Your search keyword '"Jason Waithman"' showing total 78 results

1. Transcriptional rewiring in CD8+ T cells: implications for CAR-T cell therapy against solid tumours

Author

Shamini Srinivasan, Jesse Armitage, Jonas Nilsson, and Jason Waithman

Subjects

immunotherapy, adoptive cell therapy (ACT), transcription factor, cancer, CAR-T cell, CD8+ T cell, Immunologic diseases. Allergy, RC581-607

Abstract

T cells engineered to express chimeric-antigen receptors (CAR-T cells) can effectively control relapsed and refractory haematological malignancies in the clinic. However, the successes of CAR-T cell therapy have not been recapitulated in solid tumours due to a range of barriers such as immunosuppression, poor infiltration, and tumour heterogeneity. Numerous strategies are being developed to overcome these barriers, which include improving culture conditions and manufacturing protocols, implementing novel CAR designs, and novel approaches to engineering the T cell phenotype. In this review, we describe the various emerging strategies to improve CAR T cell therapy for solid tumours. We specifically focus on new strategies to modulate cell function and fate that have precipitated from the growing knowledge of transcriptional circuits driving T cell differentiation, with the ultimate goal of driving more productive anti-tumour T cell immunity. Evidence shows that enrichment of particular phenotypic subsets of T cells in the initial cell product correlates to improved therapeutic responses and clinical outcomes. Furthermore, T cell exhaustion and poor persistence are major factors limiting therapeutic efficacy. The latest preclinical work shows that targeting specific master regulators and transcription factors can overcome these key barriers, resulting in superior T cell therapeutic products. This can be achieved by targeting key transcriptional circuits promoting memory-like phenotypes or sustaining key effector functions within the hostile tumour microenvironment. Additional discussion points include emerging considerations for the field such as (i) targeting permutations of transcription factors, (ii) transient expression systems, (iii) tissue specificity, and (iv) expanding this strategy beyond CAR-T cell therapy and cancer.

Published

2024

2. Single cell transcriptomics reveals cell type specific features of developmentally regulated responses to lipopolysaccharide between birth and 5 years

Author

James F. Read, Michael Serralha, Jesse D. Armitage, Muhammad Munir Iqbal, Mark N. Cruickshank, Alka Saxena, Deborah H. Strickland, Jason Waithman, Patrick G. Holt, and Anthony Bosco

Subjects

single cell genomics, scRNA-Seq, toll-like receptors, lipopolysaccharide, poly(I:C), interferon, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundHuman perinatal life is characterized by a period of extraordinary change during which newborns encounter abundant environmental stimuli and exposure to potential pathogens. To meet such challenges, the neonatal immune system is equipped with unique functional characteristics that adapt to changing conditions as development progresses across the early years of life, but the molecular characteristics of such adaptations remain poorly understood. The application of single cell genomics to birth cohorts provides an opportunity to investigate changes in gene expression programs elicited downstream of innate immune activation across early life at unprecedented resolution.MethodsIn this study, we performed single cell RNA-sequencing of mononuclear cells collected from matched birth cord blood and 5-year peripheral blood samples following stimulation (18hrs) with two well-characterized innate stimuli; lipopolysaccharide (LPS) and Polyinosinic:polycytidylic acid (Poly(I:C)).ResultsWe found that the transcriptional response to LPS was constrained at birth and predominantly partitioned into classical proinflammatory gene upregulation primarily by monocytes and Interferon (IFN)-signaling gene upregulation by lymphocytes. Moreover, these responses featured substantial cell-to-cell communication which appeared markedly strengthened between birth and 5 years. In contrast, stimulation with Poly(I:C) induced a robust IFN-signalling response across all cell types identified at birth and 5 years. Analysis of gene regulatory networks revealed IRF1 and STAT1 were key drivers of the LPS-induced IFN-signaling response in lymphocytes with a potential developmental role for IRF7 regulation.ConclusionAdditionally, we observed distinct activation trajectory endpoints for monocytes derived from LPS-treated cord and 5-year blood, which was not apparent among Poly(I:C)-induced monocytes. Taken together, our findings provide new insight into the gene regulatory landscape of immune cell function between birth and 5 years and point to regulatory mechanisms relevant to future investigation of infection susceptibility in early life.

Published

2023

3. Type I interferon subtypes differentially activate the anti-leukaemic function of natural killer cells

Author

Samantha A. Barnes, Katherine M. Audsley, Hannah V. Newnes, Sonia Fernandez, Emma de Jong, Jason Waithman, and Bree Foley

Subjects

natural killer cells, leukemia, interferon subtypes, adoptive cell therapy, immunotherapy, Immunologic diseases. Allergy, RC581-607

Abstract

Natural killer (NK) cells have an intrinsic ability to detect and eliminate leukaemic cells. Cellular therapies using cytokine-activated NK cells have emerged as promising treatments for patients with advanced leukaemia. However, not all patients respond to current NK cell therapies, and thus improvements in efficacy are required. Type I interferons (IFN-I) are a family of potent immunomodulatory cytokines with a known ability to modulate NK cell responses against cancer. Although the human IFN-I family comprises 16 distinct subtypes, only IFNα2 has been widely explored as an anti-cancer agent. Here, we investigated the individual immunomodulatory effects each IFNα subtype and IFNβ had on NK cell functionality to determine whether a particular subtype confers enhanced effector activity against leukaemia. Importantly, IFNα14 and IFNβ were identified as superior activators of NK cell effector function in vitro. To test the ability of these subtypes to enhance NK cell activity in vivo, IFN-I stimulation was overlaid onto a standard ex vivo expansion protocol to generate NK cells for adoptive cell therapy. Interestingly, infusion of NK cells pre-activated with IFNα14, but not IFNβ, significantly prolonged survival in a preclinical model of leukaemia compared to NK cells expanded without IFN-I. Collectively, these results highlight the diverse immunomodulatory potencies of individual IFN-I subtypes and support further investigation into the use of IFNα14 to favourably modulate NK cells against leukaemia.

Published

2022

4. Tissue-resident memory T cells in the era of (Neo) adjuvant melanoma management

Author

Kai R. Plunkett, Jesse D. Armitage, Andrisha-Jade Inderjeeth, Alison M. McDonnell, Jason Waithman, and Peter K. H. Lau

Subjects

tissue-resident memory CD8(+) T cells, cancer immunotherapy, melanoma, immune checkpoints, neoadjuvant immunotherapy, adjuvant immunotherapy, Immunologic diseases. Allergy, RC581-607

Abstract

Tissue-resident memory T (TRM) cells have emerged as key players in the immune control of melanoma. These specialized cells are identified by expression of tissue retention markers such as CD69, CD103 and CD49a with downregulation of egress molecules such as Sphingosine-1-Phosphate Receptor-1 (S1PR1) and the lymphoid homing receptor, CD62L. TRM have been shown to be integral in controlling infections such as herpes simplex virus (HSV), lymphocytic choriomeningitis virus (LCMV) and influenza. More recently, robust pre-clinical models have also demonstrated TRM are able to maintain melanoma in a dormant state without progression to macroscopic disease reminiscent of their ability to control viral infections. The discovery of the role these cells play in anti-melanoma immunity has coincided with the advent of immune checkpoint inhibitor (ICI) therapy which has revolutionized the treatment of cancers. ICIs that target programmed death protein-1 (PD-1) and cytotoxic T lymphocyte antigen-4 (CTLA-4) have led to substantial improvements in outcomes for patients with metastatic melanoma and have been rapidly employed to reduce recurrences in the resected stage III setting. While ICIs mediate anti-tumor activity via CD8+ T cells, the specific subsets that facilitate this response is unclear. TRM invariably exhibit high expression of immune checkpoints such as PD-1, CTLA-4 and lymphocyte activating gene-3 (LAG-3) which strongly implicates this CD8+ T cell subset as a crucial mediator of ICI activity. In this review, we present pre-clinical and translational studies that highlight the critical role of TRM in both immune control of primary melanoma and as a key CD8+ T cell subset that mediates anti-tumor activity of ICIs for the treatment of melanoma.

Published

2022

5. Impaired T cell proliferation by ex vivo BET-inhibition impedes adoptive immunotherapy in a murine melanoma model

Author

Jonathan Chee, Chelsea Wilson, Anthony Buzzai, Ben Wylie, Catherine A Forbes, Mitchell Booth, Nicola Principe, Bree Foley, Mark N Cruickshank, and Jason Waithman

Subjects

cancer immunotherapy, adoptive cell therapy, t cell differentiation, melanoma, cytotoxic t lymphocytes, bet inhibition, Genetics, QH426-470

Abstract

Activation of naïve CD8+ T cells stimulates proliferation and differentiation into cytotoxic T-lymphocytes (CTLs). Adoptive T Cell Therapy (ACT) involves multiple rounds of ex vivo activation to generate enough CTLs for reinfusion into patients, but this drives differentiation into terminal effector T cells. Less differentiated CTL populations, such as stem cell memory T cells, are more ideal candidates for ACT because of increased self-renewal and persistent properties. Ex vivo targeting of T cell differentiation with epigenetic modifiers is a potential strategy to improve cytotoxic T-lymphocyte (CTL) generation for ACT. We established a pipeline to assess the effects of epigenetic modifiers on CD8+ T cell proliferation, differentiation, and efficacy in a preclinical melanoma model. Single treatment with epigenetic modifiers inhibited T cell proliferation in vitro, producing CD44hiCD62Lhi effector-like T cells rather than a stem cell memory T cell phenotype. Most epigenetic modifying agents had no significant effect on ACT efficacy with the notable exception of the bromodomain and extraterminal (BET)-inhibitor JQ1 which was associated with a decrease in efficacy compared to unmodified T cells. These findings reveal the complexity of epigenetic targeting of T cell differentiation, highlighting the need to precisely define the epigenetic targeting strategies to improve CTL generation for ACT.

Published

2020

6. IFNβ Is a Potent Adjuvant for Cancer Vaccination Strategies

Author

Katherine M. Audsley, Teagan Wagner, Clara Ta, Hannah V. Newnes, Anthony C. Buzzai, Samantha A. Barnes, Ben Wylie, Jesse Armitage, Tsuneyasu Kaisho, Anthony Bosco, Alison McDonnell, Mark Cruickshank, Vanessa S. Fear, Bree Foley, and Jason Waithman

Subjects

type I interferon, IFNβ, cancer vaccination, adjuvant, cross-priming, CD8+ T cells, Immunologic diseases. Allergy, RC581-607

Abstract

Cancer vaccination drives the generation of anti-tumor T cell immunity and can be enhanced by the inclusion of effective immune adjuvants such as type I interferons (IFNs). Whilst type I IFNs have been shown to promote cross-priming of T cells, the role of individual subtypes remains unclear. Here we systematically compared the capacity of distinct type I IFN subtypes to enhance T cell responses to a whole-cell vaccination strategy in a pre-clinical murine model. We show that vaccination in combination with IFNβ induces significantly greater expansion of tumor-specific CD8+ T cells than the other type I IFN subtypes tested. Optimal expansion was dependent on the presence of XCR1+ dendritic cells, CD4+ T cells, and CD40/CD40L signaling. Therapeutically, vaccination with IFNβ delayed tumor progression when compared to vaccination without IFN. When vaccinated in combination with anti-PD-L1 checkpoint blockade therapy (CPB), the inclusion of IFNβ associated with more mice experiencing complete regression and a trend in increased overall survival. This work demonstrates the potent adjuvant activity of IFNβ, highlighting its potential to enhance cancer vaccination strategies alone and in combination with CPB.

Published

2021

7. Diverse Anti-Tumor Immune Potential Driven by Individual IFNα Subtypes

Author

Anthony C. Buzzai, Teagan Wagner, Katherine M. Audsley, Hannah V. Newnes, Lucy W. Barrett, Samantha Barnes, Ben C. Wylie, Shane Stone, Alison McDonnell, Vanessa S. Fear, Bree Foley, and Jason Waithman

Subjects

interferon subtypes, adoptive cell therapy, tumor microenvironment, CD8+ T cells, immunotherapy, Immunologic diseases. Allergy, RC581-607

Abstract

Immunotherapies harnessing T cell immunity have shown remarkable clinical success for the management of cancer. However, only a proportion of patients benefit from these treatments. The presence of type I interferon (IFN) within the tumor microenvironment is critical for driving effective tumor-specific T cell immunity. Individuals can produce 12 distinct subtypes of IFNα, which all signal through a common receptor. Despite reported differences in anti-viral potencies, the concept that distinct IFNα subtypes can improve anti-cancer treatments remains unclear. We tested whether expression of unique IFNα subtypes confined to the tumor microenvironment enhances tumor control. This was systematically evaluated by transplantation of B16 murine melanoma cells secreting five unique IFNα subtypes (B16_IFNα2; B16_IFNα4; B16_IFNα5; B16_IFNα6; B16_IFNα9) into a pre-clinical murine model. We show that IFNα2 and IFNα9 are the only subtypes capable of completely controlling tumor outgrowth, with this protection dependent on the presence of an adaptive immune response. We next determined whether these differences extended to other model systems and found that the adoptive transfer of tumor-specific CD8+ T cells engineered to secrete IFNα9 delays tumor growth significantly and improves survival, whereas no enhanced survival was observed using T cells secreting IFNα4. Overall, our data shows that the expression of distinct IFNα subtypes within the tumor microenvironment results in different anti-tumor activities, and differentially affects the efficacy of a cancer therapy targeting established disease.

Published

2020

8. Identifying the optimal donor for natural killer cell adoptive therapy to treat paediatric B‐ and T‐cell acute lymphoblastic leukaemia

Author

Bree Foley, Clara Ta, Samantha Barnes, Emma deJong, Michelle Nguyen, Laurence C Cheung, Anthony Buzzai, Teagan Wagner, Ben Wylie, Sonia Fernandez, Mark Cruickshank, Raelene Endersby, Ursula Kees, and Jason Waithman

Subjects

acute lymphoblastic leukaemia, cellular therapy, cytomegalovirus, natural killer cells, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Objectives Natural killer (NK) cells are an attractive source of cells for an ‘off the shelf’ cellular therapy because of their innate capacity to target malignant cells, and ability to be transferred between donors and patients. However, since not all NK cells are equally effective at targeting cancer, selecting the right donor for cellular therapy is critical for the success of the treatment. Recently, cellular therapies utilising NK cells from cytomegalovirus (CMV)‐seropositive donors have been explored. However, whether these NK cells are the best source to treat paediatric acute lymphoblastic leukaemia (ALL) remains unclear. Methods Using a panel of patient‐derived paediatric B‐ and T‐ALL, we assessed the ability of NK cells from 49 healthy donors to mount an effective functional response against these two major subtypes of ALL. Results From this cohort, we have identified a pool of donors with superior activity against multiple ALL cells. While these donors were more likely to be CMV+, we identified multiple CMVneg donors within this group. Furthermore, NK cells from these donors recognised B‐ and T‐ALL through different activating receptors. Dividing functional NK cells into 29 unique subsets, we observed that within each individual the same NK cell subsets dominated across all ALL cells. Intriguingly, this occurred despite the ALL cells in our panel expressing different combinations of NK cell ligands. Finally, we can demonstrate that cellular therapy products derived from these superior donors significantly delayed leukaemia progression in preclinical models of ALL. Conclusions We have identified a pool of superior donors that are effective against a range of ALL cells, representing a potential pool of donors that can be used as an adoptive NK cell therapy to treat paediatric ALL.

Published

2020

9. Tissue-resident memory T cells orchestrate tumour-immune equilibrium

Author

Simone L. Park, Laura K. Mackay, Jason Waithman, and Thomas Gebhardt

Subjects

melanoma, cancer-immune equilibrium, tissue-resident memory T cells, Medicine, Biology (General), QH301-705.5

Abstract

The immune system can prevent tumour development by engaging in a process termed cancer immunosurveillance, during which immune cells such as T cells restrict tumour growth either by completely eradicating cancer cells in a process of ‘elimination’ or by suppressing cancer cell outgrowth by establishing a state of tumour-immune ‘equilibrium’. Most cancers develop within epithelial layers of tissues but circulating T cells are largely excluded from these epithelial tissue compartments in the absence of infection or overt inflammation. In contrast, CD8+ tissue-resident memory T (TRM) cells reside permanently within epithelial layers of peripheral tissues without recirculating in blood. Accumulating evidence suggests that TRM cells are found in diverse human solid cancers where they correlate with improved prognosis and can protect against tumour challenge in mice. However, the mechanisms through which these cells mediate cancer protection are poorly understood. In our recent study (Park SL et al, Nature 565(7739), 2019) we developed a melanoma model that allowed us to identify a critical role for TRM cells in the establishment and maintenance of tumour-immune equilibrium in skin. Our findings provide insight into the immune cell populations important for maintaining long-term tumour dormancy in peripheral tissues and imply that targeting TRM cells may serve as a novel cancer treatment strategy.

Published

2019

10. Editorial: Insights Into Biomarkers, Cytokines, and Chemokines in Skin Cancer

Author

Lucy W. Barrett, Elin S. Gray, James W. Wells, and Jason Waithman

Subjects

skin cancer, immunology, biomarkers, chemokines, cytokines, immunotherapy, Medicine (General), R5-920

Published

2019

11. Acquired resistance during adoptive cell therapy by transcriptional silencing of immunogenic antigens

Author

Ben Wylie, Jonathan Chee, Catherine A Forbes, Mitchell Booth, Shane R Stone, Anthony Buzzai, Ana Abad, Bree Foley, Mark N Cruickshank, and Jason Waithman

Subjects

cancer, immunotherapy, adoptive cell therapy, acquired resistance, epigenetic modifiers, immunoediting, transcriptional silencing, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Immunotherapies such as adoptive cell therapy (ACT) are promising treatments for solid cancers. However, relapsing disease remains a problem and the molecular mechanisms underlying resistance are poorly defined. We postulated that the deregulated epigenetic landscape in cancer cells could underpin the acquisition of resistance to immunotherapy. To address this question, two preclinical models of ACT were employed to study transcriptional and epigenetic regulatory processes within ACT-treated cancer cells. In these models ACT consistently causes robust tumor regression, but resistance develops and tumors relapse. We identified down-regulated expression of immunogenic antigens at the mRNA level correlated with escape from immune control. To determine whether this down-regulation was under epigenetic control, we treated escaped tumor cells with DNA demethylating agents, azacytidine (AZA) and decitabine (DEC). AZA or DEC treatment restored antigen expression in a proportion of the tumor population. To explore the importance of other epigenetic modifications we isolated tumor cells refractory to DNA demethylation and screened clones against a panel of 19 different epigenetic modifying agents (EMAs). The library of EMAs included inhibitors of a range of chromosomal and transcription regulatory protein complexes, however, when tested as single agents none restored further antigen expression. These findings suggest that tumor cells employ multiple epigenetic and genetic mechanisms to evade immune control, and a combinatorial approach employing several EMAs targeting transcription and genome stability may be required to overcome tumor resistance to immunotherapy.

Published

2019

12. CD8+XCR1neg Dendritic Cells Express High Levels of Toll-Like Receptor 5 and a Unique Complement of Endocytic Receptors

Author

Ben Wylie, James Read, Anthony C. Buzzai, Teagan Wagner, Niamh Troy, Genevieve Syn, Shane R. Stone, Bree Foley, Anthony Bosco, Mark N. Cruickshank, and Jason Waithman

Subjects

dendritic cells, TLR5, XCR1, immunosurveillance, transcriptomics, microarray, Immunologic diseases. Allergy, RC581-607

Abstract

Conventional dendritic cells (cDC) resident in the lymphoid organs of mice have been classically divided into CD8+ and CD8neg subsets. It is well-established that CD8+ dendritic cells (DCs) and their migratory counterparts in the periphery comprise the cross-presenting cDC1 subset. In contrast, CD8neg DCs are grouped together in the heterogeneous cDC2 subset. CD8neg DCs are relatively poor cross-presenters and drive more prominent CD4+ T cell responses against exogenous antigens. The discovery of the X-C motif chemokine receptor 1 (XCR1) as a specific marker of cross-presenting DCs, has led to the identification of a divergent subset of CD8+ DCs that lacks the ability to cross-present. Here, we report that these poorly characterized CD8+XCR1neg DCs have a gene expression profile that is consistent with both plasmacytoid DCs (pDCs) and cDC2. Our data demonstrate that CD8+XCR1neg DCs possess a unique pattern of endocytic receptors and a restricted toll-like receptor (TLR) profile that is particularly enriched for TLR5, giving them a unique position within the DC immunosurveillance network.

Published

2019

13. Accumulation of CD103+ CD8+ T cells in a cutaneous melanoma micrometastasis

Author

Katharina Hochheiser, Han Xian Aw Yeang, Teagan Wagner, Candani Tutuka, Andreas Behren, Jason Waithman, Christopher Angel, Paul J Neeson, Thomas Gebhardt, and David E Gyorki

Subjects

melanoma, micrometastasis, tissue‐resident memory T cells, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Objective The immune system can halt cancer progression by suppressing outgrowth of clinically occult micrometastases in a state of cancer‐immune equilibrium. Cutaneous melanoma provides a unique opportunity to study the immune contexture of such lesions, as miniscule skin metastases are accessible to clinical inspection and diagnostic biopsy. Methods Here, we analysed by multiplex immunofluorescence microscopy samples from a melanoma patient presenting with an overt and an occult in‐transit metastasis (ITM), the latter of which appeared as a small erythematous papule. Results Microarchitecture and immune composition in the two lesions were vastly different. CD4+ and CD8+ T cells accumulated around the margin of the overt SOX10+ Melan A+ ITM but were largely excluded from the tumor centre. By contrast, the occult micrometastasis contained only few SOX10+ Melan A− melanoma cells which were scattered within a dense infiltrate of T cells, including a prominent population of CD103+ CD8+ T cells resembling tissue‐resident memory T (TRM) cells. Notably, almost every single melanoma cell in the micrometastasis was in close proximity to these TRM‐like cells. Conclusion Such results support the emerging concept that CD103+ CD8+ TRM cells are key mediators of cancer surveillance and imply an important function of these cells in controlling clinically occult micrometastases in humans.

Published

2019

14. Fine-Tuning the Tumour Microenvironment: Current Perspectives on the Mechanisms of Tumour Immunosuppression

Author

Jesse D. Armitage, Hannah V. Newnes, Alison McDonnell, Anthony Bosco, and Jason Waithman

Subjects

tumour, immunosuppression, tumour microenvironment, mechanisms, immunotherapy, fine-tuning, Cytology, QH573-671

Abstract

Immunotherapy has revolutionised the treatment of cancers by harnessing the power of the immune system to eradicate malignant tissue. However, it is well recognised that some cancers are highly resistant to these therapies, which is in part attributed to the immunosuppressive landscape of the tumour microenvironment (TME). The contexture of the TME is highly heterogeneous and contains a complex architecture of immune, stromal, vascular and tumour cells in addition to acellular components such as the extracellular matrix. While understanding the dynamics of the TME has been instrumental in predicting durable responses to immunotherapy and developing new treatment strategies, recent evidence challenges the fundamental paradigms of how tumours can effectively subvert immunosurveillance. Here, we discuss the various immunosuppressive features of the TME and how fine-tuning these mechanisms, rather than ablating them completely, may result in a more comprehensive and balanced anti-tumour response.

Published

2021

15. Cross-Presenting XCR1+ Dendritic Cells as Targets for Cancer Immunotherapy

Author

Katherine M. Audsley, Alison M. McDonnell, and Jason Waithman

Subjects

cross-presenting dendritic cells, dc-based therapy, immunotherapy, cancer, Cytology, QH573-671

Abstract

The use of dendritic cells (DCs) to generate effective anti-tumor T cell immunity has garnered much attention over the last thirty-plus years. Despite this, limited clinical benefit has been demonstrated thus far. There has been a revival of interest in DC-based treatment strategies following the remarkable patient responses observed with novel checkpoint blockade therapies, due to the potential for synergistic treatment. Cross-presenting DCs are recognized for their ability to prime CD8+ T cell responses to directly induce tumor death. Consequently, they are an attractive target for next-generation DC-based strategies. In this review, we define the universal classification system for cross-presenting DCs, and the vital role of this subset in mediating anti-tumor immunity. Furthermore, we will detail methods of targeting these DCs both ex vivo and in vivo to boost their function and drive effective anti-tumor responses.

Published

2020

16. Dietary Vitamin D Increases Percentages and Function of Regulatory T Cells in the Skin-Draining Lymph Nodes and Suppresses Dermal Inflammation

Author

Shelley Gorman, Sian Geldenhuys, Melinda Judge, Clare E. Weeden, Jason Waithman, and Prue H. Hart

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

Skin inflammatory responses in individuals with allergic dermatitis may be suppressed by dietary vitamin D through induction and upregulation of the suppressive activity of regulatory T (TReg) cells. Vitamin D may also promote TReg cell tropism to dermal sites. In the current study, we examined the capacity of dietary vitamin D3 to modulate skin inflammation and the numbers and activity of TReg cells in skin and other sites including lungs, spleen, and blood. In female BALB/c mice, dietary vitamin D3 suppressed the effector phase of a biphasic ear swelling response induced by dinitrofluorobenzene in comparison vitamin D3-deficient female BALB/c mice. Vitamin D3 increased the percentage of TReg (CD3+CD4+CD25+Foxp3+) cells in the skin-draining lymph nodes (SDLN). The suppressive activity of TReg cells in the SDLN, mesenteric lymph nodes, spleen, and blood was upregulated by vitamin D3. However, there was no difference in the expression of the naturally occurring TReg cell marker, neuropilin, nor the expression of CCR4 or CCR10 (skin-tropic chemokine receptors) on TReg cells in skin, SDLN, lungs, and airway-draining lymph nodes. These data suggest that dietary vitamin D3 increased the percentages and suppressive activity of TReg cells in the SDLN, which are poised to suppress dermal inflammation.

Published

2016

17. Resident CD8(+) and migratory CD103(+) dendritic cells control CD8 T cell immunity during acute influenza infection.

Author

Jason Waithman, Damien Zanker, Kun Xiao, Sara Oveissi, Ben Wylie, Royce Ng, Lars Tögel, and Weisan Chen

Subjects

Medicine, Science

Abstract

The identification of the specific DC subsets providing a critical role in presenting influenza antigens to naïve T cell precursors remains contentious and under considerable debate. Here we show that CD8(+) T lymphocyte (TCD8+) responses are severely hampered in C57BL/6 mice deficient in the transcription factor Batf3 after intranasal challenge with influenza A virus (IAV). This transcription factor is required for the development of lymph node resident CD8(+) and migratory CD103(+)CD11b(-) DCs and we found both of these subtypes could efficiently stimulate anti-IAV TCD8+. Using a similar ex vivo approach, many publications on this subject matter excluded a role for resident, non-migratory CD8(+) DC. We postulate the differences reported can partially be explained by how DC are phenotyped, namely the use of MHC class II to segregate subtypes. Our results show that resident CD8(+) DC upregulate this marker during IAV infection and we advise against its use when isolating DC subtypes.

Published

2013

18. Adoptive cellular therapy with T cells expressing the dendritic cell growth factor Flt3L drives epitope spreading and antitumor immunity

Author

Junyun Lai, Maximilien Evrard, Lauren Giuffrida, Emma V. Petley, Katherine Kedzierska, Stephin J. Vervoort, Paul A. Beavis, Joseph A. Trapani, Imran G House, Kirsten L. Todd, Jason Waithman, Jack D Chan, Sherly Mardiana, Emma M. Carrington, Kevin Sek, Phillip K. Darcy, Benjamin Solomon, Melissa A. Henderson, Andrew M. Lew, and Amanda X. Y. Chen

Subjects

0301 basic medicine, T-Lymphocytes, T cell, medicine.medical_treatment, Immunology, Receptors, Antigen, T-Cell, Mice, Transgenic, Lymphocyte Activation, Immunotherapy, Adoptive, Cell therapy, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Antigens, Neoplasm, medicine, Animals, Humans, Immunologic Factors, Immunology and Allergy, Receptors, Chimeric Antigen, Chemistry, Membrane Proteins, Dendritic Cells, Neoplasms, Experimental, Dendritic cell, Immunotherapy, Chimeric antigen receptor, Tumor antigen, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Cancer research, Chimeric Antigen Receptor T-Cell Therapy, 030215 immunology

Abstract

Adoptive cell therapies using genetically engineered T cell receptor or chimeric antigen receptor T cells are emerging forms of immunotherapy that redirect T cells to specifically target cancer. However, tumor antigen heterogeneity remains a key challenge limiting their efficacy against solid cancers. Here, we engineered T cells to secrete the dendritic cell (DC) growth factor Fms-like tyrosine kinase 3 ligand (Flt3L). Flt3L-secreting T cells expanded intratumoral conventional type 1 DCs and substantially increased host DC and T cell activation when combined with immune agonists poly (I:C) and anti-4-1BB. Importantly, combination therapy led to enhanced inhibition of tumor growth and the induction of epitope spreading towards antigens beyond those recognized by adoptively transferred T cells in solid tumor models of T cell receptor and chimeric antigen receptor T cell therapy. Our data suggest that augmenting endogenous DCs is a promising strategy to overcome the clinical problem of antigen-negative tumor escape following adoptive cell therapy.

Published

2020

19. Targeting Cross-Presentation as a Route to Improve the Efficiency of Peptide-Based Cancer Vaccines

Author

Ben Wylie, Ferrer Ong, Hanane Belhoul-Fakir, Kristin Priebatsch, Heique Bogdawa, Anja Stirnweiss, Paul Watt, Paula Cunningham, Shane R. Stone, and Jason Waithman

Subjects

Cancer Research, Oncology, cell penetrating peptide, dendritic cell, peptide vaccine, melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, cancer vaccine, cross-presentation, immunotherapy, Article, RC254-282

Abstract

Simple Summary Cancer vaccination is a potential anti-cancer therapy which may improve clinical outcomes, particularly in combination with current immunotherapies, but to date has demonstrated only limited success. Here we set out to improve the effectiveness of peptide-based cancer vaccine design by implementing a unique approach to target peptide antigens to the cross-presentation pathway within dendritic cells. We demonstrate that the addition of a short cell penetrating peptide sequence to the vaccine construct enhances the efficiency of our vaccine and improves outcomes in both a viral and a cancer model. Our findings provide a simple strategy that may enhance the effectiveness of peptide-based cancer vaccines and the priming of anti-tumor immunity. Abstract Cross-presenting dendritic cells (DC) offer an attractive target for vaccination due to their unique ability to process exogenous antigens for presentation on MHC class I molecules. Recent reports have established that these DC express unique surface receptors and play a critical role in the initiation of anti-tumor immunity, opening the way for the development of vaccination strategies specifically targeting these cells. This study investigated whether targeting cross-presenting DC by two complementary mechanisms could improve vaccine effectiveness, in both a viral setting and in a murine melanoma model. Our novel vaccine construct contained the XCL1 ligand, to target uptake to XCR1+ cross-presenting DC, and a cell penetrating peptide (CPP) with endosomal escape properties, to enhance antigen delivery into the cross-presentation pathway. Using a prime-boost regimen, we demonstrated robust expansion of antigen-specific T cells following vaccination with our CPP-linked peptide vaccine and protective immunity against HSV-1 skin infection, where vaccine epitopes were natively expressed by the virus. Additionally, our novel vaccination strategy slowed tumor outgrowth in a B16 murine melanoma model, compared to adjuvant only controls, suggesting antigen-specific anti-tumor immunity was generated following vaccination. These findings suggest that novel strategies to target the antigen cross-presentation pathway in DC may be beneficial for the generation of anti-tumor immunity.

Published

2021

20. Directing the Future Breakthroughs in Immunotherapy: The Importance of a Holistic Approach to the Tumour Microenvironment

Author

Jesse D. Armitage, Hannah V. Newnes, Katherine M. Audsley, Anthony Bosco, and Jason Waithman

Subjects

Cancer Research, Stromal cell, Response to therapy, business.industry, medicine.medical_treatment, Cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Review, Immunotherapy, multi-omics, medicine.disease, Immune system, Oncology, medicine, Cancer research, Multi omics, immunotherapy, personalised therapy, business, tumour microenvironment, RC254-282

Abstract

Simple Summary Immunotherapies have changed the way we treat cancer and, while some patients have benefitted greatly, there are still those that do not respond to therapy. Understanding why some patients respond to therapy and others do not is critical in developing new immunotherapeutic strategies. The increasing awareness of the importance of investigating the tumour in its entirety, including the surrounding tissue and role of various immune cells is helping to differentiate responders and non-responders. In addition, the resolution gained by the development of sophisticated bioinformatic technologies allows for a deeper understanding of the complex roles of individual cells in the tumour. This advancement will be critical for the development of novel therapies to treat cancer. Abstract Immunotherapy has revolutionised the treatment of cancers by exploiting the immune system to eliminate tumour cells. Despite the impressive response in a proportion of patients, clinical benefit has been limited thus far. A significant focus to date has been the identification of specific markers associated with response to immunotherapy. Unfortunately, the heterogeneity between patients and cancer types means identifying markers of response to therapy is inherently complex. There is a growing appreciation for the role of the tumour microenvironment (TME) in directing response to immunotherapy. The TME is highly heterogeneous and contains immune, stromal, vascular and tumour cells that all communicate and interact with one another to form solid tumours. This review analyses major cell populations present within the TME with a focus on their diverse and often contradictory roles in cancer and how this informs our understanding of immunotherapy. Furthermore, we discuss the role of integrated omics in providing a comprehensive view of the TME and demonstrate the potential of leveraging multi-omics to decipher the underlying mechanisms of anti-tumour immunity for the development of novel immunotherapeutic strategies.

Published

2021

21. Non-severe burn injury increases cancer incidence in mice and has long-term impacts on the activation and function of T cells

Author

Lucy W Barrett, Vanessa S Fear, Bree Foley, Katherine Audsley, Samantha Barnes, Hannah Newnes, Alison McDonnell, Fiona M Wood, Mark W Fear, and Jason Waithman

Subjects

Biomedical Engineering, Emergency Medicine, Immunology and Allergy, Surgery, Dermatology, Critical Care and Intensive Care Medicine

Abstract

Background Recent evidence suggests that burn patients are at increased risk of hospital admission for infection, mental health conditions, cardiovascular disease and cancer for many years after discharge for the burn injury itself. Burn injury has also been shown to induce sustained immune system dysfunction. This change to immune function may contribute to the increased risk of chronic disease observed. However, the mechanisms that disrupt long-term immune function in response to burn trauma, and their link to long-term morbidity, remain unknown. In this study we investigated changes to immune function after burn injury using a murine model of non-severe injury. Methods An established mouse model of non-severe burn injury (full thickness burn equivalent to 8% total body surface area) was used in combination with an orthotopic model of B16 melanoma to investigate the link between burns and cancer. Considering that CD8+ T cells are important drivers of effective tumour suppression in this model, we also investigated potential dysregulation of this immune population using mouse models of burn injury in combination with herpes simplex virus infection. Flow cytometry was used to detect and quantify cell populations of interest and changes in immune function. Results We demonstrate that 4 weeks after a non-severe burn injury, mice were significantly more susceptible to tumour development than controls using an orthotopic model of B16 melanoma. In addition, our results reveal that CD8+ T cell expansion, differentiation and memory potential is significantly impaired at 1 month post-burn. Conclusions Our data suggests that CD8+ T cell-mediated immunity may be dysfunctional for a sustained period after even non-severe burn injury. Further studies in patients to validate these findings may support clinical intervention to restore or protect immunity in patients after burn injury and reduce the increased risk of secondary morbidities observed.

Published

2021

22. Impaired T cell proliferation by ex vivo BET-inhibition impedes adoptive immunotherapy in a murine melanoma model

Author

Catherine A. Forbes, Mark N. Cruickshank, Anthony Buzzai, Chelsea Wilson, Bree Foley, Ben Wylie, Nicola Principe, Jason Waithman, Jonathan Chee, and Mitchell Booth

Subjects

0301 basic medicine, Cancer Research, T cell, medicine.medical_treatment, Biology, 03 medical and health sciences, CTL, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Cancer immunotherapy, 030220 oncology & carcinogenesis, T cell differentiation, medicine, Cancer research, Cytotoxic T cell, Stem cell, Molecular Biology, Memory T cell, CD8

Abstract

Activation of naive CD8+ T cells stimulates proliferation and differentiation into cytotoxic T-lymphocytes (CTLs). Adoptive T Cell Therapy (ACT) involves multiple rounds of ex vivo activation to generate enough CTLs for reinfusion into patients, but this drives differentiation into terminal effector T cells. Less differentiated CTL populations, such as stem cell memory T cells, are more ideal candidates for ACT because of increased self-renewal and persistent properties. Ex vivo targeting of T cell differentiation with epigenetic modifiers is a potential strategy to improve cytotoxic T-lymphocyte (CTL) generation for ACT. We established a pipeline to assess the effects of epigenetic modifiers on CD8+ T cell proliferation, differentiation, and efficacy in a preclinical melanoma model. Single treatment with epigenetic modifiers inhibited T cell proliferation in vitro, producing CD44hiCD62Lhi effector-like T cells rather than a stem cell memory T cell phenotype. Most epigenetic modifying agents had no significant effect on ACT efficacy with the notable exception of the bromodomain and extraterminal (BET)-inhibitor JQ1 which was associated with a decrease in efficacy compared to unmodified T cells. These findings reveal the complexity of epigenetic targeting of T cell differentiation, highlighting the need to precisely define the epigenetic targeting strategies to improve CTL generation for ACT.

Published

2019

23. Fine-Tuning the Tumour Microenvironment: Current Perspectives on the Mechanisms of Tumour Immunosuppression

Author

Hannah V. Newnes, Anthony Bosco, Jason Waithman, Alison M. McDonnell, and Jesse D. Armitage

Subjects

Stromal cell, medicine.medical_treatment, Review, Immune system, Neoplasms, medicine, Tumor Microenvironment, Humans, lcsh:QH301-705.5, Immunosuppression Therapy, Clinical Trials as Topic, mechanisms, immunosuppression, business.industry, tumour, Immunosuppression, General Medicine, Immunotherapy, Immunosurveillance, lcsh:Biology (General), Cancer research, Metabolome, Treatment strategy, Cytokines, sense organs, immunotherapy, business, tumour microenvironment, fine-tuning

Abstract

Immunotherapy has revolutionised the treatment of cancers by harnessing the power of the immune system to eradicate malignant tissue. However, it is well recognised that some cancers are highly resistant to these therapies, which is in part attributed to the immunosuppressive landscape of the tumour microenvironment (TME). The contexture of the TME is highly heterogeneous and contains a complex architecture of immune, stromal, vascular and tumour cells in addition to acellular components such as the extracellular matrix. While understanding the dynamics of the TME has been instrumental in predicting durable responses to immunotherapy and developing new treatment strategies, recent evidence challenges the fundamental paradigms of how tumours can effectively subvert immunosurveillance. Here, we discuss the various immunosuppressive features of the TME and how fine-tuning these mechanisms, rather than ablating them completely, may result in a more comprehensive and balanced anti-tumour response.

Published

2020

24. Cross-Presenting XCR1+ Dendritic Cells as Targets for Cancer Immunotherapy

Author

Alison M. McDonnell, Katherine M. Audsley, and Jason Waithman

Subjects

0301 basic medicine, XCR1, cross-presenting dendritic cells, medicine.medical_treatment, T cell, 03 medical and health sciences, 0302 clinical medicine, Cancer immunotherapy, Immunity, Medicine, cancer, lcsh:QH301-705.5, business.industry, General Medicine, Immunotherapy, Blockade, 030104 developmental biology, medicine.anatomical_structure, dc-based therapy, lcsh:Biology (General), 030220 oncology & carcinogenesis, Cancer research, immunotherapy, business, CD8, Ex vivo

Abstract

The use of dendritic cells (DCs) to generate effective anti-tumor T cell immunity has garnered much attention over the last thirty-plus years. Despite this, limited clinical benefit has been demonstrated thus far. There has been a revival of interest in DC-based treatment strategies following the remarkable patient responses observed with novel checkpoint blockade therapies, due to the potential for synergistic treatment. Cross-presenting DCs are recognized for their ability to prime CD8+ T cell responses to directly induce tumor death. Consequently, they are an attractive target for next-generation DC-based strategies. In this review, we define the universal classification system for cross-presenting DCs, and the vital role of this subset in mediating anti-tumor immunity. Furthermore, we will detail methods of targeting these DCs both ex vivo and in vivo to boost their function and drive effective anti-tumor responses.

Published

2020

25. Cross-Presenting XCR1

Author

Katherine M, Audsley, Alison M, McDonnell, and Jason, Waithman

Subjects

Cross-Priming, cross-presenting dendritic cells, Neoplasms, Animals, Humans, cancer, Dendritic Cells, Immunotherapy, Review, immunotherapy, DC-based therapy, Cancer Vaccines, Receptors, G-Protein-Coupled

Abstract

The use of dendritic cells (DCs) to generate effective anti-tumor T cell immunity has garnered much attention over the last thirty-plus years. Despite this, limited clinical benefit has been demonstrated thus far. There has been a revival of interest in DC-based treatment strategies following the remarkable patient responses observed with novel checkpoint blockade therapies, due to the potential for synergistic treatment. Cross-presenting DCs are recognized for their ability to prime CD8+ T cell responses to directly induce tumor death. Consequently, they are an attractive target for next-generation DC-based strategies. In this review, we define the universal classification system for cross-presenting DCs, and the vital role of this subset in mediating anti-tumor immunity. Furthermore, we will detail methods of targeting these DCs both ex vivo and in vivo to boost their function and drive effective anti-tumor responses.

Published

2020

26. Identifying the optimal donor for natural killer cell adoptive therapy to treat paediatric B‐ and T‐cell acute lymphoblastic leukaemia

Author

Jason Waithman, Bree Foley, Laurence C. Cheung, Clara Ta, Ben Wylie, Michelle Nguyen, Sonia Fernandez, Anthony Buzzai, Teagan Wagner, Raelene Endersby, Ursula R. Kees, Emma de Jong, Mark N. Cruickshank, and Samantha Barnes

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, acute lymphoblastic leukaemia, Immunology, Cell, Natural killer cell, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, Immunology and Allergy, Off the shelf, Medicine, Malignant cells, cytomegalovirus, General Nursing, natural killer cells, business.industry, T-cell acute lymphoblastic leukaemia, Cancer, Original Articles, cellular therapy, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, T cell subset, Original Article, business, lcsh:RC581-607, 030215 immunology

Abstract

Objectives Natural killer (NK) cells are an attractive source of cells for an ‘off the shelf’ cellular therapy because of their innate capacity to target malignant cells, and ability to be transferred between donors and patients. However, since not all NK cells are equally effective at targeting cancer, selecting the right donor for cellular therapy is critical for the success of the treatment. Recently, cellular therapies utilising NK cells from cytomegalovirus (CMV)‐seropositive donors have been explored. However, whether these NK cells are the best source to treat paediatric acute lymphoblastic leukaemia (ALL) remains unclear. Methods Using a panel of patient‐derived paediatric B‐ and T‐ALL, we assessed the ability of NK cells from 49 healthy donors to mount an effective functional response against these two major subtypes of ALL. Results From this cohort, we have identified a pool of donors with superior activity against multiple ALL cells. While these donors were more likely to be CMV+, we identified multiple CMVneg donors within this group. Furthermore, NK cells from these donors recognised B‐ and T‐ALL through different activating receptors. Dividing functional NK cells into 29 unique subsets, we observed that within each individual the same NK cell subsets dominated across all ALL cells. Intriguingly, this occurred despite the ALL cells in our panel expressing different combinations of NK cell ligands. Finally, we can demonstrate that cellular therapy products derived from these superior donors significantly delayed leukaemia progression in preclinical models of ALL. Conclusions We have identified a pool of superior donors that are effective against a range of ALL cells, representing a potential pool of donors that can be used as an adoptive NK cell therapy to treat paediatric ALL., Natural killer (NK) cells are an attractive source of cells for an ‘off the shelf’ cellular therapy; however, since not all NK cells are equally effective at targeting cancer, selecting the right donor for cellular therapy is critical for the success of the treatment. We identified a group of donors who exhibited superior responses against multiple acute lymphoblastic leukaemia (ALL) cells, representing a potential pool of donors that could be used to develop an adoptive NK cell therapy capable of treating a range of ALL subtypes.

Published

2020

27. Tissue-resident memory CD8+ T cells promote melanoma–immune equilibrium in skin

Author

Anthony Buzzai, Robyn McConville, Teagan Wagner, Umaimainthan Palendira, Katharina Hochheiser, Thomas Tüting, James S. Wilmott, David E. Gyorki, Jai Rautela, Jason Waithman, Jyh Liang Hor, Richard A. Scolyer, Jarem Edwards, Maike Effern, Nathan McBain, Scott N. Mueller, Sammy Bedoui, Simone L Park, Michael Hölzel, Laura K. Mackay, Nicholas D. Huntington, and Thomas Gebhardt

Subjects

0301 basic medicine, Multidisciplinary, Epidermis (botany), Tumor-infiltrating lymphocytes, Melanoma, Biology, medicine.disease, Immunosurveillance, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, Cancer cell, medicine, Cancer research, Cytotoxic T cell, CD8, 030215 immunology

Abstract

The immune system can suppress tumour development both by eliminating malignant cells and by preventing the outgrowth and spread of cancer cells that resist eradication1. Clinical and experimental data suggest that the latter mode of control-termed cancer-immune equilibrium1-can be maintained for prolonged periods of time, possibly up to several decades2-4. Although cancers most frequently originate in epithelial layers, the nature and spatiotemporal dynamics of immune responses that maintain cancer-immune equilibrium in these tissue compartments remain unclear. Here, using a mouse model of transplantable cutaneous melanoma5, we show that tissue-resident memory CD8+ T cells (TRM cells) promote a durable melanoma-immune equilibrium that is confined to the epidermal layer of the skin. A proportion of mice (~40%) transplanted with melanoma cells remained free of macroscopic skin lesions long after epicutaneous inoculation, and generation of tumour-specific epidermal CD69+ CD103+ TRM cells correlated with this spontaneous disease control. By contrast, mice deficient in TRM formation were more susceptible to tumour development. Despite being tumour-free at the macroscopic level, mice frequently harboured melanoma cells in the epidermal layer of the skin long after inoculation, and intravital imaging revealed that these cells were dynamically surveyed by TRM cells. Consistent with their role in melanoma surveillance, tumour-specific TRM cells that were generated before melanoma inoculation conferred profound protection from tumour development independently of recirculating T cells. Finally, depletion of TRM cells triggered tumour outgrowth in a proportion (~20%) of mice with occult melanomas, demonstrating that TRM cells can actively suppress cancer progression. Our results show that TRM cells have a fundamental role in the surveillance of subclinical melanomas in the skin by maintaining cancer-immune equilibrium. As such, they provide strong impetus for exploring these cells as targets of future anticancer immunotherapies.

Published

2018

28. Accumulation of CD103+ CD8+ T cells in a cutaneous melanoma micrometastasis

Author

Thomas Gebhardt, Katharina Hochheiser, Jason Waithman, Paul J Neeson, Candani Tutuka, Christopher Angel, Andreas Behren, Teagan Wagner, David E. Gyorki, and Han Xian Aw Yeang

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Pathology, medicine.medical_specialty, micrometastasis, Immunology, Population, Case Report, Case Reports, Metastasis, tissue‐resident memory T cells, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, melanoma, Immunology and Allergy, Cytotoxic T cell, education, General Nursing, education.field_of_study, business.industry, Melanoma, Micrometastasis, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Cutaneous melanoma, lcsh:RC581-607, business, CD8

Abstract

Objective The immune system can halt cancer progression by suppressing outgrowth of clinically occult micrometastases in a state of cancer‐immune equilibrium. Cutaneous melanoma provides a unique opportunity to study the immune contexture of such lesions, as miniscule skin metastases are accessible to clinical inspection and diagnostic biopsy. Methods Here, we analysed by multiplex immunofluorescence microscopy samples from a melanoma patient presenting with an overt and an occult in‐transit metastasis (ITM), the latter of which appeared as a small erythematous papule. Results Microarchitecture and immune composition in the two lesions were vastly different. CD4+ and CD8+ T cells accumulated around the margin of the overt SOX10+ Melan A+ ITM but were largely excluded from the tumor centre. By contrast, the occult micrometastasis contained only few SOX10+ Melan A− melanoma cells which were scattered within a dense infiltrate of T cells, including a prominent population of CD103+ CD8+ T cells resembling tissue‐resident memory T (TRM) cells. Notably, almost every single melanoma cell in the micrometastasis was in close proximity to these TRM‐like cells. Conclusion Such results support the emerging concept that CD103+ CD8+ TRM cells are key mediators of cancer surveillance and imply an important function of these cells in controlling clinically occult micrometastases in humans., Analysing an occult in‐transit metastasis in a melanoma patient, we identify CD103+CD8+ T cells with a resident memory phenotype as the dominant T‐cell subset. Such results support the emerging concept that CD103+CD8+ tissue‐resident memory T cells are key mediators of cancer surveillance and imply an important function of these cells in controlling clinically occult micrometastases in humans.

Published

2019

29. PTPN2 phosphatase deletion in T cells promotes anti-tumour immunity and CAR T-cell efficacy in solid tumours

Author

Conor J. Kearney, Jason Waithman, Pei K Goh, Paul A. Beavis, Melissa A. Henderson, Shuwei Liang, Sheng Zhang, Xin Du, Simone L Park, Kun-Hui Lu, Florian Wiede, Thomas Gebhardt, Zhong Yin Zhang, Tony Tiganis, Phillip K. Darcy, Katharina Hochheiser, Deborah Meyran, Garron T. Dodd, and Jane Oliaro

Subjects

Male, Adoptive cell transfer, Receptor, ErbB-2, TCR signalling, STAT‐5 signalling, Immunology, Receptors, Antigen, T-Cell, Mice, Transgenic, Biology, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Immunotherapy, Adoptive, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Immunity, Neoplasms, adoptive T‐cell therapy, Animals, Humans, Src family kinase, Molecular Biology, 030304 developmental biology, Cancer, Mice, Knockout, 0303 health sciences, Antigen Presentation, Protein Tyrosine Phosphatase, Non-Receptor Type 2, CAR T cells, General Immunology and Microbiology, General Neuroscience, protein tyrosine phosphatase N2, Articles, Adoptive Transfer, Chimeric antigen receptor, 3. Good health, Immunosurveillance, Cancer research, CXCL9, Female, 030217 neurology & neurosurgery, CD8, Homing (hematopoietic), Signal Transduction

Abstract

Although adoptive T‐cell therapy has shown remarkable clinical efficacy in haematological malignancies, its success in combating solid tumours has been limited. Here, we report that PTPN2 deletion in T cells enhances cancer immunosurveillance and the efficacy of adoptively transferred tumour‐specific T cells. T‐cell‐specific PTPN2 deficiency prevented tumours forming in aged mice heterozygous for the tumour suppressor p53. Adoptive transfer of PTPN2‐deficient CD8+ T cells markedly repressed tumour formation in mice bearing mammary tumours. Moreover, PTPN2 deletion in T cells expressing a chimeric antigen receptor (CAR) specific for the oncoprotein HER‐2 increased the activation of the Src family kinase LCK and cytokine‐induced STAT‐5 signalling, thereby enhancing both CAR T‐cell activation and homing to CXCL9/10‐expressing tumours to eradicate HER‐2+ mammary tumours in vivo. Our findings define PTPN2 as a target for bolstering T‐cell‐mediated anti‐tumour immunity and CAR T‐cell therapy against solid tumours., Protein tyrosine phosphatase N2 inhibits tumour T‐cell infiltration and CAR T‐cell cytotoxicity and may thus be a therapeutic target to enhance solid‐tumour immunotherapy.

Published

2019

30. PTPN2 deletion in T cells promotes anti-tumour immunity and CAR T cell efficacy in solid tumours

Author

Kun-Hui Lu, Conor J. Kearney, Garron T. Dodd, Jason Waithman, Jane Oliaro, Phillip K. Darcy, Paul A. Beavis, Florian Wiede, Tony Tiganis, Sheng Zhang, Conor Kearny, Deborah Meyran, Katharina Hochheiser, Pei K Goh, Melissa A. Henderson, Zhong Yin Zhang, Xin Du, Thomas Gebhardt, Shuwei Liang, and Simone L Park

Subjects

Immunosurveillance, Adoptive cell transfer, medicine.anatomical_structure, business.industry, Immunity, T cell, Cancer research, Medicine, Src family kinase, business, CD8, Chimeric antigen receptor, Homing (hematopoietic)

Abstract

Although adoptive T cell therapy has shown remarkable clinical efficacy in hematological malignancies, its success in combating solid tumours has been limited. Here we report that PTPN2 deletion in T cells enhances cancer immunosurveillance and the efficacy of adoptively transferred tumour-specific T cells. T cell-specific PTPN2 deficiency prevented tumours forming in aged mice heterozygous for the tumour suppressor p53. Adoptive transfer of PTPN2-deficient CD8+ T cells markedly repressed tumour formation in mice bearing mammary tumours. Moreover, PTPN2 deletion in T cells expressing a chimeric antigen receptor (CAR) specific for the oncoprotein HER-2 increased the activation of the Src family kinase LCK and cytokine-induced STAT-5 signalling thereby enhancing both CAR T cell activation and homing to CXCL9/10 expressing tumours to eradicate HER-2+ mammary tumours in vivo. Our findings define PTPN2 as a target for bolstering T-cell mediated anti-tumour immunity and CAR T cell therapy against solid tumours.

Published

2019

31. Understanding acute burn injury as a chronic disease

Author

Jason Waithman, L. Barrett, Fiona M. Wood, Mark W. Fear, and Vanessa S. Fear

Subjects

medicine.medical_specialty, Burn injury, Population, Biomedical Engineering, Poison control, lcsh:Medicine, Dermatology, Disease, Review, Patient care, Critical Care and Intensive Care Medicine, Occupational safety and health, Chronic disease, 03 medical and health sciences, 0302 clinical medicine, Injury prevention, Endocrine system, medicine, Immunology and Allergy, Homeostasis, 030212 general & internal medicine, Intensive care medicine, education, Depression (differential diagnoses), education.field_of_study, Thermal injury, business.industry, lcsh:R, 030208 emergency & critical care medicine, Immune system, Emergency Medicine, Surgery, business, Burns

Abstract

While treatment for burn injury has improved significantly over the past few decades, reducing mortality and improving patient outcomes, recent evidence has revealed that burn injury is associated with a number of secondary pathologies, many of which arise long after the initial injury has healed. Population studies have linked burn injury with increased risk of cancer, cardiovascular disease, nervous system disorders, diabetes, musculoskeletal disorders, gastrointestinal disease, infections, anxiety and depression. The wide range of secondary pathologies indicates that burn can cause sustained disruption of homeostasis, presenting new challenges for post-burn care. Understanding burn injury as a chronic disease will improve patient care, providing evidence for better long-term support and monitoring of patients. Through focused research into the mechanisms underpinning long-term dysfunction, a better understanding of burn injury pathology may help with the development of preventative treatments to improve long-term health outcomes. The review will outline evidence of long-term health effects, possible mechanisms linking burn injury to long-term health and current research into burns as a chronic disease.

Published

2019

32. Impaired T cell proliferation by

Author

Jonathan, Chee, Chelsea, Wilson, Anthony, Buzzai, Ben, Wylie, Catherine A, Forbes, Mitchell, Booth, Nicola, Principe, Bree, Foley, Mark N, Cruickshank, and Jason, Waithman

Subjects

T-Lymphocytes, Indolizines, Melanoma, Experimental, Cell Differentiation, Azepines, Triazoles, Immunotherapy, Adoptive, Epigenesis, Genetic, Mice, Inbred C57BL, Benzodiazepines, Mice, Cell Line, Tumor, Animals, Sulfones, Cells, Cultured, Cell Proliferation, Research Paper

Abstract

Activation of naïve CD8(+) T cells stimulates proliferation and differentiation into cytotoxic T-lymphocytes (CTLs). Adoptive T Cell Therapy (ACT) involves multiple rounds of ex vivo activation to generate enough CTLs for reinfusion into patients, but this drives differentiation into terminal effector T cells. Less differentiated CTL populations, such as stem cell memory T cells, are more ideal candidates for ACT because of increased self-renewal and persistent properties. Ex vivo targeting of T cell differentiation with epigenetic modifiers is a potential strategy to improve cytotoxic T-lymphocyte (CTL) generation for ACT. We established a pipeline to assess the effects of epigenetic modifiers on CD8(+) T cell proliferation, differentiation, and efficacy in a preclinical melanoma model. Single treatment with epigenetic modifiers inhibited T cell proliferation in vitro, producing CD44(hi)CD62L(hi) effector-like T cells rather than a stem cell memory T cell phenotype. Most epigenetic modifying agents had no significant effect on ACT efficacy with the notable exception of the bromodomain and extraterminal (BET)-inhibitor JQ1 which was associated with a decrease in efficacy compared to unmodified T cells. These findings reveal the complexity of epigenetic targeting of T cell differentiation, highlighting the need to precisely define the epigenetic targeting strategies to improve CTL generation for ACT.

Published

2019

33. Acquired resistance during adoptive cell therapy by transcriptional silencing of immunogenic antigens

Author

Ana P. Abad, Catherine A. Forbes, Jason Waithman, Shane R. Stone, Jonathan Chee, Anthony Buzzai, Bree Foley, Mark N. Cruickshank, Ben Wylie, and Mitchell Booth

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, medicine.medical_treatment, Immunology, lcsh:RC254-282, Cell therapy, immunoediting, transcriptional silencing, 03 medical and health sciences, 0302 clinical medicine, medicine, Immunology and Allergy, Gene silencing, cancer, Epigenetics, Original Research, Tumor-infiltrating lymphocytes, business.industry, acquired resistance, Cancer, adoptive cell therapy, Immunotherapy, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, epigenetic modifiers, 030104 developmental biology, Oncology, Immunoediting, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, immunotherapy, business, lcsh:RC581-607

Abstract

Immunotherapies such as adoptive cell therapy (ACT) are promising treatments for solid cancers. However, relapsing disease remains a problem and the molecular mechanisms underlying resistance are poorly defined. We postulated that the deregulated epigenetic landscape in cancer cells could underpin the acquisition of resistance to immunotherapy. To address this question, two preclinical models of ACT were employed to study transcriptional and epigenetic regulatory processes within ACT-treated cancer cells. In these models ACT consistently causes robust tumor regression, but resistance develops and tumors relapse. We identified down-regulated expression of immunogenic antigens at the mRNA level correlated with escape from immune control. To determine whether this down-regulation was under epigenetic control, we treated escaped tumor cells with DNA demethylating agents, azacytidine (AZA) and decitabine (DEC). AZA or DEC treatment restored antigen expression in a proportion of the tumor population. To explore the importance of other epigenetic modifications we isolated tumor cells refractory to DNA demethylation and screened clones against a panel of 19 different epigenetic modifying agents (EMAs). The library of EMAs included inhibitors of a range of chromosomal and transcription regulatory protein complexes, however, when tested as single agents none restored further antigen expression. These findings suggest that tumor cells employ multiple epigenetic and genetic mechanisms to evade immune control, and a combinatorial approach employing several EMAs targeting transcription and genome stability may be required to overcome tumor resistance to immunotherapy.

Published

2019

34. CD8+XCR1neg Dendritic Cells Express High Levels of Toll-Like Receptor 5 and a Unique Complement of Endocytic Receptors

Author

James F. Read, Teagan Wagner, Shane R. Stone, Mark N. Cruickshank, Ben Wylie, Niamh M. Troy, Anthony Bosco, Jason Waithman, Bree Foley, Genevieve Syn, and Anthony Buzzai

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, XCR1, CD8 Antigens, T cell, Immunology, Endocytic cycle, immunosurveillance, Cell Separation, Biology, Mice, transcriptomics, 03 medical and health sciences, Chemokine receptor, Cross-Priming, 0302 clinical medicine, medicine, Animals, Immunology and Allergy, dendritic cells, Receptor, TLR5, Original Research, Oligonucleotide Array Sequence Analysis, Toll-like receptor, Gene Expression Profiling, hemic and immune systems, Flow Cytometry, Endocytosis, Cell biology, Mice, Inbred C57BL, Immunosurveillance, Toll-Like Receptor 5, 030104 developmental biology, medicine.anatomical_structure, Receptors, Pattern Recognition, Receptors, Chemokine, lcsh:RC581-607, microarray, CD8, 030215 immunology

Abstract

Conventional dendritic cells (cDC) resident in the lymphoid organs of mice have been classically divided into CD8+ and CD8neg subsets. It is well-established that CD8+ dendritic cells (DCs) and their migratory counterparts in the periphery comprise the cross-presenting cDC1 subset. In contrast, CD8neg DCs are grouped together in the heterogeneous cDC2 subset. CD8neg DCs are relatively poor cross-presenters and drive more prominent CD4+ T cell responses against exogenous antigens. The discovery of the X-C motif chemokine receptor 1 (XCR1) as a specific marker of cross-presenting DCs, has led to the identification of a divergent subset of CD8+ DCs that lacks the ability to cross-present. Here, we report that these poorly characterized CD8+XCR1neg DCs have a gene expression profile that is consistent with both plasmacytoid DCs (pDCs) and cDC2. Our data demonstrate that CD8+XCR1neg DCs possess a unique pattern of endocytic receptors and a restricted toll-like receptor (TLR) profile that is particularly enriched for TLR5, giving them a unique position within the DC immunosurveillance network.

Published

2019

35. Correction to: Tumour draining lymph node-generated CD8 T cells play a role in controlling lung metastases after a primary tumour is removed but not when adjuvant immunotherapy is used

Author

Vanessa S. Fear, Catherine A. Forbes, Samuel A. Neeve, Scott A. Fisher, Jonathan Chee, Jason Waithman, Shao Kang Ma, Richard Lake, Anna K. Nowak, Jenette Creaney, Matthew D. Brown, Christobel Saunders, and Bruce W. S. Robinson

Subjects

Cancer Research, Oncology, Immunology, Immunology and Allergy

Abstract

A correction to this paper has been published: https://doi.org/10.1007/s00262-021-02970-z

Published

2021

36. Timing of excision after a non-severe burn has a significant impact on the subsequent immune response in a murine model

Author

Bree Foley, Fiona M. Wood, Wee Peng Poh, Mark W. Fear, Vanessa S. Fear, Samantha M Valvis, and Jason Waithman

Subjects

0301 basic medicine, Chemokine, Time Factors, Neutrophils, Inflammation, Adaptive Immunity, Critical Care and Intensive Care Medicine, Monocytes, Proinflammatory cytokine, Mice, 03 medical and health sciences, Th2 Cells, 0302 clinical medicine, Immune system, Antigens, CD, medicine, Animals, Lymph node, Cell Proliferation, Innate immune system, biology, business.industry, 030208 emergency & critical care medicine, Dendritic Cells, General Medicine, Eosinophil, Natural killer T cell, Immunity, Innate, Eosinophils, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Immunology, Emergency Medicine, biology.protein, Cytokines, Female, Surgery, Lymph Nodes, Chemokines, medicine.symptom, Burns, business

Abstract

Burn excision has emerged as the dominant clinical paradigm in treatment of deep burns. Surgical intervention is common but the timing of wound excision is a balance between wound depth assessment, avoidance of infection and unnecessary intervention. However the physiological impact of timing of excision and consequences for the immune response are not well understood.Mice were subject to full-thickness burn (8% TBSA) followed by early (day 1) or late (day 8) surgical excision. Draining lymph nodes, wound tissue and sera were collected longitudinally at day 2 and day 6 after excision and analyzed for cytokine, dendritic cell and T cell profiles using FACS and multiplex ELISA assays.Delayed excision after injury initiated acute and severe inflammatory responses, with high levels of inflammatory cytokines, increased chemokine responses, and elevated Th2 promoting cytokines compared to early excision. Cellular inflammation in the wound was exacerbated with elevated neutrophils, eosinophil and monocytes. Wound cellular innate immune response decreased after late excision with a loss of inflammatory dendritic cells (DC), decreased NKT cells, and inhibition of NK cell activation. Systemically late excision increased trafficking conventional CD8α(-) DC to the lymph node, but there was no apparent DC activation. This was reflected in the induction of CD4T regulatory (Treg) cells and suppression of CD8T cell proliferation after late excision. No suppression was observed with early excision.This data suggests early excision of the wound, during the phase of immune down-regulation initiated by the burn, maintains an innate and adaptive immune cell response. In contrast, late wound excision induced a severe inflammatory response, with subsequent down-regulation of innate and adaptive immune cell responses. Therefore timing of excision is critical in affecting the immune response to burn.

Published

2016

37. Skin tumor immunity: Site does matter for antigen presentation by DCs

Author

Sammy Bedoui, Jason Waithman, and Thomas Gebhardt

Subjects

0301 basic medicine, business.industry, Immunology, Antigen presentation, Skin tumor, Cross-presentation, chemical and pharmacologic phenomena, Dendritic Cells, medicine.disease, 03 medical and health sciences, 030104 developmental biology, Immune system, Antigen, Immunity, Neoplasms, medicine, Animals, Immunology and Allergy, Lymph Nodes, Sarcoma, Lymph, business

Abstract

The immune system has the ability to specifically identify and eliminate tumors, but the underlying mechanisms responsible for this phenomenon are not fully understood. A study published in this issue of the European Journal of Immunology now provides new insights into this important problem. Joncker et al. [Eur. J. Immunol. 2016. 46: 609-618] show that the timely mobilization of tumor antigen-bearing dendritic cells (DCs) from the periphery to the lymph nodes is critical for effective antitumor T-cell immunity, and that DCs present tumor antigens much more efficiently when encountered in the skin rather than in the subcutaneous tissues.

Published

2016

38. Recapitulation of human germline coding variation in an ultra-mutated infant leukemia

Author

Parwinder Kaur, Alexander M. Gout, Ursula R. Kees, Catherine H. Cole, Rishi S. Kotecha, Jason Waithman, Charles S. Bond, Kim W. Carter, Mark N. Cruickshank, Bree Foley, and Abad A

Subjects

Genetics, 0303 health sciences, Mutation, POLD1, Point mutation, Somatic hypermutation, Biology, medicine.disease_cause, Germline, 3. Good health, Infant Acute Lymphoblastic Leukemia, 03 medical and health sciences, 0302 clinical medicine, MSH2, 030220 oncology & carcinogenesis, medicine, DNA mismatch repair, 030304 developmental biology

Abstract

BackgroundMixed lineage leukemia/Histone-lysine N-methyltransferase 2Agene rearrangements occur in 80% of infant acute lymphoblastic leukemia, but the role of cooperating events is unknown. While infant leukemias typically carry few somatic lesions, we identified a case with over 100 somatic point mutations per megabase and here report unique genomic-features of this case.ResultsThe patient presented at 82 days of age, one of the earliest manifestations of cancer hypermutation recorded. The transcriptional profile showed global similarities to canonical cases. Coding lesions were predominantly clonal and almost entirely targeting alleles reported in human genetic variation databases with a notable exception in the mismatch repair gene,MSH2. There were no rare germline alleles or somatic mutations affecting proof-reading polymerase genesPOLEorPOLD1, however there was a predicted damaging mutation in the error prone replicative polymerase,POLK. The patient’s diagnostic leukemia transcriptome was depleted of rare and low-frequency germline alleles due to loss-of-heterozygosity, while somatic point mutations targeted low-frequency and common human alleles in proportions that offset this discrepancy. Somatic signatures of ultra-mutations were highly correlated with germline single nucleotide polymorphic sites indicating a common role for 5-methylcytosine deamination, DNA mismatch repair and DNA adducts.ConclusionsThese data suggest similar molecular processes shaping population-scale human genome variation also underlies the rapid evolution of an infant ultra-mutated leukemia.

Published

2018

39. T cells recognizing a 11mer influenza peptide complexed to H‐2D b show promiscuity for peptide length

Author

Damien Zanker, Kylie M. Quinn, Nicole L. La Gruta, Weisan Chen, Roger Murphy, Roleen Lata, and Jason Waithman

Subjects

Immunology, T-Cell Antigen Receptor Specificity, Peptide, Immunodominance, CD8-Positive T-Lymphocytes, Cross Reactions, Major histocompatibility complex, Cancer Vaccines, Epitope, Cell Line, Mice, Viral Proteins, Immune Tolerance, Animals, Humans, Immunology and Allergy, Amino Acid Sequence, Histocompatibility Antigen H-2D, Peptide sequence, Mice, Knockout, chemistry.chemical_classification, biology, T-cell receptor, Cell Biology, Orthomyxoviridae, RNA-Dependent RNA Polymerase, Peptide Fragments, Mice, Inbred C57BL, Cysteine Endopeptidases, chemistry, Biochemistry, biology.protein, CD8, Protein Binding

Abstract

T-cell repertoire is selected according to self peptide-MHC (major histocompatibility complex) complexes in the thymus. Although most peripheral T cells recognize specific pathogen-derived peptides complexed to self-MHC exclusively, some possess cross-reactivity to other self or foreign peptides presented by self-MHC molecules; a phenomenon often termed T-cell receptor (TCR) promiscuity or degeneracy. TCR promiscuity has been attributed to various autoimmune conditions. On the other hand, it is considered a mechanism for a relatively limited TCR repertoire to deal with a potentially much larger antigenic peptide repertoire. Such property has also been utilized to bypass self-tolerance for cancer vaccine development. Although many studies explored such degeneracy for peptide of the same length, few studies reported such properties for peptides of different length. In this study, we finely characterized the CD8(+) T-cell response specific for a 11mer peptide derived from influenza A viral polymerase basic protein 2. The short-term T-cell line, despite possessing highly biased TCR, was able to react with multiple peptides of different length sharing the same core sequence. Out data clearly showed the importance of detailed and quantitative assessments for such T-cell specificity. Our data also emphasize the importance of biochemical demonstration of the naturally presented minimal peptide.

Published

2015

40. IFNβ inhibits the development of allergen tolerance and is conducive to the development of asthma on subsequent allergen exposure

Author

Shelley Gorman, Wee Peng Poh, Jason Waithman, Mark W. Fear, and Vanessa S. Fear

Subjects

0301 basic medicine, Allergy, Ovalbumin, Immunology, Immunoglobulin E, medicine.disease_cause, Atopy, Allergic sensitization, 03 medical and health sciences, Mice, Allergen, medicine, Hypersensitivity, Immune Tolerance, Immunology and Allergy, Eosinophilia, Animals, Humans, Lung, Asthma, Mice, Inbred BALB C, biology, business.industry, Interferon-alpha, Cell Biology, Interferon-beta, respiratory system, Allergens, medicine.disease, respiratory tract diseases, Eosinophils, Disease Models, Animal, 030104 developmental biology, biology.protein, medicine.symptom, business

Abstract

Asthma is a chronic disease affecting up to 10% of the Australian population for which medical treatment is solely aimed at relief of symptoms rather than prevention of disease. Evidence from animal and human studies demonstrates a strong link between viral respiratory infections, atopy and the development of asthma. Type I IFNs include IFNα and IFNβ, with subtype expression tailored toward the specific viral infection. We hypothesized that exposure to type I IFNs and allergen may interfere with the healthy response to innocuous airway antigen exposure. In this study, we use an ovalbumin (OVA)-induced BALB/c model of experimental allergic airways disease, where pre-exposure of the airways to OVA is protective against allergen sensitization, leading to allergen tolerance. We investigated airways pre-exposure with OVA and type I IFNs on development of allergic airways disease. We demonstrate restoration of allergic airways disease on pre-exposure with allergen and IFNβ, and not IFNα. Dysfunction in tolerance led to changes in dendritic cell antigen capture/traffic, T-cell and B-cell responses. Furthermore, exposure to IFNβ with ongoing allergen exposure led to the development of hallmark asthma features, including OVA-specific IgE and airways eosinophilia. Data indicate a role for IFNβ in linking viral infection and allergy.

Published

2017

41. Investigating the link between burn injury and tumorigenesis

Author

Fiona M. Wood, Gretchen Purcell Jackson, L. Barrett, Jason Waithman, V. Willis, N. Kutub, Mark W. Fear, and Vanessa S. Fear

Subjects

Oncology, Body surface area, medicine.medical_specialty, education.field_of_study, Burn injury, business.industry, Melanoma, Population, Cancer, Hematology, medicine.disease, medicine.disease_cause, Primary tumor, Metastasis, Internal medicine, medicine, education, business, Carcinogenesis

Abstract

Background Recent population studies have shown an increase in cancer rates in patients after burn injury over a 30-year follow-up period. This work aims to understand the mediators and mechanisms that lead to cancer susceptibility after acute burn. Methods In silico analytics with Watson for Drug Discovery were performed to interrogate networks and pathways in common between burn injury and cancer to better understand the possible mechanistic links. We then useda murine non-severe burn injury model (injury to ∼ 6% body surface area) with subsequent tumor susceptibility evaluation using B16 melanoma challenge 4 weeks after the burn injury. Primary tumor growth (n = 10) and metastasis (n = 11-13) were assessed compared to sham controls. Results Network analysis highlighted multiple overlapping pathways important in burn repair and in tumors. In particular, the evidence suggested links to pathways important in the immune response to burn injury (including well characterized pro-inflammatory genes such as IL-6 and TNF-α) and matrix remodeling (such as MMP9) to metastasis. In the murine model, at four weeks after burn injury, primary tumor growth was unaffected (mean volume 353.7mm3± 235.4 vs 256.8mm3± 122.6, burn injury and control respectively, p = 0.32). However, mean number of metastases in burn injury mice was significantly increased (7.7± 4.1 compared with 2.6 ± 1.8 for control mice (p = 0.0015)), and there was a trend for increased metastatic tumor volume (mean volume 2.7 ± 1.2 compared with 1.6 ±1.3 cm3 respectively, p = 0.08) after burn injury. Conclusions This work suggests burn injury increases cancer susceptibility, specifically through increased number and size of metastases. Further work to delineate the mechanism, potentially through modulation of in silico-identified immune system and metastasis pathways, may provide potential to improve long-term health outcomes for patients. Legal entity responsible for the study Fiona Woods Institute. Funding IBM Watson Health. Disclosure All authors have declared no conflicts of interest.

Published

2019

42. Dendritic Cells and Cancer: From Biology to Therapeutic Intervention

Author

Ben Wylie, Justine D. Mintern, Christophe Macri, and Jason Waithman

Subjects

0301 basic medicine, Cancer Research, tumor-associated dendritic cells, medicine.medical_treatment, Population, Priming (immunology), Review, Biology, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immunity, novel therapies, medicine, cancer, Antigen-presenting cell, education, Tumor microenvironment, education.field_of_study, immunosuppression, Growth factor, Immunotherapy, DC-based therapy, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immune checkpoint, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, checkpoint blockade, immunotherapy

Abstract

Inducing effective anti-tumor immunity has become a major therapeutic strategy against cancer. Dendritic cells (DC) are a heterogenous population of antigen presenting cells that infiltrate tumors. While DC play a critical role in the priming and maintenance of local immunity, their functions are often diminished, or suppressed, by factors encountered in the tumor microenvironment. Furthermore, DC populations with immunosuppressive activities are also recruited to tumors, limiting T cell infiltration and promoting tumor growth. Anti-cancer therapies can impact the function of tumor-associated DC and/or alter their phenotype. Therefore, the design of effective anti-cancer therapies for clinical translation should consider how best to boost tumor-associated DC function to drive anti-tumor immunity. In this review, we discuss the different subsets of tumor-infiltrating DC and their role in anti-tumor immunity. Moreover, we describe strategies to enhance DC function within tumors and harness these cells for effective tumor immunotherapy.

Published

2019

43. 518 Investigation of the Mechanisms Underpinning Increased Incidence of Cancer after Burn Injury Using Animal Models

Author

L. Barrett, Mark W. Fear, Vanessa S. Fear, Jason Waithman, and Fiona M. Wood

Subjects

Burn injury, Underpinning, medicine.medical_specialty, business.industry, Incidence (epidemiology), Rehabilitation, Emergency Medicine, Medicine, Cancer, Surgery, business, medicine.disease, Intensive care medicine

Published

2019

44. Author Correction: Tissue-resident memory CD8+ T cells promote melanoma–immune equilibrium in skin

Author

Teagan Wagner, Nathan McBain, Anthony Buzzai, Michael Hölzel, James S. Wilmott, Richard A. Scolyer, Scott N. Mueller, David E. Gyorki, Nicholas D. Huntington, Thomas Tüting, Jai Rautela, Robyn McConville, Maike Effern, Sammy Bedoui, Thomas Gebhardt, Jason Waithman, Jyh Liang Hor, Simone L Park, Katharina Hochheiser, Umaimainthan Palendira, Laura K. Mackay, and Jarem Edwards

Subjects

0301 basic medicine, Multidisciplinary, business.industry, Published Erratum, Melanoma, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, Text mining, 030220 oncology & carcinogenesis, Immunology, medicine, Cytotoxic T cell, business, Sentence

Abstract

Panel j was inadvertently labelled as panel k in the caption to Fig. 4. Similarly, 'Fig. 4k' should have been 'Fig. 4j' in the sentence beginning 'TNF-α-deficient gBT-I cells were…'. In addition, the surname of author Umaimainthan Palendira was misspelled 'Palendria'. These errors have been corrected online.

Published

2019

45. Prostaglandin E2 imprints a long-lasting effect on dendritic cell progenitors in the bone marrow

Author

Royce L. X. Ng, Shelley Gorman, Jason Waithman, Naomi M. Scott, Prue H. Hart, and Mary Norval

Subjects

Lipopolysaccharides, Time Factors, Myeloid, Neutrophils, Administration, Topical, Immunology, Bone Marrow Cells, Inflammation, Biology, Dinoprostone, Mice, Peritoneal cavity, chemistry.chemical_compound, Immune system, Hypersensitivity, medicine, Animals, Immunology and Allergy, Progenitor cell, Fluorescein isothiocyanate, Administration, Intranasal, Bone Marrow Transplantation, Chimera, Macrophages, Stem Cells, Immunity, Cell Differentiation, Dendritic Cells, Cell Biology, Dendritic cell, medicine.anatomical_structure, chemistry, Gamma Rays, Female, lipids (amino acids, peptides, and proteins), Lymph Nodes, Bone marrow, medicine.symptom, Fluorescein-5-isothiocyanate

Abstract

Dendritic cells (DCs) that differentiate in vitro from the bone marrow (BM) of mice with prostaglandin E2 (PGE2)-associated inflammation of the skin, airways, or peritoneal cavity poorly initiate immune responses. To remove in vitro differentiation and allow BM-derived DCs to seed the periphery under steady-state conditions, as well as study the molecule proposed responsible, chimeric mice were engrafted for >16 wk with BM cells from mice exposed to PGE2. Serial PGE2-chimeric mice were established with BM cells from the primary chimeric mice. Immune responses in the airways and skin of the PGE2-chimeric mice and serial PGE2-chimeric mice were significantly attenuated. After inflammatory challenges by intranasal LPS, topical fluorescein isothiocyanate, and intraperitoneal alum, DCs, macrophages, and neutrophils trafficked poorly in PGE2-chimeric mice and serial PGE2-chimeric mice. Injection of BM-differentiated DCs from nonchimeric mice restored the reduced immune responses of PGE2-chimeric mice. DCs from BM of 16-wk-engrafted PGE2-chimeric and serial PGE2-chimeric mice resembled cells differentiated from BM exposed to PGE2 for only 3 d, demonstrating the long-lasting effect of PGE2 on DC progenitors. PGE2 attenuates systemic immune responses by modulating myeloid cell progenitors in the BM such that BM-derived, terminally differentiated myeloid cells have poor trafficking ability to sites of need.

Published

2013

46. Altered Immunity and Dendritic Cell Activity in the Periphery of Mice after Long-Term Engraftment with Bone Marrow from Ultraviolet-Irradiated Mice

Author

Michele A. Grimbaldeston, Jason Waithman, Shelley Gorman, Mary Norval, Royce L. X. Ng, Naomi M. Scott, Deborah H. Strickland, Prue H. Hart, Ng, Royce LX, Scott, Naomi M, Strickland, Deborah H, Gorman, Shelley, Grimbaldeston, Michele A, Norval, Mary, Waithman, Jason, and Hart, Prue H

Subjects

Adoptive cell transfer, adoptive transfer, bone marrow transplantation, Immunology, ultraviolet rays, Biology, Immune system, cell movement, lymph nodes, Immunity, medicine, Immunology and Allergy, dendritic cells, Progenitor cell, bone marrow cells, dermatitis, membrane proteins a T-lymphocytes, Dendritic cell, immunity, cell differentiation, Haematopoiesis, Granulocyte macrophage colony-stimulating factor, medicine.anatomical_structure, chimerism, Bone marrow, interleukin-4, hypertrophy, medicine.drug

Abstract

Alterations to dendritic cell (DC) progenitors in the bone marrow (BM) may contribute to long-lasting systemic immunosuppression (>28 d) following exposure of the skin of mice to erythemal UV radiation (UVR). DCs differentiated in vitro from the BM of mice 3 d after UVR (8 kJ/m2) have a reduced capacity to initiate immunity (both skin and airways) when adoptively transferred into naive mice. Studies in IL-10−/− mice suggested that UV-induced IL-10 was not significantly involved. To investigate the immune capabilities of peripheral tissue DCs generated in vivo from the BM of UV-irradiated mice, chimeric mice were established. Sixteen weeks after reconstitution, contact hypersensitivity responses were significantly reduced in mice reconstituted with BM from UV-irradiated mice (UV-chimeric). When the dorsal skin of UV-chimeric mice was challenged with innate inflammatory agents, the hypertrophy induced in the draining lymph nodes was minimal and significantly less than that measured in control-chimeric mice challenged with the same inflammatory agent. When DCs were differentiated from the BM of UV-chimeric mice using FLT3 ligand or GM-CSF + IL-4, the cells maintained a reduced priming ability. The diminished responses in UV-chimeric mice were not due to different numerical or proportional reconstitution of BM or the hematopoietic cells in blood, lymph nodes, and skin. Erythemal UVR may imprint a long-lasting epigenetic effect on DC progenitors in the BM and alter the function of their terminally differentiated progeny.

Published

2013

47. Dietary Vitamin D Increases Percentages and Function of Regulatory T Cells in the Skin-Draining Lymph Nodes and Suppresses Dermal Inflammation

Author

Melinda A. Judge, Prue H. Hart, Sian Geldenhuys, Jason Waithman, Shelley Gorman, and Clare E. Weeden

Subjects

0301 basic medicine, Vitamin, lcsh:Immunologic diseases. Allergy, Article Subject, Immunology, Inflammation, Spleen, chemical and pharmacologic phenomena, Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Immunology and Allergy, Mesenteric lymph nodes, CCR10, IL-2 receptor, integumentary system, FOXP3, hemic and immune systems, General Medicine, 030104 developmental biology, medicine.anatomical_structure, chemistry, Lymph, medicine.symptom, lcsh:RC581-607, 030215 immunology, Research Article

Abstract

Skin inflammatory responses in individuals with allergic dermatitis may be suppressed by dietary vitamin D through induction and upregulation of the suppressive activity of regulatory T (TReg) cells. Vitamin D may also promoteTRegcell tropism to dermal sites. In the current study, we examined the capacity of dietary vitamin D3to modulate skin inflammation and the numbers and activity ofTRegcells in skin and other sites including lungs, spleen, and blood. In female BALB/c mice, dietary vitamin D3suppressed the effector phase of a biphasic ear swelling response induced by dinitrofluorobenzene in comparison vitamin D3-deficient female BALB/c mice. Vitamin D3increased the percentage ofTReg(CD3+CD4+CD25+Foxp3+) cells in the skin-draining lymph nodes (SDLN). The suppressive activity ofTRegcells in the SDLN, mesenteric lymph nodes, spleen, and blood was upregulated by vitamin D3. However, there was no difference in the expression of the naturally occurringTRegcell marker, neuropilin, nor the expression of CCR4 or CCR10 (skin-tropic chemokine receptors) onTRegcells in skin, SDLN, lungs, and airway-draining lymph nodes. These data suggest that dietary vitamin D3increased the percentages and suppressive activity ofTRegcells in the SDLN, which are poised to suppress dermal inflammation.

Published

2016

48. NLRC4 inflammasomes in dendritic cells regulate noncognate effector function by memory CD8+ T cells

Author

Thomas Gebhardt, Sammy Bedoui, Hanwei Cao, Richard A. Strugnell, William R. Heath, Kirsty R. Short, Leif E. Sander, Odilia L. C. Wijburg, Jason Waithman, Greta Guarda, Weisan Chen, Andreas Kupz, Daniel Fernandez-Ruiz, Paul G. Whitney, Jürg Tschopp, Dimitri A. Diavatopoulos, and Roy Curtiss

Subjects

Salmonella typhimurium, Inflammasomes, Interleukin-1beta, Immunology, Yersinia pseudotuberculosis Infections, Priming (immunology), CD8-Positive T-Lymphocytes, Biology, Microbiology, Genomic disorders and inherited multi-system disorders Auto-immunity, transplantation and immunotherapy [IGMD 3], Interferon-gamma, Mice, Interferon, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Pseudomonas Infections, IL-2 receptor, Salmonella Infections, Animal, Effector, Calcium-Binding Proteins, Toll-Like Receptors, Interleukin-18, Pathogenesis and modulation of inflammation Infection and autoimmunity [N4i 1], Inflammasome, Dendritic Cells, medicine.anatomical_structure, Pseudomonas aeruginosa, Apoptosis Regulatory Proteins, Immunologic Memory, Memory T cell, Spleen, CD8, Flagellin, Signal Transduction, medicine.drug

Abstract

Item does not contain fulltext Memory T cells exert antigen-independent effector functions, but how these responses are regulated is unclear. We discovered an in vivo link between flagellin-induced NLRC4 inflammasome activation in splenic dendritic cells (DCs) and host protective interferon-gamma (IFN-gamma) secretion by noncognate memory CD8(+) T cells, which could be activated by Salmonella enterica serovar Typhimurium, Yersinia pseudotuberculosis and Pseudomonas aeruginosa. We show that CD8alpha(+) DCs were particularly efficient at sensing bacterial flagellin through NLRC4 inflammasomes. Although this activation released interleukin 18 (IL-18) and IL-1beta, only IL-18 was required for IFN-gamma production by memory CD8(+) T cells. Conversely, only the release of IL-1beta, but not IL-18, depended on priming signals mediated by Toll-like receptors. These findings provide a comprehensive mechanistic framework for the regulation of noncognate memory T cell responses during bacterial immunity. 01 februari 2012

Published

2012

49. Dendritic cells and influenza A virus infection

Author

Jason Waithman and Justine D. Mintern

Subjects

Microbiology (medical), Virulence Factors, Immunology, Antigen presentation, Review, Biology, medicine.disease_cause, Microbiology, Virus, Immune system, Orthomyxoviridae Infections, Pandemic, Influenza, Human, Influenza A virus, medicine, Cytotoxic T cell, Animals, Humans, Dendritic Cells, Virology, Vaccination, antigen presentation, Disease Models, Animal, Infectious Diseases, Immunization, Host-Pathogen Interactions, Parasitology

Abstract

Influenza A virus (IAV) is a dangerous virus equipped with the potential to evoke widespread pandemic disease. The 2009 H1N1 pandemic highlights the urgency for developing effective therapeutics against IAV infection. Vaccination is a major weapon to combat IAV and efforts to improve current regimes are critically important. Here, we will review the role of dendritic cells (DCs), a pivotal cell type in the initiation of robust IAV immunity. The complexity of DC subset heterogeneity in the respiratory tract and lymph node that drains the IAV infected lung will be discussed, together with the varied and in some cases, conflicting contributions of individual DC populations to presenting IAV associated antigen to T cells.

Published

2012

50. Differential Regulation of Simultaneous Antitumor and Alloreactive CD8+ T-Cell Responses in the Same Host by Rapamycin

Author

Adil N. Shivji, Damien Zanker, S. M. M. Haeryfar, Maryam Atef Yekta, M. J. Harding, Todd D. Schell, S. Maleki Vareki, Jason Waithman, Weisan Chen, Mateusz Rytelewski, and Delfina M. Mazzuca

Subjects

Sirolimus, Transplantation, CD8-Positive T-Lymphocytes, Biology, Article, Epitope, Virus, Mice, Inbred C57BL, Mice, Antigen, Immunology, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Female, Pharmacology (medical), PI3K/AKT/mTOR pathway, CD8, medicine.drug, Minigene

Abstract

Rapamycin is an immunosuppressive agent routinely used in organ transplantation but also paradoxically exerts antiviral and antitumor activities. Pathogen-specific memory CD8(+) T-cell (T(CD8) ) responses were recently found to be augmented by rapamycin. However, whether rapamycin influences the magnitude and quality of anticancer T(CD8) responses is unknown. Importantly, how rapamycin may regulate simultaneous virus/tumor-specific and alloreactive T(CD8) in the same host remains unexplored. To answer these questions, we primed wild-type mice with allogeneic cells concomitantly expressing simian virus 40 large tumor antigen (T Ag), a viral oncoprotein with well-defined epitopes. Rapamycin selectively enhanced the cross-priming of T(CD8) specific for T Ag's most immunodominant epitope called site IV but not T(CD8) alloreactivity. Rapamycin-treated mice also had a high percentage of splenic CD127(high) KLRG1(low) T(CD8) and an increased frequency of site IV-specific T cells long after the peak of their primary response. When site IV was presented as a cytosolic minigene encoded by a recombinant vaccinia virus, rapamycin failed to boost the site IV-specific response. Therefore, the nature and presentation mode of antigen determine the susceptibility to the adjuvant effect of rapamycin. Our findings reveal the unexpected benefit of rapamycin treatment in recipients of allografts co-expressing tumor/viral Ags.

Published

2012