Immunosequencing identifies signatures of cytomegalovirus exposure history and HLA-mediated effects on the T cell repertoire

Emerson, Ryan; DeWitt, William S; Vignali, Marissa; Gravley, Jenna; Hu, Joyce; Osborne, Edward J.; Desmarais, Cindy; Klinger, Mark; Carlson, Christopher S.; Hansen, John A.; Rieder, Mark J.; Robins, Harlan

doi:10.1038/ng.3822

Cited by 469 publications

(769 citation statements)

References 62 publications

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“…Model training is done by finding model parameters that maximize the likelihood of the data, equal to the product of generation probabilities of the observed TCRs in the dataset. Here, we used IGoR to infer a generation model from the non‐functional reads in the datasets from which the productive reads used for the sharing analysis came, for human,30 and mice 23…”

Section: Methodsmentioning

confidence: 99%

“…Human dataset was used from the CMV study in 30. 658 individual samples were used, with mean number of reads ≈200 000, and mean number of unique CDR3s ≈180 000.…”

Section: Methodsmentioning

confidence: 99%

“…Such sharing of specific TCRs is expected from the relatively low diversity of antigen‐specific sequences revealed by in vitro multimer‐staining experiments 11, 12. A very similar idea has been exploited by several groups to identify TCRs specific to the Cytomegalovirus,30 Type‐1 diabetes,48, 49 arthritis50 and other immune diseases 51. In these studies, there is no theoretical expectation from the recombination model.…”

Section: Public Specific Responsementioning

confidence: 97%

“…Specifically, we re‐analyzed published TCR β‐chain nucleotide sequences of 14 Black‐6 mice23 and 658 human donors30 (Section 7). Individual samples comprised 20 000‐50 000 unique sequences for mice, and up to 400 000 for humans.…”

Section: Predicting Sharing Between Repertoiresmentioning

confidence: 99%

“…We performed the sharing analysis on 30 patients with bladder cancer, on TCR repertoires sequenced from blood samples 54. We compared it with 30 healthy individuals, chosen at random among the individuals studied in 30 to have similar sample sizes. We then downsampled the reference repertoires of the healthy individuals to have the exact same sample sizes as the cancer patients to guarantee a fair comparison.…”

Section: Public Specific Responsementioning

confidence: 99%

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Predicting the spectrum of TCR repertoire sharing with a data‐driven model of recombination

Elhanati

Sethna

Callan

et al. 2018

Immunological Reviews

126

159

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SummaryDespite the extreme diversity of T‐cell repertoires, many identical T‐cell receptor (TCR) sequences are found in a large number of individual mice and humans. These widely shared sequences, often referred to as “public,” have been suggested to be over‐represented due to their potential immune functionality or their ease of generation by V(D)J recombination. Here, we show that even for large cohorts, the observed degree of sharing of TCR sequences between individuals is well predicted by a model accounting for the known quantitative statistical biases in the generation process, together with a simple model of thymic selection. Whether a sequence is shared by many individuals is predicted to depend on the number of queried individuals and the sampling depth, as well as on the sequence itself, in agreement with the data. We introduce the degree of publicness conditional on the queried cohort size and the size of the sampled repertoires. Based on these observations, we propose a public/private sequence classifier, “PUBLIC” (Public Universal Binary Likelihood Inference Classifier), based on the generation probability, which performs very well even for small cohort sizes.

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Section: Methodsmentioning

confidence: 99%

“…Human dataset was used from the CMV study in 30. 658 individual samples were used, with mean number of reads ≈200 000, and mean number of unique CDR3s ≈180 000.…”

Section: Methodsmentioning

confidence: 99%

Section: Public Specific Responsementioning

confidence: 97%

Section: Predicting Sharing Between Repertoiresmentioning

confidence: 99%

Section: Public Specific Responsementioning

confidence: 99%

See 3 more Smart Citations

Predicting the spectrum of TCR repertoire sharing with a data‐driven model of recombination

Elhanati

Sethna

Callan

et al. 2018

Immunological Reviews

126

159

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A new clustering method identifies multiple sclerosis‐specific T‐cell receptors

Hayashi

Isobe

Glanville

et al. 2021

Ann Clin Transl Neurol

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ObjectiveTo characterize T‐cell receptors (TCRs) and identify target epitopes in multiple sclerosis (MS).MethodsPeripheral blood mononuclear cells were obtained from 39 MS patients and 19 healthy controls (HCs). TCR repertoires for α/β/δ/γ chains, TCR diversity, and V/J usage were determined by next‐generation sequencing. TCR β chain repertoires were compared with affectation status using a novel clustering method, Grouping of Lymphocyte Interactions by Paratope Hotspots (GLIPH). Cytomegalovirus (CMV)‐IgG was measured in an additional 113 MS patients and 93 HCs. Regulatory T cells (Tregs) were measured by flow cytometry.ResultsTCR diversity for all four chains decreased with age. TCRα and TCRβ diversity was higher in MS patients (P = 0.0015 and 0.024, respectively), even after age correction. TRAJ56 and TRBV4‐3 were more prevalent in MS patients than in HCs (pcorr = 0.027 and 0.040, respectively). GLIPH consolidated 208,674 TCR clones from MS patients into 1,294 clusters, among which two candidate clusters were identified. The TRBV4‐3 cluster was shared by HLA‐DRB1*04:05‐positive patients (87.5%) and predicted to recognize CMV peptides (CMV‐TCR). MS Severity Score (MSSS) was lower in patients with CMV‐TCR than in those without (P = 0.037). CMV‐IgG‐positivity was associated with lower MSSS in HLA‐DRB1*04:05 carriers (P = 0.0053). HLA‐DRB1*04:05‐positive individuals demonstrated higher CMV‐IgG titers than HLA‐DRB1*04:05‐negative individuals (P = 0.017). CMV‐IgG‐positive patients had more Tregs than CMV‐IgG‐negative patients (P = 0.054).InterpretationHigh TCRα/TCRβ diversity, regardless of age, is characteristic of MS. Association of a CMV‐recognizing TCR with mild disability indicates CMV’s protective role in HLA‐DRB1*04:05‐positive MS.

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Target Reprogramming Lysosomes of CD8+ T Cells by a Mineralized Metal–Organic Framework for Cancer Immunotherapy

Zhao

Gong

et al. 2021

Advanced Materials

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T cell immunotherapy holds significant challenges in solid tumors, mainly due to the T cells’ low activation and the decreased synthesis–release of therapeutic proteins, including perforin and granzyme B, which are present in lysosomes. In this study, a lysosome‐targeting nanoparticle (LYS‐NP) is developed by way of a mineralized metal–organic framework (MOF) coupled with a lysosome‐targeting aptamer (CD63‐aptamer) to enhance the antitumor effect of T cells. The MOF synthesized from Zn2+ and dimethylimidazole has good protein encapsulation and acid sensitivity, and is thus an ideal lysosomal delivery vector. Calcium carbonate (CaCO3) is used to induce MOF mineralization, improve the composite material's stability in encapsulating therapeutic protein, and provide calcium ions with synergistic effects. Before mineralization, perforin and granzyme B—T cell‐needed therapeutic proteins for tumors—are preloaded with the MOF. Moreover, T cells are pretreated with processed tumor‐specific antigens to activate or produce memory before reprogramming the lysosomes, facilitating the T cell receptor (TCR) for release of the therapeutic proteins. Using T cells recombined by LYS‐NPs, a significant enhancement of breast cancer control is confirmed.

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Immunosequencing identifies signatures of cytomegalovirus exposure history and HLA-mediated effects on the T cell repertoire

Cited by 469 publications

References 62 publications

Predicting the spectrum of TCR repertoire sharing with a data‐driven model of recombination

Predicting the spectrum of TCR repertoire sharing with a data‐driven model of recombination

A new clustering method identifies multiple sclerosis‐specific T‐cell receptors

Target Reprogramming Lysosomes of CD8+ T Cells by a Mineralized Metal–Organic Framework for Cancer Immunotherapy

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