免疫突触
细胞生物学
生物
转录因子
中心体
T细胞受体
免疫系统
细胞核
NFAT公司
抄写(语言学)
T细胞
核心
细胞毒性T细胞
Jurkat细胞
化学
电池极性
激活剂(遗传学)
核蛋白
核定位序列
细胞
CD8型
作者
Yukako Asano,Y. Claire,Martin M. Limback-Stokin,Adam M. Rochussen,Jane C. Stinchcombe,Gillian M. Griffiths
出处
期刊:Science immunology
[American Association for the Advancement of Science]
日期:2025-09-19
卷期号:10 (111): eadt5909-eadt5909
被引量:1
标识
DOI:10.1126/sciimmunol.adt5909
摘要
Target cell recognition by cytotoxic T lymphocytes (CTLs) triggers rapid delivery of cytolytic granules to the immune synapse directed by the centrosome. Recent studies have also identified a rapid burst of T cell receptor (TCR)-activated transcription that contributes to CTL-mediated killing. To determine how de novo transcription might be coordinated with intracellular polarization, we asked when transcription factor translocation to the nucleus occurs relative to TCR activation and centrosome polarization within individual CTLs. Upon target cell recognition, the nucleus polarized to and contacted the immune synapse, preceding centrosome docking. The nucleus distorted as it moved, with transcription factors NFAT and NF-κB accumulating in the nucleus during polarization. Inhibition or deletion of myosin IIA prevented both nuclear polarization and transcription factor translocation. Thus, nuclear polarization facilitates an early transcriptional burst that occurs as CTLs encounter targets and the consequent delivery of newly synthesized cytokines to the immune synapse.
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