Differences in autophagy marker levels at birth in preterm vs. term infants-Reference-Cited by-同舟云学术

Differences in autophagy marker levels at birth in preterm vs. term infants

Published:2024-05-29 Issue: Volume: Page:
ISSN:0031-3998
Container-title:Pediatric Research
language:en
Short-container-title:Pediatr Res

Author:

Künstle Noëmi,Gorlanova Olga,Marten Andrea,Müller Loretta,Sharma Pawan,Röösli Martin,Sinues Pablo,Schär Primo,Schürmann David,Rüttimann Céline,Da Silva Sena Carla Rebeca,Nahum Uri,Usemann Jakob,Steinberg Ruth,Yammine Sophie,Schulzke Sven,Latzin Philipp,Frey Urs^ORCID, ,Beck Fiona,Bovermann Xenia,Casaulta Carmen,Curdy Marion,Da Silva Sena Carla Rebeca,de Hoogh Kees,Frauchiger Bettina,Ho Dac Léa Kim-Mi,Kieninger Elisabeth,Korten Insa,Oestreich Marc-Alexander,Stöcklin Benjamin,Streibel Carmen,Wyler Florian

Abstract

Abstract Background Preterm infants are susceptible to oxidative stress and prone to respiratory diseases. Autophagy is an important defense mechanism against oxidative-stress-induced cell damage and involved in lung development and respiratory morbidity. We hypothesized that autophagy marker levels differ between preterm and term infants. Methods In the prospective Basel-Bern Infant Lung Development (BILD) birth cohort we compared cord blood levels of macroautophagy (Beclin-1, LC3B), selective autophagy (p62) and regulation of autophagy (SIRT1) in 64 preterm and 453 term infants. Results Beclin-1 and LC3B did not differ between preterm and term infants. However, p62 was higher (0.37, 95% confidence interval (CI) 0.05;0.69 in log2-transformed level, p = 0.025, padj = 0.050) and SIRT1 lower in preterm infants (−0.55, 95% CI −0.78;−0.31 in log2-transformed level, padj < 0.001). Furthermore, p62 decreased (padj-value for smoothing function was 0.018) and SIRT1 increased (0.10, 95% CI 0.07;0.13 in log2-transformed level, padj < 0.001) with increasing gestational age. Conclusion Our findings suggest differential levels of key autophagy markers between preterm and term infants. This adds to the knowledge of the sparsely studied field of autophagy mechanisms in preterm infants and might be linked to impaired oxidative stress response, preterm birth, impaired lung development and higher susceptibility to respiratory morbidity in preterm infants. Impact

To the best of our knowledge, this is the first study to investigate autophagy marker levels between human preterm and term infants in a large population-based sample in cord blood plasma

This study demonstrates differential levels of key autophagy markers in preterm compared to term infants and an association with gestational age

This may be linked to impaired oxidative stress response or developmental aspects and provide bases for future studies investigating the association with respiratory morbidity

Publisher

Springer Science and Business Media LLC

Link

https://www.nature.com/articles/s41390-024-03273-6.pdf

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