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首页> 美国卫生研究院文献>other >Abundances of placental imprinted genes CDKN1C PHLDA2 and IGF-2 are related to low birth weight and early catch-up growth in full-term infants born small for gestational age
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Abundances of placental imprinted genes CDKN1C PHLDA2 and IGF-2 are related to low birth weight and early catch-up growth in full-term infants born small for gestational age

机译:胎盘印记基因CDKN1CPHLDA2和IGF-2的丰富与低胎龄和小于胎龄的足月儿的早期追赶生长有关

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Children born small for gestational age (SGA) generally have a catch-up growth and rapid weight gain in the first years of life, which is a high risk of insulin resistance and cardiovascular diseases later in life. It was reported that the level of imprinted genes IGF-2, CDKN1C and PHLDA2 regulates placental growth. We assessed these imprinted genes expression levels in placental tissue and their influences on catch-up growth of full-term SGA infants. The protein and mRNA levels of placental CDKN1C, PHLDA2 and IGF-2 were analyzed in 29 full-term SGA and 29 full-term infants born appropriate for gestational age (AGA) using quantitative RT-PCR and Western blot assay, respectively. Catch-up growth was indicated by increased standard deviation score (ΔSDS) of weight at 1, 3 and 6 months relative to birth weight (BW). Correlations between indicated variables were evaluated using Pearson correlation coefficient analysis. Compared to AGA infants, CDKN1C and PHLDA2 levels were significantly increased, whereas IGF-2 was significantly reduced in SGA infants. The value of ΔSDS was significantly higher in SGA than that in AGA infants. For SGA status, Pearson analysis shows i) a negative correlation of CDKN1C and PHLDA2 abundances with BW, and a positive correlation of IGF-2 with BW, ii) no correlation between the three imprinted gene abundances and placental weight (PW), and between PW and BW, iii) a positive correlation of PHLDA2 abundance with CDKN1C, and iv) a positive correlation of CDKN1C and PHLDA2 abundances with ΔSDS, and a negative correlation of IGF-2 with ΔSDS at 1, 3 and 6 months. Taken together, increased CDKN1C and PHLDA2 and reduced IGF-2 abundances in placental tissue were related to BW and early period catch-up growth in full-term SGA infants. Placental CDKN1C, PHLDA2 and IGF-2 level monitoring may be useful for predicting and preventing the development of SGA.
机译:小于胎龄期(SGA)的儿童通常在出生后的第一年就具有追赶性的成长和快速的体重增加,这在以后的生活中存在胰岛素抵抗和心血管疾病的高风险。据报道,印迹基因IGF-2,CDKN1C和PHLDA2的水平调节胎盘的生长。我们评估了胎盘组织中这些印迹基因的表达水平及其对足月SGA婴儿追赶性生长的影响。使用定量RT-PCR和Western blot分析法分别分析了29例足月SGA和29例足月婴儿的胎盘CDKN1C,PHLDA2和IGF-2的蛋白质和mRNA水平。相对于出生体重(BW),体重增加的标准偏差评分(ΔSDS)在第1、3和6个月时表明了追赶性增长。使用Pearson相关系数分析评估了指示变量之间的相关性。与AGA婴儿相比,SGA婴儿的CDKN1C和PHLDA2水平显着升高,而IGF-2显着降低。 SGA中的ΔSDS值显着高于AGA婴儿。对于SGA状态,Pearson分析显示:i)CDKN1C和PHLDA2丰度与BW呈负相关,IGF-2与BW呈正相关,ii)三种印迹基因丰度与胎盘重量(PW)之间,以及两者之间无相关性PW和BW,iii)PHLDA2丰度与CDKN1C正相关,iv)CDKN1C和PHLDA2丰度与ΔSDS正相关, IGF-2 与ΔSDS在1,3之间呈负相关。和6个月。综上所述,胎盘组织中 CDKN1C PHLDA2 的增加以及 IGF-2 的减少与体重和全程早期追赶性生长有关。 SGA足月儿。胎盘 CDKN1C PHLDA2 IGF-2 水平监测可能有助于预测和预防SGA的发展。

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