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乳铁蛋白与早产儿晚发性败血症的预防。

Lactoferrin and prevention of late-onset sepsis in the pre-term neonates.

机构信息

Neonatal Intensive Care Units of S. Anna Hospital, Turin, Italy.

出版信息

Early Hum Dev. 2010 Jul;86 Suppl 1:59-61. doi: 10.1016/j.earlhumdev.2010.01.009. Epub 2010 Feb 6.

Abstract

Late-onset sepsis (LOS) affects a large proportion of pre-term neonates in neonatal intensive care units (NICUs) worldwide, with high morbidity and related mortality, and frequent occurrence of severe late neurodevelopmental impairment. Due to the frequency, severity and difficulties in early diagnosis and prompt therapy, prevention is crucial for decreasing the burden of infection-related complications in NICUs. It is well known that feeding with fresh maternal milk, hygiene measures and the cautious use of H2-blockers are related with a decreased risk of developing sepsis. However, evidence from randomised clinical trials exists only for fluconazole in the prevention of fungal infections in the NICU. Lactoferrin is the main whey protein in mammalian milk, and is involved in innate immune host defences. Notably, human lactoferrin can be found at increased concentrations in colostrum and in milk from mothers of premature neonates. Human (hLF) and bovine lactoferrin (bLF) share a high (77%) amino-acid homology, and the same N-terminal peptide responsible for antimicrobial activity, called lactoferricin. In vitro, bLF shows potent direct antimicrobial activity against all types of pathogens, which occurs via anti-cell wall actions and leads to disintegration of the micro-organism's membranes. bLF is also synergistic with many antimicrobials and antifungals, and promotes growth and differentiation of the immature gut. Based on this background data, a randomised clinical trial was recently conducted in very low birth weight pre-term neonates given bLF alone or with the probiotic Lactobacillus GG. The aim of the trial was to assess the ability of bLF to prevent late-onset sepsis of any origin in the studied infants during their stay in the NICU. This article discusses the preliminary data from this study, along with the proposed mechanisms of action of bLF in pre-term infants.

摘要

迟发性败血症(LOS)影响全球新生儿重症监护病房(NICU)中很大一部分早产儿,具有高发病率和相关死亡率,并且经常发生严重的晚期神经发育损伤。由于早期诊断和及时治疗的频率、严重程度和困难,预防对于减少 NICU 感染相关并发症的负担至关重要。众所周知,用新鲜的母乳喂养、卫生措施和谨慎使用 H2 阻滞剂与降低发生败血症的风险有关。然而,在预防 NICU 真菌感染方面,只有氟康唑的随机临床试验证据。乳铁蛋白是哺乳动物乳中的主要乳清蛋白,参与先天免疫宿主防御。值得注意的是,人乳铁蛋白可以在初乳和早产儿母亲的乳汁中以更高的浓度发现。人乳铁蛋白(hLF)和牛乳铁蛋白(bLF)具有很高的(77%)氨基酸同源性,并且具有相同的负责抗菌活性的 N 端肽,称为乳铁蛋白。在体外,bLF 对所有类型的病原体都表现出强大的直接抗菌活性,这种活性通过抗细胞壁作用发生,并导致微生物膜的崩解。bLF 还与许多抗菌剂和抗真菌剂协同作用,并促进未成熟肠道的生长和分化。基于这些背景数据,最近在极低出生体重早产儿中单独给予 bLF 或与益生菌鼠李糖乳杆菌 GG 进行了一项随机临床试验。该试验的目的是评估 bLF 预防研究婴儿在 NICU 期间发生任何来源的迟发性败血症的能力。本文讨论了来自该研究的初步数据,以及 bLF 在早产儿中的作用机制。

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