外力对免疫突触形成过程中肌动蛋白依赖性T细胞突起的影响

IF 2.4 4区生物学 Q4 CELL BIOLOGY

Biology of the Cell Pub Date : 2021-01-20 DOI:10.1111/boc.202000133

Andrés Ernesto Zucchetti, Noémie Paillon, Olga Markova, Stéphanie Dogniaux, Claire Hivroz, Julien Husson

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引用次数: 6

摘要

我们之前观察到，在对抗原活化的反应中，T细胞产生富含肌动蛋白的突起，产生参与T细胞活化的力。这些力受到抗原提呈细胞(APCs)机械特性的影响。然而，apc产生的外力如何影响肌动蛋白突出的动态仍然未知。在这项研究中，我们定量表征了外力对激活T细胞生长的突起动态的影响。结果利用微管力探针，我们对被抗体覆盖的微球激活的原代T淋巴细胞施加了可控的压缩或拉力，并测量了这些力对T淋巴细胞产生的突起的影响。我们发现，施加压缩力会略微降低突出物的长度、停止生长和收缩的时间以及形成突出物的速度，而拉力则会显著增加这些参数。在这两种情况下，施加的力都没有改变T细胞开始生长突起所需的时间(延迟)。研究人员发现，抑制Arp2/3复合体可降低突起的最大长度和生长速度，并增加开始生长的延迟时间，从而损害突起的动态。最后，T细胞在更生理的条件下，即被APC激活而不是被激活的微珠激活时，产生了类似的突起。结论T细胞产生力的突起的形成是由细胞内恒定时间决定的，其动态对外力敏感。他们还表明，由肌动蛋白相关蛋白Arp2/3复合物介导的肌动蛋白组装参与了突起的形成和动态。T细胞产生的富含肌动蛋白的突起是一种感觉细胞器，可作为免疫监视的执行器。我们的研究表明，这种细胞器所经历的力改变了它们的动态，这表明它们可能改变免疫反应。此外，我们分析的定量方面应该有助于深入了解参与形成突出的分子机制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Influence of external forces on actin-dependent T cell protrusions during immune synapse formation

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Influence of external forces on actin-dependent T cell protrusions during immune synapse formation

Background Information

We have previously observed that in response to antigenic activation, T cells produce actin-rich protrusions that generate forces involved in T cell activation. These forces are influenced by the mechanical properties of antigen-presenting cells (APCs). However, how external forces, which can be produced by APCs, influence the dynamic of the actin protrusion remains unknown. In this study, we quantitatively characterised the effects of external forces in the dynamic of the protrusion grown by activated T cells.

Results

Using a micropipette force probe, we applied controlled compressive or pulling forces on primary T lymphocytes activated by an antibody-covered microbead, and measured the effects of these forces on the protrusion generated by T lymphocytes. We found that the application of compressive forces slightly decreased the length, the time at which the protrusion stops growing and retracts and the velocity of the protrusion formation, whereas pulling forces strongly increased these parameters. In both cases, the applied forces did not alter the time required for the T cells to start growing the protrusion (delay). Exploring the molecular events controlling the dynamic of the protrusion, we showed that inhibition of the Arp2/3 complex impaired the dynamic of the protrusion by reducing both its maximum length and its growth speed and increasing the delay to start growing. Finally, T cells developed similar protrusions in more physiological conditions, that is, when activated by an APC instead of an activating microbead.

Conclusions

Our results suggest that the formation of the force-generating protrusion by T cells is set by an intracellular constant time and that its dynamic is sensitive to external forces. They also show that actin assembly mediated by actin-related protein Arp2/3 complex is involved in the formation and dynamic of the protrusion.

Significance

Actin-rich protrusions developed by T cells are sensory organelles that serve as actuators of immune surveillance. Our study shows that forces experienced by this organelle modify their dynamic suggesting that they might modify immune responses. Moreover, the quantitative aspects of our analysis should help to get insight into the molecular mechanisms involved in the formation of the protrusion.

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来源期刊

Biology of the Cell 生物-细胞生物学

CiteScore

5.30

自引率

0.00%

发文量

审稿时长

>12 weeks

期刊介绍： The journal publishes original research articles and reviews on all aspects of cellular, molecular and structural biology, developmental biology, cell physiology and evolution. It will publish articles or reviews contributing to the understanding of the elementary biochemical and biophysical principles of live matter organization from the molecular, cellular and tissues scales and organisms. This includes contributions directed towards understanding biochemical and biophysical mechanisms, structure-function relationships with respect to basic cell and tissue functions, development, development/evolution relationship, morphogenesis, stem cell biology, cell biology of disease, plant cell biology, as well as contributions directed toward understanding integrated processes at the organelles, cell and tissue levels. Contributions using approaches such as high resolution imaging, live imaging, quantitative cell biology and integrated biology; as well as those using innovative genetic and epigenetic technologies, ex-vivo tissue engineering, cellular, tissue and integrated functional analysis, and quantitative biology and modeling to demonstrate original biological principles are encouraged.