论文标题

机械生物学预测由配体受体活性在细胞膜上触发的筏形成

Mechanobiology predicts raft formations triggered by ligand-receptor activity across the cell membrane

论文作者

Carotenuto, A. R., Lunghi, L., Piccolo, V., Babaei, M., Dayal, K., Pugno, N. M., Zingales, M., Deseri, L., Fraldi, M.

论文摘要

在细胞膜增厚岛上不同类型的配体结合受体的聚类,即脂质筏,是一种实验观察到的现象。尽管深入研究了其对细胞反应的影响,但涉及活性受体的机械过程和多物理学之间的耦合的作用尚未被了解。具体而言,这项工作的重点是G蛋白偶联受体(GPCR),该受体通过化学信号传导途径调节特定的细胞过程,涉及循环腺苷单磷酸腺苷(CAMP)在活性GPCR产生的循环腺苷(cAMP)之间,在内细胞内环境中及其排出中介导的多发性抗蛋白质(MR)(MR)介导了多发性抗蛋白(MR)。本文根据能量学之间的相互作用,多尺度的几何变化和物种的质量平衡,即主动GPCR和MRP,包括结合和解开的动力学,开发了一种多物理学方法。因为所获得的能量取决于运动学和物种密度的变化,所以质量和线性动量的平衡是耦合的,并控制细胞膜的时空演化。涉及细胞膜脂质排序的重塑和变化的机械生物学可以预测转运蛋白和活性受体的动力学 - 与实验观察到的cAMP水平一致 - 以及后者如何在此类位点触发筏的形成和簇。 Within the current scientific debate on Severe Acute Respiratory Syndrome CoronaVirus 2 (SARS-CoV-2) and on the basis of the ascertained fact that lipid rafts often serve as an entry port for viruses, it is felt that approaches accounting for strong coupling among mechanobiological aspects could even turn helpful in better understanding membrane-mediated phenomena such as COVID-19 virus-cell interaction.

Clustering of ligand-binding receptors of different types on thickened isles of the cell membrane, namely lipid rafts, is an experimentally observed phenomenon. Although its influence on cell response is deeply investigated, the role of the coupling between mechanical processes and multiphysics involving the active receptors and the surrounding lipid membrane during ligand-binding has not yet been understood. Specifically, the focus of this work is on G-protein-coupled receptors (GPCRs), which regulate specific cell processes through chemical signalling pathways involving a synergistic balance between the cyclic Adenosine Monophosphate (cAMP) produced by active GPCRs in the intracellular environment and its efflux, mediated by Multidrug Resistance Proteins (MRPs) transporters. This paper develops a multiphysics approach based on the interplay among energetics, multiscale geometrical changes and mass balance of species, i.e. active GPCRs and MRPs, including diffusion and kinetics of binding and unbinding. Because the obtained energy depends upon both the kinematics and the changes of species densities, balance of mass and of linear momentum are coupled and govern the space-time evolution of the cell membrane. The mechanobiology involving remodelling and change of lipid ordering of the cell membrane allows to predict dynamics of transporters and active receptors -in agreement with experimentally observed cAMP levels- and how the latter trigger rafts formation and cluster on such sites. Within the current scientific debate on Severe Acute Respiratory Syndrome CoronaVirus 2 (SARS-CoV-2) and on the basis of the ascertained fact that lipid rafts often serve as an entry port for viruses, it is felt that approaches accounting for strong coupling among mechanobiological aspects could even turn helpful in better understanding membrane-mediated phenomena such as COVID-19 virus-cell interaction.

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