Your search keyword '"CD8 antigen"' showing total 104 results

1. Low on-treatment levels of serum soluble CD8 (sCD8) predict better outcomes in advanced non-small cell lung cancer patients treated with atezolizumab.

Author

Siemiątkowska, Anna, Bryl, Maciej, Kosicka-Noworzyń, Katarzyna, Tvrdoň, Jakub, Gołda-Gocka, Iwona, and Główka, Franciszek K.

Subjects

*NON-small-cell lung carcinoma, *CYTOTOXIC T cells, *CANCER patients, *ATEZOLIZUMAB, *CD8 antigen

Abstract

Background: Immunotherapy has changed the paradigm of treating non-small cell lung cancer (NSCLC). But, selecting patients who will achieve long-term benefits from treatment remains unsatisfactory. Here, we investigated the possible use of the soluble form of CD8 antigen (sCD8) in predicting durable disease control after PD-1/PD-L1 blockade. CD8 is a marker of the cytotoxic T lymphocytes. Its soluble form (sCD8) is secreted under activation of the immune system but also has immunosuppressive properties. The data about serum sCD8 in patients dosed with anti-PD-1/PD-L1 drugs are lacking. Methods and results: We included 42 NSCLC patients and collected samples at baseline and for the first 3 months of atezolizumab immunotherapy. The serum sCD8 concentrations were measured with the ELISA kit and correlated with treatment outcomes. Patients with durable (≥ 12 months) disease control presented lower serum sCD8 than those without long-term benefits. The sCD8 levels measured at the end of cycle 2 (sCD8.2) were the earliest time point that successfully differentiated patients (3.76 vs. 9.68 ng/mL, respectively, p < 0.001). Individuals with low sCD8.2 (≤ 4.09 ng/mL) presented longer progression-free survival (HR = 0.061, p < 0.001) and overall survival (HR = 0.104, p < 0.05) compared to individuals with high sCD8.2 (median values unreached vs. 4.4 months and 14.4 months for PFS and OS, respectively). Conclusions: Serum sCD8 could be an early biomarker of durable disease control after anti-PD-L1 treatment. Higher sCD8 in patients with worse outcomes could suggest the inhibitory effect of sCD8 on cytotoxic T-cells activation. [ABSTRACT FROM AUTHOR]

Published

2023

2. TCF-1 regulates NKG2D expression on CD8 T cells during anti-tumor responses.

Author

Harris, Rebecca, Mammadli, Mahinbanu, Hiner, Shannon, Suo, Liye, Yang, Qi, Sen, Jyoti Misra, and Karimi, Mobin

Subjects

*T cells, *CD8 antigen, *CELL physiology, *TRANSCRIPTION factors, *IMMUNE response

Abstract

Cancer immunotherapy relies on improving T cell effector functions against malignancies, but despite the identification of several key transcription factors (TFs), the biological functions of these TFs are not entirely understood. We developed and utilized a novel, clinically relevant murine model to dissect the functional properties of crucial T cell transcription factors during anti-tumor responses. Our data showed that the loss of TCF-1 in CD8 T cells also leads to loss of key stimulatory molecules such as CD28. Our data showed that TCF-1 suppresses surface NKG2D expression on naïve and activated CD8 T cells via key transcriptional factors Eomes and T-bet. Using both in vitro and in vivo models, we uncovered how TCF-1 regulates critical molecules responsible for peripheral CD8 T cell effector functions. Finally, our unique genetic and molecular approaches suggested that TCF-1 also differentially regulates essential kinases. These kinases, including LCK, LAT, ITK, PLC-γ1, P65, ERKI/II, and JAK/STATs, are required for peripheral CD8 T cell persistent function during alloimmunity. Overall, our molecular and bioinformatics data demonstrate the mechanism by which TCF-1 modulated several critical aspects of T cell function during CD8 T cell response to cancer. Summary Figure: TCF-1 is required for persistent function of CD8 T cells but dispensable for anti-tumor response. Here, we have utilized a novel mouse model that lacks TCF-1 specifically on CD8 T cells for an allogeneic transplant model. We uncovered a molecular mechanism of how TCF-1 regulates key signaling pathways at both transcriptomic and protein levels. These key molecules included LCK, LAT, ITK, PLC-γ1, p65, ERK I/II, and JAK/STAT signaling. Next, we showed that the lack of TCF-1 impacted phenotype, proinflammatory cytokine production, chemokine expression, and T cell activation. We provided clinical evidence for how these changes impact GVHD target organs (skin, small intestine, and liver). Finally, we provided evidence that TCF-1 regulates NKG2D expression on mouse naïve and activated CD8 T cells. We have shown that CD8 T cells from TCF-1 cKO mice mediate cytolytic functions via NKG2D. [ABSTRACT FROM AUTHOR]

Published

2023

3. Egr2 and 3 maintain anti-tumour responses of exhausted tumour infiltrating CD8 + T cells.

Author

Symonds, Alistair L. J., Miao, Tizong, Busharat, Zabreen, Li, Suling, and Wang, Ping

Subjects

*T cells, *CD8 antigen, *TRANSCRIPTION factors, *TUMOR microenvironment, *TUMOR-infiltrating immune cells

Abstract

Although T cells can develop into an exhausted state in the tumour microenvironment, tumour infiltrating T cells (TILs) are important to control tumour growth. By analysing single cell RNA-sequencing data from human tumours, we found that the transcription factors Early Growth Response 2 (EGR2) and 3 were highly induced in TILs, but not peripheral CD8 + T cells, in multiple patient cohorts. We found that deficiency of Egr2 and 3 in T cells resulted in enhanced tumour growth and fewer TILs in mouse models. Egr2 is highly expressed together with checkpoint molecules in a proportion of CD8 + TILs and Egr2high cells exhibit better survival and proliferation than Egr2-/-Egr3-/- and Egr2low TILs. Anti-PD-1 treatment increases Egr2 expression in CD8 + TILs and reduces tumour growth, while anti-PD-1 efficacy is abrogated in the absence of Egr2 and 3. Thus, Egr2 and 3 are important for maintaining anti-tumour responses of exhausted CD8 + TILs. [ABSTRACT FROM AUTHOR]

Published

2023

4. Effects of tumor-infiltrating CD8+ T cells, PD1/PD-L1 axis, and expression patterns of HLA class I on the prognosis of patients with malignant pleural mesothelioma who underwent extra-pleural pneumonectomy.

Author

Okita, Riki, Mimura-Kimura, Yuka, Kawamoto, Nobutaka, Yamamoto, Naoki, Umeda, Masashi, Okada, Masanori, Inokawa, Hidetoshi, Mimura, Yusuke, Murakami, Tomoyuki, Nakata, Masao, and Okabe, Kazunori

Subjects

*PLEURA cancer, *T cells, *HLA histocompatibility antigens, *CD8 antigen, *TUMOR-infiltrating immune cells, *HISTOCOMPATIBILITY class I antigens

Abstract

Programmed cell death protein-1 (PD1), PD1 ligand 1 (PD-L1), and human leukocyte antigen (HLA) class I molecule play pivotal roles in T cell-induced anti-tumor immunity; however, the clinical impact of these parameters in resected malignant pleural mesothelioma (MPM) cases is unknown. We immunohistochemically evaluated the tumor infiltrated lymphocytes (TILs), PD1/PD-L1 axis, and expression of HLA class I in resected specimens from 58 patients with MPM who underwent extra-pleural pneumonectomy (EPP). Higher infiltration of CD3-TIL, CD8-TIL, and PD1-TIL, loss of HLA class I, and overexpression of PD-L1 by tumor cells (PD-L1 TC) or immune cells (PD-L1 IC) were observed in 34 (58.6%), 27 (46.6%), 41 (70.7%), 45 (77.6%), 29 (50.0%), and 33 (56.4%) of 58 cases, respectively. Interestingly, the CD3-TIL score positively correlated with PD-L1 TC and PD1-TIL scores. HLA class I expression level was inversely correlated with the expression levels of PD-L1 TC and PD-L1 IC. Multivariate analysis showed that age, histology, and node metastasis were independent prognostic factors for 5-year overall survival (OS) and loss of HLA class I coincided with a positive prognosis (p = 0.011). The concomitant lack of infiltrating CD8+ T cells with no loss of HLA class I predicted worse 5-year OS (p = 0.007). Moreover, cluster classifications among multiple immunoparameters showed that categories among CD3/PD-L1 TC/HLA class I (p = 0.043), CD8/PD1/HLA class I (p = 0.032), CD8/PD-L1 TC/HLA class I (p = 0.011), and PD1/PD-L1 TC/HLA class I (p = 0.032) predicted 5-year OS in EPP cases for MPM. These immunoparameters could guide surgical indications for patients with MPM. [ABSTRACT FROM AUTHOR]

Published

2023

5. Induction of the activating transcription factor-4 in the intratumoral CD8+ T cells sustains their viability and anti-tumor activities.

Author

Lu, Zhen, Bae, Eun-Ah, Verginadis, Ioannis I., Zhang, Hongru, Cho, Christina, McBrearty, Noreen, George, Subin S., Diehl, J. Alan, Koumenis, Constantinos, Bradley, Linda M., and Fuchs, Serge Y.

Subjects

*T cells, *CELL survival, *ANTINEOPLASTIC agents, *CYTOTOXIC T cells, *CD8 antigen

Abstract

Immune suppressive factors of the tumor microenvironment (TME) undermine viability and exhaust the activities of the intratumoral cytotoxic CD8 + T lymphocytes (CTL) thereby evading anti-tumor immunity and decreasing the benefits of immune therapies. To counteract this suppression and improve the efficacy of therapeutic regimens, it is important to identify and understand the critical regulators within CD8 + T cells that respond to TME stress and tumor-derived factors. Here we investigated the regulation and importance of activating transcription factor-4 (ATF4) in CTL using a novel Atf4ΔCD8 mouse model lacking ATF4 specifically in CD8 + cells. Induction of ATF4 in CD8 + T cells occurred in response to antigenic stimulation and was further increased by exposure to tumor-derived factors and TME conditions. Under these conditions, ATF4 played a critical role in the maintenance of survival and activities of CD8 + T cells. Conversely, selective ablation of ATF4 in CD8 + T cells in mice rendered these Atf4ΔCD8 hosts prone to accelerated growth of implanted tumors. Intratumoral ATF4-deficient CD8 + T cells were under-represented compared to wild-type counterparts and exhibited impaired activation and increased apoptosis. These findings identify ATF4 as an important regulator of viability and activity of CD8 + T cells in the TME and argue for caution in using agents that could undermine these functions of ATF4 for anti-cancer therapies. [ABSTRACT FROM AUTHOR]

Published

2023

6. Identification of the molecular subtype and prognostic characteristics of pancreatic cancer based on CD8 + T cell-related genes.

Author

Xu, Dafeng, Wang, Yu, Chen, Yonghai, and Zheng, Jinfang

Subjects

*CD8 antigen, *PANCREATIC cancer, *REGULATOR genes, *IMMUNE checkpoint proteins, *GENES

Abstract

CD8 + T lymphocytes are immune cells that play a crucial anti-tumor role in the human body, and prognostic value of CD8 + T cell-related regulatory genes in PAAD remains elusive. Data on 179 expression profiles across 13 immune cell datasets were downloaded from the GEO database, and the expression profiles of CD8 + T cell-related genes were obtained using WGCNA. Molecular subtypes based on CD8 + T cell-related genes were constructed using the ConsensusClusterPlus algorithm. Lasso regression analysis was performed to build a 10-gene signature. GSVA was performed to explore the pathways related to these ten genes. The IMvigor210 cohort was used to explore the predictive efficacy of the signature in terms of immunotherapy response. Four hundred and forty-six CD8 + T cell-related genes were obtained. One hundred and nine genes in TCGA and GEO datasets were closely related to the prognosis of patients and were included in the next study. PAAD samples were divided into two subtypes (IC1 and IC2) according to consensus cluster analysis. These two immune subtypes were significantly different in terms of immune checkpoint genes, immune function, and drug treatment response. Additionally, the 10-gene signature constructed based on CD8 + T cell-related genes showed a stable prognostic performance in TCGA and GEO cohorts. Moreover, it served as an independent prognostic factor for patients with PAAD. Furthermore, the 10-gene signature could effectively predict the response to immunotherapy. The immunophenotyping-derived prognostic model based on CD8 T cell-related genes provides a basis for the clinical treatment of pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2023

7. Tcf-1 protects anti-tumor TCR-engineered CD8+ T-cells from GzmB mediated self-destruction.

Author

Zangari, Brendan, Tsuji, Takemasa, Matsuzaki, Junko, Mohammadpour, Hemn, Eppolito, Cheryl, Battaglia, Sebastiano, Ito, Fumito, Chodon, Thinle, Koya, Richard, Robert McGray, A. J., and Odunsi, Kunle

Subjects

*T cells, *CELL death, *TRANSCRIPTION factors, *CD8 antigen, *IMMUNE response

Abstract

Background: T-cell longevity is undermined by antigen-driven differentiation programs that render cells prone to attrition through several mechanisms. CD8 + T cells that express the Tcf-1 transcription factor have undergone limited differentiation and exhibit stem-cell-like replenishment functions that facilitate persistence. We engineered human CD8 + T cells to constitutively express Tcf-1 and a TCR specific for the NY-ESO-1 cancer-associated antigen. Co-engineered cells were assessed for their potential for adoptive cellular immunotherapy. Methods: Tcf-1 mRNA encoding TCF-1B and TCF-1E isoforms, along with GzmB expression were assessed in CD62L + CD57 −, CD62L − CD57 −, and CD62L − CD57 + CD8 + T cells derived from normal donor lymphocytes. The impact of stable Tcf-1B expression on CD8 + T-cell phenotype, anti-tumor activity, and cell-cycle activity was assessed in vitro and in an in vivo tumor xenograft model. Results: TCF-1B and TCF-1E were dynamically regulated during self-renewal, with progeny of recently activated naïve T cells more enriched for TCF-1B mRNA. Constitutive TCF-1B expression improved the survival of TCR-engineered CD8 + T cells upon engagement with tumor cells. Tcf-1B prohibited the acquisition of a GzmB High state, and protected T cells from apoptosis associated with elicitation of effector function, and promoted stem cell-like characteristics. Conclusions: Tcf-1 protects TCR-engineered CD8 + T cells from activation induced cell death by restricting GzmB expression. Our study presents constitutive Tcf-1B expression as a potential means to impart therapeutic T cells with attributes of persistence for durable anti-tumor activity. [ABSTRACT FROM AUTHOR]

Published

2022

8. Role of the cGAS-STING pathway in regulating the tumor-immune microenvironment in dMMR/MSI colorectal cancer.

Author

Kaneta, Akinao, Nakajima, Shotaro, Okayama, Hirokazu, Matsumoto, Takuro, Saito, Katsuharu, Kikuchi, Tomohiro, Endo, Eisei, Ito, Misato, Mimura, Kosaku, Kanke, Yasuyuki, Saito, Motonobu, Saze, Zenichiro, Fujita, Shotaro, Sakamoto, Wataru, Onozawa, Hisashi, Momma, Tomoyuki, Ohki, Shinji, and Kono, Koji

Subjects

*COLORECTAL cancer, *HEREDITARY nonpolyposis colorectal cancer, *INTERFERONS, *CD8 antigen, *CELL lines, *HUMAN genes

Abstract

Deficient mismatch repair (dMMR)/microsatellite instability (MSI) colorectal cancer (CRC) has high immunogenicity and better prognosis compared with proficient MMR (pMMR)/microsatellite stable (MSS) CRC. Although the activation of the cyclic GMP-AMP synthase (cGAS)-stimulator of interferon genes (STING) pathway has been considered to contribute to the high number of CD8+ TILs, its role in dMMR/MSI CRC is largely unknown. In this study, to examine the role of the cGAS-STING pathway on the recruitment of CD8+ TILs in dMMR/MSI CRC, we used public datasets and clinical tissue samples in our cohorts to evaluate the expression of cGAS, STING, and CD8+ TILs in pMMR/MSS and dMMR/MSI CRCs. According to the analysis of public datasets, the expression of cGAS-STING, CD8 effector gene signature, and CXCL10-CCL5, chemoattractants for CD8+ TILs which regulated by the cGAS-STING pathway, was significantly upregulated in dMMR/MSI CRC, and the expression of cGAS-STING was significantly associated with the expression of CD8 effector gene signature. Immunohistochemistry staining of the clinical tissue samples (n = 283) revealed that cGAS-STING was highly expressed in tumor cells of dMMR CRC, and higher expression of cGAS-STING in tumor cells was significantly associated with the increased number of CD8+ TILs. Moreover, we demonstrated that the downregulation of MMR gene in human CRC cell lines enhanced the activation of the cGAS-STING pathway. Taken together, for the first time, we found that dMMR/MSI CRC has maintained a high level of cGAS-STING expression in tumor cells, which might contribute to abundant CD8+ TILs and immune-active TME. [ABSTRACT FROM AUTHOR]

Published

2022

9. Targeting PD-L1 and TIGIT could restore intratumoral CD8 T cell function in human colorectal cancer.

Author

Thibaudin, Marion, Limagne, Emeric, Hampe, Léa, Ballot, Elise, Truntzer, Caroline, and Ghiringhelli, Francois

Subjects

*T cells, *CELL physiology, *COLORECTAL cancer, *TUMOR-infiltrating immune cells, *CD8 antigen, *IPILIMUMAB

Abstract

Microsatellite stable colorectal cancers (MSS-CRC) are resistant to anti-PD-1/PD-L1 therapy but the combination of immune checkpoints inhibitors (ICI) could be a clue to reverse resistance. Our aim was to evaluate ex vivo the capacity of the combination of atezolizumab (anti-PD-L1) and tiragolumab (anti-TIGIT) to reactivate the immune response of tumor infiltrating lymphocytes (TILs) in MSS-CRC. We analysed CRC tumor tissue and the associated blood sample in parallel. For each patient sample, extensive immunomonitoring and cytokine production were tested. We generated an ex vivo assay to study immune reactivity following immune stimulation with checkpoint inhibitors of tumor cell suspensions. Three microsatellite instable (MSI) and 13 MSS-CRC tumors were analysed. To generalize our observations, bioinformatics analyses were performed on public data of single cell RNA sequencing of CRC TILs and RNA sequencing data of TCGA. Atezolizumab alone could only reactivate T cells from MSI tumors. Atezolizumab and tiragolumab reactivated T cells in 46% of MSS-CRC samples. Reactivation by ICK was observed in patients with higher baseline frequency of Th1 and Tc1 cells, and was also associated with higher baseline T cell polyfunctionality and higher CD96 expression. We showed that a high frequency of CD96 expression on T cells could be a surrogate marker of atezolizumab and tiragolumab efficacy. Together these data suggest that the association of atezolizumab and tiragolumab could restore function of CD4 and CD8 TILs in MSS-CRC and could be tested in a clinical trial in colorectal cancer patients with MSS status. [ABSTRACT FROM AUTHOR]

Published

2022

10. Cross-presentation of a TAP-independent signal peptide induces CD8 T immunity to escaped cancers but necessitates anchor replacement.

Author

Marijt, Koen A., Griffioen, Lisa, Blijleven, Laura, van der Burg, Sjoerd. H., and van Hall, Thorbald

Subjects

*PEPTIDES, *CD8 antigen, *T cells, *IMMUNITY, *CANCER cells, *ANTIGENS, *T cell receptors

Abstract

Cancer cells frequently display defects in their antigen-processing pathway and thereby evade CD8 T cell immunity. We described a novel category of cancer antigens, named TEIPP, that emerge on cancers with functional loss of the peptide pump TAP. TEIPPs are non-mutated neoantigens despite their 'self' origin by virtue of their absence on normal tissues. Here, we describe the development of a synthetic long peptide (SLP) vaccine for the most immunogenic TEIPP antigen identified thus far, derived from the TAP-independent LRPAP1 signal sequence. LRPAP121–30-specific CD8 T cells were present in blood of all tested healthy donors as well as patients with non-small cell lung adenocarcinoma. SLPs with natural flanking, however, failed to be cross-presented by monocyte-derived dendritic cells. Since the C-terminus of LRPAP121–30 is an unconventional and weakly binding serine (S), we investigated if replacement of this anchor would result in efficient cross-presentation. Exchange into a valine (V) resulted in higher HLA-A2 binding affinity and enhanced T cell stimulation. Importantly, CD8 T cells isolated using the V-variant were able to bind tetramers with the natural S-variant and respond to TAP-deficient cancer cells. A functional screen with an array of N-terminal and C-terminal extended SLPs pointed at the 24-mer V-SLP, elongated at the N-terminus, as most optimal vaccine candidate. This SLP was efficiently cross-presented and consistently induced a strong polyclonal LRPAP121–30-specific CD8 T cells from the endogenous T cell repertoire. Thus, we designed a TEIPP SLP vaccine from the LRPAP1 signal sequence ready for validation in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2022

11. Imaging features of gadoxetic acid-enhanced MR imaging for evaluation of tumor-infiltrating CD8 cells and PD-L1 expression in hepatocellular carcinoma.

Author

Sun, Lin, Mu, Luwen, Zhou, Jing, Tang, Wenjie, Zhang, Linqi, Xie, Sidong, Chen, Jingbiao, and Wang, Jin

Subjects

*PROGRAMMED death-ligand 1, *MAGNETIC resonance imaging, *CD8 antigen, *HEPATOCELLULAR carcinoma, *IMMUNE checkpoint proteins

Abstract

Background: Tumor-infiltrating CD8 cells and expression of programmed cell death ligand 1 (PD-L1) are immune checkpoint markers in patients with hepatocellular carcinoma (HCC). We aimed to determine the ability of preoperative gadoxetic acid-enhanced magnetic resonance imaging (MRI) findings to predict CD8 cell density and PD-L1 expression in HCC. Methods: A total of 120 patients with HCC who underwent 3.0-T gadoxetic acid-enhanced MRI before curative resection from January 2016 to June 2020 were enrolled and divided into a training set (n = 84) and a testing set (n = 36). Thirty-four patients with advanced stage HCC who received anti-PD-1 inhibitor between January 2017 and April 2020 and underwent pretreated gadoxetic acid-enhanced MRI scans were enrolled in an independent validation set. PD-L1 expression and CD8 cell infiltration were assessed with immunohistochemical staining, respectively. Two radiologists blinded to pathology results evaluated the pretreated MR features in consensus. Logistic regression and the receiver operating characteristic curve (ROC) analyses were used to determine the value of image features to predict high CD8 cell density, PD-L1 positivity and the combination of high CD8 cell density and PD-L1 positivity in HCC in the training set and validated the findings in the testing set. The associations of MRI predictors with the objective response to immunotherapy were assessed in the independent validation. Results: In the training set, the independent MRI predictors were irregular tumor margin (ITM, P = 0.008) and peritumoral low signal intensity (PLSI) on hepatobiliary phase (HBP) images (P < 0.001) for PD-L1 positivity, absence of an enhancing capsule (AEC, P = 0.001) and PLSI on HBP images (P = 0.025) for high CD8 cell density, and PLSI on HBP images (P = 0.001) and ITM (P = 0.023) for the both. The area under the curves (AUCs) of the predictive models for evaluating PD-L1 positivity, high CD8 cell density and the combination of high CD8 cell density and PD-L1 positivity were 0.810 and 0.809, 0.740 and 0.728, and 0.809 and 0.874 in the training and testing set, respectively. The objective response was demonstrated to be associated with the combination of PLSI on HBP images and ITM (PHI, P = 0.004), and the combination of PLSI on HBP images and AEC (PHA, P = 0.012) in the independent validation set. Conclusions: Pretreated MRI features have the potential to identify patients with HCC in an immune-activated state and predict outcomes of immunotherapy. Trial registration The study was retrospectively registered on March 5, 2020 with registration no. [2020] 02–012-01. [ABSTRACT FROM AUTHOR]

Published

2022

12. Correction to: A modified immune cell infiltration score achieves ideal stratification for CD8+ T cell efficacy and immunotherapy benefit in hepatocellular carcinoma.

Author

Pan, Banglun, Luo, Yue, Ye, Dongjie, Qiu, Jiacheng, Zhang, Xiaoxia, Wu, Xiaoxuan, Yao, Yuxin, Wang, Xiaoqian, and Tang, Nanhong

Subjects

*T cells, *IMMUNOTHERAPY, *CD45 antigen, *CD3 antigen, *CD8 antigen

Abstract

This document is a correction notice for an article titled "A modified immune cell infiltration score achieves ideal stratification for CD8+ T cell efficacy and immunotherapy benefit in hepatocellular carcinoma" published in the journal Cancer Immunology, Immunotherapy. The original article contained mistakes in figure 6, specifically an overlap in the figures representing CD45 of the high ICI group and CD3 of the low ICI group. The corrected figure 6 is provided in the document. The article discusses the analysis of CD45, CD3, CD4, and CD8 expression levels in patients diagnosed with hepatocellular carcinoma and their correlation with anti-tumor efficacy of T cells infiltrating the tumor microenvironment. The publisher, Springer Nature, remains neutral with regard to jurisdictional claims and institutional affiliations. [Extracted from the article]

Published

2023

13. CD137L dendritic cells induce potent response against cancer-associated viruses and polarize human CD8+ T cells to Tc1 phenotype.

Author

Dharmadhikari, Bhushan, Nickles, Emily, Harfuddin, Zulkarnain, Ishak, Nur Diana Binte, Zeng, Qun, Bertoletti, Antonio, and Schwarz, Herbert

Subjects

*CANCER immunotherapy, *DENDRITIC cells, *T cells, *TUMOR treatment, *CD8 antigen, *EPSTEIN-Barr virus

Abstract

Therapeutic tumor vaccination based on dendritic cells (DC) is safe; however, its efficacy is low. Among the reasons for only a subset of patients benefitting from DC-based immunotherapy is an insufficient potency of in vitro generated classical DCs (cDCs), made by treating monocytes with GM-CSF + IL-4 + maturation factors. Recent studies demonstrated that CD137L (4-1BBL, TNFSF9) signaling differentiates human monocytes to a highly potent novel type of DC (CD137L-DCs) which have an inflammatory phenotype and are closely related to in vivo DCs. Here, we show that CD137L-DCs induce potent CD8+ T-cell responses against Epstein-Barr virus (EBV) and Hepatitis B virus (HBV), and that T cells primed by CD137L-DCs more effectively lyse EBV+ and HBV+ target cells. The chemokine profile of CD137L-DCs identifies them as inflammatory DCs, and they polarize CD8+ T cells to a Tc1 phenotype. Expression of exhaustion markers is reduced on T cells activated by CD137L-DCs. Furthermore, these T cells are metabolically more active and have a higher capacity to utilize glucose. CD137L-induced monocyte to DC differentiation leads to the formation of AIM2 inflammasome, with IL-1beta contributing to CD137L-DCs possessing a stronger T cell activation ability. CD137L-DCs are effective in crosspresentation. PGE2 as a maturation factor is required for enhancing migration of CD137L-DCs but does not significantly reduce their potency. This study shows that CD137L-DCs have a superior ability to activate T cells and to induce potent Tc1 responses against the cancer-causing viruses EBV and HBV which suggest CD137L-DCs as promising candidates for DC-based tumor immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2018

14. PD-L1, B7-H3, and PD-1 expression in immunocompetent vs. immunosuppressed patients with cutaneous squamous cell carcinoma.

Author

Varki, Vinod, Ioffe, Olga B., Bentzen, Soren M., Heath, Jon, Cellini, Ashley, Feliciano, Josephine, and Zandberg, Dan P.

Subjects

*IMMUNOCOMPETENT cells, *IMMUNOCOMPROMISED patients, *SQUAMOUS cell carcinoma, *T cells, *CD8 antigen

Abstract

Background: To characterize the expression of co-signaling molecules PD-L1, PD-1, and B7-H3 in cutaneous squamous cell carcinoma (cSCC) by immune status.Methods: We retrospectively analyzed 66 cases of cSCC treated with surgical resection from 2012 to 2015. Immunostained tumor sections were analyzed for percent of tumor cells expressing PD-L1 (Tum-PD-L1%), B7-H3 (Tum-B7-H3%), density of peri and intratumoral CD8 T cells (CD8 density), proportion of CD8 T cells expressing PD-1 (CD8-PD-1%) and of tumor-infiltrating immune cells (TII) expressing PD-L1 (TII-PD-L1%).Results: Of 66 cases, 42 were immunocompetent, 24 immunosuppressed (13 organ transplant, 8 HIV+, 3 other). Defining positive expression at > 5%, 26% of tumors were positive for PD-L1, 85% for B7-H3, 80% had CD8 T cells that expressed PD-1 and 55% had TII that expressed PD-L1. Tum-B7-H3% was significantly higher (median 60 vs. 28%, p = 0.025) in immunocompetent vs. immunosuppressed patients, including when factoring in cause of immunosuppression. No significant difference in Tum-PD-L1%, TII-PD-L1%, CD8 density, or CD8-PD-1% was observed. Tumors from HIV+ patients lacked PD-L1 expression, and had lower B7-H3% (median 2.5 vs. 60%, p = 0.007), and higher CD8 density (median 75% vs. 40%, p = 0.04) compared to immunocompetent patients. Higher tumor grade (Rs = 0.34, p = 0.006) and LVI (Rs = 0.61, p < 0.001) were both associated with higher Tum-PD-L1%.Conclusion: cSCC showed expression of PD-L1 on tumor in 26% of cases, and high tumor B7-H3 expression (85%) and PD-1 expression on CD8 TILs (80%). Tumor B7-H3 expression was significantly higher in immunocompetent vs. immunosuppressed patients, largely driven by very low expression in HIV+ patients. [ABSTRACT FROM AUTHOR]

Published

2018

15. Heterogeneity of CD8 tumor-infiltrating lymphocytes in non-small-cell lung cancer: impact on patient prognostic assessments and comparison of quantification by different sampling strategies.

Author

Obeid, Joseph, Wages, Nolan, Hu, Yinin, Deacon, Donna, and Slingluff, Craig

Subjects

*CD8 antigen, *LYMPHOCYTES, *PREDICATE calculus, *IMMUNOHISTOCHEMISTRY, *NON-small-cell lung carcinoma, *PATIENTS, *PROGNOSIS

Abstract

Introduction: Infiltration of non-small-cell lung cancer (NSCLC) by CD8 T lymphocytes predicts improved patient survival; however, heterogeneity of intratumoral localization complicates this assessment. Strategies for tumor sampling may not accurately represent the whole tumor. We hypothesized that sampling strategies may alter the identification of tumors with high CD8 density and affect the prognostic significance. Patients and methods: Twenty-three primary NSCLC tumors were immunohistochemically stained for CD8 and were assessed using automated software with eight different sampling strategies or the whole tumor. Results of all sampling strategies were compared to the whole tumor counts (paired t tests, Pearson's r). Associations between CD8 densities and overall survival were assessed (log-rank test). Results: Counts from all eight sampling strategies significantly correlated with whole tumor counts ( p ≤ 0.001). However, the magnitude of CD8 cell counts and categorization into high vs low infiltrate groups were affected by the sampling strategy. The most concordant values were derived from random sampling of 20 % of the tumor, a simulated core biopsy, or from sampling the tumor center. TIL infiltration was associated with survival when sampling the center ( p = 0.038), but not the invasive margin ( p > 0.2) or other strategies. Conclusion: Different tumor sampling strategies may yield discordant TIL density results and different stratification for risk assessment. Small biopsies may be particularly unrepresentative. Random sampling of larger tumor areas is recommended. Enumerating CD8 T cells in the tumor center may have prognostic value. [ABSTRACT FROM AUTHOR]

Published

2017

16. Correction to: Identification of the molecular subtype and prognostic characteristics of pancreatic cancer based on CD8 + T cell-related genes.

Author

Xu, Dafeng, Wang, Yu, Chen, Yonghai, and Zheng, Jinfang

Subjects

*PANCREATIC cancer, *CD8 antigen, *GENES

Abstract

Correction to: Identification of the molecular subtype and prognostic characteristics of pancreatic cancer based on CD8 + T cell-related genes Correction to: Cancer Immunology, Immunotherapy https://doi.org/10.1007/s00262-022-03269-3 The original version of this article unfortunately contained a mistake. The original article can be found online at https://doi.org/10.1007/s00262-022-03269-3. [Extracted from the article]

Published

2023

17. How frequently are predicted peptides actually recognized by CD8 cells?

Author

Moldovan, Ioana, Targoni, Oleg, Zhang, Wenji, Sundararaman, Srividya, and Lehmann, Paul

Subjects

*PEPTIDES, *CD8 antigen, *IMMUNE response, *HLA histocompatibility antigens, *IMMUNE recognition, *EPSTEIN-Barr virus, *DETECTION limit

Abstract

Detection of antigen-specific CD8 cells frequently relies on the use of peptides that are predicted to bind to HLA Class I molecules or have been shown to induce immune responses. There is extensive knowledge on individual HLA alleles' peptide-binding requirements, and immunogenic peptides for many antigens have been defined. The 32 individual peptides that comprise the CEF peptide pool represent such well-defined peptide determinants for Cytomegalo-, Epstein-barr-, and Influenza virus. We tested the accuracy of these peptide recognition predictions on 42 healthy human donors that have been high-resolution HLA-typed. According to the predictions, 241 recall responses should have been detected in these donors. Actual testing showed that 36 (15 %) of the predicted CD8 cell responses occurred in the high frequency range, 41 (17 %) in mid-frequencies, and 45 (19 %) were at the detection limit. In 119 instances (49 %), the predicted peptides were not targeted by CD8 cells detectably. The individual CEF peptides were recognized in an unpredicted fashion in 57 test cases. Moreover, the frequency of CD8 cells responding to a single peptide did not reflect on the number of CD8 cells targeting other determinants on the same antigen. Thus, reliance on one or a few predicted peptides provides a rather inaccurate assessment of antigen-specific CD8 cell immunity, strongly arguing for the use of peptide pools for immune monitoring. [ABSTRACT FROM AUTHOR]

Published

2016

18. Uncoupling protein 2 regulates metabolic reprogramming and fate of antigen-stimulated CD8+ T cells.

Author

Chaudhuri, Leena, Srivastava, Rupesh, Kos, Ferdynand, and Shrikant, Protul

Subjects

*UNCOUPLING proteins, *TUMOR treatment, *CELLULAR therapy, *CD8 antigen, *T cell differentiation, *FATTY acid synthesis, *PROTEIN expression

Abstract

Adoptive cell therapy (ACT) employing ex vivo-generated tumor antigen-specific CD8+ T cells shows tumor efficacy when the transferred cells possess both effector and memory functions. New strategies based on understanding of mechanisms that balance CD8+ T cell differentiation toward effector and memory responses are highly desirable. Emerging information confirms a central role for antigen-induced metabolic reprogramming in CD8+ T cell differentiation and clonal expansion. The mitochondrial protein uncoupling protein 2 (UCP2) is induced by antigen stimulation of CD8+ T cells; however, its role in metabolic reprogramming underlying differentiation and clonal expansion has not been reported. Employing genetic (siRNA) and pharmacologic (Genipin) approaches, we note that antigen-induced UCP2 expression reduces glycolysis, fatty acid synthesis and production of reactive oxygen species to balance differentiation with survival of effector CD8+ T cells. Inhibition of UCP2 promotes CD8+ T cell terminal differentiation into short-lived effector cells (CD62LKLRG1IFNγ) that undergo clonal contraction. These findings are the first to reveal a role for antigen-induced UCP2 expression in balancing CD8+ T cell differentiation and survival. Targeting UCP2 to regulate metabolic reprogramming of CD8+ T cells is an attractive new approach to augment efficacy of tumor therapy by ACT. [ABSTRACT FROM AUTHOR]

Published

2016

19. Disease progression in recurrent glioblastoma patients treated with the VEGFR inhibitor axitinib is associated with increased regulatory T cell numbers and T cell exhaustion.

Author

Four, Stephanie, Maenhout, Sarah, Benteyn, Daphné, Keersmaecker, Brenda, Duerinck, Johnny, Thielemans, Kris, Neyns, Bart, and Aerts, Joeri

Subjects

*NEOVASCULARIZATION inhibitors, *GLIOBLASTOMA multiforme, *CANCER immunotherapy, *GLIOBLASTOMA multiforme treatment, *CD4 antigen, *CD8 antigen, *T cells, *CYTOKINES, *PATIENTS, *THERAPEUTICS

Abstract

Background: Recurrent glioblastoma is associated with a poor overall survival. Antiangiogenic therapy results in a high tumor response rate but has limited impact on survival. Immunotherapy has emerged as an efficient treatment modality for some cancers, and preclinical evidence indicates that anti-VEGF(R) therapy can counterbalance the immunosuppressive tumor microenvironment. Methods: We collected peripheral blood mononuclear cells (PBMC) of patients with recurrent glioblastoma treated in a randomized phase II clinical trial comparing the effect of axitinib with axitinib plus lomustine and analyzed the immunophenotype of PBMC, the production of cytokines and expression of inhibitory molecules by circulating T cells. Results: PBMC of 18 patients were collected at baseline and at 6 weeks after initiation of study treatment. Axitinib increased the number of naïve CD8 T cells and central memory CD4 and CD8 T cells and reduced the TIM3 expression on CD4 and CD8 T cells. Patients diagnosed with progressive disease on axitinib had a significantly increased number of regulatory T cells and an increased level of PD-1 expression on CD4 and CD8 T cells. In addition, reduced numbers of cytokine-producing T cells were found in progressive patients as compared to patients responding to treatment. Conclusion: Our results suggest that axitinib treatment in patients with recurrent glioblastoma has a favorable impact on immune function. At the time of acquired resistance to axitinib, we documented further enhancement of a preexisting immunosuppression. Further investigations on the role of axitinib as potential combination partner with immunotherapy are necessary. [ABSTRACT FROM AUTHOR]

Published

2016

20. Exploiting IL-17-producing CD4 and CD8 T cells to improve cancer immunotherapy in the clinic.

Author

Majchrzak, Kinga, Nelson, Michelle, Bailey, Stefanie, Bowers, Jacob, Yu, Xue-Zhong, Rubinstein, Mark, Himes, Richard, and Paulos, Chrystal

Subjects

*INTERLEUKIN-17, *CD4 antigen, *CD8 antigen, *T cells, *CANCER immunotherapy, *CLINICAL trials

Abstract

Cancer immunotherapy is one the most effective approaches for treating patients with tumors, as it bolsters the generation and persistence of memory T cells. In preclinical work, it has been reported that adoptively transferred CD4 and CD8 lymphocytes that secrete IL-17A (i.e., Th17 and Tc17 cells) regress tumors to a greater extent than IFN-γTh1 or Tc1 cells in vivo. Herein, we review the mechanisms underlying how infused Th17 and Tc17 cells regress established malignancies in clinically relevant mouse models of cancer. We also discuss how unique signaling cues-such as co-stimulatory molecules (ICOS and 41BB), cytokines (IL-12 and IL-23) or pharmaceutical reagents (Akt inhibitors, etc.)-can be exploited to bolster the therapeutic potential of IL-17 lymphocytes with an emphasis on using this knowledge to improve next-generation clinical trials for patients with cancer. [ABSTRACT FROM AUTHOR]

Published

2016

21. Late administration of murine CTLA-4 blockade prolongs CD8-mediated anti-tumor effects following stimulatory cancer immunotherapy.

Author

Sckisel, Gail, Mirsoian, Annie, Bouchlaka, Myriam, Tietze, Julia, Chen, Mingyi, Blazar, Bruce, and Murphy, William

Subjects

*CYTOTOXIC T lymphocyte-associated molecule-4, *DRUG administration, *CD8 antigen, *ANTINEOPLASTIC agents, *CANCER immunotherapy, *INTERLEUKIN-2, *TUMOR immunology

Abstract

We have demonstrated that immunostimulatory therapies such as interleukin-2 (IL-2) and anti-CD40 (αCD40) can be combined to deliver synergistic anti-tumor effects. While this strategy has shown success, efficacy varies depending on a number of factors including tumor type and severe toxicities can be seen. We sought to determine whether blockade of negative regulators such as cytotoxic T lymphocyte antigen-4 (CTLA-4) could simultaneously prolong CD8 T cell responses and augment T cell anti-tumor effects. We devised a regimen in which anti-CTLA-4 was administered late so as to delay contraction and minimize toxicities. This late administration both enhanced and prolonged CD8 T cell activation without the need for additional IL-2. The quality of the T cell response was improved with increased frequency of effector/effector memory phenotype cells along with improved lytic ability and bystander expansion. This enhanced CD8 response translated to improved anti-tumor responses both at the primary and metastatic sites. Importantly, toxicities were not exacerbated with combination. This study provides a platform for rational design of immunotherapy combinations to maximize anti-tumor immunity while minimizing toxicities. [ABSTRACT FROM AUTHOR]

Published

2015

22. Dysfunction of PSA-specific CD8 T cells in prostate cancer patients correlates with CD38 and Tim-3 expression.

Author

Japp, Alberto, Kursunel, M., Meier, Sarah, Mälzer, Julia, Li, Xiangdong, Rahman, Nafis, Jekabsons, Waltraut, Krause, Hans, Magheli, Ahmed, Klopf, Christian, Thiel, Andreas, and Frentsch, Marco

Subjects

*PROSTATE-specific antigen, *CD8 antigen, *T cells, *PROSTATE cancer, *PROTEIN expression, *CANCER immunotherapy, *TREATMENT effectiveness

Abstract

The efficacy of immunotherapy in cancer patients is influenced by differences in their immune status. An evaluation of immunocompetence before therapy may help to predict therapeutic success and guide the selection of appropriate regimens. We assessed the preexisting cellular immunity against prostate-specific antigen (PSA) in untreated prostate cancer patients and healthy controls through measurement of the phenotype and function of CD8 T cells. Our data show that the majority of healthy men possess functional PSA-specific CD8 T cells in contrast to cancer patients, where <50 % showed a CD8 T cell response. PSA-specific CD8 T cells of these patients had a higher expression of the activation marker CD38 and the exhaustion marker Tim-3, indicating that PSA-specific cells are exhausted. The heterogeneity of the CD8 T cell response against PSA in prostate cancer patients may influence their response to therapy and is a factor to be taken into account while designing and selecting treatment regimens. [ABSTRACT FROM AUTHOR]

Published

2015

23. STING activator c-di-GMP enhances the anti-tumor effects of peptide vaccines in melanoma-bearing mice.

Author

Wang, Zili and Celis, Esteban

Subjects

*MELANOMA treatment, *INTERFERON genetics, *GUANYLIC acid, *CANCER vaccines, *ANTINEOPLASTIC agents, *CD8 antigen

Abstract

Therapeutic vaccines to induce anti-tumor CD8 T cells have been used in clinical trials for advanced melanoma patients, but the clinical response rate and overall survival time have not improved much. We believe that these dismal outcomes are caused by inadequate number of antigen-specific CD8 T cells generated by most vaccines. In contrast, huge CD8 T cell responses readily occur during acute viral infections. High levels of type-I interferon (IFN-I) are produced during these infections, and this cytokine not only exhibits anti-viral activity but also promotes CD8 T cell responses. The studies described here were performed to determine whether promoting the production of IFN-I could enhance the potency of a peptide vaccine. We report that cyclic diguanylate monophosphate (c-di-GMP), which activates the stimulator of interferon genes, potentiated the immunogenicity and anti-tumor effects of a peptide vaccine against mouse B16 melanoma. The synergistic effects of c-di-GMP required co-administration of costimulatory anti-CD40 antibody, the adjuvant poly-IC, and were mediated in part by IFN-I. These findings demonstrate that peptides representing CD8 T cell epitopes can be effective inducers of large CD8 T cell responses in vaccination strategies that mimic acute viral infections. [ABSTRACT FROM AUTHOR]

Published

2015

24. Development of a potent melanoma vaccine capable of stimulating CD8 T-cells independently of dendritic cells in a mouse model.

Author

Powell, Katie, Stephens, Alexandre, and Ralph, Stephen

Subjects

*MELANOMA, *CD8 antigen, *T cells, *DENDRITIC cells, *LABORATORY mice, *IMMUNE response, *VACCINATION

Abstract

At present, there are no vaccines approved for the prevention or treatment of malignant melanoma, despite the amount of time and resources that has been invested. In this study, we aimed to develop a self-contained vaccine capable of directly stimulating anticancer CD8 T-cell immune responses. To achieve this, three whole-cell melanoma vaccines were developed expressing 4-1BBL or B7.1 T-cell co-stimulatory molecules individually or in combination. The ability of engineered vaccine cell lines to stimulate potent anticancer immune responses in C57BL/6 mice was assessed. Mice vaccinated with cells overexpressing both 4-1BBL and B7.1 (B16-F10-4-1BBL-B7.1-IFNγ/β anticancer vaccine) displayed the greatest increases in CD8 T-cell populations (1.9-fold increase versus control within spleens), which were efficiently activated following antigenic stimulation, resulting in a 10.7-fold increase in cancer cell cytotoxicity relative to control. The enhanced immune responses in B16-F10-4-1BBL-B7.1-IFNγ/β-vaccinated mice translated into highly efficient rejection of live tumour burdens and conferred long-term protection against repeated tumour challenges, which were likely due to enhanced effector memory T-cell populations. Similar results were observed when dendritic cell (DC)-deficient LTα mice were treated with the B16-F10-4-1BBL-B7.1-IFNγ/β anticancer vaccine, suggesting that the vaccine can directly stimulate CD8 T-cell responses in the context of severely reduced DCs. This study shows that the B16-F10-4-1BBL-B7.1-IFNγ/β anticancer vaccine acted as a highly effective antigen-presenting cell and is likely to be able to directly stimulate CD8 T-cells, without requiring co-stimulatory signals from either CD4 T-cells or DCs, and warrants translation of this technology into the clinical setting. [ABSTRACT FROM AUTHOR]

Published

2015

25. Interleukin-12 enhances the function and anti-tumor activity in murine and human CD8 T cells.

Author

Rubinstein, Mark, Su, Ee, Suriano, Samantha, Cloud, Colleen, Andrijauskaite, Kristina, Kesarwani, Pravin, Schwartz, Kristina, Williams, Katelyn, Johnson, C., Li, Mingli, Scurti, Gina, Salem, Mohamed, Paulos, Chrystal, Garrett-Mayer, Elizabeth, Mehrotra, Shikhar, and Cole, David

Subjects

*INTERLEUKIN-12, *ANTINEOPLASTIC agents, *CD8 antigen, *HUMAN T cells, *MELANOMA, *CANCER immunotherapy, *LABORATORY mice, *PATIENTS

Abstract

Mouse CD8 T cells conditioned with interleukin (IL)-12 ex vivo mediate the potent regression of established melanoma when transferred into lymphodepleted mice. However, the quantitative and qualitative changes induced by IL-12 in the responding mouse CD8 T cells have not been well defined. Moreover, the mechanisms by which IL-12-conditioning impacts human CD8 T cells, and how such cells might be expanded prior to infusion into patients is not known. We found that ex vivo IL-12-conditioning of mouse CD8 T cells led to a tenfold-100-fold increase in persistence and anti-tumor efficacy upon adoptive transfer into lymphodepleted mice. The enhancing effect of IL-12 was associated with maintenance of functional avidity. Importantly, in the context of ongoing ACT clinical trials, human CD8 T cells genetically modified with a tyrosinase-specific T cell receptor (TCR) exhibited significantly enhanced functional activity when conditioned with IL-12 as indicated by heightened granzyme B expression and elevated peptide-specific CD107a degranulation. This effect was sustainable despite the 20 days of in vitro cellular expansion required to expand cells over 1,000-fold allowing adequate cell numbers for administration to cancer patients. Overall, these findings support the efficacy and feasibility of ex vivo IL-12-conditioning of TCR-modified human CD8 T cells for adoptive transfer and cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2015

26. Broadening the repertoire of melanoma-associated T-cell epitopes.

Author

Frøsig, Thomas, Lyngaa, Rikke, Met, Özcan, Larsen, Stine, Donia, Marco, Svane, Inge, thor Straten, Per, and Hadrup, Sine

Subjects

*MELANOMA immunotherapy, *T cells, *EPITOPES, *MELANOMA, *CD8 antigen, *MAJOR histocompatibility complex, *HLA histocompatibility antigens, *PATIENTS

Abstract

Immune therapy has provided a significant breakthrough in the treatment of metastatic melanoma. Despite the remarkable clinical efficacy and established involvement of effector CD8 T cells, the knowledge of the exact peptide-MHC complexes recognized by T cells on the tumor cell surface is limited. Many melanoma-associated T-cell epitopes have been described, but this knowledge remains largely restricted to HLA-A2, and we lack understanding of the T-cell recognition in the context of other HLA molecules. We selected six melanoma-associated antigens (MAGE-A3, NY-ESO-1, gp100, Mart1, tyrosinase and TRP-2) that are frequently recognized in patients with the aim of identifying novel T-cell epitopes restricted to HLA-A1, -A3, -A11 and -B7. Using in silico prediction and in vitro confirmation, we identified 127 MHC ligands and analyzed the T-cell responses against these ligands via the MHC multimer-based enrichment of peripheral blood from 39 melanoma patients and 10 healthy donors. To dissect the T-cell reactivity against this large peptide library, we used combinatorial-encoded MHC multimers and observed the T-cell responses against 17 different peptide-MHC complexes in the patient group and four in the healthy donor group. We confirmed the processing and presentation of HLA-A3-restricted T-cell epitopes from tyrosinase (TQYESGSMDK) and gp100 (LIYRRRLMK) and an HLA-A11-restricted T-cell epitope from gp100 (AVGATKVPR) via the cytolytic T-cell recognition of melanoma cell lines and/or K562 cells expressing the appropriate antigen and HLA molecule. We further found T-cell reactivity against two of the identified sequences among tumor-infiltrating lymphocytes from melanoma patients, suggesting a potential clinical relevance of these sequences. [ABSTRACT FROM AUTHOR]

Published

2015

27. siRNA silencing of PD-1 ligands on dendritic cell vaccines boosts the expansion of minor histocompatibility antigen-specific CD8 T cells in NOD/SCID/IL2Rg(null) mice.

Author

van der Waart, Anniek, Fredrix, Hanny, van der Voort, Robbert, Schaap, Nicolaas, Hobo, Willemijn, and Dolstra, Harry

Subjects

*SMALL interfering RNA, *HEMATOLOGIC malignancies, *DENDRITIC cells, *MINOR histocompatibility antigens, *STEM cell transplantation, *CD8 antigen, *LABORATORY mice

Abstract

Allogeneic stem cell transplantation (allo-SCT) can be a curative therapy for patients suffering from hematological malignancies. The therapeutic efficacy is based on donor-derived CD8 T cells that recognize minor histocompatibility antigens (MiHAs) expressed by patient's tumor cells. However, these responses are not always sufficient, and persistence and recurrence of the malignant disease are often observed. Therefore, application of additive therapy targeting hematopoietic-restricted MiHAs is essential. Adoptive transfer of MiHA-specific CD8 T cells in combination with dendritic cell (DC) vaccination could be a promising strategy. Though effects of DC vaccination in anti-cancer therapy have been demonstrated, improvement in DC vaccination therapy is needed, as clinical responses are limited. In this study, we investigated the potency of program death ligand (PD-L) 1 and 2 silenced DC vaccines for ex vivo priming and in vivo boosting of MiHA-specific CD8 T cell responses. Co-culturing CD8 T cells with MiHA-loaded DCs resulted in priming and expansion of functional MiHA-specific CD8 T cells from the naive repertoire, which was augmented upon silencing of PD-L1 and PD-L2. Furthermore, DC vaccination supported and expanded adoptively transferred antigen-specific CD8 T cells in vivo. Importantly, the use of PD-L silenced DCs improved boosting and further expansion of ex vivo primed MiHA-specific CD8 T cells in immunodeficient mice. In conclusion, adoptive transfer of ex vivo primed MiHA-specific CD8 T cells in combination with PD-L silenced DC vaccination, targeting MiHAs restricted to the hematopoietic system, is an interesting approach to boost GVT immunity in allo-SCT patients and thereby prevent relapse. [ABSTRACT FROM AUTHOR]

Published

2015

28. Blockade of CTLA-4 promotes the development of effector CD8 T lymphocytes and the therapeutic effect of vaccination with an attenuated protozoan expressing NY-ESO-1.

Author

Santos, Luara, Galvão-Filho, Bruno, Faria, Paula, Junqueira, Caroline, Dutra, Miriam, Teixeira, Santuza, Rodrigues, Maurício, Ritter, Gerd, Bannard, Oliver, Fearon, Douglas, Antonelli, Lis, and Gazzinelli, Ricardo

Subjects

*CD8 antigen, *T cells, *CANCER immunotherapy, *CANCER prevention, *GENE expression, *CYTOTOXIC T lymphocyte-associated molecule-4, *TRYPANOSOMA cruzi, *PROTOZOA

Abstract

The development of cancer immunotherapy has long been a challenge. Here, we report that prophylactic vaccination with a highly attenuated Trypanosoma cruzi strain expressing NY-ESO-1 (CL-14-NY-ESO-1) induces both effector memory and effector CD8 T lymphocytes that efficiently prevent tumor development. However, the therapeutic effect of such a vaccine is limited. We also demonstrate that blockade of Cytotoxic T Lymphocyte Antigen 4 (CTLA-4) during vaccination enhances the frequency of NY-ESO-1-specific effector CD8 T cells producing IFN-γ and promotes lymphocyte migration to the tumor infiltrate. As a result, therapy with CL-14-NY-ESO-1 together with anti-CTLA-4 is highly effective in controlling the development of an established melanoma. [ABSTRACT FROM AUTHOR]

Published

2015

29. Activated regulatory and memory T-cells accumulate in malignant ascites from ovarian carcinoma patients.

Author

Landskron, Johannes, Helland, Øystein, Torgersen, Knut, Aandahl, Einar, Gjertsen, Bjørn, Bjørge, Line, and Taskén, Kjetil

Subjects

*CD8 antigen, *ANTINEOPLASTIC agents, *CELL proliferation, *FLOW cytometry, *OVARIAN cancer treatment, *T cells, OVARIAN cancer patients

Abstract

Invasive ovarian cancer is associated with poor outcome. The presence of infiltrating regulatory T-cells (Tregs) suppresses protective anti-tumor immune responses, and their accumulation into the tumor microenvironment correlates with reduced survival in ovarian cancer patients. Here, we conducted a detailed characterization of CD4 T-cells, CD8 T-cells and Treg subsets in the peripheral blood and malignant ascites fluid from seventeen patients with ovarian carcinoma of epithelial origin. Cell distribution, activation status and proliferation status were assessed by multi-color flow cytometry. In ascites fluid, a significant accumulation of CD8 cytotoxic T-cells and Tregs was observed compared to peripheral blood. Furthermore, a skewing toward the CD45RA effector/memory compartment was observed in all T-cell subsets in the ascites fluid, but was most pronounced in the Treg population. Regulatory T-cells in the malignant ascites were more activated and had a higher proliferation rate compared to blood-derived cells from the same patient, and their number in ascites was positively correlated with the number of epithelial cells in effusion. In summary, we demonstrate an accumulation of activated CD4, CD8 and regulatory T-cells in the cancer microenvironment of ovarian carcinoma. [ABSTRACT FROM AUTHOR]

Published

2015

30. Shaping of an effective immune microenvironment to and by cancer cells.

Author

Becht, Etienne, Goc, Jeremy, Germain, Claire, Giraldo, Nicolas, Dieu-Nosjean, Marie-Caroline, Sautès-Fridman, Catherine, and Fridman, Wolf-Herman

Subjects

*CANCER cells, *T cells, *CD8 antigen, *IMMUNOTHERAPY, *GENETIC mutation, *CYTOKINES, *LYMPH nodes

Abstract

A high density of intratumoral effector memory CD8+/Th1 T cells is associated with favorable prognosis in most cancers and may be induced or increased by immunotherapy. Efficient adaptive immune reactions are shaped in tumor adjacent tertiary lymphoid structures, which exhibit all characteristics of immunity generating lymphoid formations in reactive lymph nodes. Malignant tumor cells impact favorably or deleteriously their immune microenvironment if they bear genetic mutations that result in neo-antigens or by producing chemokines and cytokines that recruit lymphocytes and myeloid cells or increase inflammation and neo-angiogenesis. This intricate network of interactions results in control or escape of tumors, and its understanding will help define goals to monitor efficiency of immunotherapies. [ABSTRACT FROM AUTHOR]

Published

2014

31. Intrinsically de-sialylated CD103 CD8 T cells mediate beneficial anti-glioma immune responses.

Author

Jouanneau, Emmanuel, Black, Keith, Veiga, Lucia, Cordner, Ryan, Goverdhana, Shyam, Zhai, Yuying, Zhang, Xiao-xue, Panwar, Akanksha, Mardiros, Armen, Wang, HongQiang, Gragg, Ashley, Zandian, Mandana, Irvin, Dwain, and Wheeler, Christopher

Subjects

*CD8 antigen, *T cells, *GLIOMAS, *IMMUNE response, *ANTINEOPLASTIC agents, *CANCER vaccines, *BRAIN tumors

Abstract

Background: Cancer vaccines reproducibly cure laboratory animals and reveal encouraging trends in brain tumor (glioma) patients. Identifying parameters governing beneficial vaccine-induced responses may lead to the improvement of glioma immunotherapies. CD103 CD8 T cells dominate post-vaccine responses in human glioma patients for unknown reasons, but may be related to recent thymic emigrant (RTE) status. Importantly, CD8 RTE metrics correlated with beneficial immune responses in vaccinated glioma patients. Methods: We show by flow cytometry that murine and human CD103 CD8 T cells respond better than their CD103 counterparts to tumor peptide-MHC I (pMHC I) stimulation in vitro and to tumor antigens on gliomas in vivo. Results: Glioma responsive T cells from mice and humans both exhibited intrinsic de-sialylation-affecting CD8 beta. Modulation of CD8 T cell sialic acid with neuraminidase and ST3Gal-II revealed de-sialylation was necessary and sufficient for promiscuous binding to and stimulation by tumor pMHC I. Moreover, de-sialylated status was required for adoptive CD8 T cells and lymphocytes to decrease GL26 glioma invasiveness and increase host survival in vivo. Finally, increased tumor ST3Gal-II expression correlated with clinical vaccine failure in a meta-analysis of high-grade glioma patients. Conclusions: Taken together, these findings suggest that de-sialylation of CD8 is required for hyper-responsiveness and beneficial anti-glioma activity by CD8 T cells. Because CD8 de-sialylation can be induced with exogenous enzymes (and appears particularly scarce on human T cells), it represents a promising target for clinical glioma vaccine improvement. [ABSTRACT FROM AUTHOR]

Published

2014

32. B7-H1 signaling is integrated during CD8 T cell priming and restrains effector differentiation.

Author

Gibbons, Rachel, Liu, Xin, Harrington, Susan, Krco, Christopher, Kwon, Eugene, and Dong, Haidong

Subjects

*CELLULAR signal transduction, *CD8 antigen, *CANCER cell differentiation, *T cells, *CANCER immunotherapy, *DENDRITIC cells, *CANCER vaccines

Abstract

A promising strategy in tumor immunotherapy is the use of activated dendritic cells as vehicles for tumor vaccines with the goal of activating anti-tumor T cell responses. Current formulations for dendritic cell-based immunotherapies have limited effects on patient survival, providing motivation for further investigation of ways to enhance dendritic cell priming of anti-tumor T cell responses. Using a brief in vitro priming model, we have found that B7-H1 expressed by activated dendritic cells is integrated during priming of naïve CD8 T cells and functions to limit the differentiation of effector T cell responses. CD8 T cells primed by B7-H1-deficient dendritic cells exhibit increased production of IFN-γ, enhanced target cell killing, and improved anti-tumor activity. Additionally, enhanced memory populations arise from CD8 T cells primed by B7-H1-deficient dendritic cells. Based on these findings, we suggest that early blockade of B7-H1 signaling should be investigated as a strategy to improve dendritic cell-based anti-tumor immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2014

33. Effective TRAIL-based immunotherapy requires both plasmacytoid and CD8α dendritic cells.

Author

James, Britnie, Brincks, Erik, Kucaba, Tamara, Boon, Louis, and Griffith, Thomas

Subjects

*IMMUNOTHERAPY, *DENDRITIC cells, *CD8 antigen, *T cells, *IMMUNITY, *TREATMENT effectiveness, *ANTINEOPLASTIC agents, *RENAL cell carcinoma

Abstract

It is now appreciated that there are distinct subsets of dendritic cells (DC) with specialized functions. Plasmacytoid DC (pDC) and CD8α DC can contribute to the priming, activation and function of antitumor CD8 T cells; however, their specific roles and necessity in stimulating antitumor immunity are not clearly understood. We examined the importance of pDC and CD8α DC during immunotherapy of an orthotopic model of metastatic renal cell carcinoma. Immunotherapy that utilizes a recombinant adenovirus encoding tumor necrosis factor-related apoptosis-inducing ligand (Ad5-TRAIL) in combination with an immunostimulatory CpG-containing oligodeoxynucleotide (CpG) resulted in the clearance of primary and metastatic tumors in wild-type (WT) replete BALB/c mice and prolonged survival. In comparison, mice deficient in either pDC (accomplished using a depleting mAb specific for PDCA1) or CD8α DC (through utilization of CD8α DC-deficient Batf3 BALB/c mice) had uncontrolled tumor growth and high mortality after Ad5-TRAIL/CpG administration. The ineffectiveness of Ad5-TRAIL/CpG therapy in the anti-PDCA1-treated and Batf3 BALB/c mice was marked by an altered activation phenotype of the DC, as well as significantly reduced expression of type I IFN-stimulated genes and IL-15/IL-15R complex production. In addition, pDC-depleted and Batf3 BALB/c mice had significantly decreased effector CD8 T cell infiltration in the primary tumor site compared with WT mice after therapy. These data collectively suggest that pDC and CD8α DC carry out independent, but complementary, roles that are necessary to initiate an efficacious antitumor immune response after Ad5-TRAIL/CpG therapy. [ABSTRACT FROM AUTHOR]

Published

2014

34. Self-reactive T cells: suppressing the suppressors.

Author

Becker, Jürgen, Straten, Per, and Andersen, Mads

Subjects

*T cells, *IMMUNE system, *IMMUNOREGULATION, *HOMEOSTASIS, *CYTOTOXIC T cells, *CELLULAR immunity, *CD8 antigen

Abstract

The immune system is a tightly regulated and complex system. An important part of this immune regulation is the assurance of tolerance toward self-antigens to maintain immune homeostasis. However, in recent years, antigen-specific cellular immune responses toward several normal self-proteins expressed in regulatory immune cells have been reported, especially in patients with cancer. The seemingly lack of tolerance toward such proteins is interesting, as it suggests a regulatory function of self-reactive T (srT) cells, which may be important for the fine tuning of the immune system. In particular, surprising has been the description of cytotoxic srT cells that are able to eliminate normal regulatory immune cells. Such srT cells may be important as effector cells that suppress regulatory suppressor cells. The current knowledge of the nature and function of srT cells is still limited. Still, the therapeutic targeting of srT cells offers a novel approach to harness immune-regulatory networks in cancer. [ABSTRACT FROM AUTHOR]

Published

2014

35. Concomitant gemcitabine therapy negatively affects DC vaccine-induced CD8 T-cell and B-cell responses but improves clinical efficacy in a murine pancreatic carcinoma model.

Author

Bauer, Christian, Sterzik, Alexander, Bauernfeind, Franz, Duewell, Peter, Conrad, Claudius, Kiefl, Rosemarie, Endres, Stefan, Eigler, Andreas, Schnurr, Max, and Dauer, Marc

Subjects

*PANCREATIC cancer treatment, *T cells, *CD8 antigen, *CANCER chemotherapy, *CLINICAL trials, *PHARMACODYNAMICS, *LABORATORY mice

Abstract

Background: Multiple studies have shown that dendritic cell (DC)-based vaccines can induce antitumor immunity. Previously, we reported that gemcitabine enhances the efficacy of DC vaccination in a mouse model of pancreatic carcinoma. The present study aimed at investigating the influence of gemcitabine on vaccine-induced anti-tumoral immune responses in a syngeneic pancreatic cancer model. Materials and methods: Subcutaneous or orthotopic pancreatic tumors were induced in C57BL/6 mice using Panc02 cells expressing the model antigen OVA. Bone marrow-derived DC were loaded with soluble OVA protein (OVA-DC). Animals received gemcitabine twice weekly. OVA-specific CD8 T-cells and antibody titers were monitored by FACS analysis and ELISA, respectively. Results: Gemcitabine enhanced clinical efficacy of the OVA-DC vaccine. Interestingly, gemcitabine significantly suppressed the vaccine-induced frequency of antigen-specific CD8 T-cells and antibody titers. DC migration to draining lymph nodes and antigen cross-presentation were unaffected. Despite reduced numbers of tumor-reactive T-cells in peripheral blood, in vivo cytotoxicity assays revealed that cytotoxic T-cell (CTL)-mediated killing was preserved. In vitro assays revealed sensitization of tumor cells to CTL-mediated lysis by gemcitabine. In addition, gemcitabine facilitated recruitment of CD8 T-cells into tumors in DC-vaccinated mice. T- and B-cell suppression by gemcitabine could be avoided by starting chemotherapy after two cycles of DC vaccination. Conclusions: Gemcitabine enhances therapeutic efficacy of DC vaccination despite its negative influence on vaccine-induced T-cell proliferation. Quantitative analysis of tumor-reactive T-cells in peripheral blood may thus not predict vaccination success in the setting of concomitant chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2014

36. Phase I trial of a recombinant yeast-CEA vaccine (GI-6207) in adults with metastatic CEA-expressing carcinoma.

Author

Bilusic, Marijo, Heery, Christopher, Arlen, Philip, Rauckhorst, Myrna, Apelian, David, Tsang, Kwong, Tucker, Jo, Jochems, Caroline, Schlom, Jeffrey, Gulley, James, and Madan, Ravi

Subjects

*CANCER vaccines, *RECOMBINANT microorganisms, *TUMOR proteins, *TUMOR immunology, *CARCINOEMBRYONIC antigen, *CLINICAL trials, *CD8 antigen

Abstract

Yeast-CEA (GI-6207) is a therapeutic cancer vaccine genetically modified to express recombinant carcinoembryonic antigen (CEA) protein, using heat-killed yeast ( Saccharomyces cerevisiae) as a vector. In preclinical studies, yeast-CEA induced a strong immune response to CEA and antitumor responses. Patients received subcutaneous vaccines every 2 weeks for 3 months and then monthly. Patients were enrolled at 3 sequential dose levels: 4, 16, and 40 yeast units (10 yeast particles/unit). Eligible patients were required to have serum CEA > 5 ng/mL or > 20 % CEA tumor block, ECOG PS 0-2, and no history of autoimmunity. Restaging scans were performed at 3 months and then bimonthly. Peripheral blood was collected for the analysis of immune response (e.g., by ELISPOT assay). Twenty-five patients with metastatic CEA-expressing carcinomas were enrolled. Median patient age was 52 (range 39-81). A total of 135 vaccines were administered. The vaccine was well tolerated, and the most common adverse event was grade 1/2 injection-site reaction. Five patients had stable disease beyond 3 months (range 3.5-18 months), and each had CEA stabilization while on-study. Some patients showed evidence post-vaccination of increases in antigen-specific CD8 T cells and CD4 T lymphocytes and decreases in regulatory T cells. Of note, a patient with medullary thyroid cancer had substantial T cell responses and a vigorous inflammatory reaction at sites of metastatic disease. Yeast-CEA vaccination had minimal toxicity and induced some antigen-specific T cell responses and CEA stabilization in a heterogeneous, heavily pre-treated patient population. Further studies are required to determine the clinical benefit of yeast-CEA vaccination. [ABSTRACT FROM AUTHOR]

Published

2014

37. Type I interferons induced by radiation therapy mediate recruitment and effector function of CD8 T cells.

Author

Lim, Joanne, Gerber, Scott, Murphy, Shawn, and Lord, Edith

Subjects

*CANCER radiotherapy, *INTERFERONS, *CD8 antigen, *T cells, *CANCER immunology, *DENDRITIC cells, *HEALTH outcome assessment

Abstract

The need for an intact immune system for cancer radiation therapy to be effective suggests that radiation not only acts directly on the tumor but also indirectly, through the activation of host immune components. Recent studies demonstrated that endogenous type I interferons (type I IFNs) play a role in radiation-mediated anti-tumor immunity by enhancing the ability of dendritic cells to cross-prime CD8 T cells. However, it is still unclear to what extent endogenous type I IFNs contribute to the recruitment and function of CD8 T cells. Little is also known about the effects of type I IFNs on myeloid cells. In the current study, we demonstrate that type I and type II IFNs (IFN-γ) are both required for the increased production of CXCL10 (IP-10) chemokine by myeloid cells within the tumor after radiation treatment. Radiation-induced intratumoral IP-10 levels in turn correlate with tumor-infiltrating CD8 T cell numbers. Moreover, type I IFNs promote potent tumor-reactive CD8 T cells by directly affecting the phenotype, effector molecule production, and enhancing cytolytic activity. Using a unique inducible expression system to increase local levels of IFN-α exogenously, we show here that the capacity of radiation therapy to result in tumor control can be enhanced. Our preclinical approach to study the effects of local increase in IFN-α levels can be used to further optimize the combination therapy strategy in terms of dosing and scheduling, which may lead to better clinical outcome. [ABSTRACT FROM AUTHOR]

Published

2014

38. Critical role of spatial interaction between CD8 and Foxp3 cells in human gastric cancer: the distance matters.

Author

Feichtenbeiner, Anita, Haas, Matthias, Büttner, Maike, Grabenbauer, Gerhard, Fietkau, Rainer, and Distel, Luitpold

Subjects

*STOMACH cancer treatment, *CD8 antigen, *FORKHEAD transcription factors, *PROTEIN-protein interactions, *CELL communication, *T cells, *HEALTH outcome assessment, *CANCER immunology

Abstract

Purpose: In various cancer types, an abundance of FoxP3 regulatory T cells (Treg) has been associated with an unfavorable outcome. Yet, the role of Treg on cancer immunity has been shown to be complex. In single cell marker technique, other tumor-infiltrating lymphocytes (TILs) such as cytotoxic CD8 T cells (CTL) also influenced prognosis. This study for the first time investigates the concurrent spatial distribution pattern of CD8 and FoxP3 TILs and their prognostic impact in human gastric cancer. Materials and methods: Tumor tissue microarrays of 50 patients with surgically treated adenocarcinoma of the cardia were studied. An immunohistochemical double staining of CD8 and FoxP3 TILs was performed. Cell counts and cell-to-cell distances in tumor epithelium and stroma were evaluated with image-processing software. Metastasis-free survival, no-evidence-of-disease survival, and overall survival were investigated (mean follow-up time 6.9 years). Results: High intraepithelial infiltration of CD8 and FoxP3 TIL was associated with the improved 10-year metastasis-free survival (83 vs. 54 %, p = 0.04 and 85 vs. 59 %, p = 0.09, respectively). Considering cell-to-cell distance and comparing patients with functional (30-110 μm) versus nonfunctional distances of CD8 and FoxP3 TILs, 10-year survival rates differed between 89 and 55 % ( p = 0.009), respectively. Conclusion: Prognostic influence of tumor-infiltrating immune cells in gastric cancer critically depends on their cell-to-cell distance. FoxP3 TILs must be located within a distance between 30 and 110 μm of CD8 T cells to positively impact on prognosis. [ABSTRACT FROM AUTHOR]

Published

2014

39. CD8+ T-cell priming and boosting: more antigen-presenting DC, or more antigen per DC?

Author

Schaft, Niels, Wellner, Verena, Wohn, Christian, Schuler, Gerold, and Dörrie, Jan

Subjects

*CD8 antigen, *T cells, *ANTIGEN presenting cells, *DENDRITIC cells, *ANTIGENS, *CANCER vaccines, *ELECTROPORATION therapy, *GENE transfection

Abstract

RNA transfection is a standard method to load dendritic cells (DC) with antigen for therapeutic cancer vaccination. While electroporation yields high transfection efficiency and satisfying expression levels, lipofection results in only few cells expressing high amounts of antigen. We compared antigen loading of human monocyte-derived DC by MelanA RNA electroporation and lipofection. No differences in phenotype or migrational capacity were detected, but lipofected DC induced stronger cytokine secretion by antigen-specific T cells and were superior in priming and boosting of MelanA-specific CD8 + T cells. Interestingly, T cells stimulated with the differently transfected DC did not differ in their functional avidity. To determine whether the amount of antigen per cell is indeed responsible for the superiority of the lipofected DC, we increased the amount of MelanA RNA fivefold and mixed those DC with mock-electroporated ones to mimic the antigen distribution of lipofected cells. This significantly improved the stimulatory capacity, indicating that indeed the amount of antigen per cell seems to be the responsible feature for the observed superiority of lipofected DCs. These data suggest that a few DC that express high amounts of antigen are more immunogenic than many DC expressing lower amounts, although this needs to be tested in a two-armed immunogenicity trial. [ABSTRACT FROM AUTHOR]

Published

2013

40. Expanded CD8 T cells of murine and human CLL are driven into a senescent KLRG1 effector memory phenotype.

Author

Göthert, Joachim, Eisele, Lewin, Klein-Hitpass, Ludger, Weber, Stefanie, Zesewitz, Marie-Louise, Sellmann, Ludger, Röth, Alexander, Pircher, Hanspeter, Dührsen, Ulrich, and Dürig, Jan

Subjects

*CD8 antigen, *CHRONIC lymphocytic leukemia, *KILLER cell receptors, *PHENOTYPES, *GENE expression, *T cell receptors, *CADHERINS, *PATIENTS

Abstract

Altered numbers and functions of T cells have previously been demonstrated in chronic lymphocytic leukemia (CLL) patients. However, dynamics and specific T-cell subset alterations have not been studied in great detail. Therefore, we studied CLL blood lymphocyte subsets of individual patients in a longitudinal manner. Dynamic expansions of blood CD4 and CD8 T-cell numbers were consistently associated with a progressively increasing CLL leukemic compartment. Interestingly, the T-cell subset expansion over time was more pronounced in CD38 CLL. Additionally, we performed gene expression profiling of CD3 T cells of CLL patients and normal donors. Using gene set enrichment analysis, we found significant enrichment of genes with higher expression in CLL T cells within CD8 effector memory and terminal effector T-cell gene signatures. In agreement with these data, we observed a marked expansion of phenotypic CD8 effector memory T cells in CLL by flow cytometry. Moreover, we observed that increments of CD8 effector memory T cells in human CLL and also mouse CLL (Eμ-TCL1 model) were due to an expansion of the inhibitory killer cell lectin-like receptor G1 (KLRG1) expressing cellular subset. Furthermore, higher plasma levels of the natural KLRG1 ligand E-cadherin were detected in CLL patients compared to normal donor controls. The predominance of KLRG1 expression within CD8 T cells in conjunction with increased systemic soluble E-cadherin might significantly contribute to CLL immune dysfunction and might additionally represent an important component of the CLL microenvironment. [ABSTRACT FROM AUTHOR]

Published

2013

41. A novel recombinant protein of IP10-EGFRvIIIscFv and CD8 cytotoxic T lymphocytes synergistically inhibits the growth of implanted glioma in mice.

Author

Wang, Xuan, Lu, Xiao-Ling, Zhao, Hong-Yang, Zhang, Fang-Cheng, and Jiang, Xiao-Bing

Subjects

*RECOMBINANT proteins, *CD8 antigen, *CYTOTOXIC T cells, *CANCER immunotherapy, *GLIOMA treatment, *EPIDERMAL growth factor receptors, *GENE expression, *LABORATORY mice

Abstract

The epidermal growth factor receptor (EGFR) mutant of EGFRvIII is highly expressed on glioma cells and has been thought to be an excellent target molecule for immunotherapy. IP-10 is a potent chemokine and can recruit CXCR3 T cells, including CD8 T cells that are important for the control of tumor growth. This study is aimed at investigating the therapeutic efficacy of a novel fusion protein of IP10-EGFRvIIIscFv (IP10-scFv) in combination with glioma lysate-pulsed DCs-activated CD8 cytotoxic T lymphocytes (CTLs) in a mouse model of glioma. A plasmid of pET-IP10-scFv was generated by linking mouse IP-10 gene with the DNA fragment for anti-EGFRvIIIscFv, a (GlySer) flexible linker and a His-tag. The recombinant IP10-scFv in E. coli was purified by affinity chromatography and characterized for its anti-EGFRvIII immunoreactivity and chemotactic activity. C57BL/6 mice were inoculated with mouse glioma GL261 cells in the brain and treated intracranially with IP10-scFv and/or intravenously with CTL for evaluating the therapeutic effect. The glioma-specific immune responses were examined. The IP10-scFv retained anti-EGFRvIII immunoreactivity and IP-10-like chemotactic activity. Treatment with both IP10-scFv and CTL synergistically inhibited the growth of glioma and prolonged the survival of tumor-bearing mice, accompanied by increasing the numbers of brain-infiltrating lymphocytes (BILs) and the frequency of CXCR3CD8 T cells, enhancing glioma-specific IFN-γ responses and cytotoxicity, and promoting glioma cell apoptosis in mice. Our novel data indicate that IP10-scFv and CTL have synergistic therapeutic effects on inhibiting the growth of mouse glioma in vivo. [ABSTRACT FROM AUTHOR]

Published

2013

42. Elevated level of peripheral CD8CD28 T lymphocytes are an independent predictor of progression-free survival in patients with metastatic breast cancer during the course of chemotherapy.

Author

Song, Guohong, Wang, Xiaoli, Jia, Jun, Yuan, Yanhua, Wan, Fengling, Zhou, Xinna, Yang, Huabing, Ren, Jun, Gu, Jiezhun, and Lyerly, Herbert

Subjects

*BREAST cancer patients, *T cells, *CANCER chemotherapy, *CD8 antigen, *CD28 antigen, *METASTASIS, *CELLULAR immunity, *CARCINOGENESIS

Abstract

Purpose: Suppression of cellular immunity resulting from tumorigenesis and/or therapy might promote cancer cells' growth, progression and invasion. Here, we explored whether T lymphocyte subtypes from peripheral blood of metastatic breast cancer (MBC) female patients could be used as alternative surrogate markers for cancer progress. Additionally, plasma levels of interleukin (IL)-2, IL-4, IL-6, IL-10, IFN-γ, and transforming growth factor-β1 were quantitated from MBC and healthy volunteers. Experimental design: This study included 89 female MBC patients during the post-salvage chemotherapy follow-up and 50 age- and sex-matched healthy volunteers as control. The percentages of T lymphocyte subpopulations from peripheral blood and plasma levels of cytokines were measured. Results: Both CD8CD28 and CD4CD25 were elevated in MBC patients compared to the control cohort ( P < 0.05). In contrast, CD3 and CD8CD28cells were significantly lower in MBC patients ( P < 0.0001, P = 0.045, respectively). MBC patients had elevated levels of immunosuppressive cytokines IL-6 and IL-10. Patients with elevated CD8CD28 and CD4CD25 cells showed increased levels of IL-6, and only patients with elevated CD8CD28 had decreased interferon-γ. Univariate analysis indicated increased CD3CD4 or CD8CD28correlated with prolonged progression-free survival (PFS), while elevated CD8CD28associated with shorten PFS. The percent of CD8CD28 T lymphocytes is an independent predictor for PFS through multivariate analysis. Conclusions: This study suggests that progressive elevated levels of CD8CD28 suppressor T lymphocytes represent a novel independent predictor of PFS during post-chemotherapy follow-up. [ABSTRACT FROM AUTHOR]

Published

2013

43. Long-term survival and immunological parameters in metastatic melanoma patients who responded to ipilimumab 10 mg/kg within an expanded access programme.

Author

Di Giacomo, Anna, Calabrò, Luana, Danielli, Riccardo, Fonsatti, Ester, Bertocci, Erica, Pesce, Isabella, Fazio, Carolina, Cutaia, Ornella, Giannarelli, Diana, Miracco, Clelia, Biagioli, Maurizio, Altomonte, Maresa, and Maio, Michele

Subjects

*METASTASIS, *MELANOMA, *IPILIMUMAB, *BIOMARKERS, *CD4 antigen, *CD8 antigen, *T cells, *PATIENTS

Abstract

Background: Ipilimumab can result in durable clinical responses among patients with advanced melanoma. However, no predictive marker of clinical activity has yet been identified. We provide preliminary data describing the correlation between immunological parameters and response/survival among patients with advanced melanoma who received ipilimumab 10 mg/kg in an expanded access programme. Methods: Patients received ipilimumab 10 mg/kg every 3 weeks (Q3W) for four doses (induction) and Q12W from week 24 (W24) as maintenance therapy. Tumor assessments were conducted Q12W. Expression of inducible T cell costimulator (ICOS) on CD4 and CD8 T cells was assessed at baseline, W7, W12 and W24, and the ratio between absolute neutrophils (N) and lymphocytes (L) determined at baseline, W4, W7 and W10. Results: Median overall survival among 27 patients was 9.6 months (95 % CI 3.2-16.1), with 3- and 4-year survival rates of 20.4 %. Five patients survived >4 years. Patients with an increase in the number of circulating ICOS T cells at W7 were more likely to experience disease control and have improved survival. An N/L ratio below the median at W7 and W10 was also associated with better survival compared with an N/L ratio above the median. Conclusions: Ipilimumab can induce long-term survival benefits in heavily pretreated patients with metastatic melanoma. Changes in the number of circulating ICOS T cells or N/L ratio during ipilimumab treatment may represent early markers of response. However, given the limited sample size, further investigation is required. [ABSTRACT FROM AUTHOR]

Published

2013

44. CD39 is highly involved in mediating the suppression activity of tumor-infiltrating CD8+ T regulatory lymphocytes.

Author

Parodi, Alessia, Battaglia, Florinda, Kalli, Francesca, Ferrera, Francesca, Conteduca, Giuseppina, Tardito, Samuele, Stringara, Silvia, Ivaldi, Federico, Negrini, Simone, Borgonovo, Giacomo, Simonato, Alchiede, Traverso, Paolo, Carmignani, Giorgio, Fenoglio, Daniela, and Filaci, Gilberto

Subjects

*CD8 antigen, *EXTRACELLULAR enzymes, *T cells, *IMMUNOSUPPRESSION, *ADENOSINE triphosphate, *GENE expression, *BIOCHEMICAL mechanism of action

Abstract

CD39 is an ectoenzyme, present on different immune cell subsets, which mediates immunosuppressive functions catalyzing ATP degradation. It is not known whether CD39 is expressed and implicated in the activity of CD8+ regulatory T lymphocytes (Treg). In this study, CD39 expression and function was analyzed in both CD8+ and CD4+CD25 Treg from the peripheral blood of healthy donors as well as from tumor specimens. CD39 was found expressed by both CD8+ (from the majority of healthy donors and tumor patients) and CD4+CD25 Treg, and CD39 expression correlated with suppression activity mediated by CD8+ Treg. Importantly, CD39 counteraction remarkably inhibited the suppression activity of CD8+ Treg (both from peripheral blood and tumor microenvironment) suggesting that CD39-mediated inhibition constitutes a prevalent hallmark of their function. Collectively, these findings, unveiling a new mechanism of action for CD8+ Treg, provide new knowledge on intratumoral molecular pathways related to tumor immune escape, which could be exploited in the future for designing new biological tools for anticancer immune intervention. [ABSTRACT FROM AUTHOR]

Published

2013

45. Peripheral CD8 T cell proliferation is prognostic for patients with advanced thoracic malignancies.

Author

McCoy, Melanie, Nowak, Anna, Most, Robbert, Dick, Ian, and Lake, Richard

Subjects

*CD8 antigen, *CANCER cell proliferation, *T cells, *CHEST diseases, *CANCER prognosis, *IMMUNE system, *HEALTH outcome assessment, *MESOTHELIOMA

Abstract

There is a complex interplay between the immune system and a developing tumor that is manifest in the way that the balance of T cell subsets in the local tumor environment reflects clinical outcome. Tumor infiltration by CD8 T cells and regulatory T cells (Treg) is associated with improved and reduced survival, respectively, in many cancer types. However, little is known of the prognostic value of immunological parameters measured in peripheral blood. In this study, peripheral CD8 T cells and Treg from 43 patients with malignant mesothelioma or advanced non-small-cell lung cancer scheduled to commence palliative chemotherapy were assessed by flow cytometry and evaluated for association with patient survival. Patients had a higher proportion of peripheral Treg, proliferating CD8 T cells and CD8 T cells with an activated effector phenotype compared with age-matched healthy controls. Higher proportions of Treg and proliferating CD8 T cells were both associated with poor survival in univariate analyses (hazard ratio [HR] 3.81, 95 % CI 1.69-8.57; p < 0.01 and HR 2.86, 95 % CI 1.26-6.50; p < 0.05, respectively). CD8 T cell proliferation was independently predictive of reduced survival in multivariate analysis (HR 2.58, 95 % CI 1.01-6.61; p < 0.05). These findings suggest that peripheral CD8 T cell proliferation can be a useful prognostic marker in patients with thoracic malignancies planned for palliative chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2013

46. Mimicking homeostatic proliferation in vitro generates T cells with high anti-tumor function in non-lymphopenic hosts.

Author

Kaiser, Andrew, Gadiot, Jules, Guislain, Aurelie, and Blank, Christian

Subjects

*HOMEOSTASIS, *CANCER cell proliferation, *T cells, *ANTINEOPLASTIC agents, *LYMPHOPENIA, *CD8 antigen, *HUMAN phenotype

Abstract

CD8 T cells undergoing homeostatic proliferation (HP) in a lymphopenic environment acquire a central memory-like phenotype (CD44 CD62L Ly6c). Such cells are readily functional in vitro, with a strong capacity to secrete IFNγ and IL-2 and to lyse target cells upon antigen recognition. In vivo, these memory-like T cells display potent anti-tumor reactivity. When addressing whether these remarkable properties were 'acquired' or dependent on sustained HP, we observed, for the first time, that memory-like T cells retained full anti-tumor functions even when removed from their lymphopenic environment and retransferred into non-lymphopenic P14/Rag2 recipients (where HP is prevented). Moreover, memory-like T cells were superior to in vitro expanded effector T cells. We next sought to determine the conditions required to reproduce such a potent phenotype in vitro, in order to obtain optimal cells for adoptive cell transfer therapy. Assessing ex vivo lymph node cultures, dendritic cells, fibroblastic reticular cells, and HP-associated cytokines, we found that stimulation of naïve T cells with anti-CD3/CD28 beads and IL-15 (IL-7 was dispensable) led to the generation of memory-like T cell with a similar phenotype. Both in vitro and in vivo memory-like T cells retained the capacity to efficiently control tumor growth in non-lymphopenic hosts upon adoptive cell transfer. A similar phenotype could be imparted to human peripheral blood leukocytes with comparable culture conditions. Our data reinforce the idea that in vitro -generated memory-like T cells could benefit adoptive cell transfer therapies. [ABSTRACT FROM AUTHOR]

Published

2013

47. Distinct in vivo CD8 and CD4 T cell responses against normal and malignant tissues.

Author

Coe, David, Addey, Caroline, White, Matthew, Harwood, Nida, Dyson, Julian, and Chai, Jian-Guo

Subjects

*CD8 antigen, *T cells, *IMMUNE response, *TISSUES, *SKIN grafting, *CANCER immunotherapy

Abstract

Normal tissue and tumour grafts expressing the same alloantigens often elicit distinct immune responses whereby only normal tissue is rejected. To investigate the mechanisms that underlie these distinct outcomes, we compared the responses of adoptively transferred HY-specific conventional (CD8 and CD4) or regulatory T (Treg) cells in mice bearing HY-expressing tumour, syngeneic male skin graft or both. For local T cell priming, T cell re-circulation, graft localization and retention, skin grafts were more efficient than tumours. Skin grafts were also capable of differentiating CD4 T cells into functional Th1 cells. Donor T cell responses were inversely correlated with tumour progression. When skin graft and tumour transplants were performed sequentially, contemporary graft and tumour burden enhanced CD8 but reduced CD4 T cell responses causing accelerated skin-graft rejection without influencing tumour growth. Although both skin grafts and tumours were able to expand HY-specific Treg cells in draining lymph node (dLN), the proportion of tumour-infiltrating Treg cells was significantly higher than that within skin grafts, correlating with accelerated tumour growth. Moreover, there was a higher level of HY antigen presentation by host APC in tumour-dLN than in graft-dLN. Finally, tumour tissues expressed a significant higher level of IDO, TGFβ, IL10 and Arginase I than skin grafts, indicating that malignant but not normal tissue represents a stronger immunosuppressive environment. These comparisons provide important insight into the in vivo mechanisms that conspire to compromise tumour-specific adaptive immunity and identify new targets for cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2013

48. The simultaneous ex vivo detection of low-frequency antigen-specific CD4+ and CD8+ T-cell responses using overlapping peptide pools.

Author

Singh, Satwinder, Meyering, Maaike, Ramwadhdoebe, Tamara, Stynenbosch, Linda, Redeker, Anke, Kuppen, Peter, Melief, Cornelis, Welters, Marij, and Burg, Sjoerd

Subjects

*CD4 antigen, *CD8 antigen, *T cells, *PEPTIDES, *CYTOKINES, *CANCER immunotherapy, *CANCER vaccines

Abstract

The ability to measure antigen-specific T cells at the single-cell level by intracellular cytokine staining (ICS) is a promising immunomonitoring tool and is extensively applied in the evaluation of immunotherapy of cancer. The protocols used to detect antigen-specific CD8+ T-cell responses generally work for the detection of antigen-specific T cells in samples that have undergone at least one round of in vitro pre-stimulation. Application of a common protocol but now using long peptides as antigens was not suitable to simultaneously detect antigen-specific CD8+ and CD4+ T cells directly ex vivo in cryopreserved samples. CD8 T-cell reactivity to monocytes pulsed with long peptides as antigens ranged between 5 and 25 % of that observed against monocytes pulsed with a direct HLA class I fitting minimal CTL peptide epitope. Therefore, we adapted our ICS protocol and show that the use of tenfold higher concentration of long peptides to load APC, the use of IFN-α and poly(I:C) to promote antigen processing and improve T-cell stimulation, does allow for the ex vivo detection of low-frequency antigen-specific CD8+ and CD4+ T cells in an HLA-independent setting. While most of the improvements were related to increasing the ability to measure CD8+ T-cell reactivity following stimulation with long peptides to at least 50 % of the response detected when using a minimal peptide epitope, the final analysis of blood samples from vaccinated patients successfully showed that the adapted ICS protocol also increases the ability to ex vivo detect low-frequency p53-specific CD4+ T-cell responses in cryopreserved PBMC samples. [ABSTRACT FROM AUTHOR]

Published

2012

49. Intratumoral electroporation of IL-12 cDNA eradicates established melanomas by Trp2-specific CD8+ CTLs in a perforin/granzyme-mediated and IFN-γ-dependent manner: application of Trp2 peptides.

Author

Sin, Jeong-Im, Park, Jae-Bok, Lee, In, Park, Daehan, Choi, Youn, Choe, Jongseon, and Celis, Esteban

Subjects

*ELECTROPORATION, *INTERLEUKIN-12, *ANTISENSE DNA, *MELANOMA treatment, *CD8 antigen, *PERFORINS, *GRANZYMES, *PEPTIDES

Abstract

Intratumoral electroporation (IT-EP) with IL-12 cDNA (IT-EP/IL12) can lead to the eradication of established B16 melanoma tumors in mice. Here, we explore the immunological mechanism of the antitumor effects generated by this therapy. The results show that IT-EP/IL12 applied only once resulted in eradication in 70% animals with large established B16 tumors. Tumor eradication required the participation of CD8+ T cells, but not CD4+ T cells and NK cells. IT-EP/IL12 induced antigen-specific CD8+ T cell responses against the immunodominant Trp2 epitope and generated a systemic response, resulting in significant therapeutic effects against distal, untreated tumors. The therapeutic effect of IT-EP/IL12 was absent in perforin-deficient mice, indicating that tumor elimination occurred through conventional perforin/granzyme lysis by CTLs. Moreover, this therapy induced some degree of immunological memory that protected approximately one-third of the cured mice against a subsequent tumor challenge. Moreover, antitumor efficacy and long-term protection against B16 were significantly improved by concurrent Trp2 peptide immunization through more induction of Ag-specific CTL responses and more attraction of IFN-γ-expressing CD8+ T cells into tumor sites. The antitumor effect of IT-EP/IL12 required the participation of IFN-γ, which was shown to induce MHC class I expression on B16 cells and increase the lytic activity of the CD8+ CTL generated by IT-EP/IL12. The results from these animal studies may help in the development of IT-EP/IL12 for cancer patients. [ABSTRACT FROM AUTHOR]

Published

2012

50. TriVax-HPV: an improved peptide-based therapeutic vaccination strategy against human papillomavirus-induced cancers.

Author

Barrios, Kelly and Celis, Esteban

Subjects

*PAPILLOMAVIRUSES, *CERVICAL cancer, *CD8 antigen, *AUTOIMMUNITY, *VACCINATION, *IMMUNE response, *ANIMAL models in research, *LABORATORY mice

Abstract

Background: Therapeutic vaccines for cancer are an attractive alternative to conventional therapies, since the later result in serious adverse effects and in most cases are not effective against advanced disease. Human papillomavirus (HPV) is responsible for several malignancies such as cervical carcinoma. Vaccines targeting oncogenic viral proteins like HPV16-E6 and HPV16-E7 are ideal candidates to elicit strong immune responses without generating autoimmunity because: (1) these products are not expressed in normal cells and (2) their expression is required to maintain the malignant phenotype. Our group has developed peptide vaccination strategy called TriVax, which is effective in generating vast numbers of antigen-specific T cells in mice capable of persisting for long time periods. Materials and methods: We have used two HPV-induced mouse cancer models (TC-1 and C3.43) to evaluate the immunogenicity and therapeutic efficacy of TriVax prepared with the immunodominant CD8 T-cell epitope HPV16-E7, mixed with poly-IC adjuvant and costimulatory anti-CD40 antibodies. Results: TriVax using HPV16-E7 induced large and persistent T-cell responses that were therapeutically effective against established HPV16-E7 expressing tumors. In most cases, TriVax was successful in attaining complete rejections of 6-11-day established tumors. In addition, TriVax induced long-term immunological memory, which prevented tumor recurrences. The anti-tumor effects of TriVax were independent of NK and CD4 T cells and, surprisingly, did not rely to a great extent on type-I or type-II interferon. Conclusions: These findings indicate that the TriVax strategy is an appealing immunotherapeutic approach for the treatment of established viral-induced tumors. We believe that these studies may help to launch more effective and less invasive therapeutic vaccines for HPV-mediated malignancies. [ABSTRACT FROM AUTHOR]

Published

2012