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FcγRn 电化学受体传感器及其动力学研究。

Study on FcγRn Electrochemical Receptor Sensor and Its Kinetics.

机构信息

College of Biotechnology & Food Science, Tianjin University of Commerce, Tianjin 300314, China.

Tianjin Key Laboratory of Food Biotechnology, Tianjin University of Commerce, Tianjin 300314, China.

出版信息

Molecules. 2020 Jul 14;25(14):3206. doi: 10.3390/molecules25143206.

Abstract

Neonatal γ-immunoglobulin (IgG) Fc receptor (FcγRn) is a receptor that transports IgG across the intestinal mucosa, placenta, and mammary gland, ensuring the balance of IgG and albumin in the body. These functions of FcγRn depend on the intracellular signal transduction and activation caused by the combination of its extracellular domain and IgG Fc domain. Nevertheless, there are still no kinetic studies on this interaction. Consequently, in the present study, we successfully constructed the human FcγRn (hFcγRn) electrochemical receptor sensor. The signal amplification system formed by chitosan nanogold-hFcγRn protein and horseradish peroxidase was used to simulate the cell signal amplification system in vivo, and the kinetic effects between seven IgG and hFcγRn receptors from different species were quantitatively measured. The results showed that the interaction of these seven IgGs with hFcγRn was similar to the catalytic kinetics of enzyme and substrate, and there was a ligand-receptor saturation effect. The order of the interconnect allosteric constants (K), which is similar to the Michaelis constant (K), was human IgG < bovine IgG < horse IgG < rabbit IgG < sheep IgG < donkey IgG < quail IgY. The results showed that hFcγRn had the strongest ability to transport human IgG, which was consistent with the evolution of the system. Therefore, our hFcγRn electrochemical receptor sensor can be used to measure and evaluate the interconnected allosteric network. It is also an essential parameter of the interaction between hFcγRn and different IgGs and, thus, provides a new detection and evaluation method for immunoemulsion, therapeutic monoclonal antibody therapy, heteroantibody treatment, and half-life research.

摘要

新生儿 γ-免疫球蛋白 (IgG) Fc 受体 (FcγRn) 是一种跨肠黏膜、胎盘和乳腺转运 IgG 的受体,确保 IgG 与白蛋白在体内保持平衡。FcγRn 的这些功能依赖于其细胞外结构域与 IgG Fc 结构域结合引起的细胞内信号转导和激活。然而,目前针对这种相互作用还没有动力学研究。因此,在本研究中,我们成功构建了人 FcγRn(hFcγRn)电化学受体传感器。壳聚糖纳米金-hFcγRn 蛋白与辣根过氧化物酶形成的信号放大系统模拟了体内细胞信号放大系统,定量测量了来自不同物种的 7 种 IgG 与 hFcγRn 受体之间的动力学效应。结果表明,这 7 种 IgG 与 hFcγRn 的相互作用类似于酶和底物的催化动力学,存在配体-受体饱和效应。连接变构常数(K)的顺序与米氏常数(K)相似,即人 IgG <牛 IgG <马 IgG <兔 IgG <羊 IgG <驴 IgG <鹌鹑 IgY。结果表明,hFcγRn 转运人 IgG 的能力最强,这与系统的进化是一致的。因此,我们的 hFcγRn 电化学受体传感器可用于测量和评估连接变构网络。它也是 hFcγRn 与不同 IgG 相互作用的重要参数,为免疫乳剂、治疗性单克隆抗体治疗、异抗体治疗和半衰期研究提供了新的检测和评估方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c0/7397135/0952059c8dfa/molecules-25-03206-g001.jpg

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