsion RT-PCR

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