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早产儿的端粒比足月儿长得多。

Preterm infants have significantly longer telomeres than their term born counterparts.

作者信息

Vasu Vimal, Turner Kara J, George Shermi, Greenall John, Slijepcevic Predrag, Griffin Darren K

机构信息

Department of Child Health, East Kent Hospitals University Foundation NHS Trust, William Harvey Hospital, Ashford, Kent, United Kingdom.

University of Kent, School of Biosciences, Giles Lane, Canterbury, Kent, United Kingdom.

出版信息

PLoS One. 2017 Jun 28;12(6):e0180082. doi: 10.1371/journal.pone.0180082. eCollection 2017.

Abstract

There are well-established morbidities associated with preterm birth including respiratory, neurocognitive and developmental disorders. However several others have recently emerged that characterise an 'aged' phenotype in the preterm infant by term-equivalent age. These include hypertension, insulin resistance and altered body fat distribution. Evidence shows that these morbidities persist into adult life, posing a significant public health concern. In this study, we measured relative telomere length in leukocytes as an indicator of biological ageing in 25 preterm infants at term equivalent age. Comparing our measurements with those from 22 preterm infants sampled at birth and from 31 term-born infants, we tested the hypothesis that by term equivalent age, preterm infants have significantly shorter telomeres (thus suggesting that they are prematurely aged). Our results demonstrate that relative telomere length is highly variable in newborn infants and is significantly negatively correlated with gestational age and birth weight in preterm infants. Further, longitudinal assessment in preterm infants who had telomere length measurements available at both birth and term age (n = 5) suggests that telomere attrition rate is negatively correlated with increasing gestational age. Contrary to our initial hypothesis however, relative telomere length was significantly shortest in the term born control group compared to both preterm groups and longest in the preterm at birth group. In addition, telomere lengths were not significantly different between preterm infants sampled at birth and those sampled at term equivalent age. These results indicate that other, as yet undetermined, factors may influence telomere length in the preterm born infant and raise the intriguing hypothesis that as preterm gestation declines, telomere attrition rate increases.

摘要

早产存在一些已被充分证实的相关疾病,包括呼吸系统、神经认知和发育障碍。然而,最近又出现了其他几种疾病,这些疾病在相当于足月年龄的早产儿中表现出一种“衰老”的表型。这些疾病包括高血压、胰岛素抵抗和身体脂肪分布改变。有证据表明,这些疾病会持续到成年期,这引起了重大的公共卫生问题。在本研究中,我们测量了25名相当于足月年龄的早产儿白细胞中的相对端粒长度,作为生物衰老的一个指标。将我们的测量结果与22名出生时采样的早产儿和31名足月儿的测量结果进行比较,我们检验了这样一个假设:到相当于足月年龄时,早产儿的端粒明显更短(因此表明他们过早衰老)。我们的结果表明,新生儿的相对端粒长度高度可变,并且与早产儿的胎龄和出生体重显著负相关。此外,对出生时和足月时都有端粒长度测量值的早产儿(n = 5)进行的纵向评估表明,端粒损耗率与胎龄增加呈负相关。然而,与我们最初的假设相反,与两个早产组相比,足月出生的对照组的相对端粒长度最短,而出生时早产组的相对端粒长度最长。此外,出生时采样的早产儿和相当于足月年龄采样的早产儿之间的端粒长度没有显著差异。这些结果表明,其他尚未确定的因素可能会影响早产婴儿的端粒长度,并提出了一个有趣的假设,即随着早产孕周的减少,端粒损耗率会增加。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2967/5489189/0b1d7652f5da/pone.0180082.g001.jpg

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