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控制酶活性以响应渗透压调节,模拟细胞内细胞器的动态组装。

Control of Enzyme Reactivity in Response to Osmotic Pressure Modulation Mimicking Dynamic Assembly of Intracellular Organelles.

机构信息

Centre national de la recherche scientifique, University of Bordeaux, Bordeaux INP, LCPO, UMR 5629, Pessac, F-33600, France.

出版信息

Adv Mater. 2023 Aug;35(33):e2301856. doi: 10.1002/adma.202301856. Epub 2023 Jun 28.

Abstract

In response to variations in osmotic stress, in particular to hypertonicity associated with biological dysregulations, cells have developed complex mechanisms to release their excess water, thus avoiding their bursting and death. When water is expelled, cells shrink and concentrate their internal bio(macro)molecular content, inducing the formation of membraneless organelles following a liquid-liquid phase separation (LLPS) mechanism. To mimic this intrinsic property of cells, functional thermo-responsive elastin-like polypeptide (ELP) biomacromolecular conjugates are herein encapsulated into self-assembled lipid vesicles using a microfluidic system, together with polyethylene glycol (PEG) to mimic cells' interior crowded microenvironment. By inducing a hypertonic shock onto the vesicles, expelled water induces a local increase in concentration and a concomitant decrease in the cloud point temperature (T ) of ELP bioconjugates that phase separate and form coacervates mimicking cellular stress-induced membraneless organelle assemblies. Horseradish peroxidase (HRP), as a model enzyme, is bioconjugated to ELPs and is locally confined in coacervates as a response to osmotic stress. This consequently increases local HRP and substrate concentrations and accelerates the kinetics of the enzymatic reaction. These results illustrate a unique way to fine-tune enzymatic reactions dynamically as a response to a physiological change in isothermal conditions.

摘要

为了应对渗透压力的变化,特别是应对与生物失调相关的高渗性,细胞已经开发出了复杂的机制来释放多余的水分,从而避免细胞破裂和死亡。当水被排出时,细胞会收缩并浓缩其内部的生物(大)分子物质,从而在液-液相分离(LLPS)机制的作用下形成无膜细胞器。为了模拟细胞的这种固有特性,功能性热响应弹性蛋白样多肽(ELP)生物大分子缀合物被封装到使用微流控系统自组装的脂质体中,同时使用聚乙二醇(PEG)模拟细胞内部拥挤的微环境。通过对脂质体施加高渗冲击,排出的水会导致 ELP 生物缀合物的局部浓度增加,同时伴随相分离的浊点温度(T)降低,从而形成类似细胞应激诱导的无膜细胞器组装的凝聚物。辣根过氧化物酶(HRP)作为模型酶被生物偶联到 ELP 上,并作为对渗透压的响应而被局部限制在凝聚物中。这会导致局部 HRP 和底物浓度增加,并加速酶反应的动力学。这些结果说明了一种独特的方法,可以在等温条件下动态微调酶反应,以响应生理变化。

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