血清lncRNA NEAT1和miR-29c-3p表达与癫痫患儿病情及预后的相关性

doi:10.3969/j.issn.1673-8640.2025.08.007

摘要/Abstract

摘要：

目的探讨血清长链非编码RNA（lncRNA）核富集转录体 1（NEAT1）、miR-29c-3p表达与癫痫患儿病情严重程度和预后的相关性。方法选取2020年10月—2022年10月平煤神马集团总医院癫痫患儿102例（癫痫组）、健康体检儿童110名（正常对照组）。根据儿童癫痫持续状态严重程度评分（STEPSS）量表将所有患儿分为轻度组（50例）、中度组（24例）和重度组（28例）。收集所有研究对象一般资料，并检测血清lncRNA NEAT1、miR-29c-3p相对表达量。对所有患者随访1年，根据预后情况将患儿分为预后不良组（28例，出院后复发）和预后良好组（74例，无发作或仅有先兆发作）。采用Pearson相关分析评估癫痫患儿lncRNA NEAT1与miR-29c-3p的相关性。采用受试者工作特征（ROC）曲线评价血清lncRNA NEAT1和miR-29c-3p判断癫痫患儿预后不良的效能。采用多因素Logistic回归分析评估癫痫患儿预后不良的影响因素。结果与正常对照组比较，癫痫组血清lncRNA NEAT1相对表达量升高（P<0.001），血清miR-29c-3p相对表达量降低（P<0.001）。轻度组、中度组、重度组血清lncRNA NEAT1相对表达量依次升高（P<0.001），血清miR-29c-3p相对表达量依次降低（P<0.001）。lncRNA NEAT1与miR-29c-3p呈负相关（r=-0.414，P<0.05）。与预后良好组比较，预后不良组血清lncRNA NEAT1相对表达量升高（P<0.001），血清miR-29c-3p相对表达量降低（P<0.001），其他指标2个组之间差异均无统计学意义（P>0.05）。血清lncRNA NEAT1、miR-29c-3p单项检测和联合检测判断癫痫患儿预后不良的曲线下面积（AUC）分别为0.849、0.867、0.937。lncRNA NEAT1>2.52、miR-29c-3p<0.49是癫痫患儿发生预后不良的危险因素[比值比（OR）值分别为1.869、0.769，95%可信区间（CI）分别为1.257~2.777、0.631~0.937，P<0.05]。结论癫痫患儿血清lncRNA NEAT1和miR-29c-3p表达与病情严重程度和预后密切相关，或可作为癫痫患儿病情分析和预后评估的生物标志物。

关键词: 长链非编码RNA核富集转录体 1, 微小RNA-29c-3p, 癫痫, 预后

Abstract:

Objective To investigate the correlation between serum long non-coding RNA（lncRNA） nuclear-enriched abundant transcript 1（NEAT1）and miR-29c-3p expression and the severity and clinical prognosis of epilepsy in children.Methods Totally，102 children with epilepsy（epilepsy group）and 110 healthy subjects（healthy control group）were enrolled from General Hospital of Pingmei Shenma Group from October 2020 to October 2022. According to the Status Epilepticus in Pediatric Patients Severity Score（STEPSS），all the children were classified into mild group（50 cases），moderate group（24 cases）and severe group（28 cases）. The general data were collected，and the relative expression levels of serum lncRNA NEAT1 and miR-29c-3p were determined. All the chiblren were followed up for 1 year. Based on prognosis，they were classified into poor prognosis group（28 cases，reoccurrence after discharge）and good prognosis group （74 cases，non-occurrence or only precursor occurence）. Pearson correlation analysis was used to evaluate the correlation between lncRNA NEAT1 and miR-29c-3p in children with epilepsy. Using receiver operating characteristic（ROC） curve，the efficacy of serum lncRNA NEAT1 and miR-29c-3p in predicting poor prognosis in children with epilepsy was evaluated. Using multiple Logistic regression analysis，the influencing factors of poor prognosis in epilepsy patients were evaluated. Results Compared with healthy control group，the relative expression level of serum lncRNA NEAT1 in epilepsy group was increased（P<0.001），and the relative expression level of serum miR-29c-3p was decreased（P<0.001）. The relative expression levels of serum lncRNA NEAT1 in the mild，moderate and severe groups were increased sequentially（P<0.001），while the relative expression levels of serum miR-29c-3p were decreased sequentially（P<0.001）. There was a negative correlation between lncRNA NEAT1 and miR-29c-3p（r=-0.414，P<0.05）. Compared with good prognosis group，the relative expression level of serum lncRNA NEAT1 was increased and the relative expression level of serum miR-29c-3p was decreased in poor prognosis group（P<0.001）. There was no statistical significance in the other indicators between the 2 groups（P>0.05）. The areas under curves（AUC） of single and combined determinations of serum lncRNA NEAT1 and miR-29c-3p for predicting poor prognosis in children with epilepsy were 0.849，0.867 and 0.937，respectively. The lncRNA NEAT1>2.52 and miR-29c-3p<0.49 were risk factors for poor prognosis in children with epilepsy [odds ratios（OR）were 1.869 and 0.769，95% confidence intervals（CI） 1.257-2.777 and 0.631-0.937，respectively，P<0.05]. Conclusions The expressions of serum lncRNA NEAT1 and miR-29c-3p in children with epilepsy are related to the severity and prognosis of the disease，and they may serve as biological markers for analyzing the condition and evaluating the prognosis of children with epilepsy.

Key words: Long non-coding RNA nuclear-enriched abundant transcript 1, MicroRNA-29c-3p, Epilepsy, Prognosis

中图分类号:

R446.62

郭漫漫, 张鹏, 王润智, 史珑. 血清lncRNA NEAT1和miR-29c-3p表达与癫痫患儿病情及预后的相关性[J]. 检验医学, 2025, 40(8): 763-768.

GUO Manman, ZHANG Peng, WANG Runzhi, SHI Long. Correlation between the expression of serum lncRNA NEAT1，miR-29c-3p and the disease status，clinical prognosis of epilepsy in children[J]. Laboratory Medicine, 2025, 40(8): 763-768.

图/表 8

参考文献 18

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基因名称	上游引物（5'~3'）	下游引物（5'~3'）
lncRNA NEAT1	CTTCCTCCCTTTAACTTATCCATTCAC	CTCTTCCTCCACCATTACCAACAATAC
GAPDH	GCACCGTCAAGGCTGAGAAC	ATGGTGGTGAAGACGCCAGT
miR-29c-3p	GCCGAGCTTTTTGCGGTCTGGG	CTCAACTGGTGTCGTGGA
U6	GCTACGCGCGACCGTGGGCA	CACAGTGGTCTGACACTACGC

基因名称	上游引物（5'~3'）	下游引物（5'~3'）
lncRNA NEAT1	CTTCCTCCCTTTAACTTATCCATTCAC	CTCTTCCTCCACCATTACCAACAATAC
GAPDH	GCACCGTCAAGGCTGAGAAC	ATGGTGGTGAAGACGCCAGT
miR-29c-3p	GCCGAGCTTTTTGCGGTCTGGG	CTCAACTGGTGTCGTGGA
U6	GCTACGCGCGACCGTGGGCA	CACAGTGGTCTGACACTACGC

组别	例数	lncRNA NEAT1	miR-29c-3p
癫痫组	102	2.51±0.56	0.63±0.15
正常对照组	110	1.19±0.30	1.03±0.11
t值		17.649	-22.252
P值		<0.001	<0.001

组别	例数	lncRNA NEAT1	miR-29c-3p
癫痫组	102	2.51±0.56	0.63±0.15
正常对照组	110	1.19±0.30	1.03±0.11
t值		17.649	-22.252
P值		<0.001	<0.001

组别	例数	lncRNA NEAT1	miR-29c-3p
轻度组	50	2.23±0.51	0.73±0.09
中度组	24	2.59±0.47^*	0.61±0.11^*
重度组	28	2.93±0.41^*#	0.47±0.13^*#
F值		19.946	53.651
P值		<0.001	<0.001