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磷酸胆碱修饰的 PPI 树状聚合物模拟细胞膜磷酸胆碱簇并调节 C 反应蛋白的固有免疫活性。

Phosphocholine-Decorated PPI-Dendrimers Mimic Cell Membrane Phosphocholine Clusters and Tune the Innate Immune Activity of C-Reactive Protein.

机构信息

Innate Immunology Group, National Veterinary Institute, Technical University of Denmark, Lyngby 2800, Denmark.

Department of Chemistry, Technical University of Denmark, Lyngby 2800, Denmark.

出版信息

Biomacromolecules. 2021 Apr 12;22(4):1664-1674. doi: 10.1021/acs.biomac.1c00085. Epub 2021 Mar 8.

Abstract

C-reactive protein (CRP) is widely used as biomarkers of infection and inflammation. It has a well-described ability to bind phosphocholine (PC), as well as PC-clusters from compromised and inflamed cell membranes and tissues. The binding of PC-clusters to CRP is of interest as this binding determines subsequent innate immune activity. We investigated PC-decorated dendrimers as mimics for PC-clusters. Five generations of poly(propylene imine) (PPI) dendrimers were modified with PC surface groups via a three-step synthetic sequence obtaining the PC-decorated dendrimers in high purity. The dendrimers were analyzed by NMR and infrared spectroscopy as well as HPLC. We developed immunoassays to show that dendrimer-PC binding to CRP was Ca-dependent with an apparent overall of 11.9 nM for first generation (G1) PPI-PC, while G2-PPI-PC and G3-PPI-PC had slightly higher affinities, and G4-PPI-PC and G5-PPI-PC had slightly lower affinities. For all PC-dendrimers, the affinity was orders of magnitude higher than the affinity of free phosphocholine (PC), indicating a PC-cluster effect. Next, we investigated the binding of CRP:PPI-PC complexes to complement component C1q. C1q binding to CRP was dependent on the generation of PPI-PC bound to CRP, with second and third generation PPI-PCs leading to the highest affinity. The dendrimer-based approach to PC-cluster mimics and the simple binding assays presented here hold promise as tools to screen PC-compounds for their abilities to tune the innate immune activity of CRP.

摘要

C-反应蛋白(CRP)被广泛用作感染和炎症的生物标志物。它具有与磷酸胆碱(PC)结合的良好能力,以及与受损和发炎的细胞膜和组织中的 PC 簇结合的能力。PC 簇与 CRP 的结合很有趣,因为这种结合决定了随后的固有免疫活性。我们研究了 PC 修饰的树突状聚合物作为 PC 簇的模拟物。通过三步合成序列,将五代聚(丙烯亚胺)(PPI)树突状聚合物用 PC 表面基团修饰,以高纯度获得 PC 修饰的树突状聚合物。通过 NMR 和红外光谱以及 HPLC 对树突状聚合物进行了分析。我们开发了免疫测定法来表明树突状聚合物-PC 与 CRP 的结合是 Ca 依赖性的,第一代(G1)PPI-PC 的表观整体为 11.9 nM,而 G2-PPI-PC 和 G3-PPI-PC 的亲和力略高,G4-PPI-PC 和 G5-PPI-PC 的亲和力略低。对于所有 PC 树突状聚合物,亲和力的数量级都高于游离磷酸胆碱(PC)的亲和力,表明存在 PC 簇效应。接下来,我们研究了 CRP:PPI-PC 复合物与补体成分 C1q 的结合。C1q 与 CRP 的结合依赖于与 CRP 结合的 PPI-PC 的代,第二代和第三代 PPI-PC 导致最高的亲和力。基于树突状聚合物的 PC 簇模拟物和提出的简单结合测定法有望成为筛选 PC 化合物的工具,以评估它们调节 CRP 固有免疫活性的能力。

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