The T-cell Receptor Repertoire Influences the Tumor Microenvironment and Is Associated with Survival in Aggressive B-cell Lymphoma

Keane, Colm; Gould, Clare; Jones, Kimberley; Hamm, David; Talaulikar, Dipti; Ellis, Jonathan; Vari, Frank; Birch, Simone; Han, Eui-Ryoung; Wood, Peter; Cao, Kim-Anh Lê; Green, Michael R.; Crooks, Pauline; Jain, Sanjiv; Tobin, Joshua W.D.; Steptoe, Raymond J.; Gandhi, Maher K.

doi:10.1158/1078-0432.ccr-16-1576

Cited by 71 publications

(93 citation statements)

References 37 publications

(43 reference statements)

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“…19 Furthermore, substantially higher clonal T-cell responses were observed in EBV -pos vs EBV -neg DLBCL. 19 Although the prognostic impact of the TME in de novo DLBCL is well-established, [20][21][22][23][24] it remains untested as to whether the TME is associated with differential survival in EBV -pos DLBCL.…”

Section: Introductionmentioning

confidence: 99%

The tumour microenvironment is immuno‐tolerogenic and a principal determinant of patient outcome in EBV‐positive diffuse large B‐cell lymphoma

Keane

Tobin

Gunawardana

et al. 2019

European J of Haematology

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ObjectiveEpstein‐Barr virus‐positive diffuse large B‐cell lymphoma (EBV‐pos DLBCL) is a recently identified entity. Data regarding outcome to frontline immuno‐chemotherapy are conflicting. Although the prognostic impact of the tumour microenvironment (TME) in EBV‐neg DLBCL is well‐established, it remains untested whether the TME influences survival in EBV‐pos DLBCL. There are no data with new digital gene expression technologies that simultaneously interrogate the virus, B cells and the tumour microenvironment (TME).MethodsWe used the NanoString™ platform in a population‐based cohort of 433 patients to establish if the technology could detect EBV in the tumour biopsies and to investigate the influence that EBV has on the complex tumour microenvironment of DLBCL.ResultsIncidence of EBV‐pos DLBCL was 6.9% with 5‐year survival of 65% vs 82% in EBV‐neg DLBCL (P = 0.018). EBV‐pos tissues had similar expression of T‐cell genes compared to EBV‐neg DLBCL but higher levels of the antigen‐presenting molecule B2M. This was countered by elevated PD‐L1, PD‐L2, LAG3 and TIM3 immune checkpoints and a higher CD163/CD68 “M2” macrophage score.ConclusionIn EBV‐pos DLBCL, the TME is immuno‐tolerogenic and may explain the poor outcomes seen in this subtype of DLBCL.

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Section: Introductionmentioning

confidence: 99%

The tumour microenvironment is immuno‐tolerogenic and a principal determinant of patient outcome in EBV‐positive diffuse large B‐cell lymphoma

Keane

Tobin

Gunawardana

et al. 2019

European J of Haematology

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“…More recently, several additional tools that have the potential of contributing to a resolution of some of the above issues have become available. First, bioinformatics and computational approaches have made it clear that chemical and structural features of the TCR complementarity‐determining region 3 (CDR3) can correlate with a specific immune response . This development points to the second development, the employment of which offers promise for learning more about specific cancer patient, TCR CDR3, mutant peptide interactions, namely the vast databases now available representing cancer patient mutant amino acids (aa) and tens of thousands of TCR CDR3s for the corresponding TILs.…”

Section: Introductionmentioning

confidence: 99%

A scoring system for the electrostatic complementarities of T‐cell receptors and cancer‐mutant amino acids: multi‐cancer analyses of associated survival rates

et al. 2020

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Summary The anti‐tumor immune response is considered to be due to the T‐cell receptor (TCR) binding to tumor antigens, which can be either wild‐type, early stem cell proteins, presumably foreign to a developed immune system; or mutant peptides, foreign to the immune system because of a mutant amino acid (aa) or otherwise somatically altered aa sequence. Recently, very large numbers of TCR complementarity‐determining region‐3 (CDR3) aa sequences obtained from tumor specimens have become available. We developed a novel algorithm for assessing the complementarity of tumor mutant peptides and TCR CDR3s, based on the retrieval of TCR CDR3 aa sequences from both tumor specimen and patient blood exomes and by using an automated process of assessing CDR3 and mutant aa electrical charges. Results indicated many instances where high electrostatic complementarity was associated with a higher survival rate. In particular, our approach led to the identification of specific genes contributing significantly to the complementary, TCR CDR3‐mutant aa. These results suggest a novel approach to tumor immunoscoring and may lead to the identification of high‐priority neo‐antigen, peptide vaccines; or to the identification of ex vivo stimulants of tumor‐infiltrating lymphocytes.

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“…The diversity of circulating TCR repertoire is gradually decreasing during tumor progression in patients with cervical cancer (Cui et al, ). Elsewhere, high dominant clones within tumor microenvironment were associated with poor outcome in diffuse large B‐cell lymphoma (Keane et al, ).…”

Section: Introductionmentioning

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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The T-cell Receptor Repertoire Influences the Tumor Microenvironment and Is Associated with Survival in Aggressive B-cell Lymphoma

Cited by 71 publications

References 37 publications

The tumour microenvironment is immuno‐tolerogenic and a principal determinant of patient outcome in EBV‐positive diffuse large B‐cell lymphoma

The tumour microenvironment is immuno‐tolerogenic and a principal determinant of patient outcome in EBV‐positive diffuse large B‐cell lymphoma

A scoring system for the electrostatic complementarities of T‐cell receptors and cancer‐mutant amino acids: multi‐cancer analyses of associated survival rates

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

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