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纳米颗粒与肺表面活性剂接触后的蛋白质组学和脂质组学分析揭示了蛋白质组成的差异,但脂质组成没有差异。

Proteomic and Lipidomic Analysis of Nanoparticle Corona upon Contact with Lung Surfactant Reveals Differences in Protein, but Not Lipid Composition.

机构信息

Department of Pharmacy, Saarland University , 66123 Saarbruecken, Germany.

HIPS - Helmholtz Institute for Pharmaceutical Research Saarland , Helmholtz Centre for Infection Research, 66123 Saarbruecken, Germany.

出版信息

ACS Nano. 2015 Dec 22;9(12):11872-85. doi: 10.1021/acsnano.5b04215. Epub 2015 Nov 20.

Abstract

Pulmonary surfactant (PS) constitutes the first line of host defense in the deep lung. Because of its high content of phospholipids and surfactant specific proteins, the interaction of inhaled nanoparticles (NPs) with the pulmonary surfactant layer is likely to form a corona that is different to the one formed in plasma. Here we present a detailed lipidomic and proteomic analysis of NP corona formation using native porcine surfactant as a model. We analyzed the adsorbed biomolecules in the corona of three NP with different surface properties (PEG-, PLGA-, and Lipid-NP) after incubation with native porcine surfactant. Using label-free shotgun analysis for protein and LC-MS for lipid analysis, we quantitatively determined the corona composition. Our results show a conserved lipid composition in the coronas of all investigated NPs regardless of their surface properties, with only hydrophilic PEG-NPs adsorbing fewer lipids in total. In contrast, the analyzed NP displayed a marked difference in the protein corona, consisting of up to 417 different proteins. Among the proteins showing significant differences between the NP coronas, there was a striking prevalence of molecules with a notoriously high lipid and surface binding, such as, e.g., SP-A, SP-D, DMBT1. Our data indicate that the selective adsorption of proteins mediates the relatively similar lipid pattern in the coronas of different NPs. On the basis of our lipidomic and proteomic analysis, we provide a detailed set of quantitative data on the composition of the surfactant corona formed upon NP inhalation, which is unique and markedly different to the plasma corona.

摘要

肺表面活性剂(PS)构成了深部肺部宿主防御的第一道防线。由于其高含量的磷脂和表面活性剂特异性蛋白,吸入的纳米颗粒(NPs)与肺表面活性剂层的相互作用很可能形成一个不同于在血浆中形成的冠。在这里,我们使用天然猪肺表面活性剂作为模型,对 NP 冠形成的脂质组学和蛋白质组学进行了详细分析。我们分析了三种具有不同表面性质的 NP(PEG-、PLGA-和脂质-NP)与天然猪肺表面活性剂孵育后在冠中的吸附生物分子。使用无标记的 shotgun 分析进行蛋白质分析和 LC-MS 进行脂质分析,我们定量确定了冠的组成。我们的结果表明,无论 NP 的表面性质如何,在所有研究的 NP 的冠中都存在保守的脂质组成,只有亲水性的 PEG-NP 总吸附的脂质较少。相比之下,所分析的 NP 在蛋白质冠中表现出明显的差异,包含多达 417 种不同的蛋白质。在 NP 冠之间表现出显著差异的蛋白质中,有一种明显的倾向,即存在许多具有高脂质和表面结合的分子,例如 SP-A、SP-D 和 DMBT1。我们的数据表明,蛋白质的选择性吸附介导了不同 NP 冠中的相对相似的脂质模式。基于我们的脂质组学和蛋白质组学分析,我们提供了关于吸入 NP 后形成的表面活性剂冠的组成的详细定量数据集,这是独特的,与血浆冠明显不同。

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