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CCR7 + CD4 T细胞免疫监视在恒河猴大脑慢性SIV诱导的神经炎症中受到破坏。

CCR7+ CD4 T Cell Immunosurveillance Disrupted in Chronic SIV-Induced Neuroinflammation in Rhesus Brain.

作者信息

Elizaldi Sonny R, Hawes Chase E, Verma Anil, Dinasarapu Ashok R, Lakshmanappa Yashavanth Shaan, Schlegel Brent T, Rajasundaram Dhivyaa, Li Jie, Durbin-Johnson Blythe P, Ma Zhong-Min, Beckman Danielle, Ott Sean, Lifson Jeffrey, Morrison John H, Iyer Smita S

出版信息

bioRxiv. 2023 Aug 31:2023.08.28.555037. doi: 10.1101/2023.08.28.555037.

Abstract

UNLABELLED

CD4 T cells survey and maintain immune homeostasis in the brain, yet their differentiation states and functional capabilities remain unclear. Our approach, combining single-cell transcriptomic analysis, ATAC-seq, spatial transcriptomics, and flow cytometry, revealed a distinct subset of CCR7+ CD4 T cells resembling lymph node central memory (T ) cells. We observed chromatin accessibility at the CCR7, CD28, and BCL-6 loci, defining molecular features of T . Brain CCR7+ CD4 T cells exhibited recall proliferation and interleukin-2 production ex vivo, showcasing their functional competence. We identified the skull bone marrow as a local niche for these cells alongside other CNS border tissues. Sequestering T cells in lymph nodes using FTY720 led to reduced CCR7+ CD4 T cell frequencies in the cerebrospinal fluid, accompanied by increased monocyte levels and soluble markers indicating immune activation. In macaques chronically infected with SIVCL57 and experiencing viral rebound due to cessation of antiretroviral therapy, a decrease in brain CCR7+ CD4 T cells was observed, along with increased microglial activation and initiation of neurodegenerative pathways. Our findings highlight a role for CCR7+ CD4 T cells in CNS immune surveillance and their decline during chronic SIV-induced neuroinflammation highlights their responsiveness to neuroinflammatory processes.

IN BRIEF

Utilizing single-cell and spatial transcriptomics on adult rhesus brain, we uncover a unique CCR7+ CD4 T cell subset resembling central memory T cells (T ) within brain and border tissues, including skull bone marrow. Our findings show decreased frequencies of this subset during SIV- induced chronic neuroinflammation, emphasizing responsiveness of CCR7+ CD4 T cells to CNS disruptions.

HIGHLIGHTS

CCR7+ CD4 T cells survey border and parenchymal CNS compartments during homeostasis; reduced presence of CCR7+ CD4 T cells in cerebrospinal fluid leads to immune activation, implying a role in neuroimmune homeostasis. CNS CCR7+ CD4 T cells exhibit phenotypic and functional features of central memory T cells (T ) including production of interleukin 2 and the capacity for rapid recall proliferation. Furthermore, CCR7+ CD4 T cells reside in the skull bone marrow. CCR7+ CD4 T cells are markedly decreased within the brain parenchyma during chronic viral neuroinflammation.

摘要

未标记

CD4 T细胞在大脑中监测并维持免疫稳态,但其分化状态和功能能力仍不清楚。我们结合单细胞转录组分析、ATAC测序、空间转录组学和流式细胞术的方法,揭示了一个独特的CCR7+ CD4 T细胞亚群,类似于淋巴结中央记忆(T )细胞。我们观察到CCR7、CD28和BCL-6基因座处的染色质可及性,确定了T 的分子特征。脑内CCR7+ CD4 T细胞在体外表现出回忆增殖和白细胞介素-2的产生,展示了它们的功能能力。我们确定颅骨骨髓以及其他中枢神经系统边界组织是这些细胞的局部微环境。使用FTY720将T 细胞隔离在淋巴结中导致脑脊液中CCR7+ CD4 T细胞频率降低,同时单核细胞水平和表明免疫激活的可溶性标志物增加。在慢性感染SIVCL57并因停止抗逆转录病毒治疗而出现病毒反弹的猕猴中,观察到脑内CCR7+ CD4 T细胞减少,同时小胶质细胞激活增加和神经退行性途径启动。我们的研究结果突出了CCR7+ CD4 T细胞在中枢神经系统免疫监测中的作用,以及它们在慢性SIV诱导的神经炎症期间的减少突出了它们对神经炎症过程的反应性。

简而言之

利用对成年恒河猴大脑的单细胞和空间转录组学,我们在大脑和边界组织(包括颅骨骨髓)中发现了一个独特的类似于中央记忆T细胞(T )的CCR7+ CD4 T细胞亚群。我们的研究结果表明,在SIV诱导的慢性神经炎症期间,该亚群频率降低,强调了CCR7+ CD4 T细胞对中枢神经系统破坏反应性。

亮点

在稳态期间,CCR7+ CD4 T细胞监测中枢神经系统边界和实质区室;脑脊液中CCR7+ CD4 T细胞数量减少导致免疫激活,暗示其在神经免疫稳态中的作用。中枢神经系统CCR7+ CD4 T细胞表现出中央记忆T细胞(T )的表型和功能特征,包括白细胞介素2的产生和快速回忆增殖的能力。此外,CCR7+ CD4 T细胞存在于颅骨骨髓中。在慢性病毒神经炎症期间,脑实质内CCR7+ CD4 T细胞明显减少。

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