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早产儿相关阻塞性肺疾病与慢性阻塞性肺疾病的代谢组学紊乱的相似性。

Similarities of metabolomic disturbances in prematurity-associated obstructive lung disease to chronic obstructive pulmonary disease.

机构信息

Department of Child Health, School of Medicine, Cardiff University, Heath Park, Cardiff, CF14 4XN, UK.

Faculty of Life Sciences, University of Bristol, Bristol, UK.

出版信息

Sci Rep. 2024 Oct 7;14(1):23294. doi: 10.1038/s41598-024-73704-1.

Abstract

Prematurity-associated lung disease (PLD) is a long-term consequence of preterm-birth. Since the underlying mechanisms of PLD remain poorly characterised, we compared the urinary metabolome between recently described spirometry phenotypes of PLD. Preterm- and term-born children aged 7-12 years, from the Respiratory Health Outcomes in Neonates (RHiNO) cohort, underwent spirometry and urine collection. The urinary metabolome was analysed by gas chromatography time-of-flight mass spectrometry. Preterm-born children were classified into phenotypes of prematurity-associated obstructive lung disease (POLD, Forced expiratory volume in 1 s (FEV) < lower limit of normal (LLN), FEV/Forced Vital Capacity (FVC) < LLN), prematurity-associated preserved ratio impaired spirometry (pPRISm, FEV < LLN, FEV/FVC ≥ LLN) and Preterm/Term controls (FEV ≥ LLN). Metabolite set enrichment analysis was used to link significantly altered metabolites between the groups with metabolic pathways. Univariable and multivariable linear regression models examined associations between early and current life factors and significantly altered metabolites of interest. Urine from 197 preterm- and 94 term-born children was analysed. 23 and 25 were classified into POLD and pPRISm groups respectively. Of 242 identified metabolites, 49 metabolites were significantly altered in the POLD group compared with Preterm controls. Decreased capric acid (log fold change - 0.23; p = 0.003), caprylic acid (- 0.18; 0.003) and ceratinic acid (- 0.64; 0.014) in the POLD group, when compared to preterm controls, were linked with reduced β-oxidation of very long chain fatty acids (p = 0.004). Reduced alanine (log fold change - 0.21; p = 0.046), glutamic acid (- 0.24; 0.023), and pyroglutamic acid (- 0.17; 0.035) were linked with decreased glutathione metabolism (p = 0.008). These metabolites remained significantly associated with POLD in multivariable models adjusting for early/current life factors. The pPRISm urinary metabolome was minimally changed when compared with preterm-born controls. When compared to term-born subjects, alterations in tryptophan metabolism were implicated (p = 0.01). The urinary metabolome in POLD showed significantly altered β-oxidation of fatty acids and glutathione metabolism, implying alterations in cellular metabolism and oxidative stress. Similar findings have been noted in adults with chronic obstructive pulmonary disease. Given the similarity of findings between the POLD group and those reported for COPD, the POLD group should be considered at future risk of developing COPD.

摘要

早产儿相关肺病(PLD)是早产儿出生的长期后果。由于 PLD 的潜在机制仍未得到很好的描述,我们比较了最近描述的 PLD 肺功能表型之间的尿代谢组。来自新生儿呼吸健康结果(RHiNO)队列的 7-12 岁的早产儿和足月儿接受了肺功能检查和尿液采集。通过气相色谱飞行时间质谱分析尿代谢组。将早产儿分为与早产相关的阻塞性肺病(POLD,1 秒用力呼气量(FEV)<正常下限(LLN),FEV/用力肺活量(FVC)<LLN)、与早产相关的保留比值受损的肺功能表型(pPRISm,FEV<LLN,FEV/FVC≥LLN)和早产/足月对照(FEV≥LLN)。代谢物集富集分析用于将组间差异显著的代谢物与代谢途径联系起来。单变量和多变量线性回归模型研究了早期和当前生活因素与感兴趣的代谢物变化之间的关联。对 197 名早产儿和 94 名足月儿的尿液进行了分析。23 名和 25 名分别被分类为 POLD 和 pPRISm 组。在 242 种鉴定出的代谢物中,与早产儿对照组相比,POLD 组有 49 种代谢物发生了显著改变。与早产儿对照组相比,POLD 组中的癸酸(对数倍数变化-0.23;p=0.003)、辛酸(-0.18;0.003)和角鲨烯酸(-0.64;0.014)减少,表明极长链脂肪酸的β-氧化减少(p=0.004)。与早产儿对照组相比,丙氨酸(对数倍数变化-0.21;p=0.046)、谷氨酸(-0.24;0.023)和焦谷氨酸(-0.17;0.035)减少与谷胱甘肽代谢减少有关(p=0.008)。这些代谢物在调整早期/当前生活因素的多变量模型中与 POLD 仍有显著关联。与早产儿对照组相比,pPRISm 的尿代谢组变化很小。与足月出生的受试者相比,色氨酸代谢的改变被牵连(p=0.01)。POLD 组的尿代谢组显示脂肪酸的β-氧化和谷胱甘肽代谢发生明显改变,表明细胞代谢和氧化应激发生改变。在慢性阻塞性肺疾病(COPD)的成年人中也发现了类似的发现。鉴于 POLD 组与 COPD 报告的结果之间存在相似性,应考虑 POLD 组在未来有患 COPD 的风险。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ad86/11458810/ba52a5b2dca6/41598_2024_73704_Fig1_HTML.jpg

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