吗啡暴露和早产会影响早产儿的闪光视觉诱发电位

IF 2 Q3 NEUROSCIENCES
Caterina Coviello , Silvia Lori , Giovanna Bertini , Simona Montano , Simonetta Gabbanini , Maria Bastianelli , Cesarina Cossu , Sara Cavaliere , Clara Lunardi , Carlo Dani
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引用次数: 0

摘要

本研究旨在首先探讨围产期风险因素对一组足月等效年龄(TEA)早产儿闪光 VEP 波和形态的影响。方法:研究对象为出生时胎龄(GA)为 32 周且无严重脑损伤的早产儿。对每个因变量N2、P2、N3潜伏期和P2振幅分别进行多变量回归分析。逻辑回归用于研究 N4 成分(存在/不存在)和 VEP 形态(规则/不规则)。预测因素包括GA、支气管肺发育不良(BPD)、VEP登记时的月经后年龄、吗啡和芬太尼累积剂量以及疼痛过程。最后,建立了线性回归模型,以评估2岁CA时Bayley-III认知和运动评分与VEP形态之间的关系,以及与GA、BPD、疼痛程序和吗啡累积剂量之间的关系。吗啡是N2(R2 = 0.09,p = 0.006)、P2(R2 = 0.11,p = 0.002)和N3(R2 = 0.13,p = 0.003)潜伏期的预测因子。较年轻的 GA 与较低的振幅相关(R2 = 0.05,p = 0.029)。在逻辑分析中,没有一个自变量能预测 N4 成分的存在或 VEP 形态。结论吗啡治疗和早产是导致TEA时VEPs参数改变的风险因素。在我们的队列中,VEP 形态学并不能预测神经系统的预后。重要意义使用吗啡应根据潜在的风险和益处进行评估,并根据疼痛和舒适度评分,考虑到可能出现神经发育障碍的风险,单独确定剂量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Morphine exposure and prematurity affect flash visual evoked potentials in preterm infants

Objective

The present study aimed to explore first the impact of perinatal risk factors on flash-VEP waves and morphology in a group of preterm infants studied at term equivalent age (TEA). Second, to correlate VEP morphology with neurological outcome at 2 years corrected age (CA).

Methods

Infants with a gestational age (GA) at birth <32 weeks, without major brain injury, were enrolled. Multivariate regression analyses were performed, and the models were run separately for each dependent variable N2, P2, N3 latencies and P2 amplitude. Logistic regression was applied to study N4 component (present/absent) and VEP morphology (regular/irregular). The predictors were GA, bronchopulmonary dysplasia (BPD), postmenstrual age at VEP registration, cumulative morphine and fentanyl dose, and painful procedures. Lastly, linear regression models were performed to assess the relation between the Bayley-III cognitive and motor scores at 2 years CA and VEP morphology, in relation to GA, BPD, painful procedures and cumulative morphine dose.

Results

Eighty infants were enrolled. Morphine was the predictor of N2 (R2 = 0.09, p = 0.006), P2 (R2 = 0.11, p = 0.002), and N3 (R2 = 0.13, p = 0.003) latencies. Younger GA was associated with lower amplitude (R2 = 0.05, p = 0.029). None of the independent variables predicted the presence of N4 component, nor VEP morphology in the logistic analysis. VEP morphology was not associated with cognitive and motor scores at 2 years.

Conclusions

Morphine treatment and prematurity were risk factors for altered VEPs parameters at TEA. In our cohort VEP morphology did not predict neurological outcome.

Significance

Morphine administration should be evaluated according to potential risks and benefits, and dosage individually accustomed, according to pain and comfort scores, considering the possible risk for neurodevelopmental impairment.

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来源期刊
CiteScore
3.90
自引率
0.00%
发文量
47
审稿时长
71 days
期刊介绍: Clinical Neurophysiology Practice (CNP) is a new Open Access journal that focuses on clinical practice issues in clinical neurophysiology including relevant new research, case reports or clinical series, normal values and didactic reviews. It is an official journal of the International Federation of Clinical Neurophysiology and complements Clinical Neurophysiology which focuses on innovative research in the specialty. It has a role in supporting established clinical practice, and an educational role for trainees, technicians and practitioners.
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