Lamerton Rachel E, Lightfoot Abbey, Nieves Daniel J, Owen Dylan M
Institute of Immunology and Immunotherapy, School of Mathematics and Centre of Membrane Proteins and Receptors (COMPARE), University of Birmingham, Birmingham, United Kingdom.
Front Immunol. 2021 Mar 9;12:600961. doi: 10.3389/fimmu.2021.600961. eCollection 2021.
Lymphocytes must strike a delicate balance between activating in response to signals from potentially pathogenic organisms and avoiding activation from stimuli emanating from the body's own cells. For cells, such as T or B cells, maximizing the efficiency and fidelity, whilst minimizing the crosstalk, of complex signaling pathways is crucial. One way of achieving this control is by carefully orchestrating the spatiotemporal organization of signaling molecules, thereby regulating the rates of protein-protein interactions. This is particularly true at the plasma membrane where proximal signaling events take place and the phenomenon of protein microclustering has been extensively observed and characterized. This review will focus on what is known about the heterogeneous distribution of proteins and lipids at the cell surface, illustrating how such distributions can influence signaling in health and disease. We particularly focus on nanoscale molecular organization, which has recently become accessible for study through advances in microscope technology and analysis methodology.
淋巴细胞必须在响应潜在致病生物体发出的信号而激活与避免被机体自身细胞发出的刺激激活之间达成微妙的平衡。对于T细胞或B细胞等细胞而言,最大化复杂信号通路的效率和保真度,同时最小化串扰至关重要。实现这种控制的一种方法是精心编排信号分子的时空组织,从而调节蛋白质-蛋白质相互作用的速率。在发生近端信号事件的质膜处尤其如此,并且蛋白质微簇集现象已得到广泛观察和表征。本综述将聚焦于细胞表面蛋白质和脂质的异质分布情况,阐明这种分布如何在健康和疾病状态下影响信号传导。我们特别关注纳米级分子组织,近年来借助显微镜技术和分析方法的进步,这已成为可研究的对象。
