早产儿视网膜病变单胺系统水平的实验预测价值。

IF 1.1 Q4 MEDICINE, RESEARCH & EXPERIMENTAL Sovremennye Tehnologii v Medicine Pub Date : 2021-01-01 Epub Date: 2021-06-28 DOI:10.17691/stm2021.13.3.05
L А Katargina, N А Osipova, А Y Panova, N S Bondarenko, Yu О Nikishina, А R Murtazina, М V Ugrumov
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引用次数: 0

摘要

该研究的目的是研究左旋多巴、多巴胺和去甲肾上腺素的全身水平,并评估它们在实验性疾病模型早产儿视网膜病变(ROP)发展中的预后价值。材料与方法:选取Wistar幼鼠(n=36),分为研究组(实验性ROP幼鼠,n=17)和对照组(n=19)。两组动物分别于第14、21-23和28-30天处死。在一个实验中,指示周期的选择与ROP发展的关键阶段相对应,并基于我们之前的组织学研究结果。测定幼鼠血浆样本中的多巴胺、左旋多巴和去甲肾上腺素水平。结果:实验第14天(应用模型病理新生血管诱导和儿童临床前ROP对应的时间),ROP组大鼠的平均左旋多巴水平(0.31 ng/ml)明显低于对照组(0.42 ng/ml) (p≤0.01)。在实验第21-23天(应用模型病理视网膜外新生血管生长和儿童ROP 3期对应的时间),研究组全身左旋多巴水平(0.87 ng/ml)仍低于对照组(1.53 ng/ml) (p≤0.01)。在实验的第28-30天(对应于应用模型的新生血管回归和儿童自发ROP回归阶段),研究组血浆中L-DOPA水平(0.33 ng/ml)与对照组(0.21 ng/ml)相比有不显著的上升趋势。在所有随访期间,各组的平均多巴胺和去甲肾上腺素水平没有差异。结论:在实验性ROP的临床前阶段,低的全身左旋多巴水平可作为发展中的病理过程的实验室预后标准;这将有助于在制定优化现有儿童疾病筛查系统的措施时使用该标准。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Prognostic Value Estimation of Monoamines Systemic Level in Retinopathy of Prematurity in Experiment.

The aim of the investigation was to study a systemic level of L-DOPA, dopamine, and norepinephrine, and assess their prognostic value in retinopathy of prematurity (ROP) development on an experimental disease model.

Materials and methods: The investigation was carried out on infant Wistar rats (n=36) divided into a study group (rat infants with experimental ROP, n=17) and a control group (n=19). The animals of both groups were sacrificed on days 14, 21-23, and on days 28-30. The choice of the indicated periods corresponded to the key stages of ROP development in an experiment and was based on the findings of our previous histological studies. Dopamine, L-DOPA, and norepinephrine levels in infant rat blood plasma samples were determined.

Results: On day 14 of the experiment (the period corresponds to the pathological neovascularization induction in the applied model and preclinical ROP in children), mean L-DOPA level in infant rats with ROP (0.31 ng/ml) was significantly decreased compared to that in the controls (0.42 ng/ml) (p≤0.01). On days 21-23 of the experiment (the period corresponds to the growth of pathological extraretinal neovascularization in the applied model and ROP stage 3 in children) the systemic level of L-DOPA was still statistically reduced in the study group (0.87 ng/ml) compared to the control group (1.53 ng/ml) (p≤0.01). On days 28-30 of the experiment (the period corresponds to the regress of neovasculature in the applied model and a spontaneous ROP regress stage in children) the L-DOPA level in blood plasma in the study group (0.33 ng/ml) showed an insignificant upward tendency in reference to the controls (0.21 ng/ml). Mean dopamine and norepinephrine levels had no difference in the groups under study of infant rats within all follow-up periods.

Conclusion: Low systemic level of L-DOPA at the preclinical stage of experimental ROP should be considered as a laboratory prognostic criterion of a developing pathological process; it will enable to use the criterion when working out the measures to optimize the existing screening system for the disease in children.

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来源期刊
Sovremennye Tehnologii v Medicine
Sovremennye Tehnologii v Medicine MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
1.80
自引率
0.00%
发文量
38
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