Microglia Require CD4 T Cells to Complete the Fetal-to-Adult Transition

Pasciuto Emanuela; Burton Oliver T.; Roca Carlos P.; Lagou Vasiliki; Rajan Wenson D.; Theys Tom; Mancuso Renzo; Tito Raul Y.; Kouser Lubna; Callaerts-Vegh Zsuzsanna; de la Fuente Alerie G.; Prezzemolo Teresa; Mascali Loriana G.; Brajic Aleksandra; Whyte Carly E.; Yshii Lidia; Martinez-Muriana Anna; Naughton Michelle; Young Andrew; Moudra Alena; Lemaitre Pierre; Poovathingal Suresh; Raes Jeroen; De Strooper Bart; Fitzgerald Denise C.; Dooley James; Liston Adrian

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Microglia Require CD4 T Cells to Complete the Fetal-to-Adult Transition

机译：微胶质细胞需要CD4 T细胞完成胎对成人过渡

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The brain is a site of relative immune privilege. Although CD4 T cells have been reported in the central nervous system, their presence in the healthy brain remains controversial, and their function remains largely unknown. We used a combination of imaging, single cell, and surgical approaches to identify a CD69(+) CD4 T cell population in both the mouse and human brain, distinct from circulating CD4 T cells. The brain-resident population was derived through in situ differentiation from activated circulatory cells and was shaped by self-antigen and the peripheral microbiome. Single-cell sequencing revealed that in the absence of murine CD4 T cells, resident microglia remained suspended between the fetal and adult states. This maturation defect resulted in excess immature neuronal synapses and behavioral abnormalities. These results illuminate a role for CD4 T cells in brain development and a potential interconnected dynamic between the evolution of the immunological and neurological systems.

机译：大脑是相对免疫特权的场所。尽管CD4 T细胞已被报道存在于中枢神经系统中，但它们在健康大脑中的存在仍存在争议，其功能在很大程度上仍不清楚。我们采用成像、单细胞和外科手术相结合的方法，在小鼠和人脑中识别出CD69（+）CD4 T细胞群，这与循环中的CD4 T细胞不同。居住在大脑中的人群是通过激活的循环细胞原位分化而来，并由自身抗原和外周微生物群形成的。单细胞测序显示，在缺乏小鼠CD4 T细胞的情况下，驻留的小胶质细胞在胎儿和成人状态之间仍然处于悬浮状态。这种成熟缺陷导致过度不成熟的神经元突触和行为异常。这些结果阐明了CD4 T细胞在大脑发育中的作用，以及免疫系统和神经系统进化之间潜在的相互关联的动态。

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《Cell》 |2020年第3期|共40页
作者
Pasciuto Emanuela; Burton Oliver T.; Roca Carlos P.; Lagou Vasiliki; Rajan Wenson D.; Theys Tom; Mancuso Renzo; Tito Raul Y.; Kouser Lubna; Callaerts-Vegh Zsuzsanna; de la Fuente Alerie G.; Prezzemolo Teresa; Mascali Loriana G.; Brajic Aleksandra; Whyte Carly E.; Yshii Lidia; Martinez-Muriana Anna; Naughton Michelle; Young Andrew; Moudra Alena; Lemaitre Pierre; Poovathingal Suresh; Raes Jeroen; De Strooper Bart; Fitzgerald Denise C.; Dooley James; Liston Adrian;
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作者单位

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

Babraham Inst Lab Lymphocyte Signalling &

Dev Cambridge CB22 3AT England;

Babraham Inst Lab Lymphocyte Signalling &

Dev Cambridge CB22 3AT England;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

UZ Leuven Dept Neurosurg B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

KU Leuven Univ Leuven Dept Microbiol &

Immunol B-3000 Leuven Belgium;

Babraham Inst Lab Lymphocyte Signalling &

Dev Cambridge CB22 3AT England;

KU Leuven Univ Leuven Dept Brain &

Cognit B-3000 Leuven Belgium;

Queens Univ Belfast Sch Med Dent &

Biomed Sci Wellcome Wolfson Inst Expt Med Belfast BT7 1NN Antrim North Ireland;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

Babraham Inst Lab Lymphocyte Signalling &

Dev Cambridge CB22 3AT England;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

Queens Univ Belfast Sch Med Dent &

Biomed Sci Wellcome Wolfson Inst Expt Med Belfast BT7 1NN Antrim North Ireland;

Queens Univ Belfast Sch Med Dent &

Biomed Sci Wellcome Wolfson Inst Expt Med Belfast BT7 1NN Antrim North Ireland;

Babraham Inst Lab Lymphocyte Signalling &

Dev Cambridge CB22 3AT England;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

KU Leuven Univ Leuven Dept Microbiol &

Immunol B-3000 Leuven Belgium;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

Queens Univ Belfast Sch Med Dent &

Biomed Sci Wellcome Wolfson Inst Expt Med Belfast BT7 1NN Antrim North Ireland;

Babraham Inst Lab Lymphocyte Signalling &

Dev Cambridge CB22 3AT England;

VIB VIB Ctr Brain &

Dis Res B-3000 Leuven Belgium;

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正文语种 eng
中图分类细胞生物学;
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2. CD4~+Foxp3~+ regulatory T cells converted by rapamycin from peripheral CD4~+ CD25~-naive T cells display more potent regulatory ability in vitro [J] . CHEN Jian-fei, GAO Jie, ZHANG Dong, 中华医学杂志（英文版） . 2010,第007期
3. 2-Gy whole-body irradiation significantly alters the balance of CD4^(+)CD25^(-) T effector cells and CD4^(+)CD25^(+)Foxp3^(+) T regulatory cells in mice [J] . Yanyan Qu, Baojun Zhang, Shuchun Liu, 细胞与分子免疫学：英文版 . 2010,第006期
4. MSH2 is required for cell proliferation,cell cycle control and cell invasiveness in colorectal cancer cells [J] . SHEN Kai, YE YingJiang, JIANG KeWei, 中国科学通报：英文版 . 2012,第020期
5. Internalization of NK cells into tumor cells requires ezrin and leads to programmed cell-in-cell death [J] . Shan Wang, Zhen Guo, Peng Xia, 细胞研究：英文版 . 2009,第012期
6. MHCII is required for α-Synuclein-induced activation of microglia, CD4 T cell proliferation, and dopaminergic neurodegeneration [J] . HarmA.S., CaoS., RowseA.L., The Journal of Neuroscience: The Official Journal of the Society for Neuroscience . 2013,第23期

机译：MHCII是α-突触核蛋白诱导的微胶质细胞，CD4 T细胞增殖和多巴胺能神经变性的激活
7. Single-Cell Mapping of Progressive Fetal-to-Adult Transition in Human Naive T Cells [J] . Daniel G. Bunis, Yelena Bronevetsky, Elisabeth Krow-Lucal, Cell Reports . 2021,第1期

机译：人幼稚T细胞逐步胎儿对成人过渡的单细胞映射
8. Functional Domains of Runx1 Are Differentially Required for CD4 Repression, TCRβ Expression, and CD4/8 Double-Negative to CD4/8 Double-Positive Transition in Thymocyte Development [J] . Masahito Kawazu, Takashi Asai, Motoshi Ichikawa, The journal of immunology . 2005,第6期

机译：Runx1的功能域是胸腺细胞发育中CD4抑制，TCRβ表达和CD4 / 8双负向CD4 / 8双正向转变的差异性要求。
9. Production of inflammatory cytokines by murine microglia cells requires the presence of microRNA-155 [C] . Fahad Gulraiz, Ellen Boelen, Sara Walbers, European Meeting on Glial Cells in Health and Disease . 2009

机译：鼠髓细胞产生炎性细胞因子需要MicroRNA-155的存在
10. Single-Cell Mapping of Progressive Fetal-To-Adult Transition in Human na?ve T Cells [D] . Bunis, Daniel. 2020

机译：人na ve t细胞中逐步胎儿对成人过渡的单细胞映射
11. MHCII Is Required for α-Synuclein-Induced Activation of Microglia CD4 T Cell Proliferation and Dopaminergic Neurodegeneration [O] . Ashley S. Harms, Shuwen Cao, Amber L. Rowse, 2013

机译：MHCII是α-突触核蛋白诱导的小胶质细胞活化CD4 T细胞增殖和多巴胺能神经变性所必需的
12. Microglia Require CD4 T Cells to Complete the Fetal-to-Adult Transition [O] . Emanuela Pasciuto, Oliver T. Burton, Carlos P. Roca, 2020

机译：微胶质细胞需要CD4 T细胞完成胎对成人过渡
13. Signal Transduction through CD4 Receptors: Stimulatory Versus Inhibitory Activity is Regulated by CD4 Proximity to the CD3/T Cell Receptor [R] . Ledbetter, J. A., June, C. H., Rabinovitch, P. S., 1988

机译：通过CD4受体的信号转导：刺激与抑制活性受CD4接近CD3 / T细胞受体的调节

Microglia Require CD4 T Cells to Complete the Fetal-to-Adult Transition

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