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钙信号相关蛋白与支气管肺发育不良的进展有关。

Calcium signaling-related proteins are associated with broncho-pulmonary dysplasia progression.

机构信息

ProMiFa, Protein Microsequencing Facility, San Raffaele Scientific Institute, Milan, Italy.

出版信息

J Proteomics. 2013 Dec 6;94:401-12. doi: 10.1016/j.jprot.2013.10.007. Epub 2013 Oct 16.

Abstract

UNLABELLED

Broncho-pulmonary dysplasia (BPD) is a chronic pulmonary disorder that follows premature birth. It is preceded by respiratory distress syndrome (RDS), characterized by acute respiratory failure due to deficiency of surfactant at birth. Clinical characteristics of infants affected by BPD have widely changed in the last decades: they are extraordinarly immature, with impaired alveolar and vascular lung development. To build up new therapeutic strategies for BPD babies, it is necessary to understand the pathogenic mechanisms, which are complicated by environmental risk factors and genetic predisposition. Therefore, the aim of this study was to highlight protein changes in the broncho-alveolar lavage fluid (BALF), thus providing an appropriate picture on what is happening in the locus of injury. We analyzed BALF samples from preterm babies, born at different stages of lung development. We confirmed that gestational age is relevant for BPD progression, but we also detected few de-regulated proteins in the younger babies; we discovered less abundant calcium signaling-related proteins, consistent with BPD severity, comparing severe to mild BPD babies with matched gestational age. In conclusion, this study suggests a subset of proteins to be investigated to better treat BPD babies and facilitate the definition of potential drug targets for novel therapies.

BIOLOGICAL SIGNIFICANCE

Pulmonary biomarkers are needed to predict the clinical course of lung disease, status, progression and response to treatment. A key aspect in biomarker discovery is uncovering molecules that appear early during disease initiation, when the natural history of the disease can be modified. Using a proteomic-based approach we compared broncho-alveolar lavage fluid (BALF) protein profile from preterm neonates at different postmenstrual ages, to have a molecular description of broncho-pulmonary dysplasia (BPD) progression. BALF provided a snapshot of local molecular changes, which are relevant for early diagnosis, assessment and characterization of lung disorders. We showed that even if the studied patients had similar clinical phenotype (they all developed severe BPD and they were all cured in the same way in terms of mechanical ventilation, surfactant administration, antenatal steroid treatment and ibuprofen treatment for patent ductus arteriosus), however their BALF protein profiling displayed significant differences in a subset of proteins, which could be exploited to facilitate the development of novel effective therapies, distinct for age and severity of the disease.

摘要

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支气管肺发育不良(BPD)是一种早产儿发生的慢性肺部疾病。它以前是呼吸窘迫综合征(RDS),其特征是由于出生时缺乏表面活性剂而导致急性呼吸衰竭。过去几十年,受 BPD 影响的婴儿的临床特征发生了广泛变化:他们极其不成熟,肺泡和血管肺发育受损。为了为 BPD 婴儿建立新的治疗策略,有必要了解发病机制,这些机制受到环境风险因素和遗传易感性的影响。因此,本研究的目的是强调支气管肺泡灌洗液(BALF)中的蛋白质变化,从而提供有关损伤部位发生情况的适当图片。我们分析了来自不同肺发育阶段早产儿的 BALF 样本。我们证实胎龄与 BPD 进展有关,但我们也在年幼的婴儿中检测到了少数失调蛋白;与胎龄匹配的严重和轻度 BPD 婴儿相比,我们发现钙信号相关蛋白的丰度较低,这与 BPD 的严重程度一致。总之,这项研究提出了一组有待研究的蛋白质,以更好地治疗 BPD 婴儿,并为新疗法的潜在药物靶点的定义提供便利。

生物学意义

肺生物标志物可用于预测肺部疾病的临床过程、状态、进展和对治疗的反应。在生物标志物发现中,一个关键方面是揭示在疾病起始时出现的分子,那时疾病的自然史可以改变。我们使用基于蛋白质组学的方法比较了不同胎龄的早产儿支气管肺泡灌洗液(BALF)的蛋白质谱,以对支气管肺发育不良(BPD)的进展进行分子描述。BALF 提供了局部分子变化的快照,这些变化与早期诊断、评估和肺部疾病的特征有关。我们表明,即使研究中的患者具有相似的临床表型(他们都患有严重的 BPD,并且在机械通气、表面活性剂给药、产前类固醇治疗和前列腺素治疗动脉导管未闭方面的治疗方式相同),然而,他们的 BALF 蛋白谱在一组蛋白质中显示出显著差异,这些蛋白质可能被利用来促进新型有效疗法的开发,这些疗法针对疾病的年龄和严重程度而有所不同。

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