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Mycobacterium tuberculosis Lipoprotein and Lipoglycan Binding to Toll-Like Receptor 2 Correlates with Agonist Activity and Functional Outcomes.结核分枝杆菌脂蛋白和脂阿拉伯甘露聚糖与 Toll 样受体 2 的结合与激动剂活性和功能结果相关。
Infect Immun. 2018 Sep 21;86(10). doi: 10.1128/IAI.00450-18. Print 2018 Oct.
2
Flagellin is a Th1 polarizing factor for human CD4 T cells and induces protection in a murine neonatal vaccination model of rotavirus infection.鞭毛蛋白是人类 CD4 T 细胞的 Th1 极化因子,并在轮状病毒感染的小鼠新生疫苗接种模型中诱导保护作用。
Vaccine. 2018 Jul 5;36(29):4188-4197. doi: 10.1016/j.vaccine.2018.06.005. Epub 2018 Jun 8.
3
PPE60 antigen drives Th1/Th17 responses via Toll-like receptor 2-dependent maturation of dendritic cells.PPE60 抗原通过 Toll 样受体 2 依赖性树突状细胞成熟驱动 Th1/Th17 反应。
J Biol Chem. 2018 Jun 29;293(26):10287-10302. doi: 10.1074/jbc.RA118.001696. Epub 2018 May 8.
4
Fibroblastic reticular cells of the lymphoid tissues modulate T cell activation threshold during homeostasis via hyperactive cyclooxygenase-2/prostaglandin E axis.淋巴组织的纤维母细胞网状细胞通过高活性环氧化酶-2/前列腺素 E 轴在体内平衡时调节 T 细胞激活阈值。
Sci Rep. 2017 Jun 13;7(1):3350. doi: 10.1038/s41598-017-03459-5.
5
Alternative BCG delivery strategies improve protection against Mycobacterium tuberculosis in non-human primates: Protection associated with mycobacterial antigen-specific CD4 effector memory T-cell populations.替代卡介苗接种策略可增强非人灵长类动物对结核分枝杆菌的抵抗力:与分枝杆菌抗原特异性CD4效应记忆T细胞群体相关的抵抗力。
Tuberculosis (Edinb). 2016 Dec;101:174-190. doi: 10.1016/j.tube.2016.09.004. Epub 2016 Oct 8.
6
From discovery to licensure, the Adjuvant System story.从发现到获批上市,佐剂系统的故事。
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Different human vaccine adjuvants promote distinct antigen-independent immunological signatures tailored to different pathogens.不同的人用疫苗佐剂可促进针对不同病原体定制的独特的抗原非依赖性免疫特征。
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Lymph node fibroblastic reticular cells in health and disease.健康与疾病状态下的淋巴结成纤维细胞网状细胞
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Batf3-dependent CD103+ dendritic cells are major producers of IL-12 that drive local Th1 immunity against Leishmania major infection in mice.Batf3 依赖性 CD103+树突状细胞是产生 IL-12 的主要细胞,可驱动针对小鼠 Leishmania major 感染的局部 Th1 免疫。
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TLR2 激动剂在皮肤免疫接种过程中对 Th1 细胞的初始激活的抑制作用是由募集的 CCR2 单核细胞介导的。

Suppression of Th1 Priming by TLR2 Agonists during Cutaneous Immunization Is Mediated by Recruited CCR2 Monocytes.

机构信息

Department of Microbiology and Immunology, Albert Einstein College of Medicine, Bronx, NY 10461.

Department of Microbiology and Immunology, University of Minnesota, Minneapolis, MN 55455.

出版信息

J Immunol. 2018 Dec 15;201(12):3604-3616. doi: 10.4049/jimmunol.1801185. Epub 2018 Nov 19.

DOI:10.4049/jimmunol.1801185
PMID:30455402
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6487659/
Abstract

Effective subunit vaccines require the incorporation of adjuvants that stimulate cells of the innate immune system to generate protective adaptive immune responses. Pattern recognition receptor agonists are a growing class of potential adjuvants that can shape the character of the immune response to subunit vaccines by directing the polarization of CD4 T cell differentiation to various functional subsets. In the current study, we applied a high-throughput in vitro screen to assess murine CD4 T cell polarization by a panel of pattern recognition receptor agonists. This identified lipopeptides with TLR2 agonist activity as exceptional Th1-polarizing adjuvants. In vivo, we demonstrated that i.v. administration of TLR2 agonists with Ag in mice replicated the findings from in vitro screening by promoting strong Th1 polarization. In contrast, TLR2 agonists inhibited priming of Th1 responses when administered cutaneously in mice. This route-specific suppression was associated with infiltrating CCR2 cells in the skin-draining lymph nodes and was not uniquely dependent on any of the well characterized subsets of dendritic cells known to reside in the skin. We further demonstrated that priming of CD4 T cells to generate Th1 effectors following immunization with the bacillus Calmette-Guérin (BCG) strain, a lipoprotein-rich bacterium recognized by TLR2, was dependent on the immunization route, with significantly greater Th1 responses with i.v. compared with intradermal administration of BCG. A more complete understanding of route-dependent TLR2 responses may be critical for informed design of novel subunit vaccines and for improvement of BCG and other vaccines based on live-attenuated organisms.

摘要

有效的亚单位疫苗需要加入佐剂,以刺激固有免疫系统的细胞产生保护性的适应性免疫反应。模式识别受体激动剂是一类潜在的佐剂,它们可以通过指导 CD4 T 细胞分化为各种功能亚群,来塑造亚单位疫苗免疫反应的特征。在本研究中,我们应用高通量体外筛选方法,评估了一组模式识别受体激动剂对小鼠 CD4 T 细胞极化的影响。这鉴定出具有 TLR2 激动剂活性的脂肽是一种特殊的 Th1 极化佐剂。在体内,我们证明了 TLR2 激动剂与 Ag 静脉内给药在小鼠中复制了体外筛选的发现,促进了强烈的 Th1 极化。相比之下,TLR2 激动剂在小鼠皮内给药时抑制了 Th1 反应的启动。这种途径特异性的抑制与趋化因子受体 2(CCR2)细胞在皮肤引流淋巴结中的浸润有关,而不是依赖于已知存在于皮肤中的任何特征明确的树突状细胞亚群。我们进一步证明,用卡介苗(BCG)株(一种被 TLR2 识别的富含脂蛋白的细菌)进行免疫接种后,CD4 T 细胞产生 Th1 效应器的启动依赖于免疫途径,与皮内相比,静脉内给予 BCG 可产生更强的 Th1 反应。更深入地了解途径依赖性 TLR2 反应对于新型亚单位疫苗的合理设计以及改进基于减毒活生物体的 BCG 和其他疫苗可能至关重要。