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Insulin-like growth factor I, epidermal growth factor and transforming growth factor beta expression and their association with intrauterine fetal growth retardation, such as development during human pregnancy.

机译:胰岛素样生长因子I,表皮生长因子和转化生长因子β表达及其与宫内胎儿生长迟缓的关系,例如人体妊娠期间的发育。

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AIM: Fetal intrauterine growth retardation (IUGR) is one of the most common obstetric problems, with a frequency of 12% in Mexico. In the past, investigations have focused on extrinsic causes of IUGR. More recent studies have examined the intrinsic factors that cause fetal intrauterine growth. Maintenance of fetal growth has been attributed to insulin-like growth factor (IGF), epidermal growth factor (EGF) and transforming growth factor beta (TGF-beta). The objective of this study was to assess the levels of these growth factors during pregnancy and to determine whether or not low concentrations are associated with IUGR. METHODS: Nine women whose pregnancies were complicated by IUGR and a group of nine women whose pregnancies exhibited normal fetal intrauterine growth were studied. IUGR was determined by sonography and confirmed by weight at birth. Venous blood samples were taken from both groups of pregnant women at the end of each trimester. Enzyme-linked immunosorbent assays, immunoradiometric assays and radioimmunoassays were used to process samples, and the results were analysed by anova. RESULTS: IGF-I levels increased in both groups during pregnancy, but the increase was lower (p < 0.001) in the IUGR group throughout pregnancy and at delivery. EGF did not show any significant changes during pregnancy. Blood TGF-beta levels varied only during the first trimester of pregnancy. The differences were not statistically significant. However, TGF-beta concentrations were higher in the pregnancies with IUGR. Women in the IUGR group were smaller than in the control group (p < 0.05), and, using the covariance test (p < 0.05), this was found to be correlated with IGF-I levels but not with EGF or TGF-beta levels. CONCLUSIONS: Changes in fetal weight might be explained by the different concentrations of IGF. The structural homology between IGF-1 and insulin could mean that the presence of higher levels of IGF would result in a increased energetic metabolism that could contribute to fetal growth. EGF levels were not related to IUGR, and TGF-beta levels increased only during the first 3 months in the IUGR group. This observation correlates with the in vitro action of TGF-beta as a negative factor of growth, but as a positive support for sustaining early pregnancy. Our data illustrates that low height represents an increased risk factor for IUGR. These data also correlate with the studies involving extrinsic factors.
机译:目的:胎儿宫内生长迟缓(IUGR)是最常见的产科问题之一,墨西哥的频率为12%。在过去,调查侧重于IUGR的外在原因。最近的研究已经研究了导致胎儿宫内生长的内在因素。胎儿生长的维持归因于胰岛素样生长因子(IGF),表皮生长因子(EGF)和转化生长因子β(TGF-β)。本研究的目的是评估怀孕期间这些生长因子的水平,并确定低浓度是否与IUGR相关。方法:IUGR和一群怀孕表现出正常胎儿宫内生产的九名妇女的九个妇女进行了九个妇女。 IUGR由超声检查确定并在出生时得到重量。在每个三月末的孕妇两组中取静脉血样。使用酶联免疫吸附测定,免疫放射性测定和放射免疫测定法用于处理样品,并通过ANOVA分析结果。结果:IGF-I水平在怀孕期间两组增加,但在整个妊娠和交付时,IUGR组的增加较低(P <0.001)。 EGF在怀孕期间没有显示任何重大变化。血液TGF-β水平仅在怀孕的第一个三个月时变化。差异没有统计学意义。然而,IUGR妊娠的TGF-β浓度较高。 IUGR组中的女性小于对照组(P <0.05),并且使用协方差测试(P <0.05),发现该妇女与IGF-I水平相关,但不具有EGF或TGF-β水平的相关性。结论:胎儿重量的变化可能是通过不同浓度的IGF解释。 IGF-1和胰岛素之间的结构性同源性可能意味着较高水平的IGF的存在会导致有助于胎儿生长的高能量代谢。 EGF水平与IUGR无关,TGF-Beta水平仅在IUGR组的前3个月内增加。该观察结果与TGF-β的体外作用相关,作为生长的负面因素,而是作为维持早期妊娠的阳性载体。我们的数据说明了低高度代表了IUGR的危险因素增加。这些数据也与涉及外在因素的研究相关。

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