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首页> 外文期刊>Epilepsy & behavior: E&B >Prognostic factors in epileptic encephalopathies at onset in the first 2 years of life: The experience of a tertiary healthcare center in Italy
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Prognostic factors in epileptic encephalopathies at onset in the first 2 years of life: The experience of a tertiary healthcare center in Italy

机译:生命前2年癫痫脑病的预后因素:意大利第三节医疗中心的经验

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摘要

Introduction: The aim of this retrospective cohort study was to identify some prognostic factors in anamnestic/clinical/instrumental data at the onset of epileptic encephalopathy (EE), for multiple outcome measures. Methods: We recruited patients diagnosed as affected by EE at Sant'Anna University Hospital, with onset in the first 24 months of life, with follow-up lasting longer than 3 years. Results: At the end of the follow-up, 6 patients (14%) died within 2 years of age; 20 patient (49%) had a drug-resistant epilepsy (DRE); 9 patients (22%) had a language development delay (LDD); 12 patients (30%) had an autism spectrum disorder (ASD); 20 patients (49%) had a global psychomotor impairment (GPI); 9 patients (22%) needed palliative care; and nobody had a normal psychomotor development. Preexisting developmental delay predicts death (p = 0.009), and in survivors, it is associated with a GPI (p < 0.001); patients with normal neurological examination at the onset of EE only develop a LDD (p = 0.020). Neuroimaging structural alterations are associated with DRE (p = 0.012) and with a GPI (p = 0.013). The history of perinatal risk factors predicts the worst prognosis (death: p = 0.035, GPI: p = 0.015, and access to palliative care: p = 0.007). The absence of early response to treatment is correlated to a poor long-term prognosis (GPI, p = 0.019; DRE, p = 0.001). The multivariate analysis confirms that a normal development at onset predicts the most favorable prognosis, both in terms of survival and cognitive outcome (OR [odds ratio] = 0.1). An early response to treatment is a protective factor for DRE (OR = 0.1). A perinatal pathology is confirmed as an independent prognostic factor of severe comorbidities (access to palliative care: OR = 10.4). Significance: This study was conducted to recognize possible prognostic factors among onset data of patients with EE, considering multiple outcome measures. This study design represents an innovative element compared to available papers, which were centered on isolated endpoints of prognosis, such as the prediction of neurocognitive development impairment or drug resistance. The data obtained from the study confirm that EEs prognosis is generally, but not universally, poor. Structural etiology and/or lack of response to antiepileptic drug (AED) within three months are main risk factors for DRE. Normal development at the onset of EEs and early response to treatment are the main positive prognostic factors.
机译:介绍:该回顾性队列队列研究的目的是在癫痫脑病(EE)发作的厌氧/临床/乐器数据中识别一些预后因素,用于多种结果措施。方法:我们招募诊断为Sant'anna大学医院患病的患者,在生命的前24个月内发病,随访时间超过3年。结果:在随访结束时,6名患者(14%)在2岁内死亡; 20例患者(49%)有耐药性癫痫(DRE); 9名患者(22%)有语言发展延误(LDD); 12名患者(30%)具有自闭症谱系障碍(ASD); 20名患者(49%)有全球性能损伤(GPI); 9名患者(22%)需要姑息治疗;没有人有正常的精神运动发展。预先存在的发育延迟预测死亡(P = 0.009),并且在幸存者中,它与GPI相关(P <0.001); EE发作时神经检查正常的患者仅开发LDD(P = 0.020)。神经影像体结构改变与DRE(P = 0.012)和GPI相关联(P = 0.013)。围产期危险因素的历史预测预后最差(死亡:P = 0.035,GPI:P = 0.015,以及获得姑息治疗:P = 0.007)。没有早期对治疗的反应与差的长期预后(GPI,P = 0.019; DRE,P = 0.001)相关。多变量分析证实,发病的正常发展预测了在存活和认知结果(或[odds比] = 0.1)方面的最有利预后。对治疗的早期反应是DRE的保护因子(或= 0.1)。围产期病理学被证实为严重组合性的独立预后因子(获得姑息治疗:或= 10.4)。意义:考虑到多种结果措施,进行了本研究以识别EE患者的发病数据中可能的预后因素。与可用论文相比,该研究表明是一种创新的元素,其以预后的孤立终点为中心,例如神经认知发展障碍或耐药性的预测。从研究中获得的数据证实,EES预后通常,但不普遍,差。在三个月内对抗癫痫药物(AED)的结构性病因和/或缺乏反应是RE的主要危险因素。 EES发作和早期对治疗的正常发展是主要的正预后因素。

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