新生儿呼吸窘迫综合征中 LPCAT1-rs9728 多态性与脐带血 IL-10、MIF 和 VEGF 水平的关系:一项病例对照研究

Khalid M. Mohany, Ahmed Abdelrasoul Sayed, Osama Mahmoud El-Asheer, Yaser F. Abdel Raheem, Ahmed Mohamed Abbas, Ahmed Mohamed Fawzy, Mona Abd El-Hamid Hassan El-Baz
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摘要

溶血磷脂酰基转移酶(LPCAT)对表面活性剂的生物合成至关重要。它由 LPCAT 基因编码。我们研究了新生儿呼吸窘迫综合征(NRDS)病例中的 LPCAT1-rs9728 基因型及其与脐带动脉血清白细胞介素-10(IL-10)、巨噬细胞迁移抑制因子(MIF)和血管内皮生长因子(VEGF)水平的可能关联。该研究包括 160 名新生儿,分为 G1 组(60 名健康新生儿)和 G2 组(100 名 NRDS 病例)。IL-10、MIF和血管内皮生长因子水平通过相应的试剂盒进行测定。使用 Gene JETTM 全血基因组 DNA 纯化迷你试剂盒从新生儿静脉血中提取 DNA。采用实时定量聚合酶链反应对 LPCAT1-rs9728 进行基因分型。G2期的IL-10和MIF水平明显高于G1期,而VEGF水平则明显低于G1期。G2 中 LPCAT1-rs9728 AA 和 LPCAT1-rs9728 AG 基因型的百分比明显高于 G1。LPCAT1-rs9728 AA 基因型新生儿的 IL-10 和 MIF 水平明显高于 LPCAT1-rs9728 AG 和 LPCAT1-rs9728 GG 基因型新生儿,而 LPCAT1-rs9728 AG 基因型新生儿的血管内皮生长因子水平、出生体重以及 1 分钟和 5 分钟的 APGAR 评分则明显低于 LPCAT1-rs9728 GG 基因型新生儿。LPCAT1-rs9728 AA 基因型及其 A 等位基因与 NRDS 的发展和严重程度存在关联。进一步的研究可能会更好地了解这种关联,从而有助于未来的管理。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The association of LPCAT1-rs9728 polymorphism with cord blood IL-10, MIF, and VEGF levels in neonatal respiratory distress syndrome: a case–control study
Lysophospholipid acyltransferase (LPCAT) is crucial for surfactant biosynthesis. It is encoded by LPCAT genes. We investigated the LPCAT1-rs9728 genotypes in neonatal respiratory distress syndrome (NRDS) cases and their possible association with the cord arterial serum interleukin-10 (IL-10), macrophage migration inhibitory factor (MIF), and vascular endothelial growth factor (VEGF) levels. The study included 160 neonates grouped into G1: 60 healthy neonates and G2: 100 NRDS cases. IL-10, MIF, and VEGF levels were measured by their corresponding kits. The Gene JETTM Whole Blood Genomic DNA Purification Mini Kit was used to extract the DNA from the newborn venous blood. The quantitative real-time polymerase chain reaction was carried out for LPCAT1-rs9728 genotyping. The IL-10 and MIF levels were significantly higher, while VEGF levels were significantly lower in G2 than in G1. The percentages of LPCAT1-rs9728 AA and LPCAT1-rs9728 AG genotypes were significantly higher in G2 than in G1. The IL-10 and MIF levels were significantly higher, while the VEGF levels, birth weight, and APGAR score at 1 and 5 min were significantly lower in neonates with LPCAT1-rs9728 AA genotype than in neonates with LPCAT1-rs9728 AG and LPCAT1-rs9728 GG genotypes and in neonates with LPCAT1-rs9728 AG genotype than in neonates with LPCAT1-rs9728 GG genotype. There is an association between the LPCAT1-rs9728 AA genotype and its A allele and the NRDS development and severity. Further research may provide a better understanding of this association to help future management.
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