Your search keyword '"Lee, Peter A"' showing total 44 results

1. Immune overdrive signature in colorectal tumor subset predicts poor clinical outcome

Author

Fakih, Marwan, Ouyang, Ching, Wang, Chongkai, Tu, Travis Yiwey, Gozo, Maricel C., Cho, May, Sy, Marvin, Longmate, Jeffrey A., and Lee, Peter P.

Subjects

United States. National Cancer Institute, Genetic aspects, Prognosis, Patient outcomes, Cancer genetics -- Genetic aspects -- Prognosis -- Patient outcomes, Genes, Immunohistochemistry, Medical research, Tumors -- Genetic aspects -- Prognosis -- Patient outcomes, Colorectal cancer -- Genetic aspects -- Prognosis -- Patient outcomes, Genomes, Gastrointestinal diseases -- Genetic aspects -- Prognosis -- Patient outcomes, Immune response, Gene expression, Genomics, T cells, Transforming growth factors, Biochemistry, Recurrence (Disease), Phenotypes, Macrophages, Bone morphogenetic proteins

Abstract

Introduction Since the seminal report on association between infiltrating cytotoxic and memory T cells with decreased lymphatic invasion and improved patient outcome in colorectal cancer (CRC) (1), the prognostic value [...], The prognostic value of immune cell infiltration within the tumor microenvironment (TME) has been extensively investigated via histological and genomic approaches. Based on the positive prognostic value of T cell infiltration, Immunoscore has been developed and validated for predicting risk of recurrence for colorectal cancer (CRC). Also, association between a consensus T helper 1 (Th-1) immune response and favorable clinical outcomes has been observed across multiple cancer types. Here, we reanalyzed public genomic data sets from The Cancer Genome Atlas (TCGA) and NCBI Gene Expression Omnibus (NCBI-GEO) and performed multispectral immunohistochemistry (IHC) on a cohort of colorectal tumors. We identified and characterized a risk group, representing approximately 10% of CRC patients, with high intratumoral [CD8.sup.+] T cell infiltration, but poor prognosis. These tumors included both microsatellite instable (MSI) and stable (MSS) phenotypes and had a high density of tumor-associated macrophages (TAMs) that expressed CD274 (programmed death-ligand 1 [PD-L1]), TGF-[beta] activation, and an immune overdrive signature characterized by the overexpression of immune response and checkpoint genes. Our findings illustrate that CRC patients may have poor prognosis despite high [CD8.sup.+] T cell infiltration and provide CD274 as a simple biomarker for identifying these patients.

Published

2019

2. Mature Dendritic Cells May Promote High-Avidity Tuning of Vaccine T Cell Responses.

Author

Kumbhari, Adarsh, Egelston, Colt A., Lee, Peter P., and Kim, Peter S.

Subjects

DENDRITIC cells, CYTOTOXIC T cells, T cells, VACCINES

Abstract

Therapeutic vaccines can elicit tumor-specific cytotoxic T lymphocytes (CTLs), but durable reductions in tumor burden require vaccines that stimulate high-avidity CTLs. Recent advances in immunotherapy responses have led to renewed interest in vaccine approaches, including dendritic cell vaccine strategies. However, dendritic cell requirements for vaccines that generate potent anti-tumor T-cell responses are unclear. Here we use mathematical modeling to show that, counterintuitively, increasing levels of immature dendritic cells may lead to selective expansion of high-avidity CTLs. This finding is in contrast with traditional dendritic cell vaccine approaches that have sought to harness ex vivo generated mature dendritic cells. We show that the injection of vaccine antigens in the context of increased numbers of immature dendritic cells results in a decreased overall peptide:MHC complex load that favors high-avidity CTL activation and expansion. Overall, our results provide a firm basis for further development of this approach, both alone and in combination with other immunotherapies such as checkpoint blockade. [ABSTRACT FROM AUTHOR]

Published

2020

3. Predicting Relapse in Patients With Triple Negative Breast Cancer (TNBC) Using a Deep-Learning Approach.

Author

Yu, Guangyuan, Li, Xuefei, He, Ting-Fang, Gruosso, Tina, Zuo, Dongmei, Souleimanova, Margarita, Ramos, Valentina Muñoz, Omeroglu, Atilla, Meterissian, Sarkis, Guiot, Marie-Christine, Yang, Li, Yuan, Yuan, Park, Morag, Lee, Peter P., and Levine, Herbert

Subjects

TRIPLE-negative breast cancer, T cells

Abstract

The abundance and/or location of tumor infiltrating lymphocytes (TILs), especially CD8+ T cells, in solid tumors can serve as a prognostic indicator in various types of cancer. However, it is often difficult to select an appropriate threshold value in order to stratify patients into well-defined risk groups. It is also important to select appropriate tumor regions to quantify the abundance of TILs. On the other hand, machine-learning approaches can stratify patients in an unbiased and automatic fashion. Based on immunofluorescence (IF) images of CD8+ T lymphocytes and cancer cells, we develop a machine-learning approach which can predict the risk of relapse for patients with Triple Negative Breast Cancer (TNBC). Tumor-section images from 9 patients with poor outcome and 15 patients with good outcome were used as a training set. Tumor-section images of 29 patients in an independent cohort were used to test the predictive power of our algorithm. In the test cohort, 6 (out of 29) patients who belong to the poor-outcome group were all correctly identified by our algorithm; for the 23 (out of 29) patients who belong to the good-outcome group, 17 were correctly predicted with some evidence that improvement is possible if other measures, such as the grade of tumors, are factored in. Our approach does not involve arbitrarily defined metrics and can be applied to other types of cancer in which the abundance/location of CD8+ T lymphocytes/other types of cells is an indicator of prognosis. [ABSTRACT FROM AUTHOR]

Published

2020

4. Occupancy and Fractal Dimension Analyses of the Spatial Distribution of Cytotoxic (CD8+) T Cells Infiltrating the Tumor Microenvironment in Triple Negative Breast Cancer.

Author

Wortman, Juliana C., He, Ting-Fang, Rosario, Anthony, Wang, Roger, Schmolze, Daniel, Yuan, Yuan, Yost, Susan E., Li, Xuefei, Levine, Herbert, Atwal, Gurinder, Lee, Peter, and Yu, Clare C.

Subjects

TRIPLE-negative breast cancer, FRACTAL dimensions, FRACTAL analysis, TUMOR microenvironment, T cells, CYTOTOXIC T cells, CANCER relapse

Abstract

Favorable outcomes have been associated with high densities of tumor infiltrating lymphocytes (TILs) such as cytotoxic ( CD8 + ) T cells. However, the clinical significance of the spatial distribution of TILs is less well understood. We have developed novel statistical techniques to characterize the spatial distribution of TILs at various length scales. These include a box counting method that we call "occupancy" and novel applications of fractal dimensions. We apply these techniques to the spatial distribution of CD8 + T cells in the tumor microenvironment of tissue resected from 35 triple negative breast cancer patients. We find that there is a distinct difference in the spatial distribution of CD8 + T cells between good clinical outcome (no recurrence within at least 5 years of diagnosis) and poor clinical outcome (recurrence within 3 years of diagnosis). The statistical significance of the difference between good and poor outcome in the occupancy, fractal dimension (FD), and FD difference of CD8 + T cells is comparable to that of the CD8 + T cell density. Even when we randomly exclude some of the cells so that the images have the same cell density, we still find that the fractal dimension at short length scales is correlated with cancer recurrence, implying that the actual spatial distribution of CD8 + cells, and not just the CD8 + cell density, is associated with clinical outcome. The occupancy and FD difference indicate that the CD8 + T cells are more spatially dispersed in good outcome and more aggregated in poor outcome. We discuss possible interpretations. [ABSTRACT FROM AUTHOR]

Published

2020

5. Escherichia coli adhesion portion FimH functions as an adjuvant for cancer immunotherapy.

Author

Zhang, Wei, Xu, Li, Park, Hae-Bin, Hwang, Juyoung, Kwak, Minseok, Lee, Peter C. W., Liang, Guang, Zhang, Xiaoyan, Xu, Jianqing, and Jin, Jun-O

Subjects

DENDRITIC cells, ESCHERICHIA coli, IMMUNOTHERAPY, ADHESION, TOLL-like receptors, ANIMAL models in research, CYTOTOXIC T cells, T cells

Abstract

Induction of antigen-specific immune activation by the maturation of dendritic cells (DCs) is a strategy used for cancer immunotherapy. In this study, we find that FimH, which is an Escherichia coli adhesion portion, induces toll-like receptor 4-dependent and myeloid differentiation protein 2-independent DC maturation in mice in vivo. A combined treatment regimen with FimH and antigen promotes antigen-specific immune activation, including proliferation of T cells, production of IFN-γ and TNF-α, and infiltration of effector T cells into tumors, which consequently inhibits tumor growth in mice in vivo against melanoma and carcinoma. In addition, combined therapeutic treatment of anti-PD-L1 antibodies and FimH treatment efficiently inhibits CT26 tumor growth in BALB/c mice. Finally, FimH promotes human peripheral blood DC activation and syngeneic T-cell proliferation and activation. Taken together, these findings demonstrate that FimH can be a useful adjuvant for cancer immunotherapy. TLR4 agonists have been proposed as immunotherapeutics in cancer. Here, the authors show the TLR4-dependent adjuvant effect of FimH, an E. coli adhesin, in promoting dendritic cell mediated-T cell activation and response to immune checkpoint blockade in preclinical cancer models. [ABSTRACT FROM AUTHOR]

Published

2020

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

Author

Munson, Daniel J., Egelston, Colt A., Chiotti, Kami E., Parra, Zuly E., Bruno, Tullia C., Moore, Brandon L., Nakano, Taizo A., Simons, Diana L., Jimenez, Grecia, Yim, John H., Rozanov, Dmitri V., Falta, Michael T., Fontenot, Andrew P., Reynolds, Paul R., Leach, Sonia M., Borges, Virginia F., Kappler, John W., Spellman, Paul T., Lee, Peter P., and Slansky, Jill E.

Subjects

BREAST cancer research, T cell receptors, T cells, REVERSE transcriptase polymerase chain reaction, CANCER immunotherapy, PHYSIOLOGY

Abstract

Infiltration of T cells in breast tumors correlateswith improved survival of patients with breast cancer, despite relatively few mutations in these tumors. To determine if T-cell specificity can be harnessed to augment immunotherapies of breast cancer, we sought to identify the alpha-beta paired T-cell receptors (TCRs) of tumor-infiltrating lymphocytes shared between multiple patients. Because TCRs function as heterodimeric proteins, we used an emulsion-based RT-PCR assay to link and amplify TCR pairs. Using this assay on engineered T-cell hybridomas, we observed ~85% accurate pairing fidelity, although TCR recovery frequency varied. When we applied this technique to patient samples, we found that for any given TCR pair, the dominant alpha- or beta-binding partner comprised ~90% of the total binding partners. Analysis of TCR sequences from primary tumors showed about fourfold more overlap in tumor-involved relative to tumor-free sentinel lymph nodes. Additionally, comparison of sequences from both tumors of a patient with bilateral breast cancer showed 10% overlap. Finally, we identified a panel of unique TCRs shared between patients' tumors and peripheral blood that were not found in the peripheral blood of controls. These TCRs encoded a range of V, J, and complementarity determining region 3 (CDR3) sequences on the alpha-chain, and displayed restricted V-beta use. The nucleotides encoding these shared TCR CDR3s varied, suggesting immune selection of this response. Harnessing these T cells may provide practical strategies to improve the shared antigen-specific response to breast cancer. [ABSTRACT FROM AUTHOR]

Published

2016

7. A Theory of Immunodominance and Adaptive Regulation.

Author

Kim, Peter, Lee, Peter, and Levy, Doron

Subjects

*T cells, *EPITOPES, *IMMUNE response, *ANTIGEN presenting cells, *MAJOR histocompatibility complex, *COMPETITION (Biology), *BIOLOGICAL adaptation, *DELAY differential equations

Abstract

Immunodominance refers to the phenomenon in which simultaneous T cell responses against multiple target epitopes organize themselves into distinct and reproducible hierarchies. In many cases, eliminating the response to the most dominant epitope allows responses to subdominant epitopes to expand more fully. The mechanism that drives immunodominance is still not well understood, although various hypotheses have been proposed. One of the more prevalent views is that immunodominance is driven by passive T cell competition for space on antigen presenting cells (APCs) or for access to specific MHC:epitope complexes on the surface of APCs. However, several experimental studies suggest that passive competition alone may not fully explain the robustness of immunodominance under physiological conditions or varying proportions of antigen-specific precursor T cells and APCs. These studies propose that a mechanism of active suppression among T cells gives rise to immunodominance. In this work, we present the novel hypothesis that mutual suppression of simultaneous T cell responses results from the appearance of adaptive regulatory T cells (iTregs) during the course of the overall T cell expansion. We extend the mathematical model of T cell expansion proposed in Kim et al. (Bull. Math. Biol. , doi:) to consider multiple, concurrent T cell responses. The model is formulated as a system of independent feedback loops, in which antigen-specific T cell population produces a nonspecific feedback response. Our simulations show that the fastest response to expand gives rise to a de novo generated population of iTregs that induces a premature contraction in slower or weaker T cell responses, leading to a hierarchical expansion as observed in immunodominance. Furthermore, in some cases, removing the dominant T cell response allows previously subdominant responses to develop more fully. [ABSTRACT FROM AUTHOR]

Published

2011

8. T cell state transition produces an emergent change detector

Author

Kim, Peter S. and Lee, Peter P.

Subjects

*T cells, *ANTIGENS, *DETECTORS, *CELL populations, *DIFFERENTIAL equations, *DYNAMICS

Abstract

Abstract: We model the stages of a T cell response from initial activation to T cell expansion and contraction using a system of ordinary differential equations. Results of this modeling suggest that state transitions enable the T cell population to detect change and respond effectively to changes in antigen stimulation levels, rather than simply the presence or absence of antigen. A key component of the system that gives rise to this emergent change detector is initial activation of naïve T cells. The activation step creates a barrier that separates the long-term, slow dynamics of naïve T cells from the short-term, fast dynamics of effector T cells. This separation allows the T cell population to compare current, up-to-date changes in antigen levels to long-term, steady state levels. As a result, the T cell population responds very effectively to sudden shifts in antigen levels, even if the antigen were already present prior to the change. This feature provides a mechanism for T cells to react to rapidly expanding sources of antigen stimulation, such as viruses, while maintaining tolerance to constant or slowly fluctuating sources of stimulation, such as healthy tissue during growth. In addition to modeling T cell activation, we also formulate a model of the proliferation of effector T cells in response to the consumption of positive growth signal, secreted throughout the T cell response. We discuss how the interaction between T cells and growth signal generates an emergent threshold detector that responds preferentially to large changes in antigen stimulation while ignoring small ones. As a final step, we discuss how the de novo generation of adaptive regulatory T cells during the latter phase of the T cell response creates a negative feedback loop that controls the duration and magnitude of the T cell response. Hence, the immune network continually adjusts to a shifting baseline of (self and non-self) antigens, and responds primarily to abrupt changes in these antigens rather than merely their presence or absence. [Copyright &y& Elsevier]

Published

2011

9. Quantitative, Architectural Analysis of Immune Cell Subsets in Tumor-Draining Lymph Nodes from Breast Cancer Patients and Healthy Lymph Nodes.

Author

Setiadi, A. Francesca, Ray, Nelson C., Kohrt, Holbrook E., Kapelner, Adam, Carcamo-Cavazos, Valeria, Levic, Edina B., Yadegarynia, Sina, van der Loos, Chris M., Schwartz, Erich J., Holmes, Susan, and Lee, Peter P.

Subjects

BREAST cancer, LYMPH nodes, IMAGE analysis, QUANTITATIVE research, SPATIAL analysis (Statistics), B cells, T cells, HISTOLOGY, IMMUNITY, TUMORS

Abstract

Background: To date, pathological examination of specimens remains largely qualitative. Quantitative measures of tissue spatial features are generally not captured. To gain additional mechanistic and prognostic insights, a need for quantitative architectural analysis arises in studying immune cell-cancer interactions within the tumor microenvironment and tumordraining lymph nodes (TDLNs). Methodology/Principal Findings: We present a novel, quantitative image analysis approach incorporating 1) multi-color tissue staining, 2) high-resolution, automated whole-section imaging, 3) custom image analysis software that identifies cell types and locations, and 4) spatial statistical analysis. As a proof of concept, we applied this approach to study the architectural patterns of T and B cells within tumor-draining lymph nodes from breast cancer patients versus healthy lymph nodes. We found that the spatial grouping patterns of T and B cells differed between healthy and breast cancer lymph nodes, and this could be attributed to the lack of B cell localization in the extrafollicular region of the TDLNs. Conclusions/Significance: Our integrative approach has made quantitative analysis of complex visual data possible. Our results highlight spatial alterations of immune cells within lymph nodes from breast cancer patients as an independent variable from numerical changes. This opens up new areas of investigations in research and medicine. Future application of this approach will lead to a better understanding of immune changes in the tumor microenvironment and TDLNs, and how they affect clinical outcomes. [ABSTRACT FROM AUTHOR]

Published

2010

10. Emergent Group Dynamics Governed by Regulatory Cells Produce a Robust Primary T Cell Response.

Author

Kim, Peter, Lee, Peter, and Levy, Doron

Subjects

*T cells, *ANTIGENS, *MATHEMATICAL models, *IMMUNE response, *LYMPHOCYTES

Abstract

The currently accepted paradigm for the primary T cell response is that effector T cells commit to autonomous developmental programs. This concept is based on several experiments that have demonstrated that the dynamics of a T cell response is largely determined shortly after antigen exposure and that T cell dynamics do not depend on the level and duration of antigen stimulation. Another experimental study has also shown that T cell responses are robust to variations in antigen-specific precursor frequency. Various mathematical models have corroborated the first result that programmed T cell responses are insensitive to the level of antigen stimulation. However, this paper proposes that programmed responses do not entirely explain the robustness of T cell dynamics to variations in precursor frequency. This work studies the hypothesis that the dynamics of a T cell response may also be governed by a feedback loop involving adaptive regulatory cells rather than by intrinsic developmental programs. We formulate two mathematical models based on T cell developmental programs. In one model, effector cells undergo a fixed number of divisions before dying. In the second model, effector cells live for a fixed time during which they may divide. The study of these models suggests that developmental programs are not sufficiently robust as they produce an immune response that directly scales with precursor frequencies. Consequently, we derive a third model based on the principle that adaptive regulatory T cells develop in the course of an immune response and suppress effector cells. Our simulations show that this feedback mechanism responds robustly over a range of at least four orders of magnitude of precursor frequencies. We conclude that the proliferation program paradigm does not entirely capture the observed robustness of T cell responses to variations in precursor frequency. We propose an alternative mechanism by which the primary T cell response is governed by an emergent group dynamic and not by individual T cell programs. [ABSTRACT FROM AUTHOR]

Published

2010

11. Impaired interferon signaling is a common immune defect in human cancer.

Author

Critchley-Thorne, Rebecca J., Simons, Diana L., Ning Yan, Miyahira, Andrea K., Dirbas, Frederick M., Johnson, Denise L., Swetter, Susan M., Carlson, Robert W., Fisher, George A., Koong, Albert, Holmes, Susan, and Lee, Peter P.

Subjects

CANCER, INTERFERONS, CANCER invasiveness, LYMPHOCYTES, T cells, B cells

Abstract

Immune dysfunction develops in patients with many cancer types and may contribute to tumor progression and failure of immunotherapy. Mechanisms underlying cancer-associated immune dysfunction are not fully understood. Efficient IFN signaling is critical to lymphocyte function; animals rendered deficient in IFN signaling develop cancer at higher rates. We hypothesized that altered IFN signaling may be a key mechanism of immune dysfunction common to cancer. To address this, we assessed the functional responses to IFN in peripheral blood lymphocytes from patients with 3 major cancers: breast cancer, melanoma, and gastrointestinal cancer. Type-I IFN (IFN-α)-induced signaling was reduced in T cells and B cells from all 3 cancer-patient groups compared to healthy controls. Type-II IFN (IFN-γ)-induced signaling was reduced in B cells from all 3 cancer patient groups, but not in T cells or natural killer cells. Impaired-IFN signaling was equally evident in stage II, Ill, and IV breast cancer patients, and downstream functional defects in T cell activation were identified. Taken together, these findings indicate that defects in lymphocyte IFN signaling arise in patients with breast cancer, melanoma, and gastrointestinal cancer. and these defects may represent a common cancer-associated mechanism of immune dysfunction. [ABSTRACT FROM AUTHOR]

Published

2009

12. Comparison of the local immune response against Giardia lamblia cyst wall protein 2 induced by recombinant Lactococcus lactis and Streptococcus gordonii

Author

Lee, Peter, Abdul-Wahid, Aws, and Faubert, Gaétan M.

Subjects

*IMMUNE response, *LACTOCOCCUS lactis, *GIARDIA lamblia, *ANTIGENS, *IMMUNOGLOBULIN A, *MEMBRANE proteins, *CYTOKINES, *T cells, *B cells, *LABORATORY mice

Abstract

Abstract: Lactococcus lactis and Streptococcus gordonii are lactic acid bacteria (LAB) currently being advocated for use as live antigen delivery vehicles to mucosal sites. Since both vehicles differ in their capability to persist within the small intestine and in their mode of antigen delivery, we sought to compare them to determine which one was superior. In this study, we compared the efficacy of recombinant L. lactis and S. gordonii to stimulate intestinal immune responses against Giardia lamblia cyst wall protein-2 in BALB/c mice. Oral administration of either vector significantly increased the number of CD4+ T helper and B-cells in the mesenteric lymph nodes (MLN) and Peyer''s patches (PP) of immunized animals. Delivery of recombinant CWP2 (rCWP2) by L. lactis stimulated a balanced IFN-γ/IL-4 response (MLN and PP cells) and a CWP2-specific intestinal IgA antibody response. Alternatively, delivery of rCWP2 by S. gordonii stimulated a higher frequency of IFN-γ secreting MLN and PP cells, as well as doubling the amount of CWP2-specific intestinal IgA. In challenge studies, L. lactis and S. gordonii reduced cyst output by 71 and 90%, respectively. When compared to each other, S. gordonii-immunized animals shed 65% fewer cysts than their L. lactis-immunized counterparts. Based on these findings, we concluded that S. gordonii was superior to L. lactis as an intestinal vaccine delivery vehicle. [Copyright &y& Elsevier]

Published

2009

13. Dynamics and Potential Impact of the Immune Response to Chronic Myelogenous Leukemia.

Author

Kim, Peter S., Lee, Peter P., and Levy, Doron

Subjects

*CHRONIC myeloid leukemia, *IMMUNE response, *IMMUNOLOGY, *T cells, *CELL proliferation, *FUNCTIONAL differential equations

Abstract

Recent mathematical models have been developed to study the dynamics of chronic myelogenous leukemia (CML) under imatinib treatment. None of these models incorporates the anti-leukemia immune response. Recent experimental data show that imatinib treatment may promote the development of anti-leukemia immune responses as patients enter remission. Using these experimental data we develop a mathematical model to gain insights into the dynamics and potential impact of the resulting anti-leukemia immune response on CML. We model the immune response using a system of delay differential equations, where the delay term accounts for the duration of cell division. The mathematical model suggests that anti-leukemia T cell responses may play a critical role in maintaining CML patients in remission under imatinib therapy. Furthermore, it proposes a novel concept of an ''optimal load zone'' for leukemic cells in which the anti-leukemia immune response is most effective. Imatinib therapy may drive leukemic cell populations to enter and fall below this optimal load zone too rapidly to sustain the anti-leukemia T cell response. As a potential therapeutic strategy, the model shows that vaccination approaches in combination with imatinib therapy may optimally sustain the anti-leukemia T cell response to potentially eradicate residual leukemic cells for a durable cure of CML. The approach presented in this paper accounts for the role of the anti-leukemia specific immune response in the dynamics of CML. By combining experimental data and mathematical models, we demonstrate that persistence of anti-leukemia T cells even at low levels seems to prevent the leukemia from relapsing (for at least 50 months). As a consequence, we hypothesize that anti-leukemia T cell responses may help maintain remission under imatinib therapy. The mathematical model together with the new experimental data imply that there may be a feasible, low-risk, clinical approach to enhancing the effects of imatinib treatment. [ABSTRACT FROM AUTHOR]

Published

2008

14. Modeling regulation mechanisms in the immune system

Author

Kim, Peter S., Lee, Peter P., and Levy, Doron

Subjects

*LYMPHOCYTES, *T cells, *IMMUNE system, *ANATOMY

Abstract

Abstract: We develop a mathematical framework for modeling regulatory mechanisms in the immune system. The model describes dynamics of key components of the immune network within two compartments: lymph node and tissue. We demonstrate using numerical simulations that our system can eliminate virus-infected cells, which are characterized by a tendency to increase without control (in absence of an immune response), while tolerating normal cells, which are characterized by a tendency to approach a stable equilibrium population. We experiment with different combinations of T cell reactivities that lead to effective systems and conclude that slightly self-reactive T cells can exist within the immune system and are controlled by regulatory cells. We observe that CD8+ T cell dynamics has two phases. In the first phase, CD8+ cells remain sequestered within the lymph node during a period of proliferation. In the second phase, the CD8+ population emigrates to the tissue and destroys its target population. We also conclude that a self-tolerant system must have a mechanism of central tolerance to ensure that self-reactive T cells are not too self-reactive. Furthermore, the effectiveness of a system depends on a balance between the reactivities of the effector and regulatory T cell populations, where the effectors are slightly more reactive than the regulatory cells. [Copyright &y& Elsevier]

Published

2007

15. Marked Differences in Human Melanoma Antigen-Specific T Cell Responsiveness after Vaccination Using a Functional Microarray.

Author

Chen, Daniel S., Soen, Yoav, Stuge, Tor B., Lee, Peter P., Weber, Jeffrey S., Brown, Patrick O., and Davis, Mark M.

Subjects

CELLULAR immunity, T cells, MELANOMA, CANCER vaccines, PEPTIDES, MAJOR histocompatibility complex, IMMUNOGLOBULINS

Abstract

Background: In contrast to many animal model studies, immunotherapeutic trials in humans suffering from cancer invariably result in a broad range of outcomes, from long-lasting remissions to no discernable effect. Methods and Findings: In order to study the T cell responses in patients undergoing a melanoma-associated peptide vaccine trial, we have developed a high-throughput method using arrays of peptide-major histocompatibility complexes (pMHC) together with antibodies against secreted factors. T cells were specifically immobilized and activated by binding to particular pMHCs. The antibodies, spotted together with the pMHC, specifically capture cytokines secreted by the T cells. This technique allows rapid, simultaneous isolation and multiparametric functional characterization of antigen-specific T cells present in clinical samples. Analysis of CD8+ lymphocytes from ten melanoma patients after peptide vaccination revealed a diverse set of patient- and antigen-specific profiles of cytokine secretion, indicating surprising differences in their responsiveness. Four out of four patients who showed moderate or greater secretion of both interferon-γ (IFNγ) and tumor necrosis factor-α (TNFα) in response to a gp100 antigen remained free of melanoma recurrence, whereas only two of six patients who showed discordant secretion of IFNγ and TNFα did so. Conclusion: Such multiparametric analysis of T cell antigen specificity and function provides a valuable tool with which to dissect the molecular underpinnings of immune responsiveness and how this information correlates with clinical outcome. [ABSTRACT FROM AUTHOR]

Published

2005

16. Memory T cells have gene expression patterns intermediate between naïve and effector.

Author

Holmes, Susan, He, Michael, Xu, Tong, and Lee, Peter P.

Subjects

T cells, GENE expression, VACCINES, GENETIC regulation, LYMPHOCYTES, MULTIVARIATE analysis

Abstract

The biological basis underlying differentiation of naïve (NAI) T cells into effector (EFFE) and memory (MEM) cells is incompletely understood. Furthermore, whether NAI T cells serially differentiate into EFFE and then MEM cells (linear differentiation) or whether they concurrently differentiate into either EFFE or MEM cells (parallel differentiation) remains unresolved. We isolated NAI, EFFE, and MEM CD8+ I cell subsets from human peripheral blood and analyzed their gene expression by using microarrays. We identified 156 genes that strongly differentiate NAI, EFFE, and MEM CD8+ T cells; these genes provide previously unrecognized markers to help identify each cell type. Using several statistical approaches to analyze and group the data (standard heat-map and hierarchical clustering, a unique circular representation, multivariate analyses based on principal components, and a clustering method based on phylogenetic parsimony analysis), we assessed the lineage relationships between these subsets and showed that MEM cells have gene expression patterns intermediate between NAI and EFFE T cells. Our analysis suggests a common differentiation pathway to an intermediate state followed by a split into EFFE or MEM cells, hence supporting the parallel differentiation model. As such, conditions under which NAI T cells are activated may determine the magnitude of both EFFE and MEM cells, which arise subsequently. A better understanding of these conditions may be very useful in the design of future vaccine strategies to maximize MEM cell generation. [ABSTRACT FROM AUTHOR]

Published

2005

17. Diversity and Recognition Efficiency of T Cell Responses to Cancer.

Author

Stuge, Tor B., Holmes, Susan P., Saharan, Sahdev, Tuettenberg, Andrea, Roederer, Mario, Weber, Jeffrey S., and Lee, Peter P.

Subjects

CANCER treatment, T cells, ANTIGENS, IMMUNOTHERAPY, TUMORS

Abstract

Melanoma patients vaccinated with tumor-associated antigens frequently develop measurable peptide-specific CD8 + T cell responses; however, such responses often do not confer clinical benefit. Understanding why vaccine-elicited responses are beneficial in some patients but not in others will be important to improve targeted cancer immunotherapies. Methods and Findings We analyzed peptide-specific CD8 + T cell responses in detail, by generating and characterizing over 200 cytotoxic T lymphocyte clones derived from T cell responses to heteroclitic peptide vaccination, and compared these responses to endogenous anti-tumor T cell responses elicited naturally (a heteroclitic peptide is a modification of a native peptide sequence involving substitution of an amino acid at an anchor residue to enhance the immunogenicity of the peptide). We found that vaccine-elicited T cells are diverse in T cell receptor variable chain beta expression and exhibit a different recognition profile for heteroclitic versus native peptide. In particular, vaccine-elicited T cells respond to native peptide with predominantly low recognition efficiency--a measure of the sensitivity of a T cell to different cognate peptide concentrations for stimulation--and, as a result, are inefficient in tumor lysis. In contrast, endogenous tumor-associated-antigen-specific T cells show a predominantly high recognition efficiency for native peptide and efficiently lyse tumor targets. Conclusions These results suggest that factors that shape the peptide-specific T cell repertoire after vaccination may be different from those that affect the endogenous response. Furthermore, our findings suggest that current heteroclitic peptide vaccination protocols drive expansion of peptide-specific T cells with a diverse range of recognition efficiencies, a significant proportion of which are unable to respond to melanoma cells. Therefore, it is critical that the recognition efficiency of vaccine-elicited T cells be... [ABSTRACT FROM AUTHOR]

Published

2004

18. Ex vivo identification, isolation and analysis of tumor-cytolytic T cells.

Author

Rubio, Valerie, Stuge, Tor B, Singh, Naileshni, Betts, Michael R., Weber, Jeffrey S., Roederer, Mario, and Lee, Peter P.

Subjects

T cells, MEMBRANE proteins, CANCER vaccines, MAJOR histocompatibility complex, IMMUNOTHERAPY

Abstract

We isolated pure, viable populations of tumor-cytolytic T cells directly from patient blood samples using flow cytometric quantification of the surface mobilization of CD107a-an integral membrane protein in cytolytic granules-as a marker for degranulation after tumor stimulation. We show that tumor-cytolytic T cells are indeed elicited in patients after cancer vaccination, and that tumor reactivity is strongly correlated with efficient T-cell recognition of peptide-bearing targets. We combined CD107a mobilization with peptide-major histocompatibility complex (P-MHC) tetramer staining to directly correlate antigen specificity and cytolytic ability on a single-cell level. This showed that tumor-cytolytic T cells with high recognition efficiency represent only a minority of peptide-specific T cells elicited in patients after heteroclitic peptide vaccination. We were also able to expand these cells to high numbers ex vivo while maintaining their cytolytic potential. These techniques will be useful not only for immune monitoring of cancer vaccine trials, but also for adoptive cellular immunotherapy after ex vivo expansion. The ability to rapidly identify and isolate tumor-cytolytic T cells would be very useful in cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2003

19. Chronic myelogenous leukemia shapes host immunity by selective deletion of high-avidity leukemia-specific T cells.

Author

Molldrem, Jeffrey J., Lee, Peter P., Kant, Shreya, Wieder, Eric, Weidong Jiang, Sijie Lu, Changqing Wang, Davis, Mark M., Jiang, Weidong, Lu, Sijie, and Wang, Changqing

Subjects

*T cells, *CELL-mediated cytotoxicity, *CANCER, *APOPTOSIS, *COMPARATIVE studies, *IMMUNITY, *RESEARCH methodology, *MEDICAL cooperation, *PROTEINS, *PROTEOLYTIC enzymes, *RESEARCH, *HLA-B27 antigen, *EVALUATION research, *CHRONIC myeloid leukemia

Abstract

We have shown that cytotoxic T lymphocytes specific for PR1, an HLA-A2-restricted nonopeptide derived from proteinase 3, kill leukemia cells and may contribute to the elimination of chronic myelogenous leukemia (CML) after treatment with IFN or allogeneic bone marrow transplant. Some patients with persistent disease also have circulating PR1-specific T cells, however, suggesting the likelihood of immune tolerance. Here we show that both high- and low-avidity PR1-specific T cells from the peripheral blood of healthy donors can be identified and selectively expanded in vitro. Although high-avidity PR1-specific T cells killed CML more effectively than low-avidity T cells, only high-avidity T cells underwent apoptosis when stimulated with high PR1 peptide concentration or when exposed to leukemia that overexpressed proteinase 3. No high-avidity PR1-specific T cells could be identified or expanded from newly diagnosed leukemia patients, whereas low-avidity T cells were readily expanded. Circulating high-avidity PR1-specific T cells were identified in IFN-sensitive patients in cytogenetic remission, however. These results provide evidence that CML shapes the host immune response and that leukemia outgrowth may result in part from leukemia-induced selective deletion of high-avidity PR1-specific T cells. [ABSTRACT FROM AUTHOR]

Published

2003

20. Evidence that specific T lymphocytes may participate in the elimination of chronic myelogenous leukemia.

Author

Molldrem, Jeffrey J., Lee, Peter P., Wang, Changqing, Felio, Kyrie, Kantarjian, Hagop M., Champlin, Richard E., and Davis, Mark M.

Subjects

*T cells, *LYMPHOCYTES, *MYELOID leukemia, *LEUKEMIA

Abstract

Although the immune system has long been implicated in the control of cancer, evidence for specific and efficacious immune responses in human cancer has been lacking. In the case of chronic myelogenous leukemia (CML), either allogeneic bone marrow transplant (BMT) or interferon-a2b (IFN-a2b) therapy can result in complete remission, but the mechanism for prolonged disease control is unknown and may involve immune anti-leukemic responses. We previously demonstrated that PR1, a peptide derived from proteinase 3, is a potential target for CML-specific T cells. Here we studied 38 CML patients treated with allogeneic BMT, IFN- a2b or chemotherapy to look for PR1-specific T cells using PR1/HLA-A*0201 tetrameric complexes. There was a strong correlation between the presence of PR1-specific T cells and clinical responses after IFN-a and allogeneic BMT. This provides for the first time direct evidence of a role for T-cell immunity in clearing malignant cells. [ABSTRACT FROM AUTHOR]

Published

2000

21. Ubiquitin Activating Enzyme UBA6 Regulates Th1 and Tc1 Cell Differentiation.

Author

Lee, Ji Yeon, An, Eun-Koung, Hwang, Juyoung, Jin, Jun-O., and Lee, Peter C. W.

Subjects

UBIQUITINATION, TH1 cells, UBIQUITIN, T cells, KILLER cells, CELL differentiation, T cell receptors

Abstract

Ubiquitination is a crucial mechanism in regulating the immune response, setting the balance between immunity and tolerance. Here, we investigated the function of a poorly understood alternative branch of the ubiquitin-activating E1 enzyme UBA6 in activating immune cells. UBA6 expression levels were elevated in T cells by toll-like receptor agonists and anti-CD3/28 antibody stimulation, but not in dendritic cells, macrophages, B cells, and natural killer cells. Additionally, we generated T cell-specific UBA6-deficient mice and found that UBA6-deficient CD4 and CD8 T cells elevated the production of interferon-gamma (IFN-γ). Moreover, the transfer of UBA6-deficient CD4 and CD8 T cells in RAG1-knockout mice exacerbated the development of multi-organ inflammation compared with control CD4 and CD8 T cell transfer. In human peripheral blood CD4 and CD8 T cells, basal levels of UBA6 in lupus patients presented much lower than those in healthy controls. Moreover, the IFN-γ production efficiency of CD4 and CD8 T cells was negatively correlated to UBA6 levels in patients with lupus. Finally, we found that the function of UBA6 was mediated by destabilization of IκBα degradation, thereby increasing NF-κB p65 activation in the T cells. Our study identifies UBA6 as a critical regulator of IFN-γ production in T cells by modulating the NF-κB p65 activation pathway. [ABSTRACT FROM AUTHOR]

Published

2022

22. Enhancement of Immune Checkpoint Inhibitor-Mediated Anti-Cancer Immunity by Intranasal Treatment of Ecklonia cava Fucoidan against Metastatic Lung Cancer.

Author

Zhang, Wei, Hwang, Juyoung, Yadav, Dhananjay, An, Eun-Koung, Kwak, Minseok, Lee, Peter Chang-Whan, and Jin, Jun-O

Subjects

IMMUNE checkpoint proteins, INTRANASAL administration, LUNG cancer, CYTOTOXIC T cells, METASTASIS, KILLER cells, LUNGS, T cells

Abstract

Although fucoidan, a well-studied seaweed-extracted polysaccharide, has shown immune stimulatory effects that elicit anticancer immunity, mucosal adjuvant effects via intranasal administration have not been studied. In this study, the effect of Ecklonia cava-extracted fucoidan (ECF) on the induction of anti-cancer immunity in the lung was examined by intranasal administration. In C57BL/6 and BALB/c mice, intranasal administration of ECF promoted the activation of dendritic cells (DCs), natural killer (NK) cells, and T cells in the mediastinal lymph node (mLN). The ECF-induced NK and T cell activation was mediated by DCs. In addition, intranasal injection with ECF enhanced the anti-PD-L1 antibody-mediated anti-cancer activities against B16 melanoma and CT-26 carcinoma tumor growth in the lungs, which were required cytotoxic T lymphocytes and NK cells. Thus, these data demonstrated that ECF functioned as a mucosal adjuvant that enhanced the immunotherapeutic effect of immune checkpoint inhibitors against metastatic lung cancer. [ABSTRACT FROM AUTHOR]

Published

2021

23. Characterization of circulating T cells specific for tumor-associated antigens in melanoma patients.

Author

Lee, Peter P., Yee, Cassian, Savage, Peter A., Fong, Lawrence, Brockstedt, Dirk, Weber, Jeffrey S., Johnson, Denise, Swetter, Susan, Thompson, John, Greenberg, Philip D., Roederer, Mario, and Davis, Mark M.

Subjects

*T cells, *TUMOR antigens, *MELANOMA, *TUMOR growth

Abstract

We identified circulating CD8[sup +] T-cell populations specific for the tumor-associated antigens (TAAs) MART-1 (27-35) or tyrosinase (368-376) in six of eleven patients with metastatic melanoma using peptide/HLA-A[sup *]0201 tetramers. These TAA-specific populations were of two phenotypically distinct types: one, typical for memory/effector T cells; the other, a previously undescribed phenotype expressing both naive and effector cell markers. This latter type represented more than 2% of the total CD8[sup +] T cells in one patient, permitting detailed phenotypic and functional analysis. Although these cells have many of the hallmarks of effector T cells, they were functionally unresponsive, unable to directly lyse melanoma target cells or produce cytokines in response to mitogens. In contrast, CD8[sup +] T cells from the same patient were able to lyse EBVpulsed target cells and showed robust allogeneic responses. Thus, the clonally expanded TAA-specific population seems to have been selectively rendered anergic in vivo. Peptide stimulation of the TAA-specific T-cell populations in other patients failed to induce substantial upregulation of CD69 expression, indicating that these cells may also have functional defects, leading to blunted activation responses. These data demonstrate that systemic TAA-specific T-cell responses can develop de novo in cancer patients, but that antigen-specific unresponsiveness may explain why such cells are unable to control tumor growth. [ABSTRACT FROM AUTHOR]

Published

1999

24. Impaired release of a T-cell specific suppressor factor in rheumatoid arthritis.

Author

Lau, C., Budz-Tymkewycz, Stella, Ramsen, Michael, Lee, Peter, and Keystone, Edward C.

Subjects

T cells, RHEUMATOID arthritis, SCLERODERMA (Disease), LYMPHOBLASTOID cell lines, AUTOIMMUNE diseases, BLOOD

Abstract

Peripheral blood T cells from patients with rheumatoid arthritis (RA) and scleroderma (PSS) were assessed for their ability to release T-cell-specific suppressor activity (TRSA) upon incubation with a suppressor activating factor (SAF) derived from a human lymphoblastoid cell line (CEM). T cells from 11/20(55%) RA patients exhibited impaired TRSA release in contrast to 1/12 (8%) of PSS patients. RA patients demonstrating impaired TRSA release exhibited more active arthritis than patients demonstrating normal TRSA release. [ABSTRACT FROM AUTHOR]

Published

1985

25. Angiocentric T-cell lymphoma presenting as lethal midline granuloma.

Author

Lee, Peter Y., Freeman, Nancy J., Khorsand, Jila, and Weinstock, Martin A.

Subjects

GRANULOMA, T cells, LYMPHOMAS, EPSTEIN-Barr virus, PROGNOSIS, SKIN diseases

Abstract

Background Lethal midline granuloma (LMG) is a rare condition characterized by rapidly progressive midfacial destruction. Most LMG cases are angiocentric T-cell lymphomas and an association with Epstein-Barr virus (EBV) has been reported. Cutaneous involvement is poorly described and the prognosis not well documented. Methods We report a case of angiocentric T-cell lymphoma of the palate that presented as LMG with concurrent discrete skin lesions composed of two distinct morphologic appearances: indurated nodules and annular plaques. The English language literature for LMG-type angiocentric T-cell lymphoma is reviewed and a survival analysis of 58 cases with follow-up data (including our own case) is performed. Results The 1- and 5-year survival rates were 45% ± 7% and 22% ± 9%, respectively. Poor survival was associated with advanced age and stage. EBV DNA was detected in 16 out of 21 reported cases in which it was sought (including our case). Conclusions We present photographic documentation of a broader spectrum of cutaneous lesions in the LMG-type angiocentric T-cell lymphoma than has previously been described, and have confirmed the association with EBV. The prognosis is poor. Aggressive therapy such as bone marrow transplantation should be considered early in the course. [ABSTRACT FROM AUTHOR]

Published

1997

26. Lipid-coated gold nanorods for photoimmunotherapy of primary breast cancer and the prevention of metastasis.

Author

Kim, So-Jung, Park, Hae-Bin, An, Eun-Koung, Ryu, Dayoung, Zhang, Wei, Pack, Chan-Gi, Kim, HyunCheol, Kwak, Minseok, Im, Wonpil, Ryu, Ja-Hyoung, Lee, Peter C.W., and Jin, Jun-O

Subjects

*THERAPEUTICS, *CANCER relapse, *BILAYER lipid membranes, *LUNG development, *BREAST cancer, *T cells

Abstract

Nanomedicines hold promise for the treatment of various diseases. However, treating cancer metastasis remains highly challenging. In this study, we synthesized gold nanorods (AuNRs) containing (α-GC), an immune stimulator, for the treatment of primary cancer, metastasis, and recurrence of the cancer. Therefore, the AuNR were coated with lipid bilayers loaded with α-GC (α-LA). Upon irradiation with 808 nm light, α-LA showed a temperature increase. Intra-tumoral injection of α-LA in mice and local irradiation of the 4T1 breast cancer tumor effectively eliminated tumor growth. We found that the presence of α-GC in α-LA activated dendritic cells and T cells in the spleen, which completely blocked the development of lung metastasis. In mice injected with α-LA for primary breast cancer treatment, we observed antigen-specific T cell responses and increased cytotoxicity against 4T1 cells. We conclude that α-LA is promising for the treatment of both primary breast cancer and its metastasis. Schematic illustration of α-LA-mediated photo-immunotherapy for treatment of primary tumor and prevention of metastatic lung cancer. [Display omitted] • For PTT, AuNRs were coated with lipid film comprising α-galactosylceramide (α-LA). • α-LA with 808 nm laser irradiation eliminated orthotopic 4 T1 breast cancer by PTT. • α-LA also prevented recurrence of lung metastatic 4 T1 cancer. • Anti-metastatic effect of a-LA was mediated by cancer antigen-specific immunity. [ABSTRACT FROM AUTHOR]

Published

2024

27. Phenotypic Switching of Naïve T Cells to Immune-Suppressive Treg-Like Cells by Mutant KRAS.

Author

Kalvala, Arjun, Wallet, Pierre, Yang, Lu, Wang, Chongkai, Li, Haiqing, Nam, Arin, Nathan, Anusha, Mambetsariev, Isa, Poroyko, Valeriy, Gao, Hanlin, Chu, Peiguo, Sattler, Martin, Bild, Andrea, Manuel, Edwin R., Lee, Peter P., Jolly, Mohit Kumar, Kulkarni, Prakash, and Salgia, Ravi

Subjects

RAS oncogenes, T cells, NON-small-cell lung carcinoma, RAS proteins, SUPPRESSOR cells, CELLS

Abstract

Oncogenic (mutant) Ras protein Kirsten rat sarcoma viral oncogene homolog (KRAS) promotes uncontrolled proliferation, altered metabolism, and loss of genome integrity in a cell-intrinsic manner. Here, we demonstrate that CD4+ T cells when incubated with tumor-derived exosomes from mutant (MT) KRAS non-small-cell lung cancer (NSCLC) cells, patient sera, or a mouse xenograft model, induce phenotypic conversion to FOXP3+ Treg-like cells that are immune-suppressive. Furthermore, transfecting T cells with MT KRAS cDNA alone induced phenotypic switching and mathematical modeling supported this conclusion. Single-cell sequencing identified the interferon pathway as the mechanism underlying the phenotypic switch. These observations highlight a novel cytokine-independent, cell-extrinsic role for KRAS in T cell phenotypic switching. Thus, targeting this new class of Tregs represents a unique therapeutic approach for NSCLC. Since KRAS is the most frequently mutated oncogene in a wide variety of cancers, the findings of this investigation are likely to be of broad interest and have a large scientific impact. [ABSTRACT FROM AUTHOR]

Published

2019

28. γδ T Cells Predict Outcome in Zoledronate-Treated Breast Cancer Patients.

Author

Welton, Joanne L., Martí, Salvador, Mahdi, Mohammed H., Boobier, Clare, Barrett‐Lee, Peter J., and Eberl, Matthias

Subjects

PREVENTION of disease progression, ZOLEDRONIC acid, BREAST tumors, COMBINED modality therapy, CONFIDENCE intervals, STATISTICS, T cells, U-statistics, DATA analysis, RECEIVER operating characteristic curves, THERAPEUTICS

Abstract

The biological mechanism underlying the antitumor role of zoledronate is unclear. The analysis in this letter illustrates the diagnostic and prognostic potential of a γδ T‐cell‐based blood test and implies a link between immune responsiveness and positive outcome with zoledronate therapy. [ABSTRACT FROM AUTHOR]

Published

2013

29. Down-regulation of the interferon signaling pathway in T lymphocytes from patients with metastatic melanoma.

Author

Critchley-Thorne, Rebecca J., Ning Yan, Nacu, Serban, Weber, Jeffrey, Holmes, Susan P., Lee, Peter P., and Yan, Ning

Subjects

INTERFERONS, ANTINEOPLASTIC agents, T cells, MELANOMA, NEUROENDOCRINE tumors, TYROSINE metabolism, ANTIGENS, BIOCHEMISTRY, CARRIER proteins, CELL physiology, CELLULAR signal transduction, COMPARATIVE studies, HETEROCYCLIC compounds, IMMUNOLOGICAL adjuvants, IMMUNOTHERAPY, KILLER cells, PHENOMENOLOGY, RESEARCH methodology, MEDICAL cooperation, PHOSPHORYLATION, PROTEINS, RESEARCH, RESEARCH funding, SKIN tumors, SULFUR compounds, EVALUATION research, OLIGONUCLEOTIDE arrays, IN vitro studies, PHARMACODYNAMICS

Abstract

Background: Dysfunction of the immune system has been documented in many types of cancers. The precise nature and molecular basis of immune dysfunction in the cancer state are not well defined.Methods and Findings: To gain insights into the molecular mechanisms of immune dysfunction in cancer, gene expression profiles of pure sorted peripheral blood lymphocytes from 12 patients with melanoma were compared to 12 healthy controls. Of 25 significantly altered genes in T cells and B cells from melanoma patients, 17 are interferon (IFN)-stimulated genes. These microarray findings were further confirmed by quantitative PCR and functional responses to IFNs. The median percentage of lymphocytes that phosphorylate STAT1 in response to interferon-alpha was significantly reduced (Delta = 16.8%; 95% confidence interval, 0.98% to 33.35%) in melanoma patients (n = 9) compared to healthy controls (n = 9) in Phosflow analysis. The Phosflow results also identified two subgroups of patients with melanoma: IFN-responsive (33%) and low-IFN-response (66%). The defect in IFN signaling in the melanoma patient group as a whole was partially overcome at the level of expression of IFN-stimulated genes by prolonged stimulation with the high concentration of IFN-alpha that is achievable only in IFN therapy used in melanoma. The lowest responders to IFN-alpha in the Phosflow assay also showed the lowest gene expression in response to IFN-alpha. Finally, T cells from low-IFN-response patients exhibited functional abnormalities, including decreased expression of activation markers CD69, CD25, and CD71; TH1 cytokines interleukin-2, IFN-gamma, and tumor necrosis factor alpha, and reduced survival following stimulation with anti-CD3/CD28 antibodies compared to controls.Conclusions: Defects in interferon signaling represent novel, dominant mechanisms of immune dysfunction in cancer. These findings may be used to design therapies to counteract immune dysfunction in melanoma and to improve cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2007

30. Research Highlights.

Author

Dempsey, Laurie A., Lee, Peter T., and Wilson, Jamie D. K.

Subjects

*IMMUNOLOGY, *MEMBRANE proteins, *T cells, *LYMPHOCYTES, *MAST cells, *CONNECTIVE tissue cells

Abstract

The article presents brief information on research papers related to the field of immunology published in various science journals as of August 2005. A research paper on the trapping of membrane proteins published in a 2005 issue of the journal "Cell," describes the dynamics by which specialized CD2-rich membrane domains are formed in activated T cells. Another research paper published in a 2005 issue of "Journal of Experimental Medicine" investigates how the release and migration of mast cells to tissues is controlled.

Published

2005

31. Research Notes.

Author

Dempsey, Laurie A., Lee, Peter I., and Wilson, Jamie D. K.

Subjects

*IMMUNOLOGY, *MEMORY, *T cells, *B cells, *IMMUNOGLOBULINS, *LYMPHOCYTES

Abstract

The article presents research notes on issues dealing with nature immunology. Although most primary effector T cells die during the contraction phase, small numbers survive to become memory cells. A study links expression of homodimeric CD8 α chains to CD8 memory cell generation. Terminally differentiated B cells secrete antibodies, but additional factors influence whether these cells undergo further immunoglobulin gene diversification, such as somatic hypermutation and class-switch recombination.

Published

2004

32. Research notes.

Author

Dempsey, Laurie A., Lee, Peter T., and Wilson, Jamie D.K.

Subjects

*IMMUNOLOGY, *NF-kappa B, *T cells

Abstract

Reports on developments in immunology as of November 2003. Functions of NF-kappaB in T cell development; Effect of the recognition of pathogen-associated molecular patterns by surfactant proteins; Finding that neutrophils can cause substantial collateral tissue damage if unchecked.

Published

2003

33. P-type pilus PapG protein elicits toll-like receptor 2-mediated immune activation during cancer immunotherapy.

Author

Zhang, Wei, Park, Hae-Bin, Yadav, Dhananjay, An, Eun-Koung, Kim, So-Jung, Ryu, Dayoung, Agrawal, Richa, Ryu, Ja-Hyoung, Kwak, Minseok, Lee, Peter C.W., and Jin, Jun-O

Subjects

*ESCHERICHIA coli, *MAJOR histocompatibility complex, *TOLL-like receptors, *DENDRITIC cells, *CYTOTOXINS, *T cells

Abstract

The immune activation ability of FimH, an adhesion protein in pili of Escherichia coli (E. coli), has been recently reported. However, studies on the immune activity of PapG, another major pili terminal protein, have not been well explored. In this study, the immune stimulatory effect of purified recombinant PapG was evaluated. PapG treatment promoted dramatic changes in dendritic morphology of the bone marrow-derived dendritic cells (BMDCs) and induced upregulation of co-stimulatory molecule levels, major histocompatibility complex (MHC) I and II expression, and pro-inflammatory cytokine production in BMDCs. To identify the stimulatory receptor of PapG, an in silico study was performed. PapG exhibited strong binding affinity with murine toll-like receptor 2 (TLR2). In addition, PapG-induced activation of splenic DC and its subsets was unsuccessful in TLR2-knock out mice. Combination of PapG and ovalbumin (OVA) elicited OVA-specific T cell proliferation and cytokine production and cytotoxicity that consequently promoted anti-cancer immune responses against OVA-expressing B16 melanoma. Furthermore, PapG treatment induced activation of peripheral blood DCs and its subsets in humans in a TLR2 dependent manner. PapG-stimulated human conventional DC2 promoted syngeneic T cell proliferation and activation. The findings of this study demonstrated that PapG could be a useful immune stimulator for immunotherapy against cancer. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

34. Polysaccharides from Astragalus membranaceus elicit T cell immunity by activation of human peripheral blood dendritic cells.

Author

An, Eun-Koung, Zhang, Wei, Kwak, Minseok, Lee, Peter Chang-Whan, and Jin, Jun-O

Subjects

*ASTRAGALUS membranaceus, *BLOOD cells, *T cells, *DENDRITIC cells, *MONONUCLEAR leukocytes, *IMMUNOREGULATION, *POLYSACCHARIDES

Abstract

Astragalus membranaceus is a widely used herbal medicine in Asia. It has been recognized as possessing various biological properties, however, studies on the activity of the A. membranaceus polysaccharide (AMP), a major component of A. membranaceus , on human peripheral blood dendritic cells (PBDCs) have not been thoroughly investigated. In this study, we found that AMP induced changes in dendritic morphology and the upregulation of activation marker expression and inflammatory cytokine production in human blood monocyte-derived dendritic cells (MDDCs). The AMP promoted the activation of both blood dendritic cell antigen 1+ (BDCA1+) and BDCA3+ PBDCs. AMP-induced secretion of cytokines in the peripheral blood mononuclear cells (PBMCs) was mainly due to PBDCs. Finally, activated BDCA1+ and BDCA3+ PBDCs by AMP elicited proliferation and activation of autologous T cells, respectively. Hence, these data demonstrated that AMPs could activate dendritic and T cells in human blood, and may provide a new direction for the application of AMPs in the regulation of human immunity. • AMP induces activation of human monocyte-derived DCs. • AMP promotes maturation of BDCA1+ and BDCA3+ human peripheral blood DCs. • AMP-stimulated PBDCs elicit proliferation and activation of CD4 and CD8 T cells. [ABSTRACT FROM AUTHOR]

Published

2022

35. Cancer immunotherapy by immune checkpoint blockade and its advanced application using bio-nanomaterials.

Author

Yadav, Dhananjay, Kwak, Minseok, Chauhan, Pallavi Singh, Puranik, Nidhi, Lee, Peter C.W., and Jin, Jun-O

Subjects

*IMMUNOTHERAPY, *IMMUNE checkpoint proteins, *IMMUNE checkpoint inhibitors, *IPILIMUMAB, *CANCER treatment, *IMMUNE response, *T cells

Abstract

Cancer is the second leading cause of death worldwide. Traditional approaches, such as surgery, chemotherapy, and radiotherapy have been the main cancer therapeutic modalities in recent years. Cancer immunotherapy is a novel therapeutic modality that potentiates the immune responses of patients against malignancy. Immune checkpoint proteins expressed on T cells or tumor cells serve as a target for inhibiting T cell overactivation, maintaining the balance between self-reactivity and autoimmunity. Tumors essentially hijack the immune checkpoint pathway in order to survive and spread. Immune checkpoint inhibitors (ICIs) are being developed as a result to reactivate the anti-tumor immune response. Recent advances in nanotechnology have contributed to the development of successful, safe, and efficient anticancer drug systems based on nanoparticles. Nanoparticle-based cancer immunotherapy overcomes numerous challenges and offers novel strategies for improving conventional immunotherapies. The fundamental and physiochemical properties of nanoparticles depend on various cancer therapeutic strategies, such as chemotherapeutics, nucleic acid-based treatments, photothermal therapy, and photodynamic agents. The review discusses the use of nanoparticles as carriers for delivering immune checkpoint inhibitors and their efficacy in cancer combination therapy. [ABSTRACT FROM AUTHOR]

Published

2022

36. The Immune Landscape in Women Cancers

Author

Timperi, Eleonora, Vissio, Elena, Marchiò, Caterina, Romano, Emanuela, Rosen, Steven T., Series Editor, Lee, Peter P., editor, and Marincola, Francesco M., editor

Published

2020

37. Astragalus membranaceus polysaccharides potentiate the growth-inhibitory activity of immune checkpoint inhibitors against pulmonary metastatic melanoma in mice.

Author

Hwang, Juyoung, Zhang, Wei, Dhananjay, Yadav, An, Eun-Koung, Kwak, Minseok, You, SangGuan, Lee, Peter Chang-Whan, and Jin, Jun-O

Subjects

*ASTRAGALUS membranaceus, *IMMUNE checkpoint inhibitors, *BRAF genes, *MELANOMA, *IMMUNE checkpoint proteins, *POLYSACCHARIDES, *T cells

Abstract

Astragalus membranaceus (A. membranaceus) is commonly used in various herbal formulations to treat several human and animal diseases. Polysaccharides, which are the major bioactive components in the A. membranaceus , exhibit various bioactive properties. However, the ability of A. membranaceus polysaccharides (APS) to activate the mucosal immune response has not been examined. We examined the effect of intranasal administration of APS on mucosal immune cell activation and the growth-inhibitory activity against pulmonary metastatic melanoma in mice by combination treatment with immune checkpoint blockade. The intranasal treatment of APS increased the number of lineage−CD11c+ dendritic cell (DCs) in the mesenteric lymph nodes (mLN) through the upregulation of CC-chemokine receptor 7 expression. Moreover, intranasal treatment of APS activated DCs, which further stimulated natural killer (NK) and T cells in the mLN. The APS/anti-PD-L1 antibody combination inhibited the pulmonary infiltration of B16 melanoma cells. The depletion of NK cells and CD8 T cells in mice mitigated the anti-cancer effect of this combination, thereby highlighting the critical role of NK cells and CD8 T cells in mediating anti-cancer immunity. These findings demonstrated that APS could be used as a topical mucosal adjuvant to enhance the immune check point inhibitor anti-cancer effect. [ABSTRACT FROM AUTHOR]

Published

2021

38. Myeloid cell-targeted STAT3 inhibition sensitizes head and neck cancers to radiotherapy and T cell-mediated immunity.

Author

Moreira, Dayson, Sampath, Sagus, Haejung Won, White, Seok Voon, Yu-Lin Su, Alcantara, Marice, Chongkai Wang, Lee, Peter, Maghami, Ellie, Massarelli, Erminia, Kortylewski, Marcin, Won, Haejung, Su, Yu-Lin, and Wang, Chongkai

Subjects

*CELLULAR immunity, *SUPPRESSOR cells, *CANCER radiotherapy, *CETUXIMAB, *GENE expression profiling, *HEAD & neck cancer, *T cells, *RESEARCH, *ANIMAL experimentation, *RESEARCH methodology, *EVALUATION research, *COMPARATIVE studies, *RESEARCH funding, *MYELOID cells, *CELL lines, *MICE

Abstract

The tumor microenvironment affects the outcome of radiotherapy against head and neck squamous cell carcinoma (HNSCC). We recently found that tolerogenic myeloid cells accumulate in the circulation of HNSCC patients undergoing radiotherapy. Here, we analyzed tumor-containing lymph node biopsies collected from these patients. After 2 weeks of radiotherapy, we found an increase in tumor-associated macrophages (TAMs) with activated STAT3, while CD8+ T cells were reduced as detected using multiplex IHC. Gene expression profiling indicated upregulation of M2 macrophage-related genes (CD163, CD206), immunosuppressive mediators (ARG1, LIF, TGFB1), and Th2 cytokines (IL4, IL5) in irradiated tumors. We next validated STAT3 as a potential target in human HNSCC-associated TAMs, using UM-SCC1 xenotransplants in humanized mice. Local injections of myeloid cell-targeted STAT3 antisense oligonucleotide (CpG-STAT3ASO) activated human DCs/macrophages and promoted CD8+ T cell recruitment, thereby arresting UM-SCC1 tumor growth. Furthermore, CpG-STAT3ASO synergized with tumor irradiation against syngeneic HPV+ mEERL and HPV- MOC2 HNSCC tumors in mice, triggering tumor regression and/or extending animal survival. The antitumor immune responses were CD8+ and CD4+ T cell dependent and associated with the activation of antigen-presenting cells (DCs/M1 macrophages) and increased CD8+ to regulatory T cell ratio. Our observations suggest that targeted inhibition of STAT3 in tumor-associated myeloid cells augments the efficacy of radiotherapy against HNSCC. [ABSTRACT FROM AUTHOR]

Published

2021

39. Optimisation of anti-cancer peptide vaccines to preferentially elicit high-avidity T cells.

Author

Kumbhari, Adarsh, Kim, Peter S., and Lee, Peter P.

Subjects

*CYTOTOXIC T cells, *T cells, *CANCER vaccines, *VACCINES, *ORDINARY differential equations, *CANCER cells

Abstract

• Therapeutic peptide vaccines stimulate CTLs that can eliminate cancer cells. • In clinical trials vaccines did not work despite eliciting large numbers of CTLs. • Vaccines elicit low-avidity CTLs that don't kill cancer, but stop high-avidity CTLs. • Goal of vaccines should be to elicit high-avidity CTLs that can kill cancer cells. • Using an ODE model, we optimise dosage to preferentially elicit high-avidity CTLs. Therapeutic cancer vaccines often do not substantially reduce tumour burden, despite stimulating anti-tumour cytotoxic T lymphocytes (CTLs). Recent experiments have shown that the majority of vaccine-elicited CTLs may be of low-avidity. Moreover, low-avidity CTLs, which are abundant, do not kill cancer cells and potentially inhibit the ability of high-avidity T cells to kill cancer cells. By modelling CTL selection using a system of ordinary differential equations, we show that the efficacy of the peptide vaccine may be improved by controlling its delivery and dosage to preferentially elicit high-avidity CTLs. Our simulations predict that weekly, reduced doses of a vaccine may result in a greater than 90% reduction in cancer concentration. By contrast, a standard vaccine protocol such as a high-dose injection given every 2 weeks induces only a 65% reduction. Our model demonstrates a proof-of-concept approach to targeting immune responses for CTL selection, thereby offering a technique to potentially improve existing therapies. [ABSTRACT FROM AUTHOR]

Published

2020

40. Immunosuppressive nanoparticles containing recombinant PD-L1 and methotrexate alleviate multi-organ inflammation.

Author

An, Eun-Koung, Zhang, Wei, Park, Hae-Bin, Kim, So-Jung, Eom, Hee-Yun, Hwang, Juyoung, Kwak, Minseok, Lee, Ji Yeon, Lee, Peter Chang-Whan, and Jin, Jun-O

Subjects

*IMMUNE checkpoint proteins, *REGULATORY T cells, *PROGRAMMED death-ligand 1, *IMMUNOREGULATION, *PROGRAMMED cell death 1 receptors, *T cell differentiation, *T cells, *T helper cells

Abstract

Multi-organ inflammatory diseases are one of the most serious autoimmune diseases worldwide. The regulation of immune responses by immune checkpoint proteins influences the development and treatment of cancer and autoimmune diseases. In this study, recombinant murine PD-L1 (rmPD-L1) was used for controlling T cell immunity to treat multi-organ inflammation. To enhance the immunosuppressive effect, we incorporated methotrexate, an anti-inflammatory drug, into hybrid nanoparticles (HNPs) and decorated the surface of HNPs with rmPD-L1 to produce immunosuppressive HNPs (IsHNPs). IsHNP treatment effectively targeted PD-1-expressing CD4 and CD8 T cells in the splenocytes; additionally, it promoted the production of Foxp3-expressing regulatory T cells, which suppressed the differentiation of helper T cells. IsHNP treatment also inhibited anti-CD3 antibody-mediated activation of CD4 and CD8 T cells in mice in vivo. This treatment protected mice from multi-organ inflammation induced by the adoptive transfer of naïve T cells to recombination-activating gene 1 knockout mice. The results of this study imply the therapeutic potential of IsHNPs in the treatment of multi-organ inflammation and other inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2023

41. Recombinant programmed cell death protein 1 functions as an immune check point blockade and enhances anti-cancer immunity.

Author

Hwang, Juyoung, An, Eun-Koung, Zhang, Wei, Park, Hae-Bin, Kim, So-Jung, Yadav, Dhananjay, Kim, Jihoe, Choi, Inho, Kwak, Minseok, Lee, Peter CW., Zhang, Xiaoyan, Xu, Jianqing, and Jin, Jun-O

Subjects

*T cells, *PROGRAMMED cell death 1 receptors, *DENDRITIC cells, *IMMUNOLOGIC memory, *IMMUNE checkpoint proteins, *IMMUNITY, *CELLULAR immunity, *TUMOR growth

Abstract

Effective cancer therapy aims to treat not only primary tumors but also metastatic and recurrent cancer. Immune check point blockade-mediated immunotherapy showed promising effect against tumors; however, it still has a limited effect in metastatic or recurrent cancer. Here, we extracted recombinant murine programmed death-1 (rmPD-1) proteins. The extracted rmPD-1 effectively bound to CT-26 and 4T1 cells expressing PD-L1 and PD-L2. The rmPD-1 did not alter the activation of dendritic cells (DCs); however, rmPD-1 promoted T cell-mediated anti-cancer immunity against CT-26 tumors in mice. Moreover, rmPD-1 decorated thermal responsive hybrid nanoparticles (piHNPs) promoted apoptotic and necrotic cell death of CT-26 cells in response to laser irradiation at 808 nm consequently, it promoted anti-tumor effects against the 1st challenged CT-26 tumors in mice. In addition, piHNP-mediated cured mice from 1st challenged CT-26 was also prevented the 2nd challenged lung metastatic tumor growth, which was dependent of cancer antigen-specific memory T cell immunity. It was also confirmed that the lung metastatic growth of 2nd challenged 4T1 breast cancer was also prevented in cured mice from 1st challenged 4T1 by piHNP. Thus, these data demonstrate that rmPD-1 functions as an immune checkpoint blockade for the treatment of tumors, and piHNPs could be a novel therapeutic agent for preventing cancer metastasis and recurrence. [ABSTRACT FROM AUTHOR]

Published

2022

42. Agent-based modeling of the context dependency in T cell recognition

Author

Casal, Arancha, Sumen, Cenk, Reddy, Timothy E., Alber, Mark S., and Lee, Peter P.

Subjects

*T cells, *PEPTIDES, *MOLECULAR immune response, *CELLULAR immunity

Abstract

Abstract: Antigen recognition by T cells is a key event in the adaptive immune response. T cells scan the surface of antigen-presenting cells (APCs) or target cells for specific peptides bound to MHC molecules. In the physiological setting, a typical APC presents tens of thousands of diverse endogenous self-derived peptides complexed to MHC (pMHC complexes). When ‘foreign’ peptides are presented, they constitute a small fraction of the total surface peptide repertoire. As T cells seem to be capable of discerning minute amounts of ‘foreign’ peptides among a complex background of self-peptides, endogenous peptides are generally assumed to play no role in recognition. However, recent results suggest that these background peptides may alter the sensitivity of T cells to foreign peptides. Current experimental limitations preclude analysis of peptide mixtures approaching physiological complexity, making it difficult to further address the role of complex background peptides. In this paper, we present a computational model to test how complex, varied peptide populations on an APC could potentially modulate a T cell''s ability to detect the presence of small numbers of agonist peptides among a diverse population. We use the model to investigate the notion that under physiological conditions, T cell recognition of foreign peptides is context dependent, that is, T cells process signals gathered from all pMHC interactions, not just from a few agonist peptides while ignoring all others. [Copyright &y& Elsevier]

Published

2005

43. Post-transplantation dynamics of the immune response to chronic myelogenous leukemia

Author

DeConde, Rob, Kim, Peter S., Levy, Doron, and Lee, Peter P.

Subjects

*IMMUNE response, *LYMPHOCYTES, *T cells, *MYELOID leukemia

Abstract

Abstract: We model the immune dynamics between T cells and cancer cells in leukemia patients after bone marrow transplants, using a system of six delay differential equations to track the various cell-populations. Our approach incorporates time delays and accounts for the progression of cells through different modes of behavior. We explore possible mechanisms behind a successful cure, whether mediated by a blood-restricted immune response or a cancer-specific graft-versus-leukemia (GVL) effect. Characteristic features of this model include sustained proliferation of T cells after initial stimulation, saturated T cell proliferation rate, and the possible elimination of cancer cells, independent of fixed-point stability. In addition, we use numerical simulations to examine the effects of varying initial cell concentrations on the likelihood of a successful transplant. Among the observed trends, we note that higher initial concentrations of donor-derived, anti-host T cells slightly favor the chance of success, while higher initial concentrations of general host blood cells more significantly favor the chance of success. These observations lead to the hypothesis that anti-host T cells benefit from stimulation by general host blood cells, which induce them to proliferate to sufficient levels to eliminate cancer. [Copyright &y& Elsevier]

Published

2005

44. Inhibitory effect of porphyran on lipopolysaccharide-induced activation of human immune cells.

Author

Wang, Yuhua, Hwang, Juyoung, Yadav, Dhananjay, Oda, Tatsuya, Lee, Peter Chang-Whan, and Jin, Jun-O

Subjects

*BLOOD cells, *SEPTIC shock, *CELLS, *T cells, *TOLL-like receptors, *LIPOPOLYSACCHARIDES, *DENDRITIC cells, *CELL proliferation

Abstract

• Pyropia yezoensis porphyran inhibits LPS-induced proinflammatory cytokines in human PBMCs. • Porphyran suppresses LPS-induced human MODC and PBDC activation. • LPS binding to TLR4/MD2 complex is interrupted by porphyran in human PBDCs. In mice, porphyran extracted from Pyropia yezoensis exerts anti-inflammatory effects and suppresses lipopolysaccharide (LPS)-induced immune activation and sepsis. Here, we investigated inhibition of LPS-induced activation of human immune cells by porphyran and the underlying mechanisms. We demonstrated that porphyran may inhibit LPS-induced proinflammatory cytokine production in peripheral blood mononuclear cells, monocyte-derived dendritic cells, and peripheral blood dendritic cells. We also observed that porphyran-mediated LPS-induced activation of DC suppressed syngeneic T cell proliferation, resulting in reduced production of interferon-γ. The mechanism of LPS-induced immune cell activation requires the activation of toll like receptor 4 following binding of LPS to myeloid differentiation factor 2 (MD2). Additionally, we show that porphyran competes with LPS for binding to MD2 and thereby suppresses immune cell activation. Porphyran may, therefore, be a promising therapeutic candidate for the treatment of endotoxin-mediated septic shock and inflammation in humans. [ABSTRACT FROM AUTHOR]

Published

2020