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多功能活性蛋白质组学在发育肺中的应用。

Multifunctional Activity-Based Protein Profiling of the Developing Lung.

机构信息

Biological Sciences Division , Pacific Northwest National Laboratory , Richland , Washington 99352 , United States.

Texas Advanced Computing Center , University of Texas at Austin , Austin , Texas 78758 , United States.

出版信息

J Proteome Res. 2018 Aug 3;17(8):2623-2634. doi: 10.1021/acs.jproteome.8b00086. Epub 2018 Jul 18.

Abstract

Lung diseases and disorders are a leading cause of death among infants. Many of these diseases and disorders are caused by premature birth and underdeveloped lungs. In addition to developmentally related disorders, the lungs are exposed to a variety of environmental contaminants and xenobiotics upon birth that can cause breathing issues and are progenitors of cancer. In order to gain a deeper understanding of the developing lung, we applied an activity-based chemoproteomics approach for the functional characterization of the xenometabolizing cytochrome P450 enzymes, active ATP and nucleotide binding enzymes, and serine hydrolases using a suite of activity-based probes (ABPs). We detected P450 activity primarily in the postnatal lung; using our ATP-ABP, we characterized a wide range of ATPases and other active nucleotide- and nucleic acid-binding enzymes involved in multiple facets of cellular metabolism throughout development. ATP-ABP targets include kinases, phosphatases, NAD- and FAD-dependent enzymes, RNA/DNA helicases, and others. The serine hydrolase-targeting probe detected changes in the activities of several proteases during the course of lung development, yielding insights into protein turnover at different stages of development. Select activity-based probe targets were then correlated with RNA in situ hybridization analyses of lung tissue sections.

摘要

肺部疾病和障碍是婴儿死亡的主要原因之一。这些疾病和障碍中的许多是由早产和肺部发育不良引起的。除了与发育有关的疾病外,出生后肺部还会接触到各种环境污染物和外源性化学物质,这些物质会导致呼吸问题,并引发癌症。为了更深入地了解发育中的肺部,我们应用基于活性的化学蛋白质组学方法,使用一系列基于活性的探针(ABPs)来研究异种代谢细胞色素 P450 酶、活跃的 ATP 和核苷酸结合酶以及丝氨酸水解酶的功能特征。我们主要在出生后的肺部中检测到 P450 活性;使用我们的 ATP-ABP,我们在整个发育过程中描述了一系列广泛的与细胞代谢的多个方面有关的 ATP 酶和其他活跃的核苷酸和核酸结合酶。ATP-ABP 的靶标包括激酶、磷酸酶、NAD 和 FAD 依赖性酶、RNA/DNA 解旋酶等。靶向丝氨酸水解酶的探针在肺发育过程中检测到几种蛋白酶活性的变化,深入了解了不同发育阶段的蛋白质周转情况。然后,选择基于活性的探针靶标与肺组织切片的 RNA 原位杂交分析相关联。

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