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肌醇与磷脂酰肌醇4,5-二磷酸/磷脂酰肌醇-3,4,5-三磷酸比值:细胞与其微环境之间生物动力学界面的交叉点

Inositol and PIP2/PIP3 Ratio: At the Crossroad of the Biodynamic Interface Between Cells and Their Microenvironment.

作者信息

Lentini Guglielmo, Querqui Alessandro, Giuliani Alessandro, Verna Roberto, Bizzarri Mariano

机构信息

Space Biomedicine Laboratory, Department of Experimental Medicine, University Sapienza, 00161 Rome, Italy.

Environment and Health Department, Istituto Superiore di Sanità, 00161 Rome, Italy.

出版信息

Biomolecules. 2025 Mar 20;15(3):451. doi: 10.3390/biom15030451.

Abstract

Plasma membrane plays a pivotal role in orchestrating motility and invasive processes, as well as mitosis and genome expression. Indeed, specialized regions of the plasma membrane enriched in phosphoinositides-namely PIP2 and PIP3-can accommodate the requirements of the dynamic interface, which mediates the interplay between cells and their microenvironment. The fine-tuned balance between the two phosphoinositides is instrumental in regulating cytoskeleton organization, motility, ion channel activation, and membrane traffic. The balanced expression of PIP2/PIP3 fulfills these functions by activating pathways through several transporter and receptor proteins. These dynamic interactions modulate the interplay with the extracellular environment by decreasing/increasing their exposure on the cell surface. In this way, lipid structures can rapidly either dismiss or recruit specific proteins, eventually favoring their cooperation with membrane receptors and ion channels. Particularly, exposure of proteins can be managed through the internalization of plasma membrane segments, while receptor signaling can be desensitized by their removal from the cell surface. Notably, the equilibrium between PIP2 and PIP3 is largely dependent on inositol availability, as inositol addition enhances PIP2 content while reducing PIP3 via PI3K inhibition. Pharmacological modulation of PIP2/PIP3 balance promises to be an interesting target in different clinical settings.

摘要

质膜在协调细胞运动和侵袭过程以及有丝分裂和基因组表达中起着关键作用。实际上,富含磷酸肌醇(即PIP2和PIP3)的质膜特殊区域能够满足动态界面的需求,该界面介导细胞与其微环境之间的相互作用。这两种磷酸肌醇之间的精细平衡有助于调节细胞骨架组织、运动性、离子通道激活和膜运输。PIP2/PIP3的平衡表达通过激活几种转运蛋白和受体蛋白的途径来实现这些功能。这些动态相互作用通过减少/增加它们在细胞表面的暴露来调节与细胞外环境的相互作用。通过这种方式,脂质结构可以迅速去除或招募特定蛋白质,最终促进它们与膜受体和离子通道的协同作用。特别是,蛋白质的暴露可以通过质膜片段的内化来控制,而受体信号可以通过将它们从细胞表面去除而脱敏。值得注意的是,PIP2和PIP3之间的平衡在很大程度上取决于肌醇的可用性,因为添加肌醇会增加PIP2含量,同时通过抑制PI3K降低PIP3含量。PIP2/PIP3平衡的药理学调节有望成为不同临床环境中一个有趣的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99e3/11940430/5003a5a14277/biomolecules-15-00451-g001.jpg

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