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Impact of Immunotherapy after Resection of Pancreatic Cancer.胰腺癌切除术后免疫治疗的影响。
J Am Coll Surg. 2019 Jul;229(1):19-27.e1. doi: 10.1016/j.jamcollsurg.2019.01.016. Epub 2019 Feb 10.
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Anti-cancer Therapies Employing IL-2 Cytokine Tumor Targeting: Contribution of Innate, Adaptive and Immunosuppressive Cells in the Anti-tumor Efficacy.采用 IL-2 细胞因子靶向肿瘤的抗癌疗法:固有、适应性和免疫抑制细胞在抗肿瘤疗效中的贡献。
Front Immunol. 2018 Dec 18;9:2905. doi: 10.3389/fimmu.2018.02905. eCollection 2018.
4
Vaccination With Mitoxantrone-Treated Primary Colon Cancer Cells Enhances Tumor-Infiltrating Lymphocytes and Clinical Responses in Colorectal Liver Metastases.用米托蒽醌处理的原发性结肠癌细胞进行免疫接种可增强结直肠癌肝转移灶中的肿瘤浸润淋巴细胞并改善临床应答。
J Surg Res. 2019 Jan;233:57-64. doi: 10.1016/j.jss.2018.07.068. Epub 2018 Aug 17.
5
Critical role of OX40 signaling in the TCR-independent phase of human and murine thymic Treg generation.OX40 信号在人类和鼠类胸腺 Treg 产生的 TCR 非依赖性阶段的关键作用。
Cell Mol Immunol. 2019 Feb;16(2):138-153. doi: 10.1038/cmi.2018.8. Epub 2018 Mar 26.
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PKC-ѳ is dispensable for OX40L-induced TCR-independent Treg proliferation but contributes by enabling IL-2 production from effector T-cells.PKC-ѳ 对于 OX40L 诱导的 TCR 非依赖性 Treg 增殖是可有可无的,但它通过促进效应 T 细胞产生 IL-2 而做出贡献。
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Utilization and impact of adjuvant chemotherapy among patients with resected stage II colon cancer: a multi-institutional analysis.辅助化疗在II期结肠癌切除患者中的应用及影响:一项多机构分析
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Cytotherapy. 2017 Jun;19(6):689-702. doi: 10.1016/j.jcyt.2017.03.067. Epub 2017 Apr 11.
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LIGHT Elevation Enhances Immune Eradication of Colon Cancer Metastases.光增强促进结肠癌转移灶的免疫清除。
Cancer Res. 2017 Apr 15;77(8):1880-1891. doi: 10.1158/0008-5472.CAN-16-1655. Epub 2017 Mar 1.

LIGHT 与白细胞介素-2 联合免疫疗法可增加体内 CD8 中央记忆 T 细胞。

Combination Immunotherapy With LIGHT and Interleukin-2 Increases CD8 Central Memory T-Cells In Vivo.

机构信息

Division of Surgical Oncology, Department of Surgery, University of Illinois at Chicago, Chicago, Illinois.

Division of Surgical Oncology, Department of Surgery, University of Illinois at Chicago, Chicago, Illinois.

出版信息

J Surg Res. 2021 Jul;263:44-52. doi: 10.1016/j.jss.2021.01.010. Epub 2021 Feb 22.

DOI:10.1016/j.jss.2021.01.010
PMID:33631377
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8169541/
Abstract

BACKGROUND

The generation of long-term durable tumor immunity and prolonged disease-free survival depends on the ability to generate and support CD8+ central memory T-cells. Microsatellite-stable colon cancer is resistant to currently available immunotherapies; thus, development of novel mechanisms to increase both lymphocyte infiltration and central memory formation are needed to improve outcomes in these patients. We have previously demonstrated that both interleukin-2 (IL-2) and LIGHT (TNFSF14) independently enhance antitumor immune responses and hypothesize that combination immunotherapy may increase the CD8+ central memory T-cell response.

METHODS

Murine colorectal cancer tumors were established in syngeneic mice. Tumors were treated with control, soluble, or liposomal IL-2 at established intervals. A subset of animal tumors overexpressed tumor necrosis superfamily factor LIGHT (TNFSF14). Peripheral blood, splenic, and tumor-infiltrating lymphocytes were isolated for phenotypic studies and flow cytometry.

RESULTS

Tumors exposed to a combination of LIGHT and IL-2 experienced a decrease in tumor size compared with IL-2 alone that was not demonstrated in wild-type tumors or between other treatment groups. Combination exposure also increased splenic central memory CD8+ cells compared with IL-2 administration alone, while not increasing tumor-infiltrating lymphocytes. In the periphery, the combination enhanced levels of circulating CD8 T-cells and central memory T-cells, while also increasing circulating T-regulatory cells.

CONCLUSIONS

Combination of IL-2, whether soluble or liposomal, with exposure to LIGHT results in increased CD8+ central memory cells in the spleen and periphery. New combination immunotherapy strategies that support both effector and memory T-cell functions are critical to enhancing durable antitumor responses and warrant further investigation.

摘要

背景

长期持久的肿瘤免疫和无病生存的延长取决于产生和支持 CD8+中央记忆 T 细胞的能力。微卫星稳定的结肠癌对目前可用的免疫疗法有抵抗力;因此,需要开发新的机制来增加淋巴细胞浸润和中央记忆形成,以改善这些患者的预后。我们之前已经证明,白细胞介素-2 (IL-2) 和 LIGHT (TNFSF14) 都可以独立增强抗肿瘤免疫反应,并假设联合免疫疗法可以增加 CD8+中央记忆 T 细胞反应。

方法

在同基因小鼠中建立了鼠结直肠癌细胞肿瘤。肿瘤用对照、可溶性或脂质体 IL-2 以既定间隔进行治疗。一部分动物肿瘤过表达肿瘤坏死超家族因子 LIGHT (TNFSF14)。分离外周血、脾和肿瘤浸润淋巴细胞进行表型研究和流式细胞术分析。

结果

与单独使用 IL-2 相比,暴露于 LIGHT 和 IL-2 联合治疗的肿瘤体积减小,而野生型肿瘤或其他治疗组之间则没有这种情况。联合暴露还增加了脾中央记忆 CD8+细胞,而单独使用 IL-2 则没有增加肿瘤浸润淋巴细胞。在体外,联合治疗增强了循环 CD8 T 细胞和中央记忆 T 细胞的水平,同时也增加了循环 T 调节细胞。

结论

IL-2(无论是可溶性还是脂质体)与 LIGHT 的联合暴露导致脾和外周血中 CD8+中央记忆细胞增加。支持效应和记忆 T 细胞功能的新联合免疫治疗策略对于增强持久的抗肿瘤反应至关重要,值得进一步研究。