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血浆蛋白质组学揭示了机械通气对不同胎龄的特异性反应,并确定了引发早产儿肺损伤的机制途径。

Plasma proteomics reveals gestational age-specific responses to mechanical ventilation and identifies the mechanistic pathways that initiate preterm lung injury.

机构信息

Neonatal Research, Murdoch Childrens Research Institute, Parkville, Australia.

Department of Paediatrics, University of Melbourne, Parkville, Australia.

出版信息

Sci Rep. 2018 Aug 22;8(1):12616. doi: 10.1038/s41598-018-30868-x.

Abstract

The preterm lung is particularly vulnerable to ventilator-induced lung injury (VILI) as a result of mechanical ventilation. However the developmental and pathological cellular mechanisms influencing the changing patterns of VILI have not been comprehensively delineated, preventing the advancement of targeted lung protective therapies. This study aimed to use SWATH-MS to comprehensively map the plasma proteome alterations associated with the initiation of VILI following 60 minutes of standardized mechanical ventilation from birth in three distinctly different developmental lung states; the extremely preterm, preterm and term lung using the ventilated lamb model. Across these gestations, 34 proteins were differentially altered in matched plasma samples taken at birth and 60 minutes. Multivariate analysis of the plasma proteomes confirmed a gestation-specific response to mechanical ventilation with 79% of differentially-expressed proteins altered in a single gestation group only. Six cellular and molecular functions and two physiological functions were uniquely enriched in either the extremely preterm or preterm group. Correlation analysis supported gestation-specific protein-function associations within each group. In identifying the gestation-specific proteome and functional responses to ventilation we provide the founding evidence required for the potential development of individualized respiratory support approaches tailored to both the developmental and pathological state of the lung.

摘要

早产儿的肺部由于机械通气而特别容易受到呼吸机引起的肺损伤(VILI)的影响。然而,影响 VILI 变化模式的发育和病理细胞机制尚未得到全面阐述,这阻碍了针对肺保护治疗的进展。本研究旨在使用 SWATH-MS 全面绘制与出生后 60 分钟标准化机械通气开始时 VILI 相关的血浆蛋白质组改变,在三种明显不同的发育肺状态下使用通气羊模型;极早产儿、早产儿和足月产肺。在这些妊娠期间,出生时和 60 分钟时采集的匹配血浆样本中有 34 种蛋白质发生了差异改变。对血浆蛋白质组的多元分析证实了机械通气的胎龄特异性反应,只有 79%的差异表达蛋白在单个胎龄组中发生改变。6 个细胞和分子功能以及 2 个生理功能仅在极早产儿或早产儿组中得到了独特的富集。相关性分析支持了每个组内的胎龄特异性蛋白-功能关联。在确定胎龄特异性蛋白质组和对通气的功能反应时,我们提供了潜在发展个体化呼吸支持方法所需的基础证据,这些方法针对肺的发育和病理状态进行了调整。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/17eb/6105628/eee687cf5834/41598_2018_30868_Fig1_HTML.jpg

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